UNITED STATES
SECURITIES AND EXCHANGE COMMISSION
Washington, D.C. 20549
FORM 20-F
(Mark One)
 
o
 REGISTRATION STATEMENT PURSUANT TO SECTION 12(b) OR (g) OF THE SECURITIES EXCHANGE ACT OF 1934
 
OR
 
x
ANNUAL REPORT PURSUANT TO SECTION 13 OR 15(d) OF THE SECURITIES EXCHANGE
ACT OF 1934
For the fiscal year ended December 31, 2012
OR
 
o
TRANSITION REPORT PURSUANT TO SECTION 13 OR 15(d) OF THE SECURITIES EXCHANGE
ACT OF 1934
For the transition period from ________________ to ________________
 
OR
 
o
SHELL COMPANY REPORT PURSUANT TO SECTION 13 OR 15(d) OF THE SECURITIES EXCHANGE
ACT OF 1934
Date of event requiring this shell company report  ________________
 
For the transition period from ________________ to ________________
 

Commission file number:  001-11960
 
ASTRAZENECA PLC
(Exact name of Registrant as specified in its charter)
 
England
(Jurisdiction of incorporation or organization)
 
2 Kingdom Street, London W2 6BD
(Address of principal executive offices)
Adrian Kemp
AstraZeneca PLC
2 Kingdom Street, London W2 6BD
Telephone: +44 20 7604 8000
Facsimile number: +44 20 7604 8151
(Name, Telephone, E-Mail or Facsimile number and Address of Company Contact Person)
 
Securities registered or to be registered pursuant to Section 12(b) of the Act:
 
Title of each class
Name of each exchange on which registered
American Depositary Shares, each representing one Ordinary Share of 25¢ each
The New York Stock Exchange
Ordinary Shares of 25¢ each
The New York Stock Exchange*
5.40% Notes due 2014
The New York Stock Exchange
5.90% Notes due 2017
The New York Stock Exchange
1.95% Notes due 2019
The New York Stock Exchange
7.00% Notes due 2023
The New York Stock Exchange
6.45% Notes due 2037
The New York Stock Exchange
4.00% Notes due 2042
The New York Stock Exchange
* Not for trading, but only in connection with the registration of American Depositary Shares representing such Ordinary Shares pursuant to the requirements of the Securities and Exchange Commission.
 
Securities registered or to be registered pursuant to Section 12(g) of the Act:
None
(Title of Class)
 
 
 
 
 
Securities for which there is a reporting obligation pursuant to Section 15(d) of the Act:
 
None
(Title of Class)
 
Indicate the number of outstanding shares of each of the issuer’s classes of capital or common stock as of the close of the period covered by the annual report.
 
The number of outstanding shares of each class of stock of AstraZeneca PLC as of December 31, 2012 was:
 
Ordinary Shares of 25¢ each: 1,246,779,548
Redeemable Preference Shares of £1 each: 50,000

Indicate by check mark if the registrant is a well-known seasoned issuer, as defined in Rule 405 of the Securities Act.
 
x   Yes o   No
 
  If this report is an annual or transition report, indicate by check mark if the registrant is not required to file reports pursuant to Section 13 or 15(d) of the Securities Exchange Act of 1934.
 
o   Yes x   No
 
Note — checking the box above will not relieve any registrant required to file reports pursuant to Section 13 or 15(d) of the Securities Exchange Act of 1934 from their obligations under those Sections.
 
Indicate by check mark whether the registrant (1) has filed all reports required to be filed by Section 13 or 15(d) of the Securities Exchange Act of 1934 during the preceding 12 months (or for such shorter period that the registrant was required to file such reports), and (2) has been subject to such filing requirements for the past 90 days.
 
x   Yes o   No
 
Indicate by check mark whether the registrant has submitted electronically and posted on its corporate Web site, if any, every Interactive Data File required to be submitted and posted pursuant to Rule 405 of Regulation S-T (§232.405 of this chapter) during the preceding 12 months (or for such shorter period that the registrant was required to submit and post such files).
 
o   Yes o   No
 
Indicate by check mark whether the registrant is a large accelerated filer, an accelerated filer, or a non-accelerated filer. See definition of “accelerated filer and large accelerated filer” in Rule 12b-2 of the Exchange Act. (Check one):
 
Large accelerated filer  x
Accelerated filer  o
Non-accelerated filer  o

Indicate by check mark which basis of accounting the registrant has used to prepare the financial statements included in this filing:
 
U.S. GAAP  o
International Financial Reporting Standards as issued
by the International Accounting Standards Board  x
Other  o
 
If “Other” has been checked in response to the previous question, indicate by check mark which financial statement item the registrant has elected to follow.
o   Item 17 o   Item 18
 
If this is an annual report, indicate by check mark whether the registrant is a shell company (as defined in Rule 12b-2 of the Exchange Act).
 
o   Yes x   No
 
(APPLICABLE ONLY TO ISSUERS INVOLVED IN BANKRUPTCY PROCEEDINGS DURING THE PAST FIVE YEARS)
 
Indicate by check mark whether the registrant has filed all documents and reports required to be filed by Sections 12, 13 or 15(d) of the Securities Exchange Act of 1934 subsequent to the distribution of securities under a plan confirmed by a court.
 
o   Yes o   No
 
 
 
 
 
 
Pursuant to Rule 12b-23(a) of the Securities Exchange Act of 1934, as amended, the information for the 2012 Form 20-F of AstraZeneca PLC (“AstraZeneca” or the “Company”) set out below is being incorporated by reference from the Company’s “Annual Report and Form 20-F Information 2012” included as exhibit 15.1 to this Form 20-F dated and submitted on March 25, 2013.
 
References below to major headings include all information under such major headings, including subheadings, unless such reference is a reference to a subheading, in which case such reference includes only the information contained under such subheading. Graphs and tabular data are not included unless specifically identified below. Photographs are also not included.
 
In addition to the information set out below, the information (including tabular data) set forth under the headings “Important information for readers of this Annual Report”, “Definitions”, “Use of terms”,  and “Statements of dates” on the inside front cover, “Cautionary statement regarding forward-looking statements”, “Inclusion of reported performance, Core financial measures and constant exchange rate growth rates”, “Statements of competitive position, growth rates and sales”, “AstraZeneca websites”, “External/third party websites” and “Figures” on the inside back cover, “Glossary” on pages 209 to 210, and “Trade marks” on page 211, in each case of the Company’s “Annual Report and Form 20-F Information 2012” included as exhibit 15.1 to this Form 20-F dated March 25, 2013 is incorporated by reference.
 
PART 1
 
ITEM 1. IDENTITY OF DIRECTORS, SENIOR MANAGEMENT AND ADVISERS
 
Not applicable.
 
ITEM 2. OFFER STATISTICS AND EXPECTED TIMETABLE
 
Not applicable.
 
ITEM 3. KEY INFORMATION
 
A. Selected Financial Data
 
The information (including graphs and tabular data) set forth under the headings “Financial Statements—Group Financial Record” on page 198 and the first table that appears under “Additional Information—Shareholder Information—AstraZeneca PLC share listings and prices” on page 203, in each case of the Company’s “Annual Report and Form 20-F Information 2012” included as exhibit 15.1 to this Form 20-F dated March 25, 2013 is incorporated by reference. The selected financial data incorporated by reference herein is derived from audited financial statements of the Company and its consolidated entities, prepared in accordance with International Financial Reporting Standards (“IFRS”) as adopted by the European Union and as issued by the International Accounting Standards Board, included in the Company’s “Annual Report and Form 20-F Information 2012” included as exhibit 15.1 to this Form 20-F dated March 25, 2013.
 
B. Capitalization and Indebtedness
 
Not applicable.
 
C. Reason for the Offer and Use of Proceeds
 
Not applicable.
 
D. Risk Factors
 
The information (including tabular data) set forth or referenced under the heading “Performance—Risk—Principal risks and uncertainties” on pages 75 to 85 of the Company’s “Annual Report and Form 20-F Information 2012” included as exhibit 15.1 to this Form 20-F dated March 25, 2013 is incorporated by reference.
 
 
1
 
 
Item 4. INFORMATION ON THE COMPANY
 
A. History and Development of the Company
 
The information (including tabular data) set forth under the headings “Additional Information—Corporate Information—History and development of the Company” on page 208, “Performance—Financial Review—Financial position – 2012—Investments, divestments and capital expenditure” on page 93 and “Financial Statements—Notes to the Group Financial Statements—Note 22—Acquisitions and disposals” on pages 173 to 174, in each case of the Company’s “Annual Report and Form 20-F Information 2012” included as exhibit 15.1 to this Form 20-F dated March 25, 2013 is incorporated by reference.
 
B. Business Overview
 
The information (including graphs and tabular data) set forth under the headings “Overview—AstraZeneca at a glance” on pages 2 to 5, “—Chairman’s Statement” on pages 6 to 7, “—Chief Executive Officer’s Review” on pages 8 to 9, “Strategy” on pages 12 to 21, “Performance—Our performance in 2012” on pages 24 to 29, “—Business Review” on pages 30 to 49, “—Therapy Area Review” on pages 50 to 69, “—Geographical Review” on pages 70 to 73, “Performance—Risk—Managing Risk”, “—Embedded in business processes” and “—Key responsibilities” on pages 74 to 75, “Additional Information—Development Pipeline” on pages 199 to 202, “Financial Statements—Notes to the Group Financial Statements—Note 1—Product revenue information” on page 150, “—Note 6—Segment Information” on pages 155 to 156, and “Statements of competitive position, growth rates and sales” on the inside back cover, in each case of the Company’s “Annual Report and Form 20-F Information 2012” included as exhibit 15.1 to this Form 20-F dated March 25, 2013 is incorporated by reference.
 
Strategy update
 
Strategy to return to growth and achieve scientific leadership
 
On March 21, 2013, AstraZeneca announced its strategy to return to growth and achieve scientific leadership, which is the result of AstraZeneca’s annual strategy review. AstraZeneca’s strategic priorities are:
 
 
·
Driving our on-market growth platforms to return to growth as we move through a period of patent expiries and revenue declines;
 
 
·
Progressing the Phase II pipeline with the goal of increasing our Phase III asset volume and delivering on the potential of our biologics portfolio;
 
 
·
Launching a steady flow of specialty care products, balancing AstraZeneca’s historic strength in primary care;
 
 
·
Rebuilding AstraZeneca’s R&D platform through innovation and distinctive science supported by co-location of our teams and better access to globally recognised science clusters;
 
 
·
Significantly simplifying the business, improving productivity and building a culture that supports long-term success;
 
 
·
Leveraging business development and acquisition opportunities to strengthen the product pipeline.
 
Achieving scientific leadership
 
AstraZeneca is committed to executing a focused innovation-driven global biopharmaceuticals strategy, exploiting its combination of strengths in large and small molecules, immunotherapies and protein engineering technologies.
 
We will strive for our research and development efforts to be more focused. In large and small molecule R&D, we will concentrate our scientific efforts and the weight of our investment, including business development, on three core therapy areas:
 
 
2
 
 
 
·
Respiratory, Inflammation & Autoimmunity
 
 
·
Cardiovascular & Metabolic Disease
 
 
·
Oncology
 
We will continue to be active in Infection & Vaccines and in Neuroscience, though our investments will be more opportunity-driven. Within our chosen therapy areas, we will tighten our disease focus. This approach is designed to improve our likelihood of success while allowing us to meet our goal of funding our growing portfolio of late stage medicines to 2016 with R&D expenditure that we expect to be comparable with current levels.
 
By accelerating development of several new molecular entities (NMEs), we believe our Phase III pipeline has the potential to double in size by 2016. Acceleration of these key NMEs, combined with our ongoing efforts to progress a strong Phase II biologics pipeline into late stage development, will create a portfolio more weighted towards specialty care, balancing our traditional strengths in primary care. We are also increasing our investment in life cycle management to support key on-market and late stage pipeline products such as Brilinta , FORXIGA TM , BYDUREON TM and lesinurad.
 
We intend to transform the way we carry out research and development. To help achieve sustainable scientific leadership and improve pipeline productivity, we will reshape our footprint and evolve our operating model. As discussed below in “—Strategy update—AstraZeneca to establish strategic R&D centres to enhance innovation and pipeline productivity”, we are proposing to increase our proximity to bioscience clusters and bring our research, development and commercial people together in three strategic R&D centres. We believe that these proposals will make it easier for our researchers to collaborate with external partners and with each other. The creation of autonomous biologics and small molecules biotech units is designed to improve innovation and accelerate decision-making. Additionally, we intend to increase our emphasis on novel biology and personalised healthcare and to continue to partner with leading academic institutions to increase our understanding of disease biology.
 
Return to growth
 
By seeking to maximize the potential of our current portfolio of products and product candidates, we expect to navigate a period of revenue decline during which some of our major products are scheduled to lose exclusivity. Through this organic strategy we will target a return to growth. We will focus investment and resources on five key growth platforms:
 
 
·
Ensuring Brilinta reaches the patients who can benefit, capturing the potential of this medicine;
 
 
·
Working with our partner, BMS, to achieve a leading position in the non-insulin diabetes market;
 
 
·
Investing to drive growth in our Emerging Markets;
 
 
·
Maximising the potential of our on-market respiratory portfolio, which continues to grow in key markets, and accelerate our pipeline of respiratory projects;
 
 
·
Capturing the potential from our established brands and new launches in Japan, the world’s second largest pharmaceutical market and one that is showing steady growth.
 
Through accelerated business development we will seek to deliver benefits that exceed the Company’s base plan while supporting our long-term product pipeline aspirations. There will be a more intense focus to the business development efforts of our small molecule and biologics biotech units on early stage academic and biotech alliances. We will continue to in-license to strengthen the pipeline, focusing predominately on the three core therapy areas identified above, while we will seek partnerships and bolt-on acquisitions to support the late-stage and on-market portfolio to accelerate revenues.
 
 
3
 
 
Simplification and productivity
 
We believe that transforming how we work is crucial to delivering our strategy. We are committed to significantly simplifying our organisation and our processes, while creating an innovative environment. A more focused footprint will support that aim, as will increasing autonomy to accelerate and improve decision making.  We will continue to drive productivity improvements across the Group with a view to removing complexity and to create additional headroom to invest in growing our business and providing returns to our shareholders.
 
This initivative will involve a restructuring of our selling, general and administrative (SG&A) activities that will lead to a global reduction in headcount of approximately 2,300. The majority of this headcount impact is related to restructuring programmes that have been previously announced or have otherwise already been communicated to affected employees. The new, fourth phase of our restructuring programme combines this SG&A restructuring with two previously announced programmes. These comprise the headcount reduction of 1,600 related to the proposed R&D footprint changes discussed below in “—Strategy update—AstraZeneca to establish strategic R&D centres to enhance innovation and pipeline productivity”, and the balance of the third phase of our restructuring programme announced in February 2012, which amounts to 1,150 roles. This Phase 4 restructuring programme entails an estimated global headcount reduction of about 5,050 over the period from 2013 to 2016.
 
The Phase 4 restructuring programme is estimated to result in $2.3 billion in one-time restructuring charges that will impact our income statement, of which $1.7 billion are expected to be cash costs. The Phase 4 restructuring programme is expected to result in annual benefits of approximately $800 million by 2016, of which approximately $500 million relate to the proposed SG&A restructuring and R&D footprint changes and approximately $300 million relate to the balance of the third phase of our restructuring programme announced in February 2012.
 
Financial objectives and capital allocation
 
On March 21, 2013, the Company also summarised its financial objectives and capital allocation policy:
 
 
·
Maintaining strong Core pre-R&D operating margins with a target range of 48% to 52%;
 
 
·
An expectation that up to 50% of the post-tax, pre-R&D cashflow from our on-market portfolio will be reinvested in R&D, external collaborations and in-licensing, as well as capital investment;
 
 
·
A commitment to maintain our progressive dividend policy under which we hold or grow the dividend per share with a target cover of two times core earnings over the investment cycle;
 
 
·
Allocating the balance of cashflows to fund additional value-creating business development and bolt-on acquisitions;
 
 
·
Returning cash through share repurchases over time if no value-creating business development opportunities arise.
 
In adopting a progressive dividend policy, by which AstraZeneca’s Board of Directors intends to maintain or grow the dividend each year, the Board recognises that some earnings fluctuations are to be expected as the revenue base transitions through a period of exclusivity losses and new product launches. The Board’s view is that the annual dividend will not just reflect the financial performance of a single year taken in isolation, but reflects its view of the earnings prospects for the Group over the entirety of the investment cycle.
 
Long-term incentives
 
The Company is proposing to review its long-term incentive performance metrics to maximise alignment with the strategy of returning to growth and achieving scientific leadership. The Company’s Remuneration Committee plans to consult the Group’s largest investors about its thinking in this area before any long term incentive awards are made in 2013 and will take those views into account before reaching its final decision. The Company expects to make available further information about the new performance metrics at the Company’s Annual General Meeting on April 25, 2013.
 
 
4
 
 
AstraZeneca to establish strategic R&D centres to enhance innovation and pipeline productivity
 
On March 18, 2013, the Company announced plans to invest in strategic research and development centres in the UK, the US and Sweden to improve pipeline productivity and to establish the Company as a global leader in biopharmaceutical innovation. The proposals are designed to locate more of the Company’s scientists close to globally recognised bioscience clusters, making it easier to access talent and opportunities for collaboration and partnerships; bring teams together to improve collaboration and to create an environment that prioritises scientific development and the needs of patients; and simplify the Company’s footprint to reduce complexity and eliminate unnecessary cost.
 
Under the plans, AstraZeneca’s small molecule and biologics R&D activities will be concentrated in three strategic centres: Cambridge, UK; Gaithersburg, US; and Mölndal, Sweden. The proposals are expected to be fully implemented by 2016.  Under the proposals:
 
Cambridge, UK: AstraZeneca plans to invest around $500 million to establish a new, purpose-built facility in Cambridge, a world-renowned centre for life sciences innovation with strong links to globally important research institutions in London. Consolidating the Company’s UK-based small molecule and biologics research and development at a new centre will build on AstraZeneca’s protein engineering capabilities already based in the city. Cambridge will also become AstraZeneca’s new global corporate headquarters.
 
Gaithersburg, Maryland, US: The site of MedImmune’s headquarters and the primary location for AstraZeneca’s biologics activities, Gaithersburg is expected to also become the location of much of the Company’s US-based Global Medicines Development activities for small and large molecules and to accommodate some global marketing and US specialty care commercial functions.
 
Mölndal, Sweden: AstraZeneca’s site in Mölndal, near Gothenburg, will continue to be a global centre for research and development, with a primary focus on small molecules.
 
We expect that the three strategic sites will be supported by other existing AstraZeneca facilities around the world, including Boston, Massachusetts, US, which will continue to be a centre for research and development, with a primary focus on small molecules. The consolidation of AstraZeneca’s global R&D footprint and the creation of a new headquarters will impact on other sites over the next three years, particularly in the UK and US. The main changes, as currently contemplated under our proposals, are as follows:
 
Alderley Park, Cheshire, UK: Research and development work will no longer be carried out at Alderley Park. Approximately 1,600 roles are expected to relocate from Alderley Park, with the significant majority going to the new centre in Cambridge and the remainder to the Company’s nearby Macclesfield manufacturing facility or other AstraZeneca sites overseas. At least 700 non-R&D roles are expected to remain at Alderley Park.
 
Wilmington, Delaware, US: With the move of the Global Medicines Development group and the relocation of global marketing and US specialty care commercial roles, we expect that about 1,200 roles will leave Wilmington and there will be a net increase of approximately 300 roles in Gaithersburg. The changes announced in our proposals are expected to lead to an estimated overall reduction of about 650 positions in the US; while around 170 will relocate to other AstraZeneca sites in the US or overseas. We expect that Wilmington will remain the North America commercial headquarters, with a population of about 2,000 at the AstraZeneca site.
 
London, UK: The majority of corporate and global commercial roles based in London are expected to move to the new centre in Cambridge with some going to other AstraZeneca sites. Following the transfer of the Company’s headquarters to Cambridge, AstraZeneca’s Paddington office is expected to close by 2016. Currently, around 350 roles are based in London.
 
Globally, over the 2013 to 2016 period, the proposed investment and associated changes announced on March 18, 2013 are expected to lead to the relocation of nearly 2,500 roles and an overall estimated reduction in headcount in the region of 1,600 roles. The vast majority of these will be in the UK and the US. The programme is expected to incur $1.4 billion in one-time restructuring charges, of which $800 million are likely to be cash costs. In addition, the Company will invest approximately $500 million in establishing the new centre in Cambridge. Annualised benefits of approximately $190 million are expected by 2016 for the programme. Final estimates for programme costs, benefits and headcount impact in all areas of the business are subject to completion of applicable consultation processes in accordance with local laws.
 
 
5
 
 
Readers of this “Strategy update” section should understand that the pharmaceutical sector is inherently risky and a variety of risks, uncertainties and factors outside of our control may affect our business, including our ability to successfully implement our strategy and realise the expected benefits therefrom.  If we are unsuccessful in implementing our proposed strategic initiatives or if these initiatives fail to produce the anticipated benefits (either at all, or along our anticipated timeline), this may materially adversely impact our business, financial condition and results of operations.  For more information on the principal risks and uncertainties that we consider to be material to our business, please see the information above under the heading Item 3 – “Key Information—Risk Factors.”
 
Other matters
 
AstraZeneca settles litigation over Crestor patent
 
On March 25, 2013, AstraZeneca announced that it has entered into a settlement agreement in its US patent infringement litigation against Watson Laboratories, Inc. (Watson), Actavis, Inc. (formerly known as Watson Pharmaceuticals, Inc.), and EGIS Pharmaceuticals regarding Watson’s proposed rosuvastatin zinc product.  Watson, a successor of Cobalt, has also agreed not to further appeal a decision by the US Court of Appeals for the Federal Circuit that upheld the validity and enforceability of the Crestor (rosuvastatin calcium) substance patent.  Shionogi is also a party to the settlement agreement.
 
Under the agreement, Watson and EGIS have conceded that the Crestor substance patent is valid, enforceable and would be infringed by Watson’s rosuvastatin zinc product and its rosuvastatin calcium product.  The settlement agreement permits Watson to begin selling its generic version of Crestor and its rosuvastatin zinc product beginning May 2, 2016, at a fee to AstraZeneca of 39% of net sales of Watson’s products until the end of pediatric exclusivity on July 8, 2016.  The entry date could be earlier and the fees eliminated in certain circumstances.
 
All claims and counterclaims will be dismissed in a consent judgment entered by the US District Court for the District of Delaware. All other terms of the settlement remain confidential.  The substance patent protecting Crestor expires on January 8, 2016, and the pediatric exclusivity period expires on July 8, 2016.  In compliance with the Medicare Prescription Drug, Improvement, and Modernization Act of 2003, AstraZeneca will file the settlement agreement with the US Federal Trade Commission and US Department of Justice.
 
US Court of Appeals affirms decision finding Seroquel XR formulation patent valid and infringed
 
On February 14, 2013, the US Court of Appeals for the Federal Circuit summarily upheld a lower court ruling that had found AstraZeneca’s formulation patent protecting Seroquel XR (quetiapine fumarate) extended release tablets in the US to be valid and infringed.
 
Results from long-term safety trial of naloxe gol
 
On February 26, 2013, the Company announced high-level results from KODIAC-08, an open-label, randomised, 52-week, long-term safety trial of naloxegol versus usual care (UC) in patients with non-cancer related pain and opioid-induced constipation (OIC). UC was defined as the investigator’s choice of an existing laxative treatment regimen for OIC. This is the fourth trial in the naloxegol Phase III development program, and was designed to evaluate the long-term safety and adverse event (AE) profile of naloxegol in patients taking 25 mg once daily, as compared to UC.
 
In the trial, a total of 534 patients received naloxegol once daily for up to 52 weeks, while 270 patients received UC for OIC during the same treatment period. The most commonly reported AEs occurring more frequently on naloxegol than on usual care included abdominal pain, diarrhoea, nausea and headache. The trial reported no imbalances in serious adverse events. In addition, there were a low number of major adverse cardiovascular events, as adjudicated by an independent external committee, and there was no imbalance of these events across naloxegol and UC arms.
 
There were no increases from baseline levels in mean daily pain scores or mean total daily opioid dose in either the naloxegol or the UC arm. Additionally, there were no reports of opioid withdrawal AEs which could be attributed to naloxegol. A full assessment of the safety and tolerability findings is ongoing.
 
A New Drug Application (NDA) filing in the US and a Marketing Authorisation Application filing in the EU are planned for the third quarter of 2013, pending AstraZeneca’s final preparation of the registration package and a pre-NDA meeting with the FDA.
 
Federal Court of Australia holds Crestor patents invalid
 
On March 5, 2013, the Company announced that the Federal Court of Australia found three patents protecting Crestor (rosuvastatin) to be invalid. These patents – a formulation patent (AU 200051842, with an expiry date in 2020); a second patent related to the use of rosuvastatin for treating heterozygous familial hypercholesterolemia (AU 2002214165, with an expiry date in 2021); and a third patent related to the use of rosuvastatin for treating hypercholesterolemia (AU 2000023051, with an expiry date in 2020) – were challenged by Apotex Pty Ltd, Watson Pharma Pty Ltd and Ascent Pharma Pty Ltd. The Federal Court decision is limited to Australia and has no impact on the validity of patents related to Crestor in other countries.
 
Results of real world study comparing commonly prescribed COPD medicines
 
On March 19, 2013, AstraZeneca announced that an analysis of data from real world study PATHOS, published in the Journal of Internal Medicine, shows that chronic obstructive pulmonary disease (COPD) patients treated with Symbicort Turbuhaler (budesonide/formoterol) are significantly less likely to suffer from COPD-related exacerbations – or ‘flare ups’ – and are significantly less likely to be hospitalised for COPD than those treated with Seretide™ (fluticasone/salmeterol).  PATHOS is the largest real world study to compare the effectiveness of two commonly prescribed inhaled corticosteroid and long-acting beta agonist (ICS/LABA) combination treatments for COPD with more than one year of patient follow up.
 
 
6
 
 
Overall, budesonide/formoterol reduced the annual rate of moderate to severe exacerbations by 26% compared to fluticasone/salmeterol (0.80 vs. 1.09 /patient-year; p<0.0001). The significant, and clinically relevant reduction in favour of budesonide/formoterol was apparent for all types of exacerbation event (e.g. antibiotic use, oral steroid use or hospital admission). Indeed, use of budesonide/formoterol reduced rates of COPD-related hospitalisation by 29% (0.15 vs. 0.21 /patient-year; p<0.0001) with hospital days due to COPD exacerbation 34% fewer (0.63 vs. 0.95/patient-year; p<0.0001) compared with fluticasone/salmeterol.
 
The 11-year PATHOS study, led by Uppsala University, retrospectively examined the medical records of 5,468 ICS/LABA-treated patients in Sweden from 1999 to 2009; a total of 19,000 patient years. This first published analysis of the data compares the rate of COPD exacerbations associated with two commonly prescribed combinations. To allow for a valid comparison, a cohort of patients treated with budesonide/formoterol were individually matched with an equal number of patients treated with a second ICS/LABA, fluticasone/salmeterol. Investigators used a statistical technique called “propensity score matching” to minimise bias and ensure the two ICS/LABA-treated groups were comparable in terms of variables including age, gender, and measures of disease severity such as medication use, COPD co-morbidities, previous hospitalisations for any cause and exacerbation rates for COPD, and other conditions like respiratory infections prior to the first ICS/LABA prescription. Exacerbations were defined in the study as medical interventions such as hospitalisations, emergency room visits and prescription of oral steroids or antibiotics due to COPD deterioration.
 
Exclusive agreement with Moderna Therapeutics to develop messenger RNA Therapeutics™ in cardiometabolic diseases and cancer
 
On March 21, 2013, AstraZeneca announced an exclusive agreement with Moderna Therapeutics, Inc. (Moderna) to discover, develop and commercialise messenger RNA therapeutics™ for the treatment of serious cardiovascular, metabolic and renal diseases as well as cancer. Messenger RNA therapeutics™ are a new treatment approach that enables the body to produce therapeutic protein in vivo, opening up new treatment options for a wide range of diseases that cannot be addressed at the moment using existing technologies. Effectiveness of the agreement is contingent on expiration or termination of the waiting period under the Hart-Scott-Rodino Antitrust Improvements Act.
 
Under the terms of the agreement, AstraZeneca will make an upfront payment of $240 million. AstraZeneca will have exclusive access to select any target of its choice in cardiometabolic diseases, as well as selected targets in oncology, over a period of up to five years for subsequent development of messenger RNA. In addition, Moderna is entitled to an additional $180 million for the achievement of three technical milestones. Through this agreement, AstraZeneca has the option to select up to 40 drug products for clinical development and Moderna will be entitled to development and commercial milestone payments as well as royalties on drug sales ranging from high single digits to low double digits for each product. AstraZeneca will lead the preclinical, clinical development and commercialisation of therapeutics resulting from the agreement and Moderna will be responsible for designing and manufacturing the messenger RNA against selected targets.
 
Moderna’s approach uses proprietary messenger RNA containing naturally occurring nucleotide analogues, which are designed to stimulate the body’s natural ability to produce intracellular and secreted therapeutic proteins without triggering an innate immune response. The secreted proteins will be released into the bloodstream to potentially restore function elsewhere in the body. Using messenger RNA also has the potential advantage of dramatically reducing the time and expense associated with creating therapeutic proteins using current recombinant technologies.
 
AstraZeneca and Karolinska Institutet to create Integrated Translational Research Centre
 
On March 21, 2013, AstraZeneca and the Swedish medical university Karolinska Institutet announced their intention to create an Integrated Translational Research Centre for cardiovascular and metabolic disease and regenerative medicine located at Karolinska Institutet’s site in Stockholm, Sweden. The Centre will be set up to conduct preclinical and clinical studies aimed at advancing the understanding of cardiovascular and metabolic disease pathophysiology and assessing new drug targets for AstraZeneca’s two biotech units, AstraZeneca Innovative Medicines and Early Development and MedImmune.
 
 
7
 
 
Building on the organisations’ longstanding collaboration, the Centre will initially run for a period of five years and will be made up of between 20 and 30 scientists, including a number of AstraZeneca scientists. In addition, AstraZeneca will contribute up to $20 million per annum, and Karolinska Institutet will contribute expertise and facilities. The Centre is expected to be operational by mid-2013.
 
Disclosures Under the Iran Threat Reduction and Syria Human Rights Act of 2012
 
The Company is a global, innovation-driven biopharmaceutical business with operations in over 100 countries and our innovative medicines are used by millions of patients worldwide. AstraZeneca does not have a legal entity based in Iran, or any employees or an office located in Iran. The Company, through one of its non-US Group companies that is neither a US person nor a foreign subsidiary of a US person, currently generates sales in Iran solely through a single third-party distributor. None of AstraZeneca’s US entities are involved in any business activities in Iran, or with the Iranian government. AstraZeneca has a valid and existing OFAC license covering the sale of certain US-origin medicines to its sole distributor and the three known entities used by its sole distributor in the Iranian distribution chain, although to date AstraZeneca has sold only non-US origin medicines to Iran. To the best knowledge of the management of AstraZeneca, the third-party distributor used by AstraZeneca is not owned or controlled by the Iranian government and the Company does not have any agreements, commercial arrangements, or other contracts with the Iranian government. However, the Company understands that one of the known sub-distributors (covered by the OFAC license) may be indirectly controlled by the Iranian government but the Company has not been able to confirm this. Further, in view of the types of products created and distributed by AstraZeneca, it is expected that the ultimate end-payers for our medicines may also include the Iranian government.
 
For the year ended December 31, 2012, the Company’s gross revenues and net profits attributable to the above-mentioned Iranian activities were $14 million and $6 million respectively. For the same period, the Group’s gross revenues and net profits were $27,973 million and $6,327 million respectively. Accordingly, the gross revenues and net profits attributable to the above-mentioned Iranian activities amounted to approximately 0.05% of the Group’s gross revenues and approximately 0.09% of its net profits.
 
At the time of publication, the management of AstraZeneca does not anticipate any change in its activities in Iran that would result in a material impact on the Group.
 
C. Organizational Structure
 
The information (including tabular data) set forth under the headings “Corporate Governance—Corporate Governance Report—Other matters—Subsidiaries and principal activities” on page 119 and “Financial Statements—Principal Subsidiaries” on page 191, in each case of the Company’s “Annual Report and Form 20-F Information 2012” included as exhibit 15.1 to this Form 20-F dated March 25, 2013 is incorporated by reference.
 
D. Property, Plant and Equipment
 
The information (including tabular data) set forth under the headings “Performance—Business Review—Research and Development—Our resources” on pages 32 to 33, “—Business Review—Supply and Manufacturing—Our resources” on page 41, “Performance—Financial Review—Financial position – 2012—Property, plant and equipment” and “—Financial position – 2011—Property, plant and equipment” on pages 92 and 97, respectively, “Performance—Risk—Principal risks and uncertainties—Legal, regulatory and compliance risks—Environmental and occupational health and safety liabilities” on page 83, “Financial Statements—Notes to the Group Financial Statements—Note 7—Property, plant and equipment” on page 157, “—Note 25—Commitments and contingent liabilities—Environmental costs and liabilities” on page 183 and “Additional Information—Corporate Information—Property” on page 208, in each case of the Company’s “Annual Report and Form 20-F Information 2012” included as exhibit 15.1 to this Form 20-F dated March 25, 2013 is incorporated by reference. Please also see the information above under the heading Item 4 – “Business Overview—Strategy update.”
 
 
8
 
 
ITEM 4A. UNRESOLVED STAFF COMMENTS
 
Not applicable.
 
ITEM 5. OPERATING AND FINANCIAL REVIEW AND PROSPECTS
 
The information (including graphs and tabular data) set forth under the headings “Performance—Financial Review” on pages 86 to 103, “Performance—Geographical Review” on pages 70 to 73, “Performance—Therapy Area Review—Sales by Therapy Area” (consisting of tabular data) on page 50, “—Therapy Area Review—Our financial performance” (consisting of tabular data) on page 53, “Strategy” on pages 12 to 21, “Performance—Business Review—Research and Development” on pages 30 to 34, “Corporate Governance—Corporate Governance Report—Business organisation—Portfolio Investment Board (PIB)” on page 119, “Performance—Risk—Principal risks and uncertainties—Commercialisation and business execution risks—Developing our business in Emerging Markets”, “—Pressures resulting from generic competition”, “—Price controls and reductions” and “—Economic, regulatory and political pressures” on pages 77 to 79, “Financial Statements—Notes to the Group Financial Statements—Note 14—Interest-bearing loans and borrowings” on pages 164 to 165, “—Note 15—Derivative financial instruments” on page 166, “—Note 19—Reserves” on page 172, “—Note 23—Financial risk management objectives and policies” on pages 175 to 179 and “—Note 25—Commitments and contingent liabilities” on pages 183 to 189, in each case of the Company’s “Annual Report and Form 20-F Information 2012” included as exhibit 15.1 to this Form 20-F dated March 25, 2013 is incorporated by reference.
 
Please see the information above under the heading Item 4 – “Business Overview—Strategy Update.”
 
We consider the Group’s working capital to be sufficient for its present requirements.
 
Developments in Legal Proceedings
 
For further information in respect of material legal proceedings in which the Company is currently involved, including those discussed below, please see the information (including tabular data) set forth under the heading “Financial Statements—Notes to the Group Financial Statements—Note 25—Commitments and contingent liabilities” on pages 183 to 189 of the Company’s “Annual Report and Form 20-F Information 2012” included as exhibit 15.1 to this Form 20-F dated March 25, 2013.  Unless noted below or in the Company’s “Annual Report on Form 20-F Information 2012”, no provisions have been established in respect of the proceedings discussed below.
 
Patent litigation

Crestor (rosuvastatin calcium)

Patent proceedings in the US

In January 2013, defendants Aurobindo Pharma Limited, Teva Pharmaceuticals USA, Inc., Mylan Pharmaceuticals Inc., Sun Pharmaceutical Industries, LTD., and, separately, Apotex Corp., filed petitions for rehearing and rehearing en banc of aspects of the US Court of Appeals for the Federal Circuit’s December 2012 decision in favour of AstraZeneca.  In February and March 2013, the Court of Appeals denied the petitions.
 
As previously disclosed, a December 2012 trial took place in AstraZeneca’s patent litigation in the US District Court for the District of Delaware in which it contends that a §505(b)(2) NDA for rosuvastatin zinc tablets infringes the substance patent for Crestor tablets.  On 25 March 2013, the parties entered into a settlement agreement resolving the litigation, and the case will be dismissed by consent judgment.  Under the agreement, Watson Laboratories, Inc. (Watson) and EGIS Pharmaceuticals concede that the Crestor substance patent is valid, enforceable and would be infringed by Watson’s rosuvastatin zinc product and its rosuvastatin calcium product.  The settlement agreement permits Watson to begin selling its generic version of Crestor and its rosuvastatin zinc product beginning May 2, 2016, at a fee to AstraZeneca of 39% of net sales of Watson’s products until the end of paediatric exclusivity on July 8, 2016.  The entry date could be earlier and the fees eliminated in certain circumstances.

Patent proceedings outside the US

In Australia in 2011, AstraZeneca instituted proceedings against Apotex Pty Ltd asserting infringement of various formulation and method patents for Crestor .  In January 2012, AstraZeneca instituted similar proceedings against Watson Pharma Pty Ltd. and Actavis Australia Pty Ltd.  On March 5, 2013, the Federal Court of Australia held all three patents at issue invalid.  AstraZeneca intends to appeal the decision.

 
9
 
 
Nexium (esomeprazole magnesium)

Patent proceedings in the US

In February 2013, AstraZeneca received a Paragraph IV notice letter from Watson Laboratories, Inc. (Watson), and in March 2013, AstraZeneca commenced a patent infringement action against Watson in the US District Court for the District of New Jersey regarding Watson’s generic ANDA product.

Patent proceedings outside the US

In Canada, in March 2013, the Federal Court prohibited Ranbaxy Pharmaceuticals Canada Inc. from receiving a marketing authorization for its esomeprazole magnesium product until June 2015.

Pulmicort Respules (budesonide inhalation suspension)

Patent proceedings in the US

Closing arguments in AstraZeneca’s consolidated patent infringement lawsuits in the US District Court for the District of New Jersey against various generic companies for infringement of US patents directed to methods of use and the formulation and form of active ingredient for Pulmicort Respules were held in March 2013. AstraZeneca expects a decision by the District Court before April 2013.

Seroquel (quetiapine fumarate) and Seroquel XR (quetiapine fumarate)

Patent proceedings in the US

In   February 2013, the US Court of Appeals for the Federal Circuit affirmed the March 2012 decision of the US District Court for the District of New Jersey that the Seroquel XR formulation patent is valid and infringed.

In February 2013, AstraZeneca settled its patent infringement action against Torrent Pharmaceuticals Limited and Torrent Pharma Inc. by granting a license to the Seroquel XR product patent, effective November 1, 2016, or earlier, in certain circumstances.

Patent proceedings outside the US

In March 2013, the Federal Court of Canada dismissed AstraZeneca’s application to prohibit the Canadian Minister of Health from issuing a Notice of Compliance to Teva Canada Limited (“Teva”) for its generic quetiapine fumarate product relating to Seroquel XR . Also in March 2013, AstraZeneca discontinued its application to prohibit the Canadian Minister of Health from issuing a Notice of Compliance to Sandoz Canada Inc. (Sandoz) for its generic quetiapine fumarate product relating to Seroquel XR . AstraZeneca previously filed a patent infringement action against Sandoz related to Seroquel XR.

Product liability litigation

Seroquel IR (quetiapine fumarate)

As previously disclosed, a putative class action was initiated in Ontario, Canada alleging that AstraZeneca failed to provide adequate warnings in connection with an alleged association between Seroquel IR and certain medical conditions.  In February 2013, the Ontario Divisional Court dismissed the plaintiffs’ appeal of a lower court decision denying class certification. In March 2013, the plaintiffs served notice of their motion to seek leave to appeal to the Court of Appeal for Ontario.

With regard to insurance coverage for the substantial legal defence costs and settlements that have been incurred in connection with the Seroquel IR product liability claims in the US related to alleged diabetes and/or other related injuries (which now exceed the total amount of insurance coverage available), disputes continue with insurers about the availability of coverage under certain insurance policies. These policies have aggregate coverage limits of $300 million. Legal proceedings were brought in the UK against two of the insurers in respect of policies with aggregate coverage limits of $200 million; in February 2013, the London High Court issued a judgment on preliminary legal issues which ruled that AstraZeneca was not entitled to recover under those policies. AstraZeneca intends to appeal the decision. AstraZeneca had not recognised an insurance receivable prior to this ruling.

 
10
 
 
Commercial litigation

Nexium (esomeprazole magnesium)

In a class action lawsuit against AstraZeneca based on allegations that its promotion and advertising of Nexium to physicians, consumers and third party payers was unfair, unlawful, and deceptive, the Massachusetts State Court in February 2013 granted plaintiffs’ unopposed motion for preliminary approval of the class settlement agreement. The final approval hearing is scheduled for July 31, 2013.

Toprol-XL (metoprolol succinate)

AstraZeneca is defending anti-trust claims in the US regarding the listing and enforcement of patents protecting Toprol-XL .  In March 2013, the US District Court for the District of Delaware entered an Order and Final Judgment approving the Company’s settlement agreement with the end-payers, for which a provision had been taken in 2012.

Other commercial litigation

Medco qui tam litigation (Schumann)

In February 2013, plaintiff in the qui tam litigation in the US District Court for the Eastern District of Pennsylvania filed a notice of appeal to the US Court of Appeals for the Third Circuit with regard to the District Court’s decision to dismiss AstraZeneca from the litigation with prejudice.

ITEM 6. DIRECTORS, SENIOR MANAGEMENT AND EMPLOYEES
 
A. Directors and Senior Management
 
The information (including tabular data) set forth under the headings “Corporate Governance—Board of Directors” and “—Senior Executive Team” on pages 106 to 109, “Corporate Governance—Directors’ Remuneration Report—Policy Report—Service Contracts” and “—Policy on external appointments and retention of fees” on page 126 and “Directors’ Remuneration Report—Appendix – Additional Information—Directors’ emoluments in 2012—Directors’ remuneration – US dollars” (last sentence only) on page 133, in each case of the Company’s “Annual Report and Form 20-F Information 2012” included as exhibit 15.1 to this Form 20-F dated March 25, 2013 is incorporated by reference.
 
Marc Dunoyer appointed as Executive Vice President, Global Portfolio & Product Strategy
 
On March 21, 2013, AstraZeneca announced that Marc Dunoyer is to join the Company in the newly created role of Executive Vice President, Global Portfolio & Product Strategy. He will be responsible for driving business strategy, including business development, mergers and acquisitions, portfolio and product strategies. His most critical priorities will be to bolster the core growth platforms and therapy areas through well executed business development initiatives and leadership of internal efforts.
 
Mr. Dunoyer will join AstraZeneca from GlaxoSmithKline (GSK), where, as Global Head of Rare Diseases, he established an integrated global capability in treatments for rare diseases from R&D through to commercialisation. He also serves as Chairman of GSK Japan and is a member of the Corporate Executive Team. Previously at GSK, he was President for Asia Pacific and Japan. Prior to joining GSK in 1999, he held a number of international positions in operations and general management at Hoechst Marion Roussel.
 
Mr. Dunoyer, who will join the company in the second quarter of 2013, will report to Pascal Soriot and will be a member of AstraZeneca’s Senior Executive Team. He holds an MBA from the Hautes Etudes Commerciales and has a Bachelor of Law degree from Paris University. He qualified as a Junior Certified Public Accountant in France.
 
 
11
 
 
B. Compensation
 
The information (including graphs and tabular data) set forth under the headings “Corporate Governance—Directors’ Remuneration Report” on pages 122 to 137, “Financial Statements—Notes to the Group Financial Statements—Note 18—Post-retirement benefits” on pages 167 to 172, “—Note 24—Employee costs and share plans for employees” on pages 179 to 182 and “—Note 27—Statutory and other information—Key management personnel compensation”, on page 190, in each case of the Company’s “Annual Report and Form 20-F Information 2012” included as exhibit 15.1 to this Form 20-F dated March 25, 2013 is incorporated by reference.
 
C. Board Practices
 
The information (including tabular data) set forth under the headings “Corporate Governance—Board of Directors” and “—Senior Executive Team” on pages 106 to 109, “Corporate Governance—Corporate Governance Report—Leadership” “—Reserved matters and delegation of authority”, and “—Operation of the Board” on pages 111, “—Board effectiveness” on pages 111 to 114, “—Audit Committee” on pages 115 to 117, “—Remuneration Committee”, “—Nomination and Governance Committee” and “—Science Committee”, on pages 117 to 118, “—Business organisation— Senior Executive Team” and “—Compliance and Group Internal Audit” on pages 118 to 119, “Corporate Governance—Directors’ Remuneration Report—Policy Report—Service contracts” and “—Policy on external appointments and retention of fees” on page 126 and “—Appendix – Additional Information—Non-Executive Directors” on page 132, in each case of the Company’s “Annual Report and Form 20-F Information 2012” included as exhibit 15.1 to this Form 20-F dated March 25, 2013 is incorporated by reference.

D. Employees
 
The information set forth under the headings “Performance—Business Review—People” (comprising the graphical data, and the “Managing change” and “Managing employee relations” sections only) on pages 43 to 46, “—Research and Development—Our resources” (first and second paragraphs only) on page 32, “—Supply and Manufacturing—Our resources” on page 41, “Strategy—Our strategy—Restructuring” on page 21, and “Financial Statements—Notes to the Group Financial Statements—Note 24—Employee costs and share plans for employees—Employee costs” (including the tabular data) on pages 179 to 180, in each case of the Company’s “Annual Report and Form 20-F Information 2012” included as exhibit 15.1 to this Form 20-F dated March 25, 2013 is incorporated by reference. Please see also the information above under the headings Item 4 – “Business Overview—Strategy update—Strategy to return to growth and achieve scientific leadership—Simplification and productivity” and “—AstraZeneca to establish strategic R&D centres to enhance innovation and pipeline productivity”.
 
E. Share Ownership
 
The information (including graphs and tabular data) set forth under the headings “Financial Statements—Notes to the Group Financial Statements—Note 24—Employee costs and share option plans for employees” on pages 179 to 182, “Corporate Governance—Corporate Governance Report—Other matters—Directors’ shareholdings” on page 120, “Corporate Governance—Directors’ Remuneration Report—Appendix – Additional information—Directors’ interests in shares” on pages 134 to 137, and “Additional Information—Shareholder Information—Options to purchase securities from registrant or subsidiaries” on page 205, in each case of the Company’s “Annual Report and Form 20-F Information 2012” included as exhibit 15.1 to this Form 20-F dated March 25, 2013 is incorporated by reference.
 
ITEM 7. MAJOR SHAREHOLDERS AND RELATED PARTY TRANSACTIONS
 
A. Major Shareholders
 
The information set forth under the heading “Additional Information—Shareholder Information—Major shareholdings” (including tabular data) on pages 204 to 205 of the Company’s “Annual Report and Form 20-F Information 2012” included as exhibit 15.1 to this Form 20-F dated March 25, 2013 is incorporated by reference.
 
 
12
 
 
B. Related Party Transactions
 
The information set forth under the headings “Financial Statements—Notes to the Group Financial Statements—Note 27—Statutory and other information—Related party transactions” on page 190 and “Additional Information—Shareholder Information—Related party transactions” on page 205, in each case of the Company’s “Annual Report and Form 20-F Information 2012” included as exhibit 15.1 to this Form 20-F dated March 25, 2013 is incorporated by reference.
 
C. Interests of Experts and Counsel
 
Not applicable.
 
ITEM 8. FINANCIAL INFORMATION
 
A. Consolidated Statements and Other Financial Information
 
Please see the information below under the heading Item 18 – “Financial Statements.” The information (including graphs and tabular data) set forth under the headings  “Additional Information—Shareholder Information” on pages 203 to 207, “Performance—Financial Review—Capitalisation and shareholder return—Dividend and share repurchases” on page 94 and “Corporate Governance—Corporate Governance Report—Other matters—Distributions to shareholders and dividends for 2012” on page 120, in each case of the Company’s “Annual Report and Form 20-F Information 2012” included as exhibit 15.1 to this Form 20-F dated March 25, 2013 is incorporated by reference.
 
B. Significant Changes
 
Please see the information above under the heading Item 5 – “Operating and Financial Review and Prospects—Developments in Legal Proceedings” for information as to recent developments in certain legal proceedings disclosed under the heading “Financial Statements—Notes to the Group Financial Statements—Note 25—Commitments and contingent liabilities” on pages 183 to 189, of the Company’s “Annual Report and Form 20-F Information 2012” included as exhibit 15.1 to this Form 20-F dated March 25, 2013.
 
Other than as disclosed herein, since the date of the annual consolidated financial statements included in this Form 20-F dated March 25, 2013, no significant change has occurred.
 
ITEM 9.  THE OFFER AND LISTING
 
A. Offer and Listing Details
 
The information (including tabular data) set forth under the heading “Additional Information—Shareholder Information—AstraZeneca PLC share listings and prices” on pages 203 to 204 of the Company’s “Annual Report and Form 20-F Information 2012” included as exhibit 15.1 to this Form 20-F dated March 25, 2013 is incorporated by reference.
 
In addition, the table below sets forth, for the periods indicated, the reported high and low share prices of AstraZeneca PLC, on the following bases:
 
 
·
for shares listed on the London Stock Exchange (LSE) the reported high and low middle market closing quotations are derived from the Daily Official List;
 
 
·
for shares listed on the Stockholm Stock Exchange (SSE) the high and low closing sales prices are as stated in the Official List; and
 
 
·
for American Depositary Shares (ADS) listed on the New York Stock Exchange the reported high and low sales prices are as reported by Dow Jones (ADR quotations).
 
 
13
 
 
   
Ordinary LSE
   
AstraZeneca
ADS
   
Ordinary SSE(1)
 
   
High
(GB pence)
   
Low
(GB pence)
   
High
($)
   
Low
($)
   
High
(SEK)
   
Low
(SEK)
 
2013 – February
    3068.5       2910.0       48.42       44.67       305.6       284.5  
2013 – January
    3168.0       2969.0       50.06       47.84       322.0       308.4  
2012 – December
    3042.5       2909.5       48.90       46.88       326.3       306.4  
2012 – November
    2966.5       2792.5       47.55       44.34       316.7       300.8  
2012 – October
    2951.0       2860.0       47.63       45.82       313.2       307.0  
2012 – September
    2976.0       2888.5       48.36       46.34       316.9       307.3  

   
Ordinary LSE
   
AstraZeneca
ADS
   
Ordinary SSE(1)
 
   
High
(GB pence)
   
Low
(GB pence)
   
High
($)
   
Low
($)
   
High
(SEK)
   
Low
(SEK)
 
2012
    3111.5       2591.0       48.90       40.03       329.5       286.2  
2012 – Quarter 4
    3042.5       2792.5       48.90       44.34       326.3       300.8  
2012 – Quarter 3
    3096.0       2882.0       48.36       45.01       326.4       307.3  
2012 – Quarter 2
    2867.0       2591.0       46.22       40.03       309.3       286.2  
2012 – Quarter 1
    3111.5       2778.5       48.58       44.18       329.5       294.5  

   
Ordinary LSE
   
AstraZeneca
ADS
   
Ordinary SSE(1)
 
   
High
(GB pence)
   
Low
(GB pence)
   
High
($)
   
Low
($)
   
High
(SEK)
   
Low
(SEK)
 
2011
    3194.0       2543.5       52.40       40.95       328.5       269.3  
2011 – Quarter 4
    3080.5       2731.5       49.89       42.53       319.0       293.7  
2011 – Quarter 3
    3166.5       2543.5       51.08       40.95       324.5       269.3  
2011 – Quarter 2
    3194.0       2895.0       52.40       46.60       328.5       294.2  
2011 – Quarter 1
    3073.5       2801.5       49.38       45.40       320.6       289.0  

   
Ordinary LSE
   
AstraZeneca
ADS
   
Ordinary SSE(1)
 
   
High
(GB pence)
   
Low
(GB pence)
   
High
($)
   
Low
($)
   
High
(SEK)
   
Low
(SEK)
 
2010
    3,385       2,732       53.50       40.91       382.2       309.3  
2009
    2,947       2,147       47.54       30.24       365.0       261.5  
2008
    2,888       1,748       49.85       34.10       340.5       211.5  
(1) Principally held in bearer form.


B. Plan of Distribution
 
Not applicable.
 
C. Markets
 
The information (including tabular data) set forth under the heading “Additional Information—Shareholder Information—AstraZeneca PLC share listings and prices” on pages 203 to 204 of the Company’s “Annual Report and Form 20-F Information 2012” included as exhibit 15.1 to this Form 20-F dated March 25, 2013 is incorporated by reference.
 
D. Selling Shareholders
 
Not applicable.
 
 
14
 
 
E. Dilution
 
Not applicable.
 
F. Expenses of the Issue
 
Not applicable.
 
ITEM 10. ADDITIONAL INFORMATION
 
A. Share Capital
 
Not applicable.
 
B. Memorandum and Articles of Association
 
The information set forth under the heading “Additional Information—Corporate Information—Articles” on page 208 of the Company’s “Annual Report and Form 20-F Information 2012” included as exhibit 15.1 to this Form 20-F dated March 25, 2013 is incorporated by reference.
 
C. Material Contracts
 
Not applicable.
 
D. Exchange Controls
 
The information set forth under the headings “Additional Information—Shareholder Information—Exchange controls and other limitations affecting security holders” on page 207 of the Company’s “Annual Report and Form 20-F Information 2012” included as exhibit 15.1 to this Form 20-F dated March 25, 2013 is incorporated by reference.
 
E. Taxation
 
The information set forth under the headings “Additional Information—Shareholder Information—Taxation for US residents”, “—UK and US income taxation of dividends”, “—Taxation on capital gains”, “—Passive Foreign Investment Company (PFIC) rules”, “—Information reporting and backup withholding”, “—UK inheritance tax” and “—UK stamp duty reserve tax and stamp duty” on pages 206 to 207 of the Company’s “Annual Report and Form 20-F Information 2012” included as exhibit 15.1 to this Form 20-F dated March 25, 2013 is incorporated by reference.
 
F. Dividends and Paying Agents
 
Not applicable.
 
G. Statement by Experts
 
Not applicable.
 
H. Documents on Display
 
The information set forth under the heading “Additional Information—Shareholder Information—Documents on display” on page 206 of the Company’s “Annual Report and Form 20-F Information” included as exhibit 15.1 to this Form 20-F dated March 25, 2013 is incorporated by reference.
 
In addition, we file reports and other information with the United States Securities and Exchange Commission (the “SEC”). You can read and copy these reports and other information at the SEC’s Public Reference Room at 100 F Street, N.E., Washington, D.C. 20549. You can call the SEC at 1-800-SEC-0330 for further information on the Public Reference Room. The SEC also maintains a website at www.sec.gov which contains in electronic form each of the reports and other information that we have filed electronically with the SEC.
 
 
15
 
 
I. Subsidiary Information
 
Not applicable.
 
ITEM 11. QUANTITATIVE AND QUALITATIVE DISCLOSURES ABOUT MARKET RISK
 
The information (including graphs and tabular data) set forth under the headings “Performance—Financial Review—Financial risk management” on page 99 and “Financial Statements—Note 23—Financial risk management objectives and policies” on pages 175 to 179, in each case of the Company’s “Annual Report and Form 20-F Information 2012” included as exhibit 15.1 to this Form 20-F dated March 25, 2013 is incorporated by reference.
 
ITEM 12. DESCRIPTION OF SECURITIES OTHER THAN EQUITY SECURITIES
 
A. Debt Securities
 
Not applicable.
 
B. Warrants and Rights
 
Not applicable.
 
C. Other Securities
 
Not applicable.
 
D. American Depositary Shares
 
Fees and Charges Payable by ADR Holders
 
The Company’s American Depositary Receipt (“ADR”) program is administered by JPMorgan Chase Bank, N.A. (“J.P. Morgan”), as the depositary. The holder of an ADR may have to pay the following fees and charges to J.P. Morgan in connection with ownership of the ADR:
 
Category
Depositary actions
Associated fee or charge
(a) Depositing or substituting the underlying shares
Issuances against deposits of shares, including deposits and issuances pursuant to a stock dividend or stock split declared by the Company or issuances pursuant to a merger, exchange of securities or any other transaction or event affecting the ADSs or the deposited securities
Up to $5.00 for each 100 ADSs (or portion thereof) issued or delivered (as the case may be)
 
The depositary may sell (by public or private sale) sufficient securities and property received in respect of share distributions, rights and other distributions prior to such deposit to pay such charge
(b) Receiving or distributing dividends (1)
Cash distributions made pursuant to the deposit agreement
$0.05 or less per ADS
(c) Selling or exercising rights
Distribution or sale of securities, the fee being in an amount equal to the fee for the execution and delivery of ADSs which would have been charged as a result of the deposit of such securities
Up to $5.00 for each 100 ADSs (or portion thereof)
 
 
16
 
 
Category
Depositary actions
Associated fee or charge
(d) Withdrawing, cancelling or reducing an underlying security
Acceptance of ADSs surrendered for withdrawal, cancellation or reduction of deposited securities
Up to $5.00 for each 100 ADSs (or portion thereof) surrendered, cancelled or reduced (as the case may be)
 
The depositary may sell (by public or private sale) sufficient securities and property received in respect of share distributions, rights and other distributions prior to such deposit to pay such charge
(e) Transferring, combination or split-up of receipts
Transfer, combination and split-up of ADRs
$1.50 per ADR
(f) General depositary services, particularly those charged on an annual basis (1)
Services performed by the depositary in administering the ADRs
$0.05 or less per ADS per calendar year (or portion thereof), payable at the sole discretion of the depositary by billing ADR holders or by deducting such charge from one or more cash dividends or other cash distributions
(g) Fees and expenses of the depositary
Fees and expenses incurred by the depositary or the depositary’s agents on behalf of holders, including in connection with:
Expenses payable at the sole discretion of the depositary by billing ADR holders or by deducting such charges from one or more cash dividends or other cash distributions
 
·       compliance with foreign exchange control regulations or any law or regulation relating to foreign investment
 
·       stock transfer or other taxes and governmental charges
 
·       cable, telex and facsimile transmission and delivery charges
 
·       fees for the transfer or registration of deposited securities in connection with the deposit or withdrawal of deposited securities
 
·      expenses of the depositary in connection with the conversion of foreign currency into US dollars
 
 
 
17
 
 
Category
Depositary actions
Associated fee or charge
 
·      any other charge payable by the depositary or the depositary’s agents in connection with the servicing of the shares or other deposited securities (which charge shall be assessed against holders as of the record date or dates set by the depositary)
 
(1)
J.P. Morgan has agreed that it shall not charge ADR holders any of these fees without the Company’s prior written consent. No such fees have been charged for the year ended December 31, 2012 or from January 1, 2013 to the date hereof.
 
Fees and Payments Made by the Depositary to us
 
J.P. Morgan, as ADR depositary, has agreed to reimburse certain expenses related to the Company’s ADR program and incurred by the Company in connection with the program. For the year ended December 31, 2012, the ADR depositary reimbursed to the Company, or paid on its behalf to third parties, a total sum of $1,620,852 (comprised of reimbursements of $1,279,626 and payments to third parties of $120,852, in each case as detailed in the tables below). The ADR depositary also waived certain of its fees for standard costs associated with the administration of the ADR program in a total amount of $220,374.
 
The table below sets forth the types of expenses that the ADR depositary has agreed to reimburse and the amounts reimbursed within each such category for the year ended December 31, 2012:
 
 
Category of Expenses – Direct Payments
 
Reimbursement for the year ended December 31, 2012
 
ADR program expenses, including investor relations costs and legal fees
  $ 1,279,626  
Total
  $ 1,279,626  

The ADR depositary has paid certain expenses directly to third parties on behalf of the Company and has agreed to waive certain of its fees for standard costs associated with the administration of the ADR program. The table below sets forth those expenses that the ADR depositary paid directly to third parties, and those fees waived, in each case for the year ended December 31, 2012.
 
 
Category of Expenses – Indirect Payment
 
Amount paid for the year ended
December 31, 2012
 
Expenses paid by depositary to third parties on behalf of the Company – NYSE listing fees
  $ 120,852  
Fees waived by depositary for standard ADR program costs
  $ 220,374  
Total
  $ 341,226  

Under certain circumstances, including removal of the ADR depositary or termination of the ADR program by the Company, the Company is required to repay the ADR depositary certain amounts reimbursed and/or expenses paid to or on behalf of the Company. No such repayments were made during the year ended December 31, 2012.
 
 
PART II
 
ITEM 13. DEFAULTS, DIVIDEND ARREARAGES AND DELINQUENCIES
 
Not applicable.
 
ITEM 14. MATERIAL MODIFICATIONS TO THE RIGHTS OF SECURITY HOLDERS AND USE OF PROCEEDS
 
Not applicable.
 
 
18
 
 
ITEM 15. CONTROLS AND PROCEDURES
 
The information set forth under the heading “Corporate Governance—Corporate Governance Report—Board composition, processes and responsibilities” and “—Accountability” on pages 110 and 114, respectively, “—Corporate Corporate Governance Report—Audit Committee” on pages 115 to 117 (the last four paragraphs of the “Audit Committee” section only, excluding the “Code of Conduct” section), “—US corporate governance requirements” on page 118 (the first and second paragraphs only), “—Corporate Governance Report—Business organisation—Disclosure Committee” on page 119 and “Financial Statements—Directors’ Responsibilities for, and Report on, Internal Control over Financial Reporting” on page 140, in each case of the Company’s “Annual Report and Form 20-F Information 2012” included as exhibit 15.1 to this Form 20-F dated March 25, 2013 is incorporated by reference.
 
Management’s Annual Report on Internal Control over Financial Reporting
 
As required by US regulations, management is responsible for establishing and maintaining adequate internal control over financial reporting for the Company, and is required to identify the framework used to evaluate the effectiveness of the Company’s internal control over financial reporting and to assess the effectiveness of such internal control. In this regard, management has made the same assessment and reached the same conclusion as that set forth in the section entitled “Financial Statements—Director’s Responsibilities for, and Report on, Internal Control over Financial Reporting” on page 140 of the Company’s “Annual Report and Form 20-F Information 2012” included as exhibit 15.1 to this Form 20-F dated March 25, 2013, which is incorporated herein by reference.
 
Report of Independent Registered Public Accounting Firm
 
The Board of Directors and Stockholders
AstraZeneca PLC:
 
We have audited AstraZeneca PLC’s (“the Company”) internal control over financial reporting as of 31 December 2012, based on criteria established in Internal Control – Integrated Framework issued by the Committee of Sponsoring Organizations of the Treadway Commission (“COSO”). AstraZeneca’s management is responsible for maintaining effective internal control over financial reporting and for its assessment of the effectiveness of internal control over financial reporting. Our responsibility is to express an opinion on the Company’s internal control over financial reporting based on our audit.
 
We conducted our audit in accordance with the standards of the Public Company Accounting Oversight Board (United States) (“PCAOB”). Those standards require that we plan and perform the audit to obtain reasonable assurance about whether effective internal control over financial reporting was maintained in all material respects. Our audit included obtaining an understanding of internal control over financial reporting, assessing the risk that a material weakness exists, and testing and evaluating the design and operating effectiveness of internal control based on the assessed risk. Our audit also included performing such other procedures as we considered necessary in the circumstances. We believe that our audit provides a reasonable basis for our opinion.
 
A company’s internal control over financial reporting is a process designed to provide reasonable assurance regarding the reliability of financial reporting and the preparation of financial statements for external purposes in accordance with generally accepted accounting principles. A company’s internal control over financial reporting includes those policies and procedures that (1) pertain to the maintenance of records that, in reasonable detail, accurately and fairly reflect the transactions and dispositions of the assets of the company; (2) provide reasonable assurance that transactions are recorded as necessary to permit preparation of financial statements in accordance with generally accepted accounting principles, and that receipts and expenditures of the company are being made only in accordance with authorizations of management and directors of the company; and (3) provide reasonable assurance regarding prevention or timely detection of unauthorized acquisition, use, or disposition of the company’s assets that could have a material effect on the financial statements.
 
Because of its inherent limitations, internal control over financial reporting may not prevent or detect misstatements. Also, projections of any evaluation of effectiveness to future periods are subject to the risk that controls may become inadequate because of changes in conditions, or that the degree of compliance with the policies or procedures may deteriorate.
 
 
19
 
 
In our opinion, AstraZeneca PLC maintained, in all material respects, effective internal control over financial reporting as of 31 December 2012, based on criteria established in Internal Control – Integrated Framework issued by the Committee of Sponsoring Organizations of the Treadway Commission.
 
We also have audited, in accordance with the standards of the PCAOB, the Consolidated Statement of Financial Position of AstraZeneca and subsidiaries as of 31 December 2012, 2011 and 2010, and the related Consolidated Statements of Comprehensive Income, Changes in Equity, and Cash Flows for each of the years in the three-year period ended 31 December 2012, and our report dated 31 January 2013 expressed an unqualified opinion on those Consolidated Financial Statements.
 
KPMG Audit Plc
15 Canada Square
London
United Kingdom
E14 5GL

31 January 2013

ITEM 16. RESERVED
 
ITEM 16A. AUDIT COMMITTEE FINANCIAL EXPERT
 
The information set forth under the heading “Corporate Governance—Corporate Governance Report—Board composition, processes and responsibilities—Board Committee membership” (consisting of tabular data) on page 112 and in the first paragraph under the heading “—Corporate Governance Report—Audit Committee” on page 115, in each case of the Company’s “Annual Report and Form 20-F Information 2012” included as exhibit 15.1 to this Form 20-F dated March 25, 2013 is incorporated by reference.
 
ITEM 16B. CODE OF ETHICS
 
The information set forth under the headings “Corporate Governance—Corporate Governance Report—Audit Committee—Code of Conduct” on page 117 and “Performance—Business Review—Compliance—Code of Conduct” on page 47, in each case of the Company’s “Annual Report and Form 20-F Information 2012” included as exhibit 15.1 to this Form 20-F dated March 25, 2013 is incorporated by reference.
 
The Company’s Code of Conduct is available at www.astrazeneca.com.
 
ITEM 16C. PRINCIPAL ACCOUNTANT FEES AND SERVICES
 
   
Year ended December 31,
 
   
2012
   
2011
 
   
($ million)
 
Audit Fees
    9.2       9.8  
Audit-Related Fees
    0.5       0.6  
Tax Fees
    0.9       0.9  
All Other Fees
    1.3       3.0  
Total
    11.9       14.3  

Audit fees consist of $5.0 million for the audit of subsidiaries pursuant to legislation (2011 $5.5 million), $2.2 million for the Group audit (2011 $2.4 million), $1.7 million in respect of section 404 of the Sarbanes-Oxley Act (2011 $1.9 million) and $0.3 million for assurance services provided in relation to the issuance by the Company in 2012 of $1 billion of its 1.95% notes due 2019 and $1 billion of its 4.00% notes due 2042.

 
20
 
 
Audit-related fees are $0.5 million for the audit of subsidiaries’ pension schemes (2011: $0.6 million). Tax fees consist of tax compliance services and, to a lesser extent, tax advice.

All other fees consist of fees of $1.3 million (2011: $3.0 million) for assurance services in relation to interim financial statements, the expansion of the Group’s diabetes alliance with BMS through the acquisition by BMS of Amylin, compliance with licensing agreements, review of EuropeSAP testing and follow-up, assistance with the IS/IT SOx Uplift Programme and attestation for the UK PPRS report.

The information (including tabular data) set forth under the heading “Corporate Governance—Corporate Governance Report—Audit Committee” (excluding the “Code of Conduct” section) on pages 115 to 117 of the Company’s “Annual Report and Form 20-F Information 2012” included as exhibit 15.1 to this Form 20-F dated March 25, 2013 is incorporated by reference.
 
ITEM 16D. EXEMPTIONS FROM THE LISTING STANDARDS FOR AUDIT COMMITTEES
 
Not applicable.
 
ITEM 16E. PURCHASES OF EQUITY SECURITIES BY THE ISSUER AND AFFILIATED PURCHASERS
 
 
Period
 
(a) Total number of Shares (or Units) Purchased
   
(b) Average Price Paid per Share (or Unit)
   
(c) Total Number of Shares (or Units) Purchased as Part of Publicly Announced Plans or Programs
   
(d) Maximum Number (or Approximate Dollar Value) of Shares (or Units) that May Yet Be Purchased Under the Plans or Programs
 
         
($)
         
($ billion)
 
Month #1
   Jan 1 - Jan 31
    9,407,043       47.34       9,407,043       2.2  
Month #2
   Feb 1 - Feb 28
    6,984,893       46.62       6,984,893       1.9  
Month #3
   Mar 1 - Mar 31
    6,193,262       44.99       6,193,262       1.6  
Month #4
   Apr 1 - Apr 30
    5,791,989       44.82       5,791,989       1.3  
Month #5
   May 1 - May 31
    6,912,478       42.10       6,912,478       1.0  
Month #6
   Jun 1 - Jun 30
    5,751,576       42.45       5,751,576       0.8  
Month #7
   Jul 1 - Jul 31
    9,988,454       45.79       9,988,454       0.3  
Month #8
   Aug 1 - Aug 31
    4,252,593       47.07       4,252,593       0.1  
Month #9
   Sep 1 - Sep 30
    2,535,000       47.05       2,535,000       0.0  
Month #10
   Oct 1 - Oct 31
    0       N/A       0       N/A  
Month #11
   Nov 1 - Nov 30
    0       N/A       0       N/A  
Month #12
   Dec 1 - Dec 31
    0       N/A       0       N/A  
Total
    57,817,288       45.34       57,817,288       N/A  

 
21
 
 
All of the purchases reflected in the table above were made pursuant to our publicly announced share repurchase program, which was announced by the Company on January 27, 2011 and extended on February 2, 2012, when the Company stated that, subject to market conditions and business needs, share repurchases (net of new issues) for the full year 2012 were anticipated to be approximately $4.5 billion. On October 1, 2012, the Company announced the suspension of the share repurchase program with immediate effect. On October 25, 2012, the Company announced that share repurchases (net of new issues) for the period of January 1 to September 30, 2012 amounted to $2,273 million. Excluding new issues, share repurchases for the full year amounted to $2,635 million. There have been no share repurchases since October 1, 2012, and on January 31, 2013 the Company announced that no share repurchases will take place in 2013 in order to maintain the flexibility to invest in the Company’s business.
 
ITEM 16F. CHANGE IN REGISTRANT’S CERTIFYING ACCOUNTANT
 
Not applicable.
 
ITEM 16G. CORPORATE GOVERNANCE
 
AstraZeneca PLC is a public limited company incorporated in England and Wales, admitted to the Official List of the Financial Services Authority (“FSA”) and to trading on the main market of the London Stock Exchange. As a result, it follows the UK Corporate Governance Code (the “UK Code”), the 2012 edition of which came into effect for the Company as of January 1, 2013 (formerly, the UK Combined Code on Corporate Governance), in respect of its corporate governance practices. The Company has ADRs listed on the NYSE and, under the NYSE Corporate Governance Standards (the “NYSE Standards”) applicable to listed companies, as a foreign private issuer, the Company is permitted to follow the corporate governance practice of its home country in lieu of certain provisions of the NYSE Standards.
 
A summary of the significant ways in which the Company’s corporate governance practices differ from those followed by US domestic companies under the NYSE Standards is set forth below.
 
NYSE Standards
 
AstraZeneca Corporate Governance Practice
     
1.     Under the NYSE Standards, the audit committee is to be directly responsible for the appointment, compensation, retention and oversight of a listed company’s external auditor, unless there is a conflicting requirement under the home country laws of the company.
 
Under UK company law, a company’s external auditors are appointed by its shareholders. Under the UK Code, the Company’s audit committee is responsible for making recommendations to the Board of Directors, for the Board of Directors to propose to the Company’s shareholders in general meeting, in relation to the appointment, re-appointment and removal of the external auditors, and for approving the remuneration and terms of engagement of the external auditor. If the Board of Directors does not accept the audit committee’s recommendation, it should include in the annual report, and in any papers recommending appointment or re-appointment, a statement from the audit committee explaining the recommendation and should set out reasons why the Board of Directors has taken a different position.
     
2.     Under the NYSE Standards, the nominating/corporate governance committee and compensation committee are to be composed entirely of independent directors.
 
Under the UK Code, a majority of the members of a company’s nomination committee, and all of the members of its remuneration committee, should be independent non-executive directors. The chairman of the company may be a member of, but not chair, the remuneration committee, provided he or she was considered independent on appointment as chairman (under the UK Code, the test of independence is not appropriate in relation to the chairman thereafter), and in the case of the nomination committee, the chairman may chair such committee.
 
 
22
 
 
NYSE Standards
 
AstraZeneca Corporate Governance Practice
     
   
The Company’s Nomination and Governance Committee and Remuneration Committee each includes four members, including the chairman of the Company’s Board of Directors, with the remainder all being considered by the Company’s Board of Directors to be independent in accordance with the principles and criteria of the UK Code. The Company’s chairman was considered to be independent upon his appointment as chairman.
     
3.     Under the NYSE Standards, the compensation committee is to make recommendations to the listed company’s Board of Directors with respect to non-CEO executive officer compensation and certain other compensation plans which are subject to Board approval.
 
In compliance with the UK Code, the Company’s Remuneration Committee determines the Company’s global remuneration frameworks and principles, approves individual salary decisions and related matters for members of the Company’s Board of Directors, Senior Executive Team (“SET”) and the Company Secretary, and reviews annual bonus payments for all executives reporting directly to SET members. While the Remuneration Committee does not make initial recommendations to the Board of Directors in this respect, it does report to the Board of Directors on these matters.
     
4.     Under the NYSE Standards, shareholders are entitled to vote on all equity compensation plans and material revisions thereto, with certain limited exemptions.
 
Under the listing rules of the UK Listing Authority (the “UKLA Rules”), with which the Company complies, shareholder approval is required to be obtained by the Company for the adoption of equity compensation plans which are either long-term incentive schemes in which directors of the Company can participate or schemes which may involve the issue of new shares. Under the UKLA Rules, these plans may not be changed to the benefit of the plan participants unless shareholder approval is obtained (with certain minor exceptions, for example, to benefit the administration of the plan or to take account of tax benefits). The UKLA Rules in respect of shareholder approval regarding equity compensation plans, or any material revision thereto, may differ from the NYSE Standards.
     
5.     Under the NYSE Standards, each listed company Chief Executive Officer must certify to the NYSE each year that he or she is not aware of any violation by the listed company of any NYSE corporate governance listing standards.
 
As the Company is a foreign private issuer, the Company’s Chief Executive Officer is not required to make this certification. He is, however, required to promptly notify the NYSE in writing after any executive officer of the Company becomes aware of any non-compliance with any NYSE corporate governance rules applicable to the Company.
 
The information set forth under the heading “Corporate Governance—Corporate Governance Report—US corporate governance requirements” (final paragraph only) on page 118 of the Company’s “Annual Report and Form 20-F Information 2012” included as exhibit 15.1 to this Form 20-F dated March 25, 2013 is incorporated by reference.
 
 
23
 
 
ITEM 16H. MINE SAFETY DISCLOSURE
 
Not applicable.
 
PART III
 
ITEM 17. FINANCIAL STATEMENTS
 
The Company has responded to Item 18 in lieu of this item.
 
ITEM 18. FINANCIAL STATEMENTS
 
The information set forth in Exhibit 15.2 hereto “Report of Independent Registered Public Accounting Firm to the Board of Directors and Stockholders of AstraZeneca PLC by KPMG Audit Plc” is incorporated in this section by reference. The information (including tabular data) set forth under the headings “Financial Statements” on pages 142 to 191 (including the information set forth under the subheading “Notes to the Group Financial Statements” on pages 150 to 190), “Financial Statements—Group Financial Record” on page 198 and “—Principal Subsidiaries” on page 191, in each case of the Company’s “Annual Report and Form 20-F Information 2012” included as exhibit 15.1 to this Form 20-F dated March 25, 2013 is incorporated by reference.
 
Please see the information above under the heading Item 5 – “Operating and Financial Review and Prospects—Developments in Legal Proceedings” for information as to recent developments in certain legal proceedings disclosed under the heading “Financial Statements—Notes to the Group Financial Statements—Note 25—Commitments and contingent liabilities” on pages 183 to 189, of the Company’s “Annual Report and Form 20-F Information 2012” included as exhibit 15.1 to this Form 20-F dated March 25, 2013.
 
The information set out in the above-referenced financial statements does not constitute the Company’s statutory accounts under the UK Companies Act for the years ended December 31, 2012, 2011 or 2010. Those accounts have been reported on by the Company’s auditors; their reports were unqualified and did not contain a statement under section 498(2) or (3) of the Companies Act 2006. The accounts for 2011 and 2010 have been delivered to the UK registrar of companies and those for 2012 will be delivered in due course.
 
ITEM 19. EXHIBITS
 
1.1
Articles of Association.(1)
4.1
Master Restructuring Agreement dated as of June 19, 1998 between Astra AB, Merck & Co., Inc., Astra Merck Inc., Astra USA, Inc., KB USA, L.P., Astra Merck Enterprises, Inc., KBI Sub Inc., Merck Holdings, Inc. and Astra Pharmaceuticals, L.P.(2)
4.2
Letter agreement between AstraZeneca PLC and Pascal Soriot, and Agreement for Service between AstraZeneca UK Limited and Pascal Soriot, each dated August 27, 2012.
4.3
Agreement for Service between AstraZeneca PLC and Simon Lowth, dated September 27, 2007.(3)
4.4
Agreement for Service between AstraZeneca PLC and David R. Brennan dated December 16, 2005 (effective as of January 1, 2006).(4)
4.5
Form of Deed of Indemnity for Directors.(5)
4.6
License Agreement dated April 20, 1998, by and between Shionogi & Co., Ltd. and Zeneca Limited (the “License Agreement”).(6)
4.7
Amendment Agreement dated May 14, 2002, by and between Shionogi & Co., Ltd. and AstraZeneca UK Limited, to the License Agreement.(6)
 
 
24
 
 
4.8
Amendment No. 2, effective as of April 26, 2005, to the License Agreement.(6)
4.9
Amendment No. 3, effective as of December 5, 2008, to the License Agreement.(6)
4.10
Amendment No. 4, effective as of February 19, 2009, to the License Agreement.(6)
4.11
Amendment No. 5, effective as of November 12, 2012, to the License Agreement.(6)
7.1
Statement explaining calculation of ratio of earnings to fixed charges.
8.1
List of subsidiaries.
12.1
Certification of Pascal Soriot filed pursuant to 17 CFR 240.13a-14(a).
12.2
Certification of Simon Lowth filed pursuant to 17 CFR 240.13a-14(a).
13.1
Certification of Pascal Soriot and Simon Lowth furnished pursuant to 17 CFR 240.13a-14(b) and 18 U.S.C. 1350.
15.1
Annual Report and Form 20-F Information 2012.(7)
15.2
Report of Independent Registered Public Accounting Firm to the Board of Directors and Stockholders of AstraZeneca PLC by KPMG Audit Plc.
15.3
Consent of KPMG Audit Plc, independent registered public accounting firm.
15.4
Consent of IMS Health HQ Limited.
15.5
Consent of Bureau Veritas UK Limited.
 
 
(1)
Incorporated into this Form 20-F by reference to AstraZeneca PLC’s Form 20-F filed April 28, 2011 (File No. 001-11960).
 
(2)
Incorporated into this Form 20-F by reference to AstraZeneca PLC’s Form 20-F filed March 25, 2003 (File No. 001-11960).
 
(3)
Incorporated into this Form 20-F by reference to AstraZeneca PLC’s Form 20-F filed March 12, 2008 (File No. 001-11960).
 
(4)
Incorporated into this Form 20-F by reference to AstraZeneca PLC’s Form 20-F filed March 23, 2006 (File No. 001-11960).
 
(5)
Incorporated into this Form 20-F by reference to AstraZeneca PLC’s Form 20-F filed March 27, 2007 (File No. 001-11960).
 
(6)
Incorporated into this Form 20-F by reference to AstraZeneca PLC’s Form 20-F/A filed September 21, 2012 (File No. 001-11960).
 
(7)
Certain of the information included within exhibit 15.1, which is provided pursuant to Rule 12b-23(a)(3) of the Securities Exchange Act of 1934, as amended, is incorporated by reference in this Form 20-F, as specified elsewhere in this Form 20-F. With the exception of the items and pages so specified, the Annual Report and Form 20-F Information 2012 is not deemed to be filed as part of this Annual Report on Form 20-F.
 
 
25
 
 
SIGNATURE
 
The registrant hereby certifies that it meets all of the requirements for filing on Form 20-F and that it has duly caused and authorized the undersigned to sign this annual report on its behalf.
 
 
AstraZeneca PLC
 
   
       
By:  /s/ A C N Kemp  
  Name:
A C N Kemp
 
  Title:
Authorized Signatory
 
 
London, England
March 25, 2013
 
26
 
Exhibit 4.2
[ASTRAZENECA PLC LETTERHEAD]

Strictly private and confidential
 

Mr P Soriot


27 July 2012
 

 
Dear Pascal,
 
Further to our recent discussions, I now have great pleasure in offering you the position of Chief Executive Officer of AstraZeneca PLC (“CEO”) with a Base Salary of £1,100,000.  Ideally, we would wish you to take up this position as soon as possible, and certainly envisage that you will come to the UK to take up these duties as soon as you are released from your present position.

The terms and conditions that will apply to your employment with AstraZeneca UK Limited (“the Company”) are set out in this offer letter and the enclosed Service Agreement.  If you wish to accept this offer and commence your employment with the Company, you will be eligible to receive the payments and benefits set out in this letter, on and subject to its terms.  This letter should be read in conjunction with the terms of the Service Agreement between you and the Company.  In the event of any conflict between the terms of this offer letter and the Service Agreement, this offer letter will prevail.
 
1. 
Annual Short Term Incentive (STI)
 
You will be eligible to participate in the Global Executive Bonus Plan (GEBP).  The rules of the GEBP are determined by the Remuneration Committee on an annual basis in its absolute discretion.  In the performance year 2012, this plan is based on the following measures:
 
Measure
 
Contribution
to outcome
Global Scorecard including:
   
Earnings Per Share
45%
 
Cashflow
15%
60%
Other Global Scorecard Measures
40%
 
SET Area Scorecards
  40%
 
This plan will provide you with an opportunity to be awarded an annual bonus in the range of 0%-180% of your base salary (with 100% of your base salary representing on target performance) based on the achievement of personal objectives linked to performance across all functional areas.  In the first year of your employment any award under the GEBP would be pro-rated to reflect your
 
 
 
 
 
start date part way through the performance year.  A proportion (currently one-third) of any actual bonus awarded would be paid as shares and deferred for three years. 1
 
The GEBP is discretionary and any bonuses are awarded in the absolute discretion of the Remuneration Committee and are not pensionable.
 
2. 
Long term incentives (LTIs)
 
You will be eligible for consideration annually for an award of LTIs with an expected value target of 250% and a maximum face value of 500% of your Base Salary using metrics that will measure and reward outstanding performance when compared against our industry peers.  Typically awards are granted in March.
 
For performance year 2013 you will be eligible to receive an LTI award in or around March 2013, as normal.
 
LTI awards are subject to satisfaction of appropriately stretching performance targets determined by the Remuneration Committee in its absolute discretion.  These are currently based on net cash flow and total shareholder return (TSR) in the case of Performance Shares, dividend growth and dividend cover spread in the case of the AstraZeneca Investment Plan (AZIP). 2    However, the applicable performance targets may change and are always subject to the absolute discretion of the Remuneration Committee.  LTI awards are not pensionable.
 
3. 
Sign-on arrangements
 
We understand you would be required to forego certain LTI awards on leaving Roche under the proposed circumstances and commencing employment with the Company.  After the commencement of your employment, you will receive the following awards from AstraZeneca, calculated on the basis of certain current unvested LTI awards from Roche:
 
 
·   
An award of restricted stock units to the value of £2m.  These units will vest, subject to the rules of the AstraZeneca Restricted Share Plan (as modified by this letter), on a time-elapsed basis as follows:
 
 
o   
40% on the first anniversary of the commencement of your employment with the Company;
 
 
o   
30% on the second anniversary of the commencement of your employment with the Company; and
 
 
o   
30% on the third anniversary of the commencement of your employment with the Company.
 
 
1 A copy of the plan rules relating to the deferred bonus is enclosed (the AstraZeneca Deferred Bonus Plan).
 
2 Copies of the plan rules relating to the LTI plans is enclosed (the AstraZeneca Performance Share Plan and AstraZeneca Investment Plan).
 
 
 
 
 
If the Company terminates your employment (other than in the circumstances set out at clause 15.6 of your service agreement)  at any time prior to the third anniversary of the commencement of your employment, then any tranche of the above award that has not yet vested shall not lapse and shall continue to vest on the timetable outlined above. In accordance with the rules of the Restricted Share Plan, the value of the stock for the purpose of determining the number of shares subject to the award will be the average of the middle market closing price on the date of the award.
 
 
·  
An award under the AZIP of shares to the value of £2m.  Vesting of this award will be subject to the rules of the AZIP (as modified by this letter) and to satisfaction of performance targets determined by the Remuneration Committee in its discretion.  Any AZIP award made during 2012 will have performance conditions based on the current 2012 AZIP performance schedule, which is based on dividend growth and dividend cover spread, as previously supplied to you.  The performance period for your AZIP award will be the four year period commencing on 1 January 2013, with a subsequent holding period of four years.
 
Should you leave the Company for any reason after the end of the performance period then vested amounts will be dealt with in accordance with the rules of the AZIP, save that if you give notice of the termination of your employment at any time after the end of the performance period but before the end of the holding period, you will be deemed to fall within clause 10.3(b) of the AZIP rules so that your sign-on AZIP awards will vest in accordance with the provisions of clause 10.4(b) of the AZIP rules.
 
In accordance with the rules of the AZIP, the value of the stock for the purpose of determining the number of shares subject to the award will be the average of the middle market closing price on the three consecutive Dealing Days (as defined in the rules) preceding the date of grant (or such other Dealing Day or Dealing Days as the Remuneration Committee may decide).
 
These awards will be made on a date to be agreed which shall be a date which is as soon as practicably possible during an open trading period immediately following the commencement of your employment with the Company.

In addition to the stock awards outlined above, you will also receive an award in lieu of any forfeited annual bonus at Roche.  The value of your forfeited bonus will be determined by the Remuneration Committee, in its discretion, applying appropriate pro-rating to reflect the period of the bonus year which has elapsed from 1 January 2012 to the final day of your employment with Roche.  A cash award equal to the value of such forfeited bonus amount will then be made to you, provided that you agree to apply such payment in full toward the purchase of shares in AstraZeneca to count towards meeting the share ownership expectation referred to below.  You agree that you shall work with the Board and Corporate Support Team to effect the purchase of such shares.
 
 
 
 
 
These awards are designed to compensate you for certain reward arrangements at Roche which you have advised us that you will be required to forego if you accept this offer.  The figures above will therefore be recommended for approval by the Remuneration Committee based on the information you have provided regarding your entitlements.  If this information is inaccurate, please let me know before signing this offer letter and the accompanying service agreement, as it will not be possible to increase these figures at a later date.

4. 
Share Ownership Expectation

It is the expectation of the Remuneration Committee that you will build up your own holding of shares in AstraZeneca PLC, with a value equivalent to 300% of your base salary.  This shareholding target can be reached in part through shares delivered from the various LTI arrangements, as well as the deferred part of any short-term incentive.  The expectation is that your shareholding should reach the target level within five years of the commencement of your employment and that you would not dispose of any net new shares acquired (after payment of the acquisition cost and any tax due) at least until such time as the target holding has been reached.  In addition, you will be expected to retain the net number of shares acquired through the exercise of any share options (after payment of the acquisition cost and any tax due) for at least six months.

5. 
Benefits

The Company operates a flexible benefits arrangement (AZ Advantage) which is designed to give participants flexibility over their selection of benefits.  The Advantage Fund is calculated by reference to base salary and your annual Advantage Fund will be £104,341 (excluding base salary and pension contribution).  Your Advantage Fund contains an element to reflect part of the Company’s cost of funding your Pension (24% of your annual base salary).  All contributions, which you elect to make to Pension, will be deducted from your Advantage Fund.  The Company’s contribution to pension is 24% of annual base salary.   The balance of your Advantage Fund will be used to purchase benefits from a range including private medical insurance, life assurance, Permanent Health Insurance and holidays, including benefits of your choice.  Your Advantage Fund is entirely flexible, so should you choose not to purchase from the range of benefits, including Pension, you can take the funding as cash.

The Company will fund the cost of providing a chauffeur to you after you have selected your preferred vehicle using the AZ Advantage scheme.

On commencement with AstraZeneca, we will provide reimbursement for you and your immediate family for private medical insurance cover that you may need to purchase if your cover with Roche expires before your cover with AstraZeneca commences.

6. 
Financial Planning and Tax Advice

You will be eligible for financial advice, available from a range of Independent Financial Advisers who have been appointed by the Company.  The facility is for
 
 
 
 
 
an initial assessment to the value of £2,000 plus VAT and annual reviews thereafter to the value of £1,000 plus VAT.  The cost of advice beyond these limits will be a matter for you.
 
In recognition of your change in tax status as you relocate to the UK, we will additionally provide you with additional tax preparation and planning support. PricewaterhouseCoopers LLP (PWC) in London is our preferred vendor in this regard.
 
7. 
Relocation assistance

You will be eligible for certain assistance from the Company in respect of relocation expenses on commencement of your employment and relocation to the UK, as outlined below:  

 
Sale of primary residence

Upon receipt of the signed Service Agreement, we will provide assistance for you in relation to the sale of your primary residence.  This will be subject to the terms of AstraZeneca’s Relocation Policy (Homeowner New Employee Overseas to UK) (a copy of which has been provided to you).

 
ii 
Rental Assistance and Relocation allowance

I am pleased to confirm that the Company will provide you with rental assistance, up to a value of £8,000   per month, for a period of up to 18 months (subject to your continued employment with the Company), prior to Exchange of Contracts on a purchase of your house in the UK.  The company will cover any tax due on these payments as well as any tax arising from the provision of any relocation assistance to support your relocation to London under 7(i) above.
 
 
 
 
 
This offer is based on our understanding that you are not prevented from taking up employment with the Company, for example, by any restrictions in any agreement with your current employer (save for any notice period in such agreement).  In the event that such condition is not satisfied, this offer may be withdrawn.

I very much look forward to you joining AstraZeneca.




Kind regards


/s/ Leif Johansson

Leif Johansson
Chairman
AstraZeneca PLC



I understand and accept the terms set out in this offer letter.

/s/ Pascal Soriot
..………………………
Pascal Soriot

Date:  27 August 2012
 
 
 
 
 
Dated    27 th August 2012
 
 
 
 
 
 
 
ASTRAZENECA UK LIMITED (1)
 
PASCAL SORIOT (2)
 
 
 
 
 
 
 
 
 
 
 
SERVICE AGREEMENT
 
 
 
 
 
 
 
 
 
 
 
 
Contents
 
  Clause  Page
     
1
Definitions and interpretation
2
2
Appointment
3
3
Duration of the Employment
3
4
Scope of the Employment
4
5
Hours of work
5
6
Place of work
5
7
Remuneration
5
8
Expenses
6
9
Holidays
6
10
Sickness benefits
7
11
Pension and benefits
7
12
Restrictions during the Employment
8
13
Confidential information and company documents
8
14
Inventions and other intellectual property
9
15
Termination
11
16
Restrictive covenants
13
17
Disciplinary and grievance procedures
14
18
Notices
14
19
D & O Liability Insurance
15
20
Former contracts of employment
15
21
Choice of law and submission to jurisdiction
15
22
General
15

 
 
 
 
This Agreement is made on 27 th August 2012
 
Between
 
(1) 
ASTRAZENECA UK LIMITED (registered in England and Wales under number 3674842) whose registered office is at 2 Kingdom Street, London, W2 6BD ( Company ); and
 
(2) 
PASCAL SORIOT with a service address at 2 Kingdom Street, London W2 6BD ( Executive )
 
It is agreed
 
1  
Definitions and interpretation
 
1.1  
In this Agreement unless the context otherwise requires the following expressions have the following meanings:
 
AstraZeneca means AstraZeneca PLC, a company registered in England and Wales under number 2723534.
 
AstraZeneca Board means the Board of Directors of AstraZeneca as the same may be constituted from time to time or such other person or persons as the Board of Directors of AstraZeneca may nominate as the representative of the Board of Directors for this purpose.
 
Base Salary means the salary referred to in clause 7.1.
 
Board means Board of Directors of the Company as the same may be constituted from time to time or such other person or persons as the Board of Directors of the Company may nominate as the representative of the Board of Directors for this purpose.
 
Confidential Information means information relating to the business, products, affairs and finances of the Company or of any Group Company for the time being confidential to it or to them and trade secrets (including, without limitation, technical data and know-how) relating to the business of the Company or of any Group Company, details of any of its or their suppliers, clients or customers including in particular (by way of example only and without limitation) customer requirements, prices charged to and terms of business with customers, terms of business with suppliers, marketing plans and sales forecasts, financial information, results and other forecasts (save to the extent that these are included in published audited accounts), any of the Company’s or a Group Company’s proposals relating to the acquisition or disposal of a company, or a business or any part thereof or to any proposed expansion or contraction of activities, details of employees, officers, consultants and/or contractors and of the remuneration and other benefits paid to them, information relating to research activities, inventions, secret processes, designs, formulae and product lines, any information which is treated as confidential or which the Executive is told or ought reasonably to know is confidential and any information which has been given to the Company or any Group Company in confidence by customers, suppliers and others.
 
Employment means the Executive's employment under this Agreement.
 
ERA means the Employment Rights Act 1996 as amended.
 
Group means the Company and the Group Companies.
 
Group Company means any company which is for the time being a subsidiary or holding company of the Company and any subsidiary of any such holding company and for the purposes of this Agreement the terms subsidiary and holding company shall have the
 
 
 
 
 
meanings ascribed to them by section 1159 Companies Act 2006 (and Group Companies shall be interpreted accordingly)
 
Intellectual Property means all patents, registered designs, trade marks and service marks (whether registered or not and including any applications for the foregoing), copyrights, design rights, semiconductor topography rights, database rights and all other intellectual property and similar proprietary rights subsisting in any part of the world (whether or not capable of registration) and including (without limitation) all such rights in materials, works, prototypes, inventions, discoveries, techniques, computer programs, source codes, data, technical, commercial or confidential information, trading, business or brand names, goodwill or the style of presentation of the goods or services or any improvement of any of the foregoing and the right to apply for registration or protection of any of them and in existing applications for the protection of any of the above.
 
Sensitive Data means personal data consisting of information as to racial or ethnic origin; political opinions; religious beliefs or other beliefs of a similar nature; membership of a trade union (within the meaning of the Trade Union and Labour Relations (Consolidation) Act 1992); physical or mental health or condition; sexual life; the commission or alleged commission of any offence or any proceedings for any offence committed or alleged to have been committed, including the disposal of such proceedings or the sentence of any court in such proceedings.
 
Termination Date means for the purposes of clause 16  the date of the termination of the Employment or, where the Company exercises its rights under clause 3.2 to require the Executive to remain at home, the last day on which the Executive was required to work.
 
1.2  
References to clauses and schedules are unless otherwise stated to clauses of and schedules to this Agreement.
 
1.3  
The headings to the clauses are for convenience only and shall not affect the construction or interpretation of this Agreement.
 
2  
Appointment
 
2.1  
The Company agrees to employ the Executive and the Executive agrees to act as Chief Executive Officer of the Company and of AstraZeneca on the terms of this Agreement.
 
3  
Duration of the Employment
 
3.1  
The Employment will commence on such date as you are lawfully free to do so and, subject to the provisions of this Agreement, shall continue unless and until terminated by either party giving to the other not less than 12 months' prior notice in writing, but any such notice from the Company not to expire prior to the second anniversary of the commencement date of the Employment.  Provided always, however, that in respect of the part of any period of notice which exceeds 12 months, the Executive shall be entitled to his Base Salary together with funding for any flexible benefit arrangement operated by the Company from time to time but any other remuneration (as described in clause 7) shall be determined at the sole discretion of AstraZeneca's Remuneration Committee taking account of the reason for such notice being given and in particular the Executive's actual performance assessed against his duties as set out or contemplated by this Agreement.
 
3.2  
At any time during any period of notice of termination served in accordance with clause 3.1 (whether given by the Company or the Executive), the Executive may be placed on “garden leave” in which case neither the Company nor any Group Company shall be under any
 
 
 
 
 
obligation to provide work for or assign any duties to the Executive for the whole or any part of the relevant notice period and the Company shall have the right at its absolute discretion to assign no, reduced or alternative duties to the Executive (provided these are commensurate with his status and position) and shall be entitled to require the Executive to act at the reasonable direction of the Company including the right to:
 
 
(a)  
exclude him from any premises of the Company and any other Group Company, and/or
 
 
(b)  
remove him from any or all directorships and offices held by him in the Company or in any other company in the Group (including if appropriate the office of trustee of any of the pension schemes of the Company or the Group); and/or
 
 
(c)  
prevent the Executive from discussing its affairs with the Company's or any other company in the Group's employees, agents, clients, customers; and/or
 
 
(d)  
require the Executive to refrain from business contact with any customers, clients or employees of the Company or any Group Company; and/or
 
 
(e)  
to take any holiday which has accrued under clause 9 during any period of suspension under this clause 3.2.
 
If the Company shall exercise its right under this clause, the Executive's entitlement to Base Salary and other contractual benefits shall continue as an employee for the period of garden leave, subject always to the rules of any relevant scheme or policy relating to such benefits.  For the avoidance of doubt, at all times during any period of notice of termination served in accordance with clause 3.1 (whether given by the Company or the Executive), the Executive shall continue to be bound by the same obligations as were owed to the Company prior to the commencement of the notice period including for the avoidance of doubt the duties of good faith and fidelity.
 
3.3  
For the purposes of the ERA there is no previous period of continuous employment.
 
3.4  
For the avoidance of doubt, in the event that the Company terminates the Employment without notice or on notice less than required by clause 3.1, the Executive’s entitlement to any damages or compensation arising from the termination will be subject to the Executive’s duty to mitigate his losses.
 
4  
Scope of the Employment
 
4.1  
During the Employment the Executive shall:
 
 
(a)  
devote the whole of his working time, attention and skill to the business and affairs of the Group during the hours of work described in clause 5 except during holidays and periods of absence due to ill health;
 
 
(b)  
faithfully, competently and diligently perform such duties and exercise such powers consistent with his position as may from time to time be assigned to or vested in him by the Board or the AstraZeneca Board;
 
 
(c)  
obey the reasonable and lawful directions of the Board and the AstraZeneca Board;
 
 
(d)  
comply with all the Company's and AstraZeneca’s rules, regulations, policies and procedures from time to time in force; and
 
 
 
 
 
 
(e)  
keep the Board and the AstraZeneca Board at all times promptly and fully informed (in writing if so requested) of his conduct of the business of the Company and any Group Company and provide such explanations in connection with it as the Board and the AstraZeneca Board may require.
 
4.2  
The Executive shall if and so long as the Company requires and without any further remuneration carry out his duties on behalf of any Group Company and act as a director or officer of any Group Company.
 
4.3  
The Company may at its sole discretion transfer this Agreement to any Group Company at any time.
 
4.4  
If at any time the Executive is unable to perform his duties properly because of ill health, accident or otherwise, or becomes incapable by reason of mental disorder of administering his property or managing his affairs, then the Company may appoint any other person or persons to act jointly with the Executive in any position to which he may be assigned during any resulting period of absence from work.
 
4.5  
For the purposes of the Data Protection Act 1998, the Executive consents to the Company's processing of personal data, including Sensitive Data, of which the Executive is the subject , details of which processing are specified in the Company's Data Protection Policy.
 
5  
Hours of work
 
5.1  
The Executive shall be required to work a minimum of 40 hours per week at such times to be agreed between the Executive and the Company which may involve working during normal business hours and during such additional hours as are necessary for the proper performance of his duties or as the Board or the AstraZeneca Board may reasonably require from time to time.
 
5.2  
As a senior executive the Executive’s working time is not measured or pre-determined.  The Executive is responsible for determining his own hours of work, providing that such hours are consistent with the proper performance of his duties.
 
6  
Place of work
 
6.1  
The Executive's place of work will be as determined by the AstraZeneca Board from time to time and the Company may require the Executive to travel and work at any place (whether inside or outside the United Kingdom) for such periods as the Company may from time to time reasonably require on a temporary or an indefinite basis.
 
6.2  
The Board shall have the right to require the Executive to move house to an appropriate location for the better performance of his duties.  The Executive will be given reasonable notice of any such requirement   and the Company will reimburse to him all expenses incurred by him in such a move as it may consider reasonable in all the circumstances in accordance with the relevant Relocation Policy from time to time in force for senior executives.
 
7  
Remuneration
 
7.1  
The Company shall pay to the Executive the Base Salary at the rate of £1,100,000 per annum (or such other sum as may from time to time be agreed) by equal monthly instalments in arrears by credit transfer to his bank account.  The rate of Base Salary will be reviewed annually in December, the next such review to take place in December 2013.  No salary review will be undertaken after notice has been given by either party to terminate the
 
 
 
 
 
Employment.  The Company is under no obligation to increase the Executive’s Base Salary following a salary review but will not decrease it.
 
7.2  
The Executive shall also be entitled to participate during the Employment in such discretionary performance related bonus schemes and such share incentive or option schemes as the AstraZeneca Board may in its discretion determine in accordance with the rules of any such schemes from time to time in force.  If the Company shall pay the Executive a bonus in any one year, this shall not give rise to a contractual entitlement to a bonus in future years.
 
7.3  
In the year in which the Employment terminates, any discretionary performance related bonus shall be determined at the sole discretion of AstraZeneca’s Remuneration Committee, taking account of factors including (but not limited to):
 
 
(a)  
the length of time during which the Executive has given service during the bonus year in which the Employment terminates; and
 
 
(b)  
the reason(s) for termination and in particular, the Executive’s actual performance assessed against his duties as set out in or contemplated by this Agreement.
 
7.4  
The Base Salary and any bonus/share incentives/share options shall be inclusive of any fees to which the Executive may be entitled as a director of the Company or any Group Company.
 
7.5  
Payment of the Base Salary and any bonus/share incentives/share options to the Executive shall be made either by the Company or by a Group Company and, if by more than one company, in such proportions as the Board or the AstraZeneca Board may from time to time think fit.
 
7.6  
The Executive agrees that, pursuant to Part II of the ERA, the Company shall be entitled to deduct from any sum due to the Executive under the terms of this Agreement any monies which are owed by the Executive to the Company or any Group Company.
 
8  
Expenses
 
8.1  
The Company shall reimburse the Executive in respect of all expenses reasonably incurred by him in the proper performance of his duties, subject to him providing such receipts or other appropriate evidence as the Company may require.
 
9  
Holidays
 
9.1  
The Executive shall be entitled, in addition to all Bank and Public holidays normally observed in England and any additional holidays purchased by the Executive under the Company’s flexible benefits arrangement (AstraZeneca Advantage), to 22 working days' paid holiday in each holiday year (being the period from 1 July to 30 June).  The Executive may take holiday only at such times as are agreed with the Board.
 
9.2  
In the respective holiday years in which the Employment commences or terminates, the Executive's entitlement to holiday shall accrue on a pro rata basis for each completed calendar month of service during the relevant year.
 
9.3  
If, on the termination of the Employment, the Executive has exceeded his accrued holiday entitlement, the value of such excess, calculated on the basis that each day of paid holiday is equivalent to 1/260 th of the Executive’s Base Salary, may be deducted by the Company from any sums due to him.  If the Executive has any unused holiday entitlement, the Company
 
 
 
 
 
shall at its discretion either require the Executive to take such unused holiday during any notice period or make a payment to him in lieu of it, calculated in accordance with this clause.
 
9.4  
Holiday entitlement for one holiday year cannot be taken in subsequent holiday years unless otherwise agreed by the Board.  Failure to take holiday entitlement in the appropriate holiday year will lead to forfeiture of any accrued holiday not taken without any right to payment in lieu of it.
 
10  
Sickness benefits
 
10.1  
Subject to clause 15 the Company shall continue to pay the Base Salary for:
 
 
(a)  
up to a maximum of 130 working days' absence on medical grounds in any period of 12 calendar months; or
 
 
(b)  
for the first 130 working days' absence on medical grounds in any one continuous period of absence (or two or more linked periods as determined by the Social Security Contributions and Benefits Act 1992, as amended from time to time)
 
whichever is the lesser, provided that the Executive shall from time to time if required supply the Company with medical certificates covering any period of sickness or incapacity exceeding seven days (including weekends).
 
10.2  
Payment in respect of any other or further period of absence shall be at the Company's discretion.  For the avoidance of doubt, the Executive will not be paid during any period of absence from work (other than due to holiday, sickness, injury or other incapacity) without the prior permission of the Board.
 
10.3  
Any payment to the Executive pursuant to clause 10.1 shall be subject to set off by the Company in respect of any Statutory Sick Pay and any Social Security Sickness Benefit or other benefits to which the Executive may be entitled.
 
10.4  
Subject to clause 10.2, when all sick pay entitlement pursuant to clause 10.1 has been exhausted, no further Base Salary will be payable by the Company to the Executive until the Executive has returned to active service of the Company.
 
10.5  
If the Executive's absence shall be occasioned by the actionable negligence of a third party in respect of which damages are recoverable, then the Executive shall:
 
 
(a)  
notify the Company immediately of all the relevant circumstances and of any claim, compromise, settlement or judgment made or awarded in co nnection with it;
 
 
(b)  
give to the Company such information concerning the above matters as the Company may reasonably require; and
 
 
(c)  
if the Company so requires, refund to the Company any amount received by him from any such third party provided that the refund shall be no more than the amount which he has recovered in respect of remuneration.
 
11  
Pension and benefits
 
11.1  
During the Employment the Executive shall be entitled to participate in the AstraZeneca Group Self Invested Personal Pension Plan ( GSIPP ) as it exists on the effective date of this Agreement and any successor plans, subject to the applicable rules from time to time in force provided that the GSIPP may be terminated or amended at any time in accordance with the
 
 
 
 
 
relevant trust deed or rules that governs it, provided always that the Executive is provided with a comparable level of benefits to those set out above in any amended or replacement plan.
 
11.2  
The Company shall, from time to time, be entitled to require the Executive to undertake a medical examination with a doctor of the Company's choice to determine the Executive’s ability to carry out his duties under this Agreement.  The Company will be entitled to receive a copy of any report produced in connection with all such examinations and to discuss the contents of the report with the doctor who produced it.
 
11.3  
The Executive shall be entitled during the Employment to such other benefits, including participation in AZ Advantage, not inconsistent with the foregoing and as may be appropriate for a person of the status of the Executive as are provided to other UK based employees in the Group.
 
12  
Restrictions during the Employment
 
12.1  
During the Employment the Executive shall not directly or indirectly be employed, engaged, concerned or interested:
 
 
(a)  
in any other business or undertaking; or
 
 
(b)  
in any activity which the Board reasonably considers may be, or become, harmful to the interests of AstraZeneca, the Company or of any Group Company or which might reasonably be considered to interfere with the performance of the Executive's duties under this Agreement.
 
12.2  
Clause 12.1 shall not apply:
 
 
(a)  
so as to prevent the Executive from holding (directly or through nominees) investments listed on the Official List of London Stock Exchange plc or in respect of which dealing takes place in the Alternative Investment Market or any recognised stock exchange as long as he does not hold more than 3  per cent of the issued shares or other securities of any class of any one company and provided always that the Executive takes reasonable care to ensure that the holding of such investments does not give rise to any actual or potential conflict of interest between the holding of such investments and the duties of the Executive as contemplated by this Service Agreement and/or which may otherwise arise as a result of any law or regulation to which any of the Executive, the Company or AstraZeneca may from time to time be subject; or
 
 
(b)  
to any act undertaken by the Executive with the prior written consent of the AstraZeneca Board.
 
12.3  
The Executive shall comply with, the UK Listing Authority's listing rules' Model Code for transactions in securities by directors of listed companies, certain employees and persons connected with them and every regulation of AstraZeneca and the Company for the time being in force in relation to dealings in shares or other securities of AstraZeneca, the Company or any Group Company.
 
13  
Confidential information and company documents
 
13.1  
The Executive shall keep secret and will not, whether during the Employment or after its termination:
 
 
 
 
 
 
(a)  
divulge or communicate to any person, company, business entity or other organisation;
 
 
(b)  
use for his own purposes or for any purposes other than those of the Company or any Group Company; or
 
 
(c)  
through any failure to exercise due care and diligence, permit or cause any unauthorised disclosure of,
 
any Confidential Information.
 
13.2  
The restrictions in clause 13.1 shall not apply:
 
 
(a)  
to any disclosure of information which is already in the public domain otherwise than by breach of this Agreement;
 
 
(b)  
to any disclosure or use authorised by the Board or required in the proper performance by the Executive of his duties under this Agreement or by any applicable laws or regulations, including, without limitation, to any disclosure required for patent purposes provided that the Executive promptly notifies the Company when any such disclosure requirement arises to enable the Company to take such action as it deems necessary, including, without limitation, to seek an appropriate protective order and/or make known to the appropriate government or regulatory authority or court the proprietary nature of the Confidential Information and make any applicable claim of confidentiality with respect hereto;
 
 
(c)  
so as to prevent the Executive from using his own personal skill, experience and knowledge in any business in which he may be lawfully engaged after the Employment is ended; or
 
 
(d)  
to prevent the Executive making a protected disclosure within the meaning of s43A of the Employment Rights Act 1996.
 
13.3  
The Executive acknowledges and agrees that all books, notes, memoranda, records, lists of customers and suppliers and employees, correspondence, documents, computer and other discs and tapes, data listings, codes, designs and drawings and other documents and material whatsoever (whether made or created by the Executive or otherwise) relating to the business of AstraZeneca, the Company or any Group Company (and any copies of the same):
 
 
(a)  
shall be and remain the property of AstraZeneca, the Company or the relevant Group Company; and
 
 
(b)  
shall be handed over by the Executive to AstraZeneca, the Company or to the relevant Group Company on demand and in any event on the termination of the Employment and the Executive shall certify that all such property has been handed over on request by the Board.
 
14  
Inventions and other intellectual property
 
14.1  
The parties foresee that the Executive may make inventions or create other Intellectual Property in the course of his duties and agree that in this respect the Executive has and shall have at all times a special responsibility to further the interests of AstraZeneca, the Company and any Group Company.
 
 
 
 
 
14.2  
Any invention, discovery, improvement, prototype, technique, design, process, information, copyright work, computer program, trade mark, trade name or get-up, work or other output ( Work ) made, created or discovered wholly or partially by the Executive during the Employment (whether capable of being patented or registered or not and whether or not made, created, developed or discovered in the course of the Employment and whether or not recorded in material form) in conjunction with or in any way affecting or relating to the business of AstraZeneca, the Company or of any Group Company or capable of being used or adapted for use in or in connection with such business, together with all Intellectual Property subsisting therein, (collectively Intellectual Property Rights ) shall be disclosed by the Executive immediately to the Company and shall (subject to sections 39 to 43 Patents Act 1977) belong to and be the absolute property of the Company or such Group Company as the Company may direct.  To the extent that any Intellectual Property Rights do not vest automatically in the Company, the Executive holds them on trust for the Company and the Executive hereby assigns to the Company with full title guarantee and by way of present assignment of future rights, all such copyright, database rights, design rights (and any other Intellectual Property capable of assignment by way of present assignment of future rights) which may fall within the definition of the Intellectual Property Rights absolutely for the full term of those rights.
 
14.3  
If and whenever required so to do by the Company, both during and after the Employment, the Executive shall, at the expense of the Company or such Group Company as the Company may direct:
 
 
(a)  
apply or join with the Company or such Group Company in applying for patent or other protection or registration in the United Kingdom and in any other part of the world for any Intellectual Property Rights; and
 
 
(b)  
promptly execute all instruments and do all things necessary for vesting all Intellectual Property Rights (including such patent or other protection or registration when so obtained) and all right, title and interest to and in them absolutely, with full title guarantee and as sole beneficial owner, in the Company or such Group Company or in such other person as the Company may specify.
 
14.4  
The Executive irrevocably and unconditionally waives all rights under Chapter IV of Part I Copyright Designs and Patents Act 1988 and all similar rights in other jurisdictions in connection with his authorship of any existing or future copyright work which forms part of the Intellectual Property Rights, in whatever part of the world such rights may be enforceable, including, without limitation:
 
 
(a)  
the right conferred by section 77 of that Act to be identified as the author of any such work; and
 
 
(b)  
the right conferred by section 80 of that Act not to have any such work subjected to derogatory treatment.
 
14.5  
The Executive irrevocably appoints the Company to be his Attorney in his name and on his behalf to execute any such instrument or do any such thing and generally to use his name for the purpose of giving to the Company or such Group Company as the Company may nominate the full benefits of this clause.  A certificate in writing in favour of any third party signed by any director or by the secretary of the Company that any instrument or act falls within the authority conferred by this Agreement shall be conclusive evidence that such is the case.
 
 
 
 
 
14.6  
The Executive acknowledges that, except as provided by law, no further remuneration or compensation other than that provided for in this Agreement is or may become due to the Executive in respect of his compliance with this clause 14.  Nothing in this clause 14 shall be construed as restricting the rights of the Executive or the Company under sections 39 to 43 Patents Act 1977.
 
15  
Termination
 
15.1  
Either party may terminate the Employment in accordance with clause 3.1.
 
15.2  
The Company may, in its sole discretion, terminate the Employment at any time with immediate effect and pay a sum in lieu of notice (the Payment in Lieu )   equal to:
 
 
(a)  
the Base Salary which the Executive would have been entitled to receive under this Agreement during the notice period referred to at clause 3.1 if notice had been given (or, if notice has already been given, during the remainder of the notice period) (the Relevant Period );
 
 
(b)  
the balance of the cost to the Company (including, for the avoidance of doubt, an amount in respect of the Company’s pension contribution) of funding any flexible benefit arrangement operated by the Company from time to time in respect of the Executive’s employment during the Relevant Period.
 
15.3  
For the avoidance of doubt:
 
 
(a)  
the Payment in Lieu shall not include any sum in lieu of bonus;
 
 
(b)  
the Executive will not be entitled to receive any payment in addition to the Payment in Lieu in respect of any holiday entitlement that would have accrued during the period for which the Payment in Lieu is made.
 
15.4  
The Payment in Lieu shall be made in full and final settlement of any contractual claims the Executive may have against the Company or any Group Company (whether known or unknown) arising from the Employment or the termination thereof or the Executive’s directorship or resignation from any directorship of the Company or any Group Company.
 
15.5  
The Payment in Lieu shall be subject to any deductions the Company may be required to make and may at the Company’s discretion be paid as a lump sum within 30 days of the date of the termination of the Employment or, alternatively, the first six months’ thereof may be paid in equal monthly instalments from the date of termination of the Employment with the balance paid in a lump sum within 30 days after the date of the last such instalment.  If the Company pays the first six months’ Payment in Lieu in instalments, and the Employee commences alternative employment or the provision of services pursuant to a consultancy arrangement at a basic salary or fee of at least £30,000 per month whilst such payments are being made, each instalment that falls due after the commencement of the alternative employment or the provision of services under the consultancy arrangement will be reduced by such sum as is equal to 50% of 1/12 th of the basic annual salary or fee the Executive is entitled to receive from the alternative employment or consultancy arrangement. In the event that the Company exercises its discretion to terminate the Executive’s employment under this clause 15, the Executive will use reasonable efforts to secure suitable alternative employment as soon as reasonably practicable and the payment of the instalments shall be conditional on the Executive providing the Company with reasonable evidence of such efforts.
 
 
 
 
 
15.6  
Notwithstanding any other provisions of this Agreement, the Company may also terminate the Employment summarily (by serving written notice on the Executive to that effect) and with no liability to make any further payment to the Executive (other than in respect of amounts accrued due at the date of termination) if the Executive:
 
 
(a)  
commits any fundamental breach of this Agreement or is guilty of any gross misconduct, gross incompetence, or any wilful neglect in the discharge of his duties;
 
 
(b)  
repeats or continues (after warning) any breach of this Agreement;
 
 
(c)  
is guilty of any fraud, dishonesty or conduct which brings, or in the reasonable opinion of the Company would bring, himself, the Company or any Group Company into disrepute;
 
 
(d)  
commits any act of bankruptcy or takes advantage of any statute for the time being in force offering relief for insolvent debtors;
 
 
(e)  
is convicted of any criminal offence (other than minor offences under the Road Traffic Acts or the Road Safety Acts for which a fine or non-custodial penalty is imposed) which might reasonably be thought to affect adversely the performance of his duties;
 
 
(f)  
is disqualified from holding office in the Company or in any other company by reason of any order made under the Company Directors Disqualification Act 1986 or any other enactment;
 
 
(g)  
resigns as, or becomes prohibited by law from being, a director of the Company or any Group Company, otherwise than at the Company's or AstraZeneca’s request.
 
This clause shall not restrict any other right the Company may have (whether at common law or otherwise) to terminate the Employment summarily.
 
Any delay by the Company in exercising such right of termination shall not constitute a waiver of it.
 
15.7  
If at any time the Executive is unable to perform his duties properly because of ill health accident or otherwise for a period or periods totalling at least 130 working days in any period of 12 calendar months, or becomes incapable by reason of mental disorder of managing and administering his property and affairs, then the Company may, notwithstanding the existence of any permanent health insurance cover provided for the Executive in its absolute discretion terminate the Employment by giving him not less than three months' written notice to that effect.
 
15.8  
If the Company believes that it may be entitled lawfully to terminate the Employment summarily, whether pursuant to clause 15.1 or otherwise, it shall be entitled (but without prejudice to its right subsequently to terminate the Employment on the same or any other ground) to suspend the Executive on full pay for such reasonable period as is necessary to conduct any investigation and to conclude any disciplinary proceedings.
 
15.9  
On the termination of the Employment or upon the Company having exercised its rights under clause 3.2, the Executive shall:
 
 
(a)  
at the request of the Board resign from office as a director of the Company and all offices held by him in any Group Company and shall transfer to the Company without payment or as the Company may direct any qualifying shares held by him as nominee for the Company or any Group Company provided however that such
 
 
 
 
 
resignation shall be without prejudice to any claims which the Executive may have against the Company or any Group Company arising out of the termination of the Employment; and
 
 
(b)  
immediately deliver to the Company all materials within the scope of clause 13.3, any Company car, mobile telephone or other Company equipment in his possession and all keys, credit cards, and other property of or relating to the business of the Company or of any Group Company which may be in his possession or under his power or control
 
and the Executive irrevocably authorises the Company to appoint any person in his name and on his behalf to sign any documents and do any things necessary or requisite to give effect to his obligations under this clause 15.9.
 
16  
Restrictive covenants
 
16.1  
The Executive will not (without the previous consent in writing of the Board) for the period of 12 months immediately after the Termination Date (save that in respect of clause 16.1(a) the period shall be 6 months) whether as principal or agent, and whether alone or jointly with, or as a director, manager, partner, shareholder, employee or consultant of any other person, directly or indirectly:
 
 
(a)  
carry on, or be engaged, concerned or interested in any business which is similar to and/ or competes with any business being carried on by the Company or by any Group Company at the Termination Date and with which the Executive was materially involved in the course of the Employment at any time during the period of 12 months immediately preceding the Termination Date;
 
 
(b)  
negotiate with, solicit business from or endeavour to entice away from AstraZeneca, the Company or any Group Company the business of any person, firm, company or organisation who or which to his knowledge is and has been a customer, client or agent of or supplier to, or who had regular business dealings with, AstraZeneca, the Company or with any Group Company during the period of 12 months immediately preceding the Termination Date and with whom he had material direct or indirect dealings or personal contact in the course of the Employment during that period provided that this restriction will be limited to activities by the Executive which will involve offering or providing services similar to those which he will have provided during the Employment;
 
 
(c)  
undertake to provide in competition with AstraZeneca, the Company or any Group Company any service or to manufacture or supply any product similar to those with which he was concerned in the course of the Employment during the period of 12 months immediately preceding the Termination Date to or for any person who is or was a customer, client or agent of or supplier to (or who had regular business dealings with) AstraZeneca, the Company or any other Group Company during the period of 12 months immediately preceding the Termination Date and with whom he had material direct or indirect dealings in the course of the Employment during that period;
 
 
(d)  
interfere with, solicit or endeavour to entice away from AstraZeneca, the Company or any Group Company any person who to his knowledge is, and within the period of  12 months immediately preceding the Termination Date had been, part of the senior management of AstraZeneca, the Company or any other Group Company and with
 
 
 
 
 
whom he had material personal dealings in the course of the Employment during that period.
 
16.2  
For the avoidance of doubt, none of the restrictions contained in clause 16.1 shall prohibit any activities by the Executive which are not in direct or indirect competition with any business being carried on by AstraZeneca, the Company or any Group Company at the Termination Date.
 
16.3  
Nothing in clause 16.1 shall preclude the Executive from holding (directly or through nominees) investments listed on the Official List of London Stock Exchange plc or in respect of which dealing takes place in the Alternative Investment Market or any recognised stock exchange as long as he does not hold more than 3 per cent of the issued shares or other securities of any class of any one company.
 
16.4  
At no time after the Termination Date shall the Executive directly or indirectly represent himself as being interested in or employed by or in any way connected with the Company or any Group Company, other than as a shareholder of AstraZeneca and former employee of the Company.
 
16.5  
The Executive agrees that, having regard to all the circumstances, the restrictions contained in this clause are reasonable and necessary for the protection of AstraZeneca, the Company or of any Group Company and that they do not bear harshly upon him and the parties agree that:
 
 
(a)  
each restriction shall be read and construed independently of the other restrictions so that if one or more are found to be void or unenforceable as an unreasonable restraint of trade or for any other reason the remaining restrictions shall not be affected; and
 
 
(b)  
if any restriction is found to be void but would be valid and enforceable if some part of it were deleted, that restriction shall apply with such deletion as may be necessary to make it valid and enforceable.
 
17  
Disciplinary and grievance procedures
 
17.1  
There are no special disciplinary or grievance rules which apply to the Executive and any such matters affecting him will be dealt with by the Board.
 
18  
Notices
 
18.1  
Any notice or other document to be given under this Agreement shall be in writing and may be given personally to the Executive or to the secretary of the Company or may be sent by first class post or other fast postal service or by facsimile transmission to, in the case of the Company, its registered office for the time being and in the case of the Executive either to his address shown on the face of this Agreement or to his last known place of residence.
 
18.2  
Any such notice shall (unless the contrary is proved) be deemed served when in the ordinary course of the means of transmission it would first be received by the addressee in normal business hours.  In the case of first class post, this shall be deemed to be no later than two working days after posting. In proving such service it shall be sufficient to prove, where appropriate, that the notice was addressed properly and posted, or that the facsimile transmission was despatched.
 
 
 
 
 
19  
D & O Liability Insurance
 
During the Employment and for six years following its termination the Executive shall be entitled to be covered by a policy of directors’ and officers’ liability insurance on terms no less favourable than those in place from time to time for other members of the Board of AstraZeneca.
 
20  
Former contracts of employment
 
This Agreement shall be in substitution for any previous contracts, whether by way of letters of appointment, agreements or arrangements, whether written, oral or implied, relating to the employment of the Executive other than the letter from the Company to the Executive dated 27 July 2012, all of which (other than the letter from the Company to the Executive dated 27 July 2012) shall be deemed to have been terminated by mutual consent as from the date of this Agreement and the Executive acknowledges that he has no outstanding claims of any kind against AstraZeneca, the Company or any Group Company in respect of any such contract.
 
21  
Choice of law and submission to jurisdiction
 
21.1  
This Agreement shall be governed by and interpreted in accordance with English law.
 
21.2  
The parties submit to the exclusive jurisdiction of the English courts.
 
22  
General
 
22.1  
The expiration or termination of this Agreement shall not prejudice any claim which either party may have against the other in respect of any pre-existing breach of or contravention of or non-compliance with any provision of this Agreement nor shall it prejudice the coming into force or the continuance in force of any provision of this Agreement which is expressly or by implication intended to or has the effect of coming into or continuing in force on or after such expiration or termination.
 
22.2  
This Agreement may be executed in any number of counterparts, each of which, when executed, shall be an original, and all the counterparts together shall constitute one and the same instrument.
 
22.3  
This Agreement constitutes the written statement of the terms of employment of the Executive provided in compliance with Part I of the ERA.
 
22.4  
A person who is not a party to this Agreement has no right under the Contracts (Rights of Third Parties) Act 1999 to enforce any term of this Agreement but this does not affect any right or remedy of a third party which exists or is available apart from that Act.
 
 
 
 
 
Executed as a deed by the Company
)
/s/ Simon Lowth
acting by two directors or by a director and its
)
Director
secretary
)
 
 
)
/s/ Adrian Kemp
 
)
Director/ Secretary


Executed as a deed by the Executive
)
 
in the presence of
)
 
 
)
/s/ Pascal Soriot
     
     
/s/ Caroline Hempstead /s/
   
Signature of witness
   
     
Name   Caroline Hempstead
   
     
Address   2 Kingdom Street, London W2 6BD
   

 
 

Exhibit 7.1
 
 
RATIO OF EARNINGS TO FIXED CHARGES
 
Our consolidated ratios of earnings to fixed charges calculated in accordance with IFRS for the twelve month periods ended December 31, 2012, 2011, 2010, 2009 and 2008 are as follows:

 
2012
2011
2010
2009
2008
IFRS
19.9  
28.5  
24.0  
19.9  
13.5  

For the purpose of computing these ratios, earnings consist of the income from continuing ordinary activities before taxation of Group companies and income received from companies owned 50% or less, plus fixed charges.  Fixed charges consist of interest on all indebtedness, amortization of debt discount and expense and that portion of rental expense representative of the interest factor.

 
 
 
Exhibit 8.1

PRINCIPAL SUBSIDIARIES

At December 31, 2012
Country
Percentage of voting share capital held (1)
Principal activity
UK
     
AstraZeneca UK Limited
England
100
Research and development, manufacturing, marketing
AstraZeneca Treasury Limited
England
100
Treasury
       
Continental Europe
     
AstraZeneca Dunkerque Production SCS
France
100
Manufacturing
AstraZeneca SAS
France
100
Research, manufacturing, marketing
Novexel SA
France
100
Research
AstraZeneca GmbH
Germany
100
Development, manufacturing, marketing
AstraZeneca Holding GmbH
Germany
100
Manufacturing, marketing
AstraZeneca SpA
Italy
100
Marketing
AstraZeneca Farmaceutica Spain SA
Spain
100
Marketing
AstraZeneca AB
Sweden
100
Research and development, manufacturing, marketing
AstraZeneca BV
Netherlands
100
Marketing
LLC AstraZeneca Pharmaceuticals
Russia
100
Marketing
       
The Americas
     
AstraZeneca do Brasil Limitada
Brazil
100
Manufacturing, marketing
AstraZeneca Canada Inc.
Canada
100
Research, marketing
AZ Reinsurance Limited
Cayman Islands
100
Insurance and reinsurance underwriting
IPR Pharmaceuticals Inc.
Puerto Rico
100
Development, manufacturing, marketing
Ardea Biosciences, Inc
US
100
Research and development
AstraZeneca LP
US
99
Research and development, manufacturing, marketing
AstraZeneca Pharmaceuticals LP
US
100
Research and development, manufacturing, marketing
Zeneca Holdings Inc.
US
100
Manufacturing, marketing
MedImmune, LLC
US
100
Research and development, manufacturing, marketing
       
Asia, Africa & Australasia
     
AstraZeneca Pty Limited
Australia
100
Development, manufacturing, marketing
AstraZeneca Pharmaceuticals Co., Limited
China
100
Research and development, manufacturing, marketing
AZ (Wuxi) Trading Co. Limited
China
100
Marketing
AstraZeneca KK
Japan
80
Manufacturing, marketing
__________________________
(1) All shares are held indirectly.
 
The companies and other entities listed above are those whose results or financial position principally affected the figures shown in the Group Financial Statements of AstraZeneca PLC (the “Company”) and its subsidiaries (together, the “Group”). A full list of subsidiaries, joint ventures and associates will be annexed to the Company’s next annual return filed with the Registrar of Companies. The country of registration or incorporation is stated alongside each company. The accounting year ends of subsidiaries and associates are December 31. AstraZeneca operates through 217 subsidiaries worldwide. Products are manufactured in 16 countries worldwide and are sold in over 100 countries. The Group Financial Statements consolidate the Financial Statements of the Company and its subsidiaries at December 31, 2012.
 

 
Exhibit 12.1
 

CERTIFICATION PURSUANT TO SECTION 302 OF THE SARBANES-OXLEY ACT 2002

 
I, Pascal Soriot, certify that:
 
 
1.
I have reviewed this annual report on Form 20-F of AstraZeneca PLC;
 
 
2.
Based on my knowledge, this report does not contain any untrue statement of a material fact or omit to state a material fact necessary to make the statements made, in light of the circumstances under which such statements were made, not misleading with respect to the period covered by this report;
 
 
3.
Based on my knowledge, the financial statements, and other financial information included in this report, fairly present in all material respects the financial condition, results of operations and cash flows of the company as of, and for, the periods presented in this report;
 
 
4.
The company’s other certifying officer(s) and I are responsible for establishing and maintaining disclosure controls and procedures (as defined in Exchange Act Rules 13a-15(e) and 15d-15(e)) and internal control over financial reporting (as defined in Exchange Act Rules 13a-15(f) and 15d-15(f)) for the company and have:
 
 
(a)  
Designed such disclosure controls and procedures, or caused such disclosure controls and procedures to be designed under our supervision, to ensure that material information relating to the company, including its consolidated subsidiaries, is made known to us by others within those entities, particularly during the period in which this report is being prepared;
 
 
(b)  
Designed such internal control over financial reporting, or caused such internal control over financial reporting to be designed under our supervision, to provide reasonable assurance regarding the reliability of financial reporting and the preparation of financial statements for external purposes in accordance with generally accepted accounting principles;
 
 
(c)  
Evaluated the effectiveness of the company’s disclosure controls and procedures and presented in this report our conclusions about the effectiveness of the disclosure controls and procedures, as of the end of the period covered by this report based on such evaluation; and
 
 
(d)  
Disclosed in this report any change in the company’s internal control over financial reporting that occurred during the period covered by the annual report that has materially affected, or is reasonably likely to materially affect, the company’s internal control over financial reporting; and
 
 
5.
The company’s other certifying officer(s) and I have disclosed, based on our most recent evaluation of internal control over financial reporting, to the company’s auditors and the audit committee of the company’s board of directors (or persons performing the equivalent functions):
 
 
(a)  
All significant deficiencies and material weaknesses in the design or operation of internal control over financial reporting which are reasonably likely to adversely affect the company’s ability to record, process, summarize and report financial information; and
 
 
(b)  
Any fraud, whether or not material, that involves management or other employees who have a significant role in the company’s internal control over financial reporting.
 
 
March 25, 2013
 
 
  /s/ Pascal Soriot
 
Pascal Soriot,
Chief Executive Officer, AstraZeneca PLC
 
 
 
 
Exhibit 12.2
 

CERTIFICATION PURSUANT TO SECTION 302 OF THE SARBANES-OXLEY ACT 2002

 
I, Simon Lowth, certify that:
 
 
1.
I have reviewed this annual report on Form 20-F of AstraZeneca PLC;
 
 
2.
Based on my knowledge, this report does not contain any untrue statement of a material fact or omit to state a material fact necessary to make the statements made, in light of the circumstances under which such statements were made, not misleading with respect to the period covered by this report;
 
 
3.
Based on my knowledge, the financial statements, and other financial information included in this report, fairly present in all material respects the financial condition, results of operations and cash flows of the company as of, and for, the periods presented in this report;
 
 
4.
The company’s other certifying officer(s) and I are responsible for establishing and maintaining disclosure controls and procedures (as defined in Exchange Act Rules 13a-15(e) and 15d-15(e)) and internal control over financial reporting (as defined in Exchange Act Rules 13a-15(f) and 15d-15(f)) for the company and have:
 
 
(a)  
Designed such disclosure controls and procedures, or caused such disclosure controls and procedures to be designed under our supervision, to ensure that material information relating to the company, including its consolidated subsidiaries, is made known to us by others within those entities, particularly during the period in which this report is being prepared;
 
 
(b)  
Designed such internal control over financial reporting, or caused such internal control over financial reporting to be designed under our supervision, to provide reasonable assurance regarding the reliability of financial reporting and the preparation of financial statements for external purposes in accordance with generally accepted accounting principles;
 
 
(c)  
Evaluated the effectiveness of the company’s disclosure controls and procedures and presented in this report our conclusions about the effectiveness of the disclosure controls and procedures, as of the end of the period covered by this report based on such evaluation; and
 
 
(d)  
Disclosed in this report any change in the company’s internal control over financial reporting that occurred during the period covered by the annual report that has materially affected, or is reasonably likely to materially affect, the company’s internal control over financial reporting; and
 
 
5.
The company’s other certifying officer(s) and I have disclosed, based on our most recent evaluation of internal control over financial reporting, to the company’s auditors and the audit committee of the company’s board of directors (or persons performing the equivalent functions):
 
 
(a)  
All significant deficiencies and material weaknesses in the design or operation of internal control over financial reporting which are reasonably likely to adversely affect the company’s ability to record, process, summarize and report financial information; and
 
 
(b)  
Any fraud, whether or not material, that involves management or other employees who have a significant role in the company’s internal control over financial reporting.
 
 
March 25, 2013
 
 
/s/ Simon Lowth
Simon Lowth,
Chief Financial Officer, AstraZeneca PLC
 
 
 
Exhibit 13.1
 
CERTIFICATION PURSUANT TO SECTION 906 OF THE SARBANES-OXLEY ACT OF 2002
(SUBSECTIONS (a) and (b) OF SECTION 1350, CHAPTER 63 OF TITLE 18, UNITED STATES CODE)
 
The certification set forth below is being submitted in connection with the Annual Report on Form 20-F of AstraZeneca PLC for the year ended December 31, 2012 (the “Report”) for the purpose of complying with Rule 13a-14(b) or Rule 15d-14(b) of the Securities Exchange Act of 1934 (the “Exchange Act”) and Section 1350 of Chapter 63 of Title 18 of the United States Code.
 
Pascal Soriot, the Chief Executive Officer and Simon Lowth, the Chief Financial Officer of AstraZeneca PLC, each certifies that, to the best of his knowledge:
 
 
1. 
the Report fully complies with the requirements of Section 13(a) or 15(d) of the Exchange Act; and
 
 
2.
the information contained in the Report fairly presents, in all material respects, the financial condition and results of operations of AstraZeneca PLC.
 



March 25, 2013



 
/s/ Pascal Soriot
Pascal Soriot,
Chief Executive Officer, AstraZeneca PLC




 
/s/ Simon Lowth
Simon Lowth,
Chief Financial Officer, AstraZeneca PLC
 
 
 
 

Exhibit 15.1

 

LOGO

Table of Contents

Innovation is at the core of everything we do at AstraZeneca – from our research into effective new medicines to how we run our business.

Our goal is to improve health for patients, bring benefits for stakeholders and deliver long-term shareholder value through continued successful innovation.

Our innovation:

 

LOGO   >    Improves health outcomes for patients    LOGO

 

LOGO

  >    Delivers economic benefits for healthcare systems    LOGO

 

LOGO

  >    Adds value beyond the medicines    LOGO

 

LOGO

  >    Contributes to our local communities    LOGO

In a world where the demand for healthcare continues to grow, the advances made through innovation are vital to address unmet medical need and deliver sustained improvement in healthcare worldwide.

 

Important information for readers of this Annual Report For further information in relation to the inclusion of reported performance, Core financial measures and constant exchange rate (CER) growth rates as used in this Overview from page 2 and throughout the Performance and Corporate Governance sections from pages 24 and 106 respectively, please refer to the Financial Review on page 88. Throughout this Annual Report, growth rates are expressed at CER unless otherwise stated.

 

Definitions The Glossary and the Market definitions table from page 209 are intended to provide a useful guide to terms and AstraZeneca’s definitions of markets, as well as to acronyms and abbreviations, used in this section and elsewhere in this Annual Report.

 

Use of terms In this Annual Report, unless the context otherwise requires, ‘AstraZeneca’, ‘the Group’, ‘we’, ‘us’ and ‘our’ refer to AstraZeneca PLC and its consolidated entities.

 

LOGO

This Annual Report

is also available on

our website,

astrazeneca.com/

annualreport2012

  

Statements of dates Except as otherwise stated, references to days and/or months in this Annual Report are references to days and/or months in 2012.

 

Cautionary statement regarding forward-looking statements A cautionary statement regarding forward-looking statements and other essential information relating to this Annual Report can be found on the inside back cover.

 

Directors’ Report The following sections make up the Directors’ Report, which has been prepared in accordance with the requirements of the Companies Act 2006:

 

> Strategy

> Performance

> Corporate Governance

> Development Pipeline

> Shareholder Information

> Corporate Information

 

 

AstraZeneca

Welcome to the AstraZeneca Annual Report and Form
20-F Information 2012 (Annual Report). You will find this Annual Report on our website, astrazeneca.com/ annualreport2012

 

 

Strategy

To compete as a global biopharmaceutical business delivering great medicines to patients through innovative science and excellence in development and commercialisation

 

 

Performance

2012 financial performance was defined by significant revenue decline associated with the loss of exclusivity for several products

 

 

Corporate Governance

In addition to the regular programme of meetings for the Board and its Committees 2012 was a busy year with new appointments, a record number of business development deals and our strategic review

 

 

Financial Statements

Met or exceeded financial targets as a result of disciplined financial management and lower Reported tax rate

 

 

Additional Information

More information about our business and about being an AstraZeneca shareholder

 

Table of Contents

LOGO

    Introduction and overview  
  2   AstraZeneca at a glance  
  6   Chairman’s Statement  
  8   Chief Executive Officer’s Review  
     
     
     
     
     
             
    Strategy  
  12   Our business model  
  14   Life-cycle of a medicine  
  16   Our industry  
  20  

Our strategy

 

 
     
     
     
     
     
             
    Performance  
  24   Key Performance Indicators  
  30   Business Review  
  50   Therapy Area Review  
  70   Geographical Review  
  74   Risk  
  86   Financial Review  
     
     
     
             
    Corporate Governance  
  106   Board of Directors and Senior Executive Team  
  110   Corporate Governance Report  
  122  

Directors’ Remuneration Report

 

 
     
     
             
    Financial Statements  
  141   Auditor’s Report  
  142   Consolidated Statements  
  150   Notes to the Group Financial Statements  
     
     
     
     
     
             
   

Additional Information

 
  199   Development Pipeline  
  203   Shareholder Information  
  208   Corporate Information  
  209   Glossary  
  212   Index  
     
     

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   1

Table of Contents

  Overview | AstraZeneca at a glance

 

LOGO

Table of Contents

LOGO

Table of Contents

 

LOGO

Table of Contents

 

LOGO

Table of Contents

Overview | Chairman’s Statement

 

LOGO

 

Dear Shareholder

I am glad I was able to meet a number of you in April 2012 when AstraZeneca held its Annual General Meeting in London. At that meeting you elected me as a Director and it is my privilege to have served as your Chairman since June.

Louis Schweitzer and David Brennan

The day of the AGM was, by any measure, an historic one for your Company. It was the day on which David Brennan announced his decision to retire from AstraZeneca as your Chief Executive Officer. It was also the day on which your previous Chairman, Louis Schweitzer, brought forward the date of his intended retirement to 1 June to coincide with that of David.

Louis had been a Director since 2004 and your Chairman for seven years. During that time he worked tirelessly to ensure that the Board was effective in its task of setting our strategy and overseeing its implementation. We are grateful to him for his efforts on your behalf.

As Chief Executive Officer, David led AstraZeneca with skill, integrity and courage during a period of enormous change for the industry and for the Company in particular. I would like to thank David for his selfless leadership during his six years at the helm.

 

Non-Executive changes

Part of the strength of any board comes from refreshing and renewing the mix of people sitting around the boardroom table. When I joined the Board, I was pleased that both Graham Chipchase and Geneviève Berger also became Non-Executive Directors. They bring, respectively, in-depth financial and scientific expertise, as well as significant international business experience to our discussions.

Also in April 2012, we said farewell to Michele Hooper who stood down from the Board. We are all grateful for her distinguished contribution to our work and her dedicated service as Chairman of the Audit Committee and senior independent Non-Executive Director. In her place, John Varley took over as senior independent Non-Executive Director and Rudy Markham became Chairman of the Audit Committee.

A new Chief Executive Officer

Upon my election to the Board I was also appointed Chairman of the Nomination Committee. This enabled me to lead the important process of selecting David Brennan’s successor. This was a process that included both internal and external candidates and culminated in the appointment of Pascal Soriot to the Board as the Company’s Chief Executive Officer on 1 October.

Pascal joined us from Roche where he had been serving as Chief Operating Officer of the company’s pharmaceuticals division. His was a key appointment at an important time for AstraZeneca. The Board is certain that Pascal’s leadership qualities, combined with his strategic thinking and extensive

experience in the industry, make him the right person to drive AstraZeneca to success over the coming years. I am confident that Pascal’s approach and his track record of delivering results in innovation-driven businesses will be valued by shareholders and employees alike.

Following David’s departure, Simon Lowth acted as Interim Chief Executive Officer. The Board and I would like to record our appreciation for his impressive leadership in this period. Supported by a highly capable and committed executive team, Simon maintained the organisation’s focus on key business priorities during a period of significant change.

Sound governance

All the changes I have outlined took place at the same time as AstraZeneca completed a record number of business development deals. We also undertook our annual strategic review, in which Pascal has been fully involved, as well as our regular programme of meetings and business activity. That we have been able to do all this is a tribute both to the sound corporate governance processes we have in place and to the dedication and hard work of my fellow Directors. I am grateful to all of them for the contribution they made in 2012.

Challenging times

We will need to harness all our skills, capabilities and experience if we are to successfully navigate the current harsh climate for the pharmaceutical sector. The world pharmaceutical market is still growing and underlying demographic trends remain favourable to long-term industry growth. However, many of the drivers of demand and supply in the industry are under pressure.

 

 

6   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

 

LOGO

 

On the demand side, we face increased competition from generic medicines as some of the world’s most successful drugs come off patent. In addition, securing recognition (through reimbursement approval) and reward (through favourable pricing and sales) for innovation is becoming more difficult in the face of intensifying pricing pressures, particularly in Established Markets facing rising healthcare costs. On the supply side, the industry faces an ongoing R&D productivity challenge. R&D costs have risen significantly over the past decade, while industry-wide probability of success continues to decline.

Strategic focus

It is for the reasons outlined above that the outcome of our current strategic review is so important. Our strategy is rooted in our heritage as a company focused on innovative science to deliver great medicines to patients. I firmly believe that it is the path we need to take if we are to remain competitive and return to growth. That path must also include a commitment to the responsible and sustainable development of our business. That is why I was so pleased that we were once again listed in the Dow Jones Sustainability World Index in 2012 and retained our listing on the European Index for the fifth year running.

Financial performance

We cannot hope to secure our long-term success if we do not meet our financial targets and deliver acceptable levels of return to our owners. Group sales in 2012 were down 15% to $27,973 million (2011: $33,591 million) and Reported operating profit was down 34% at $8,148 million (2011: $12,795 million). Revenue in the US was down 21% while revenue outside the US was down 11%.

More than 13 percentage points of the revenue decline, approximately $4.5 billion, was related to loss of exclusivity on several brands in the portfolio. Seroquel IR alone declined by more than $3 billion, while regional losses of exclusivity for Atacand, Nexium and Crestor accounted for more than $1 billion. Additionally, the disposals of Astra Tech and Aptium accounted for around 1.7 percentage points of the decline. On the other hand, taken together, Symbicort, Faslodex, Onglyza, Iressa, Brilinta/Brilique and Seroquel XR accounted for more than $600 million of revenue growth. Additionally, our diabetes alliance with BMS is strengthened by the inclusion of the Amylin portfolio and the approval of Forxiga in Europe.

Reported earnings per share were down 29% to $4.99. The decline reflects the $1.08 per share benefit in 2011 from the sale of Astra Tech and higher restructuring costs in 2012.

Returns to shareholders

Consistent with our progressive dividend policy, the Board has recommended a second interim dividend of $1.90. This brings the dividend for the full year to $2.80 (178.6 pence, SEK 18.34). In 2012, cash distributions to shareholders through dividends totalled $3,665 million and net share repurchases totalled $2,206 million. In October, we announced the suspension of our share repurchase programme for 2012 and the Board has decided that no share repurchases will take place in 2013 in order to maintain the flexibility to invest in the business.

Outlook

We believe challenging market conditions will persist in 2013, including continued government interventions in price. The revenue impact from the loss of exclusivity will also continue to affect our performance. In the context of the ongoing update to our strategy, we have withdrawn the planning assumptions for revenue and margin evolution for the period 2010 to 2014 we outlined in January 2010. We plan to hold a Capital Markets Day in March 2013 to provide a more detailed exposition of our strategic priorities.

 

LOGO

Leif Johansson

Chairman

 

 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   7

Table of Contents

Overview | Chief Executive Officer’s Review

 

LOGO

 

I am both excited and honoured to have been asked to lead AstraZeneca. Throughout my career I have had enormous respect for its people and what they have achieved. Since joining in October, I have seen for myself the passion and commitment that exists within the Group to improve the lives of patients around the world.

This level of energy should come as no surprise as our innovative medicines mean that more people than ever before are able to lead longer and healthier lives. As we seek to show throughout this Annual Report, successful pharmaceutical innovation, delivered responsibly, adds value not only for patients and shareholders but also for healthcare systems and the communities in which we work.

The challenge

Leif has already described in his Chairman’s Statement how, in addition to the well-known challenges that confront the pharmaceutical sector, the loss of exclusivity of several of our major brands largely defined AstraZeneca’s financial performance in 2012. I believe that our ability to provide an acceptable level of return to you in the years ahead will come from an undiluted focus on delivering great medicines to patients through innovative science and global excellence in development and commercialisation. Underpinning that focus are three priorities: achieving scientific leadership, returning AstraZeneca to growth and making it a great place to work.

In the Strategy section from page 12 of this Annual Report, we talk more about the background to our strategy and the review we are undertaking. For the rest of my Review I want to look at the progress we made towards our goals in 2012, as well as consider some of the setbacks we encountered.

Scientific leadership

In a research and development-based business such as AstraZeneca, I believe that everything starts with a focus on patients and great science. It is our first priority.

AstraZeneca has a unique combination of scientific capabilities in small molecules, biologics, immunotherapies and antibody engineering. This puts us in a strong position to develop the targeted novel medicines and combinations (such as drug-antibody conjugates) required to meet patient needs in the future. Reviews that we have held with scientific experts outside AstraZeneca have further reinforced my confidence in our underlying science base.

We have much to do to realise our full scientific potential but made some progress in 2012. On the regulatory front, we received approvals in Europe for Zinforo , our intravenous antibiotic, Caprelsa , our thyroid cancer treatment, and Forxiga , a product of our diabetes alliance with BMS. In the US, FluMist Quadrivalent was approved, the first four-strain influenza vaccine to be approved by the FDA.

Across the entire pipeline of 84 projects, 39 successfully progressed to the next stage of testing in 2012, including 12 projects into first human testing. Nineteen projects were withdrawn. While we met our target for Phase III investment decisions for the year, we did not meet our value targets for those projects.

To increase the value of our pipeline, we aim to access the best science and molecules regardless of origin. Our portfolio was strengthened during the year by a number of successful business development initiatives. Our collaboration with Amgen encompasses five clinical stage projects in inflammation, including brodalumab, which has already entered Phase III development. In April 2012, we entered into an agreement to acquire Ardea, which added lesinurad, a Phase III project for the treatment of gout, to our portfolio. We also significantly expanded our diabetes alliance with BMS through its acquisition of Amylin.

Overall, we completed a record number of more than 60 important business development deals in 2012 that helped us to strengthen our scientific leadership in key therapeutic areas, expand our pipeline and improve our capabilities. They also helped underpin business growth in both Established and Emerging Markets.

Return to growth

Our second priority must be to return AstraZeneca to growth. Our performance in 2012 reflected a period of significant patent expiry and tough market conditions globally. Despite the challenges we face, I am excited about AstraZeneca’s fundamental strengths, which will be key in returning AstraZeneca to growth.

 

 

8   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

 

LOGO

 

Brilinta/Brilique , our treatment for acute coronary syndromes, is now approved in 88 countries and launched in 82. I believe that, while performance since its launch has been disappointing, especially in the US, Brilinta/Brilique has the potential to become a major product for AstraZeneca, given its significant mortality benefits relative to the standard of care. We have moved quickly to improve our sales, marketing and medical support to this important medicine. Early indications from some markets, combined with the favourable profile of this medicine, suggest that we are on the right path.

Taking full advantage of our expanded diabetes alliance with BMS also presents a significant opportunity. With the addition of Amylin products such as Byetta and Bydureon , we now have treatment options for patients from early stages of Type 2 diabetes to the pre-insulin stage. The launch of the extended portfolio in the US, only a few weeks after we concluded the deal, demonstrates how swiftly we can move to bring a range of treatment options to physicians and their patients.

With our well-established commercial strength, we are in a strong position to bring our medicines to patients in Emerging Markets. Conditions have been tough in Mexico, Brazil and some other markets, but strong growth in countries such as Russia and China shows how much our products are valued in these markets.

A great place to work

Skilled, committed employees are essential if AstraZeneca is to realise its full potential. Unfortunately, the 2012 global employee survey showed a reduction in the scores in the majority of categories. These scores were disappointing. While they might be regarded as understandable given our challenging environment and the ongoing transformation of the business, my SET colleagues and I are committed to working harder to ensure employees have an improved understanding and confidence in our future direction.

More positively, it was encouraging to see the high level of motivation that exists across AstraZeneca to help us succeed. This was something I witnessed at first hand as I spent time with colleagues on site in the weeks after I joined the organisation. I want to build on this and make AstraZeneca a great place to work – a simplified business that comprises a diverse and talented workforce operating in a high performance culture, which enables us to bring great medicines to patients.

Senior Executive Team

In January 2013, we announced changes to our Senior Executive Team, which were designed to provide sharper management focus, as well as devolving and accelerating decision making. Changes include increased representation of the Company’s scientific expertise, product portfolio and key regions. Members of the new SET are shown on pages 108 and 109 and I look forward to working with them all on delivering our strategic goals. As a result

of the changes, two senior roles were eliminated – President of R&D, held by Martin Mackay, and Executive Vice-President, Global Commercial, held by Tony Zook. Both Martin and Tony left their respective roles in January 2013, and I would like to thank them for their contribution and the exemplary leadership they have shown.

Innovation and growth

In closing, I would like to thank everyone in AstraZeneca for their support and making me feel so welcome. My first three months as Chief Executive Officer confirmed the nature and scale of the challenges we face. Those months also confirmed my view that within the organisation we have both the capabilities and skills necessary to achieve scientific leadership, return to growth and be a great place to work. I am sure that by being true to our mission of bringing innovative medicines to patients we can meet our short- and medium-term goals and thereby deliver our longer term aspirations for the business.

 

LOGO

Pascal Soriot

Chief Executive Officer

 

 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   9

Table of Contents

Strategy | The value of innovation

Innovation means

 

LOGO

 

10   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

Innovation is not always about ‘breakthrough’ discoveries – medical progress can often be delivered just as effectively through incremental improvements.

 

LOGO

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   11

Table of Contents

Strategy | Our business model

 

LOGO

 

In this section, we describe our business model and review the key growth drivers and challenges that the pharmaceutical sector faces.

We then describe AstraZeneca’s response to these factors and the ongoing update to our strategy – a strategy that seeks to make a real difference to patient health, deliver long-term value for our shareholders, and add value for our other stakeholders and wider society.

Our business model

Improving health is one of the toughest challenges facing the world today. Despite all the advances in recent decades, the prevalence of major diseases is on the increase. The world’s population is growing and ageing. Health awareness and patients’ expectations are rising while healthcare systems everywhere are under pressure. It will take a sustained and significant effort to drive continued progress in healthcare.

As a global biopharmaceutical company, AstraZeneca has a key contribution to make. Our skills and resources are focused on the discovery, development, manufacturing and commercialisation of patent-protected medicines that make a meaningful difference to patients facing some of the world’s most serious health challenges: heart disease, diabetes, gastrointestinal disorders, infection,

neurological disorders, cancer, and respiratory and inflammatory conditions. This is the core of our commitment to our stakeholders and society. Successful pharmaceutical innovation, delivered responsibly, improves health for patients, brings benefits to stakeholders and delivers long-term shareholder value.

The process of getting a medicine to market, from initial discovery, through development to approval and launch is risky, costly and time consuming. Of the many thousands of compounds initially analysed, only a few make it through all stages of development. The figure overleaf illustrates the process we follow. Our activities cover the entire life-cycle of a medicine and start with the identification of an unmet medical need, and the scientific search for a potential medicine. The process continues through the phases of clinical trials and drug development, regulatory submission, and a medicine’s launch. After launch, our life-cycle management process (including line extensions) is designed to ensure a medicine’s continued safe use and to explore its potential for treating other diseases or extending its use into additional patient populations.

As the figure overleaf shows, we work in partnership with others to deliver the highest quality new medicines to market rapidly. For example, we work with those who pay for our medicines and health technology appraisers early on and throughout a

medicine’s development to understand where the greatest clinical needs are. As we develop our medicines we gather not only the clinical data required for regulatory approval but also the health economics cost/benefit and ‘value-in-use’ data required by payers.

An essential element of our business model is the creation and protection of our underlying intellectual property assets. This process is outlined in the diagram above. The development of a new medicine requires a significant investment of resources over a period of 10 or more years before product launch, with no guarantee of success. For this to be a viable investment, the resulting new medicine must be safeguarded from being copied with a reasonable amount of certainty and for a reasonable period of time. This allows time to generate a return on our investment and to reinvest in new pharmaceutical innovation.

The loss of key product patents has affected a significant proportion of sales in recent years and will continue to do so. A key goal for our planning process is therefore to ensure that we sustain the cycle of successful innovation and, as a result, continue to refresh our portfolio of patented products and so generate value for shareholders.

 

 

12   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

 

LOGO

 

Distinctive capabilities

AstraZeneca has clear strengths that allow us to create value for patients and for shareholders:

 

> Good underlying science. External opinion leaders confirm that we have strong disease knowledge, research portfolios, and related technology platforms in a number of areas, particularly in oncology, and respiratory and inflammation.
> Unique scientific capabilities. Few pharmaceutical companies in the world, if any, can match the combination of capabilities that we have in small molecules, biologics, immunotherapies and antibody engineering. These capabilities allow us to produce combination therapies (such as drug antibody conjugates and bispecifics) and customisable molecules, both targeted to specific patient populations.
> Strong therapy area franchises, brands and commercial capability . Over the past decade, we have developed strong commercial franchises that address respiratory, cardiovascular, oncology and neuroscience diseases. We continue to develop these strong therapeutic area positions: for example, Brilinta/Brilique and the diabetes portfolio we are commercialising jointly with BMS provide the next phase of development for our cardiovascular and metabolic disease franchise. We have strong commercial capability in developing, marketing and
  selling primary care, specialty care-led and specialty care products.
> Strong Emerging Markets presence. We combine global reach with local customer relationships. We do this particularly well in Emerging Markets, where we invested early and where our decentralised approach to sales and marketing has allowed us to develop and act on local customer insight. For example, we are the second largest pharmaceutical company in China by sales.

As we look ahead, the future success of an innovation-driven R&D-based business such as AstraZeneca must be based on the twin foundations of a focus on patients and great science. We are one of only a handful of companies to span the entire life-cycle of a medicine from discovery, early and late-stage development to the global commercialisation of primary care, specialty care-led and specialty care medicines. Using these skills and capabilities we can make a real difference to the health of a broad range of patients in disease areas where there is unmet medical need in more than 100 markets around the world. We also harness these skills and capabilities in partnership with others, such as the relationships we have with BMS and Amgen.

 

Health connects us all

We know we cannot deliver on our commitment to improve healthcare on our own. We work closely with others in the healthcare community to understand their needs and challenges, and how we can combine skills and resources to achieve common goals. To be able to do this, people must have confidence in both what we do and how we do it. We know that their trust depends on us acting with integrity and staying true to our core values.

The principles of Courage, Collaboration and Creativity frame our values. They describe what we stand for as a company, and the behaviours we need to demonstrate to achieve our strategic priorities. These values reflect our belief that health connects us all. They guide our actions and shape the culture that underpins our drive for business success.

 

 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   13

Table of Contents

Strategy | Life-cycle of a medicine

 

LOGO

 

14   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

 

LOGO

Table of Contents

Strategy | Our industry

 

LOGO

 

Our industry

Introduction

The pharmaceutical industry has doubled in value since 2000, driven by a large number of FDA approvals in the second half of the 1990s and by the increased use of medicines around the world in the wake of global economic growth in that period. Now, many of the drivers of demand and supply in the industry are under pressure.

Nonetheless, as the figure above shows, the world pharmaceutical market grew by 2.5% in 2012. Average revenue growth in Established Markets was 1.5% while that in Emerging Markets was over seven times higher at 11.1%. The top five pharmaceutical markets in the world remained the US, Japan, Germany, France and China, with the US representing 39.3% of global pharmaceutical sales (2011: 38.1%).

On the demand side, underlying demographic trends remain favourable to long-term industry growth. These are outlined below. However, securing recognition (through reimbursement approval) and reward (through favourable pricing and sales) for innovation is becoming more difficult, as there are intensifying pricing pressures, particularly in Established Markets which are facing rising healthcare costs. Our challenge is to work with governments and other payers to ensure they understand the value of pharmaceutical innovation in order for us to achieve adequate commercial returns on our investment. We also face increased competition from generic medicines as some of the world’s most successful drugs come off patent. Finally, greater regulatory constraints are being placed on the pharmaceutical industry by governments and those who pay for medicines.

On the supply side, the industry faces an ongoing and significant R&D productivity challenge. R&D costs have risen significantly over the past decade, while industry-wide probability of success from pre-clinical to launch continues to decline. For example, the median large pharmaceutical company success rate for 2007 to 2011 in delivering a compound from pre-clinical studies to launch was 2%. These factors are considered in more detail below.

The industry remains highly competitive. Our competitors are other large research-based pharmaceutical companies that discover, develop and sell innovative, patent-protected prescription medicines and vaccines, as well as smaller biotechnology and vaccine companies, and companies that produce generic medicines. While many of our peers are confronting similar challenges, strategically these challenges are being met in different ways. For example, while some companies have pursued a focused strategy, others have diversified by acquiring or building branded generics businesses or consumer portfolios, arguing that this enables them to better meet changing customer needs and smooth risk for shareholders.

While most companies continued to pursue their existing strategies in 2012, there were exceptions with some companies moving away from diversification. Key trends across the industry included ongoing efforts to improve R&D innovation and productivity, expansion of geographic scope, especially in Emerging Markets and Japan, and the pursuit of operational efficiency. There was an increase in business development and partnering at all stages of product development, with a continued increase in peer collaboration.

Growth drivers

Expanding patient populations

The world population is expected to rise from its current level of some seven billion and reach nine billion by 2050. In addition, the number of people who can access healthcare continues to increase, particularly among the elderly. Globally, it is estimated that between 2000 and 2050, the number of people aged 60 years and over will increase from 605 million to two billion.

Faster-developing economies, such as China, India and Brazil, offer new opportunities for the pharmaceutical industry to help an expanding number of patients who can benefit from innovative medicines. Developing markets now represent approximately 85% of the world population and over 22% of the world’s pharmaceutical revenues. Pharmaceutical revenues in those markets therefore continued to grow faster than those in Established Markets in 2012. As the Estimated pharmaceutical market growth 2011-2016 figure on page 20 shows, we expect this trend will continue.

Unmet medical need

In most developed markets, ageing populations and certain lifestyle choices such as smoking, a poor diet and lack of exercise drive an increased incidence of non-communicable diseases (NCDs) such as cancer, cardiovascular/ metabolic and respiratory diseases which require long-term management. In 2008, almost two-thirds of deaths globally were from NCDs and 80% of those were in lower and middle income countries. For example, in South Asia it is estimated that deaths from NCDs will increase from half to almost three-quarters of all deaths between 2008 and 2030. It is also estimated that nearly one-third of the world’s diabetes patients will come from

 

 

16   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

LOGO

 

India and China by 2030, by which date its prevalence in Brazil is expected to have increased by two-thirds.

Advances in science and technology

Innovation leading to new drugs is critical if we are to address unmet medical need. Existing drugs will continue to be important in meeting the growing demand for healthcare, particularly with the increasing use of generic medication. At the same time, advances in disease understanding and the application of new technologies will be required to ensure the delivery of new medicines. Such approaches include personalised healthcare and predictive science, as well as new types of therapy. With advances in the technologies for the design and testing of novel compounds, new opportunities exist for the use of innovative small molecules as new medicines. The use of large molecules, or biologics, has also become an important source of innovation, with biologics among the most commercially successful new products. Forecasts for 2018 predict that of the world’s top 100 pharmaceutical products, 49% of sales will come from biologics. This compares with only 34% in 2011 and 17% in 2004. Most pharmaceutical companies now pursue R&D in both small molecules and biologics.

The challenges

R&D productivity

Improving R&D productivity is a critical challenge for the pharmaceutical industry. As shown in the diagram above, global investment in pharmaceutical R&D reached an estimated $134 billion in 2012, a 94% increase from $69 billion in 2002. However, the annual growth in R&D spend has slowed in recent years.

The number of new drugs approved by the FDA rose from 30 in 2011 to 39 in 2012. This marks the greatest increase in annual approvals since 2004. However, the average forecast sales from these products five years post-launch is lower than the forecasts for products approved in 2010, reflecting the shift away from broad primary care indications to more specialist drugs.

To ensure it delivers a sustainable return on its R&D investment, the industry is working to increase its probability of success in developing commercially viable new drugs and is moving to a lower, more flexible cost base. It does so at a time when regulators and payers are demanding more and better evidence of comparative effectiveness of compounds, which lengthens development times and increases development costs.

The industry is using the full range of innovative technologies to achieve and accelerate product approvals. Additionally, greater emphasis has been placed on demonstrating Proof of Concept, which delivers candidate drugs with supporting data demonstrating that the drug results in a clinical change with an acceptable endpoint or surrogate in patients with the disease.

Organisationally, companies are addressing productivity challenges in a variety of ways. These include:

 

> focusing on a defined set of therapeutic areas and exiting those where success has been poor
> restructuring R&D organisations to create clearer accountabilities and smaller, more entrepreneurial units
> revamping decision making and governance, so that unsuccessful
  compounds are identified early, before significant costs have been incurred
> reducing costs and improving process efficiency, using Lean business improvement tools such as Six Sigma and outsourcing
> a collaboration-centric business model that includes academic collaborations and co-development agreements that provide for the sharing of development risks and costs with external partners
> looking externally for high quality science, technologies, targets, drug candidates, and/or entire drug pipelines.

Regulatory requirements

Our industry continues to be highly regulated. This reflects public interest in ensuring access to safe, effective and high quality medicines that are responsibly tested, manufactured and commercialised. Given the nature and geographic scope of our business, we maintain important relationships with health authorities worldwide as they assess the safety, efficacy and quality of medicines. These include the FDA in the US, the EMA in the EU, the Japan Pharmaceuticals and Medical Device Agency and the SFDA in China.

In 2012, the US re-authorised the Prescription Drug User Fee Act and the EU continued to implement pharmacovigilance legislation. These measures share the common goals of protecting patient safety, creating greater transparency in the regulatory process throughout a product’s life-cycle and taking greater account of the patient perspective in the regulatory process. There is also a global trend, led by the EU, to increase public access to the documentation companies submit to health authorities in support of marketing authorisations.

 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   17

Table of Contents

Strategy | Our industry

 

LOGO

 

So far as the development of biosimilars is concerned, health authorities continue to face the challenge of developing robust standards to ensure their safety, effectiveness and quality. For further information on biosimilars, see the Patent expiries and genericisation section below.

Efforts to harmonise regulations globally continue, yet the number of regulations and their impact continue to multiply. Clinical trials that support the registration of products in a given regulatory jurisdiction must be relevant to a variety of patient demographics. Programmes using foreign clinical trial data also need to meet each individual health authority’s requirements and be relevant to their population. Health authorities continue to redefine patient safety assessment processes. In addition, in emerging pharmaceutical markets, health authorities are developing their own individual requirements and safety initiatives.

One impact of the growing complexity and globalisation of clinical studies, and the pressure on industry and healthcare budgets, has been an increase in industry collaborations with health authorities. These are driving innovation and streamlining regulatory processes, as well as defining and clarifying approval requirements for new technology and approaches such as personalised healthcare. They are also accelerating the development of treatments that address public health priorities.

In another trend, health technology assessors and payers are increasingly assessing not only the safety of products but also their relative effectiveness and value. Consequently, there is a heightened interest by health authorities in both comparative clinical effectiveness and the ongoing benefit/risk assessment of medicines after they have been approved. This is resulting in a greater focus on incorporating validated health outcome measures into clinical trials and the development of clinical comparative evidence.

However, it remains the case that when applications are supported by strong data and compelling benefit/risk propositions, regulators are approving drugs that address unmet medical need.

Pricing pressure

The pricing and reimbursement environment in many markets continues to be highly challenging. Most pharmaceutical sales are generated in highly regulated markets where governments and private payers, such as insurance companies, exert various levels of control on pricing and reimbursement. Cost-containment, including containment of spending on pharmaceuticals, continues to be a focus. A wave of austerity programmes following the current global economic downturn further constrain healthcare providers and tougher economic conditions constrain those patients who pay directly for their medicines. Additional challenges may arise if suppliers and distributors face credit-related difficulties. At the same time, significant extra resources are required by pharmaceutical companies to demonstrate to payers the economic as well as therapeutic value of medicines.

In 2012, pressures on pricing included the implementation of a variety of drug price control mechanisms and other regulatory reforms, as well as the introduction of fixed hospital tariffs which can act as a method of controlling drug costs by incentivising hospitals to choose cheaper generic alternatives over patent-protected medicines.

In the US, the Affordable Care Act has already had a direct impact on healthcare activities despite the fact that many of the healthcare coverage expansion provisions of the Affordable Care Act do not take effect until 2014. For example, in 2010 there was an increase in the mandatory Medicaid rebates. In addition, the pharmaceutical industry, including AstraZeneca, is making prescription drugs more affordable to senior citizens through, for example, helping to close the coverage gap in the Medicare Part D prescription drug programme. The industry continues to work with policymakers and regulators with a view to ensuring that they strike a balance between containing costs, improving outcomes and promoting an environment that fosters medical innovation.

In August 2011, as part of the bipartisan agreement to raise the federal debt ceiling, the US Congress created the Joint Select Committee on Deficit Reduction (Committee). The Committee was empowered to recommend a package of $1.2 trillion in cost savings with the requirement that, if the Committee failed to reach an agreement, the savings would be achieved through across the board spending cuts (sequestration).

 

 

18   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

LOGO

 

The Committee discussions ended without reaching an agreement and, barring future action by Congress, sequestration was to take effect on 2 January 2013. Sequestration would have impacted most federal government healthcare programmes with broad reductions in federal government spending. On 3 January 2013, President Barack Obama signed a bill that avoided sequestration. The bill allowed the US Congress and the President an additional two months to address the sequestration challenge. As Congress and the President continue to discuss how to reduce government expenditure, some policymakers may look to the pharmaceutical industry to help achieve the cost savings they seek.

In Europe, governments have issued new legislation on mandatory discounts, clawbacks and referencing rules, driving prices down, especially in the distressed economies of Greece, Portugal and Spain. It has been estimated that in Greece, Ireland, Italy, Portugal and Spain the pharmaceutical industry accommodated price cuts and discounts of more than 7 billion in 2010 and 2011, which amounted to 8% of the industry’s turnover in these countries. In Germany, Europe’s largest pharmaceutical market, manufacturers are now required to prove the additional benefit of their drugs over existing alternatives. Only by showing additional benefit can the drug avoid being transferred to the German reference pricing system, where, for each drug group, a single reimbursement level or reference price is set.

Elsewhere, in China, the triennial maximum retail drug price review took place in 2012, with more stringent rules being imposed compared with previous rounds of cuts, while in Japan biennial cuts are expected to continue. In Latin America, pricing is increasingly controlled by governments, for example in Colombia and Venezuela.

More information regarding the impact of price controls and reductions, as well as the impact of healthcare reform in the US, can be found in the Principal risks and uncertainties section from page 75. The principal aspects of price regulation in our major markets are described further in the Geographical Review from page 70.

Patent expiries and genericisation

We are in the middle of a period in which some of the biggest selling drugs the industry has ever produced face patent expiry. As a consequence, payers, physicians and patients in Established Markets will have access to low price, generic alternatives in many important classes of primary care drugs. For example, in the US in 2012, generics constituted 84% of the market by volume.

Patents only protect pharmaceutical products for a finite period and the expiry or early loss of patents often leads to the availability of generics. Generic versions of drugs are very competitive with significantly lower pricing than the innovator equivalents. This is partly due to lower investment by generic manufacturers in R&D and market development. While generic competition has traditionally occurred when patents

expire, it can also occur where the validity of patents is disputed or successfully challenged before expiry. Such early challenges by generics have increased with generics companies increasingly willing to launch products ‘at risk’, for example, prior to resolution of the relevant patent litigation. This trend is likely to continue, resulting in significant market presence for the generic version during the period in which litigation remains unresolved, even though the courts may subsequently rule that the innovative product is properly protected by a valid patent. The unpredictable nature of patent litigation has led innovators to seek to settle such challenges on terms acceptable to both innovator and generic manufacturer. However, some competition authorities have sought to challenge the scope and/or availability of this type of settlement agreement.

Biologics have, to date, sustained longer life-cycles than traditional small molecule pharmaceuticals and have faced less generic competition. This is due to a more complex manufacturing process for biologics compared with small molecule medicines. It is also due to the inherent difficulties in producing a biosimilar which, as a biological equivalent, rather than an exact chemical copy, could require additional clinical trials. However, with regulatory authorities in Europe and the US continuing to implement abbreviated approvals pathways for biosimilar versions, innovative biologics are likely to become increasingly subject to competition from biosimilars.

 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   19

Table of Contents

Strategy | Our strategy

 

LOGO

 

Building trust

The pharmaceutical industry faces a challenge in building and maintaining trust, particularly with governments and regulators. The last 10 years have seen a significant increase in the number of settlements between innovator companies and governmental and regulatory authorities for violations of a variety of laws. These include breaches of sales and marketing practices, inducements of physicians to administer a company’s products and breaches of anti-trust legislation. For some audiences, there is a perception that pharmaceutical companies place their commercial goals above the interests of patients, physicians and payers. Companies are taking steps to change this perception by embedding a culture of ethics and integrity, adopting higher standards of governance and improving relationships with employees, shareholders and other stakeholders.

Our strategy

AstraZeneca’s mission is to make the most meaningful difference to health through great medicines.

Our strategic review has confirmed our belief that biopharmaceuticals remain an attractive business, with strong underlying drivers of demand: expanding and ageing populations, a growing chronic disease burden, and increasing wealth through

economic growth, especially in Emerging Markets. While the hurdles to adopting new products have been raised, there remains a willingness to pay for differentiated, innovative medicines.

We further believe that AstraZeneca has the skills and capabilities to take advantage of these opportunities and turn them into long-term value. We will do this by exploiting and further developing our competitive advantage: an innovation and science-led organisation capturing the best of biologics, small molecules, immunotherapies and antibody engineering.

Our revised strategy is to compete as a global biopharmaceutical business delivering great medicines to patients through innovative science and excellence in development and commercialisation:

 

> global – in that we believe we combine global reach with local customer relationships and have the ability to meet healthcare needs in both developed and developing markets efficiently and effectively
> biopharmaceutical – in that we will develop both chemical (small molecule) and biological (large molecule) medicines available by prescription, targeting those product categories where medical innovation or brand equity will continue to enable us to make acceptable levels of return on our investments
> innovative   science – in that we believe that innovative science must be the foundation for procuring differentiated, novel medicines that benefit patients and for which payers will pay
> excellence in development and commercialisation – in that we believe we have strong commercial franchises and capability in developing, marketing and selling primary care, specialty care-led and specialty care products.

We are currently completing the strategic review that we began in 2012. We plan to hold a Capital Markets Day in March 2013 to provide a more detailed exposition of our strategic priorities.

Changes to the Senior Executive Team

In January 2013, we unveiled changes to our Senior Executive Team that came into immediate effect. Membership of the SET has been expanded to include increased representation of AstraZeneca’s scientific expertise, key products and key markets. Changes included the creation of:

 

> three senior R&D roles responsible for discovery and early-stage development in small molecules; discovery and early-stage development in biologics; and late-stage development
> three roles representing the commercial regions: North America; Europe; and International.
 

 

20   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

LOGO

 

A further role will be responsible for global portfolio and product strategy, bridging the R&D and sales organisations. An appointment will be made at a later date.

The new SET structure is designed to provide sharper management focus on our key pipeline assets, product portfolio and key regions, as well as devolving and accelerating decision making. It draws heavily from the leadership talent within AstraZeneca, with the six new members being internal appointments. The full membership of the SET, together with information about individual members and their responsibilities, is shown in the Senior Executive Team section on pages 108 and 109.

Restructuring

Since 2007, we have undertaken significant efforts to restructure and reshape our business to improve long-term competitiveness.

The first phase was completed in 2009.

The second phase, which featured a significant change programme in R&D, began in 2010. The restructuring actions for this phase of the programme were completed in 2011, at a total programme cost of $2.1 billion. Headcount changes associated with this phase, involving an estimated 9,000 positions, were also completed. Total annual benefits of $1.9 billion were to be delivered by the end of 2014 in connection with this phase of the programme, of which $1.5 billion had been achieved by the end of 2012.

A third phase of restructuring was announced in February 2012. This phase, comprising initiatives across the supply chain, SG&A and R&D, carries an estimated programme cost of $2.1 billion (approximately $1.7 billion in cash costs). Restructuring costs of $1,558 million associated with this third phase were taken in 2012, together with $261 million that was charged in the fourth quarter of 2011. Most of the remaining costs of approximately $300 million will be taken in 2013. To date, actions involving around 6,300 of the estimated 7,300 positions to be impacted in connection with this phase of the programme have been completed. When completed, this phase is expected to deliver an estimated $1.6 billion in annual benefits by the end of 2014, of which approximately $350 million was realised by the end of 2012.

These restructuring programmes have been delivering their targeted benefits, and are designed to continue to provide the headroom to make appropriate investments to drive future growth and value, such as Emerging Markets commercial infrastructure and expansion of our research capabilities in biologics.

Medium-term planning assumptions

We believe challenging market conditions will persist in 2013, including continued government interventions in price. The revenue impact from the loss of exclusivity will also continue to affect our performance. In the context of the ongoing update to our strategy, we have withdrawn the planning assumptions for revenue and margin evolution for the period 2010 to 2014 that we had outlined in January 2010.

 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   21

Table of Contents

Performance | The value of innovation

Innovation means

LOGO

 

22   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

We are working more closely than ever before with the people who pay for healthcare to make sure we can answer their questions about the value of our medicines in delivering better, cost-effective healthcare to patients, including evidence about a medicine’s use in the ‘real world’ once it has been approved.

 

LOGO

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   23

Table of Contents

Performance | Introduction

 

LOGO

Our priorities in 2012

 

> Pipeline discovery and development of innovative, differentiated and commercially attractive medicines. We are transforming our R&D organisation to improve productivity and pioneering innovative ways of conducting research. We continue to focus on improving the quantity and quality of R&D output by building industry-leading capabilities in critical areas and being an outward-looking organisation, accessing the best science, regardless of origin.

 

> Deliver the business sales and marketing activities focused on the needs of our customers: patients, physicians and payers, and undertaken in the right way. We continue to build on our leading positions in Established Markets, to introduce innovative ways of serving our customers and pursue further growth opportunities in Emerging Markets. We have accelerated our efforts to secure late-stage/on-market product licensing, acquisition and peer collaboration opportunities in order to leverage our global development, resources, and sales and marketing capabilities to bring a broader portfolio of medicines to patients.

 

> Business shape a reliable supply and manufacturing operation, and Lean organisational infrastructure that ensure our medicines are where they need to be when they are needed. Given the pressures in the external environment, we continue to simplify the business. Simplification means not only cost reduction, but also streamlining processes and shifting to a more flexible cost base.
> People a talented and diverse workforce with the right capabilities operating in a high performance culture is critical to the successful achievement of our strategic priorities.

 

> Responsible business our commitment to enhancing the sustainability of our business by operating responsibly. Our Responsible Business Plan underpins our work and provides the framework for applying integrity and high ethical standards across all our activities.

Our performance

Within AstraZeneca, each business function is subject to an annual budget and target-setting process that includes developing financial and business forecasts, conducting sensitivity and risk analyses, and setting relevant objectives. Regular reviews are undertaken in order to monitor and assess progress against business and budget targets. During the year we also sought to manage the business appropriately, both to optimise our opportunities and to assess key risks and mitigating actions. Quarterly reports provide the SET and the Board with insight into progress against current year objectives and milestones for longer-term strategic goals. We assess performance using quantitative, comparative market, operational and financial measures, and qualitative analysis.

We have developed KPIs by which we measure our success in delivering our strategy. A description of our KPIs and how we performed against them in 2012 is shown overleaf.

Business Review

This section includes information that fulfils the requirements of a business review under the Companies Act 2006. The Strategy, Corporate Governance, Development Pipeline and Shareholder Information sections from pages 12, 106, 199, and 203, respectively, are incorporated into this section. Details of the more significant risks to AstraZeneca are set out in the Principal risks and uncertainties section from page 75. Many of our products are subject to litigation. Information about material legal proceedings can be found in Note 25 to the Financial Statements from page 184. References to prevalence of disease have been derived from a variety of sources and are not intended to be indicative of the current market or any potential market for AstraZeneca’s pharmaceutical products since, among other things, there may be no correlation between the prevalence of disease and the number of individuals who are treated for such a disease.

 

 

24   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

LOGO

 

In the remainder of this section, we review our progress in 2012 in terms of:

 

 

Key Performance Indicators

 

  P26            

 

how we performed against the indicators by which we measure our success

                 
                   
                   
                   
                   

The resources, capabilities and skills we have within the business and how we use them to ensure a focus on:

 

 

Research and Development

 

 

 

P30

 

   

 

Sales and Marketing

 

 

 

P37

   

 

Supply and Manufacturing

 

 

 

P40

 

   

 

People

 

 

 

P43

 

 

the discovery and development of innovative, differentiated and commercially attractive medicines that make a real difference to the health of patients

 

 

sales and marketing activities focused on the needs of our customers: patients, physicians and payers, and undertaken in the right way

 

 

a reliable supply and manufacturing operation that ensures our medicines are where they need to be when they are needed

 

 

a talented and diverse workforce with the right capabilities operating in a high performance culture

                   
                   

Which are supported by:

 

Intellectual Property

 

  P35    

Compliance

  P47    

Responsible Business

 

  P48      

 

a well-functioning system of intellectual property rights

 

 

employees acting with integrity

 

 

a commitment to acting responsibly and to the sustainable development of our business

   
                   
                   
                   
                   

Therapy Area Review

 

  P50    

Geographical Review

 

  P70    

Risk

  P74    

Financial Review

 

  P86

 

our chosen Therapy
Areas

 

 

the markets in which we carry out our business

 

 

the risks that might stop us from achieving our strategy and how we manage them

 

 

our finances

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   25

Table of Contents

Performance | Our performance in 2012

 

LOGO

Priority

 

     KPI      Target
LOGO Financial          

Met or exceeded targets as a result of disciplined financial management and lower Reported tax rate

     Revenue     

Sustain annual revenues of $28-$34 billion

 

    

 

Core pre-R&D operating margin

    

 

Sustain Core pre-R&D operating margins of 48%-54%

 

    

 

Core EPS

    

 

Achieve Core EPS for 2012 in the range $6.00-$6.30

 

    

 

Reinvestment rate

    

 

Reinvest 40%-50% of pre-R&D post-tax cash flows in R&D and capital investments

 

    

 

Total shareholder distribution

    

 

Provide strong cash returns to shareholders via progressive dividends and periodic share repurchases

LOGO Pipeline          

Major market approvals for  Caprelsa, FluMist Quadrivalent, Forxiga, Zinforo

     Product approvals     

One to two first major market approvals per year that support revenue target for 2014 of $2-$4 billion from recent launches, pipeline and in-licensing

 

    

 

Regulatory submissions

    

 

Major market submissions to support first approvals and line extensions for each new product, and continued marketing applications (first local authorisation and local line extensions) in additional countries to drive growth

 

 

    

 

Phase III investment decisions

    

 

 

Phase III investment decisions that support value targets for new products

 

    

 

Licensing deals/acquisitions

    

 

At least 40% of our pipeline sourced from outside our laboratories

 

 

LOGO Deliver the business          

Global revenue reduction of

15% largely as a result of loss of exclusivity on Seroquel IR . Key brands grew where we retained exclusivity

     Growth of key brands     

Drive revenue growth of key brands that retain exclusivity

 

    

 

 

Revenue from new product launches

    

 

Revenue in 2014 in the range of $2-$4 billion from recent launches, pipeline and in-licensing

 

    

 

Emerging Markets sales

    

 

25% of revenue in 2014 from Emerging Markets business

 

 

26   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

LOGO

 

2011

 

     2012      Commentary
         
         

 

$33,591 million

    

 

$27,973 million

    

 

Missed target by $27 million, primarily due to adverse exchange rates in 2012

 

 

54.2%

 

    

 

53.2%

 

    

 

Met target

 

 

$7.28

 

    

 

$6.41

 

    

 

Exceeded target

 

 

40%

 

    

 

48%

 

    

 

Met target

 

 

$2.80 dividend

 

    

 

$2.80 dividend

 

    

 

Met target. See the Financial Review from page 86 for more information

$5.6 billion net share repurchases

 

    

$2.2 billion net share repurchases

 

    
         
         

 

Brilinta approved in the US and Canada; Caprelsa approved in the US and positive CHMP opinion in the EU; 

Axanum approved in the EU;

Komboglyze approved in the EU;

Fluenz approved in the EU

 

    

 

Marketing authorisation for Caprelsa, Forxiga and Zinforo granted in the EU;  FluMist Quadrivalent approved by the FDA in the US

 

    

 

We have met our volume target and, with in-licensing, we have built a foundation for new product revenues

 

 

Nexium and Faslodex 500mg approved in Japan; dapagliflozin MAA validated by EMA; Complete Response Letter received from the FDA in the US requesting additional clinical data

 

    

 

Quadrivalent live attenuated influenza vaccine (MEDI3250) MAA submitted in September; Nexium OTC and dapagliflozin/metformin IR FDC submitted in the EU; Casodex oral tablet, Nexium Helicobacter pylori , and Arimidex Oral Dispersible Film submitted in Japan

 

    

 

On target

 

See the Research and Development section from page 30 for more information

 

Phase III trials started for NKTR-118 and initiation of Phase III programme for CAZ AVI

    

 

Lesinurad entered Phase III clinical development following the acquisition of Ardea. Positive Phase III investment decisions achieved for moxetumomab, and brodalumab

 

    

 

On target

 

6 out of 9 Phase III/Registration projects (67%) sourced externally

 

12 out of 24 Phase II projects (50%) sourced externally

 

    

 

8 out of 11 Phase III/Registration projects (73%) sourced externally

 

15 out of 25 Phase II projects (60%) sourced externally

 

    

 

Met target

         
         

 

+13% Crestor , +11% Symbicort ,

 

    

 

-4% Crestor , +5% Symbicort ,

 

    

 

On target

 

+27% Seroquel XR      +4% Seroquel XR     

Crestor overall +1% in those markets where we retained exclusivity

 

See the Intellectual Property section from page 35 and the Geographical Review from page 70 for more information

 

 

$274 million revenue from Onglyza, Vimovo, Brilinta/Brilique, Caprelsa  and Axanum

 

    

 

$633 million revenue from Onglyza, Vimovo, Brilinta/Brilique, Caprelsa, Axanum, Zinforo, Bydureon, Byetta  and Symlin

 

    

 

Meeting this target remains a challenge

 

See the Financial Review from page 86 and the Therapy Area Review from page 50 for more information

 

 

17% of revenue from Emerging Markets

 

    

 

21% of revenue from Emerging Markets

 

    

 

On target

 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   27

Table of Contents

Performance | Our performance in 2012

 

LOGO

Priority

 

     KPI      Target
LOGO Business shape

 

Met or exceeded targets with continued efficiencies across the organisation

    

 

Core gross margin

 

    

 

Maintain Core gross margin in excess of 80%

 

    

 

Core SG&A costs

 

    

 

Improve cost efficiencies and flexibility in Core SG&A costs

 

    

 

Procurement savings

 

    

 

Procurement savings across all functions

 

    

 

R&D cost efficiency

    

 

Reduced function costs across R&D to support focused R&D portfolio

 

LOGO People

 

A decrease in employee engagement in the context of a challenging business environment and the ongoing transformation of our business

    

 

Employee engagement

 

    

 

Achieve global high performing norm rating for employee engagement by 2014

 

    

 

Leadership communications

 

    

 

Further develop our leadership and management capabilities

 

    

 

Work-life balance

 

    

 

Achieve an improvement in the work-life balance of our employees

 

LOGO Responsible business

Maintained position in the World Index of the Dow Jones Sustainability Index (DJSI), as well as the elite European Index

    

 

DJSI ranking

 

    

 

Maintain position within the DJSI World Index comprising the top 10% of the largest 2,500 companies

 

    

 

Confirmed breaches of external sales and marketing codes or regulations

 

    

 

Report confirmed breaches of external codes arising from external scrutiny and voluntary disclosure by AstraZeneca

 

    

 

Number of audits conducted

 

    

 

Expand risk-based programme of responsible procurement audits, across all supplier categories and geographies

 

 

28   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

LOGO

2011

 

    

2012

 

    

Commentary

 

         
         

 

82.2%

 

    

 

81.2%

 

    

 

Met target

 

See the Financial Review from page 86 for more information

 

 

1.5% reduction in Core SG&A costs

 

    

 

12.2% reduction in Core SG&A costs

 

    

 

Met target

 

See the Financial Review from page 86 for more information

 

 

Savings of $487 million

 

    

 

Savings of $566 million

 

    

 

Exceeded target for 2012 which was $526 million

 

See the Financial Review from page 86 for more information

 

 

Achieved Core R&D efficiency savings with spend of $5 billion

 

    

 

A more variable and efficient R&D cost base achieved through accelerated strategy implementation and increased outsourcing

 

    

 

Met target

 

See the Research and Development section from page 30 for more information

 

         
         

 

84% score

 

    

 

81% score

 

    

 

Meeting this target remains a challenge

 

 

65% score

 

 

    

 

61% score

 

 

    

 

Missed target

 

 

 

67% score

 

    

 

66% score

 

    

 

Missed target

 

All percentages are the result of our global employee survey (FOCUS), percentage scores are measured on a like-for-like basis using comparable questions/categories from the 2011 FOCUS survey

 

See the People section from page 43 for more information

 

         
         

 

Top 7% of companies

 

 

    

 

Top 7% of companies

 

 

    

 

Met target

 

 

 

17 confirmed breaches of external sales and marketing regulations or codes globally

 

    

 

10 confirmed breaches of external sales and marketing regulations or codes globally

 

    

 

Met target

 

 

751 audits

 

    

 

482 audits

 

    

 

Audit programme continued. Responsible procurement assessments have been completed on suppliers who account for two-thirds of our spend

 

See the Responsible Business section from page 48 for more information

 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   29

Table of Contents

Performance | Business Review

 

LOGO

 

 4

Four major market approvals – Caprelsa, FluMist Quadrivalent, Forxiga, Zinforo

 3

Three positive Phase III investment decisions – lesinurad following the acquisition of Ardea; also moxetumomab and brodalumab

 8

Eight out of 11 Phase III/Registration projects (73%) sourced externally

 

As a research-based biopharmaceutical company, we are committed to applying innovative science and technology to invent, acquire, produce and distribute prescription medicines that make a meaningful difference to people’s health around the world. This commitment is at the core of our R&D strategy. It drives our focus to create medicines that are valued by patients and that also recognise the needs of healthcare practitioners, governments, payers and other stakeholders throughout the healthcare system.

We invest in high quality science while developing a learning-based culture which is built on high standards of leadership, ethics and transparency.

Focused R&D portfolio

We continue to prioritise our resources and focus discovery activities on those diseases within our existing Therapy Areas where we believe there is the greatest potential to meet patient need through the application of novel science. This continual process of prioritisation is designed to ensure that the projects we have in our pipeline constitute the programmes which we believe are most likely to deliver technical and commercial success.

In 2012, we continued our research focus on six Therapy Areas: Cardiovascular, Gastrointestinal, Neuroscience, Infection, Oncology and Respiratory & Inflammation. Early R&D efforts are conducted by our small molecules (Innovative Medicines) and biologics R&D groups, which are responsible for discovery and development up to and including Proof of Concept. Our Global Medicines Development (GMD) organisation progresses products through late-stage development, registration and ongoing post-launch development activities. The GMD organisation provides

 

a consistent, global platform dedicated to conducting trials for small molecules and biologics. It is accountable for delivering the regulatory packages to support launches of new medicines that have a positive benefit/ risk profile that are commercially attractive and reimbursable. In addition to our defined disease areas, we continuously assess opportunities to acquire, through purchase or partnership, development and commercialisation rights to compounds, targets and technologies.

In February 2012, as part of our accelerated R&D strategy, we created a virtual neuroscience Innovative Medicines unit (Virtual iMed) made up of a team of approximately 40 scientists conducting discovery and development externally through a network of partners in academia and industry. The team is based in our major neuroscience hubs – US (Cambridge, Massachusetts) and the UK (Cambridge) –and works closely with partners such as the Karolinska Institute in Sweden (Stockholm). The implementation of the Virtual iMed has resulted in the end of R&D activity at two sites that focused on neuroscience: in Sweden (Södertälje) and in Canada (Montreal). For more information about the Virtual iMed please see the Neuroscience section of the Therapy Area Review at page 61.

Development pipeline

Our pipeline includes 84 projects of which 71 are in the clinical phase of development. As shown in the Development projects chart below, we now have a total of 29 projects in Phase I, 25 projects in Phase II, 11 projects in late-stage development, either in Phase III or under regulatory review, and we are running 19 significant life-cycle management projects.

 

 

30   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

 

LOGO

 

Development projects

During 2012, across the clinical portfolio, 36 projects successfully progressed to their next phase (including 12 projects entering first human testing). The Pipeline delivery table overleaf summarises the milestones for products in development passed in 2012. Ten projects have successfully completed development activities and have now been launched in all relevant major markets. Nineteen projects were withdrawn in 2012. One project was withdrawn following failure to obtain the required regulatory or marketing approvals for the product candidate or the facilities in which it is manufactured and 17 projects were withdrawn following poorer than anticipated safety or efficacy results. One project was withdrawn due to the anticipated completion of the collaboration which supported that project. For more information about our pipeline, including discontinued and completed projects, see the Therapy Area Review and Development Pipeline section from page 50 and page 199 respectively. For information about the risks inherent in the clinical phase of development, please see the Principal risks and uncertainties section from page 75.

Portfolio quality

Our focus continues to be on identifying key candidate medicines that have the highest potential to deliver technical and commercial success. This includes an annual assessment of our early portfolio projects. By continuing to apply a rigorous quality approach to our candidate selection process, we expect to increase the likelihood that our most promising medicines progress into Phase III development. Our quality approach focuses on ensuring that every project in our pipeline has been assessed against a valid biological target, has sufficient exposure to demonstrate an effect on the disease, and has a strong efficacy and safety profile in the intended patient population.

Our Portfolio Investment Board (PIB) plays an important role in maintaining portfolio quality. It continuously evaluates our projects with the goal of maximising the value of our R&D investments. More detail relating to the PIB’s responsibilities can be found in the Corporate Governance Report on page 119.

For more information about our pipeline, including discontinued and completed projects, see the Development Pipeline section from page 199.

Our R&D approach

As demonstrated by the Life-cycle of a medicine diagram on page 14, our R&D activities span the entire life-cycle of a medicine. Our approach brings together drug discoverers and developers within each Therapy Area to focus and collaborate in specific disease areas, while continuing to leverage our expertise in late-stage development, product registration and life-cycle management. This model is designed to promote accountability and scientific knowledge-sharing within therapeutic areas. In addition, our R&D strategy enables more effective and efficient delivery of our research objectives across the therapeutic portfolio, regardless of geography, disease area or stage of development.

Partnering to improve health

We know that we cannot address the challenges of healthcare alone and scientific innovation does not exist solely within our own research laboratories. By engaging with partners across the healthcare delivery spectrum, we can stimulate more creativity and better develop medicines and solutions for patients. Our collaboration efforts have resulted in a combination of internally and externally sourced compounds throughout our portfolio, which include development partnerships with biotechnology firms, research institutions and other pharmaceutical companies. We aim to source at least 40% of our pipeline from outside our laboratories and we continued to deliver against this KPI in 2012 with external partnerships positively impacting our pipeline including:

 

> A collaboration with Amgen to jointly develop and commercialise five monoclonal antibodies from Amgen’s clinical inflammation portfolio including brodalumab.
> The acquisition of Ardea and their Phase III development product candidate, lesinurad, as a potential treatment for the chronic management of hyperuricaemia in patients with gout.
> An expansion of the diabetes alliance with BMS in connection with BMS’s acquisition of Amylin and the potential development and commercialisation of Amylin’s portfolio of products related to diabetes and other metabolic diseases, with a primary focus on a franchise of glucagon-like peptide 1 agonists (GLP-1 agonists) for the treatment of Type 2 diabetes. This includes Byetta (exenatide injection) and Bydureon (exenatide extended release for injectable suspension), both of which are approved for use in the US, Europe and Japan, and Symlin (pramlintide acetate), an injected amylin analogue, which is approved in the US.
> An innovative research alliance that brings four leading academic research laboratories together with AstraZeneca to study a major risk factor for Alzheimer’s disease, the apolipoprotein E4 genotype (ApoE).
> The acquisition of a portfolio of neuroscience assets from Link Medicine Corporation, a privately held biopharmaceutical company developing potential new treatments for a range of neurodegenerative diseases.
> A collaboration with the diagnostics division of Roche to develop companion diagnostics for selected products in development across all AstraZeneca Therapy Areas.
> A worldwide exclusive licensing agreement with Ardelyx in respect of their NHE3 inhibitor programme for the treatment of complications associated with end-stage renal disease (ESRD) and chronic kidney disease (CKD).
> A collaboration with Ironwood to co-develop and co-commercialise linaclotide in China. Linaclotide is a guanylate cyclase-C (GC-C) agonist for the treatment of irritable bowel syndrome with constipation (IBS-C) and chronic idiopathic constipation (CIC).
> A collaboration in China with WuXi AppTec to develop and commercialise MEDI5117, a biologic for autoimmune and inflammatory diseases.
 

 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   31

Table of Contents

Performance | Business Review

 

LOGO

Pipeline delivery

 

Milestone

   Product    2012 Achievement
Key pipeline progressions (Phase III starts and first regulatory filings)    Brodalumab    Phase III programme has commenced for brodalumab in psoriasis.
Major market approvals    Zinforo (ceftaroline fosamil)   

European marketing authorisation for Zinforo , a new intravenous cephalosporin antibiotic, for the treatment of adult patients with complicated skin and soft tissue infections (CSSTI) or community acquired pneumonia (CAP).

 

  

 

   Caprelsa (vandetanib)   

European marketing authorisation for Caprelsa for the treatment of aggressive and symptomatic medullary thyroid cancer (MTC) in patients with unresectable locally advanced or metastatic disease. Caprelsa is the first approved treatment for advanced MTC in Europe.

 

  

 

   FluMist Quadrivalent (influenza vaccine live, intra-nasal)   

FDA approval for FluMist Quadrivalent in the prevention of influenza. This marks the first four-strain influenza vaccine approved by the FDA.

 

  

 

     Forxiga (dapagliflozin)   

European marketing authorisation for Forxiga tablets for the treatment of Type 2 diabetes, as an adjunct to diet and exercise, in combination with other glucose-lowering medicinal products including insulin, and as a monotherapy in metformin intolerant patients.

 

 

> A collaboration with the Cancer Research Institute and the Ludwig Institute for Cancer Research to advance the research of immunotherapy in cancer. Specifically, the research will focus on clinical trials to test novel combinations of immunotherapies, including three investigational MAbs.
> A strategic alliance with Isis Pharmaceuticals, Inc. (Isis) for the discovery and development of novel generation antisense therapeutics against five cancer targets, which includes a licence to develop and commercialise ISIS-STAT3 RX , a drug Isis is currently evaluating in an early clinical trial in patients with advanced lymphomas.

We continue to search for opportunities to advance science and public health through research collaborations and partnerships. Initiatives that we announced in 2012 include the following:

 

> A collaboration with other pharmaceutical and biotechnology companies working alongside public partners in the NewDrugs4BadBugs research programme (part of the European Commission’s Action Plan Against the Rising Threats from Antimicrobial Resistance) which is intended to boost the current industry-wide faltering discovery and development of new antibiotics.
> A collaboration along with six other pharmaceutical companies and four research institutions, working with the Bill & Melinda Gates Foundation, with

a goal to speed the discovery of essential new treatments for tuberculosis (TB).

> Formation of a non-profit organisation called TransCelerate BioPharma Inc., along with nine other major pharmaceutical companies, to accelerate the development of new medicines by solving common challenges (initially) related to clinical study execution.
> Continued activities to meet our commitment to health research through our ongoing efforts with organisations such as the European Innovative Medicines Initiative aimed at improving tools, technologies and methodologies. We have actively shared knowledge through collaborations with the UK Medical Research Council and the World Intellectual Property Organisation (WIPO) for Neglected Tropical Diseases (NTDs). More information concerning NTDs can be found in the Therapy Area Review in the Infection section on page 58.

Investing in capabilities

A component of our R&D strategy is strengthening four core capabilities. In 2010, we announced an investment of more than $200 million over five years to develop capabilities in the areas of payer partnering, personalised healthcare, predictive science and clinical design. We have made significant progress in building these skills both internally and through external collaborations, and they are now fully integrated into most of our development programmes.

Our resources

At the end of 2012, our R&D organisation comprised approximately 9,800 people at 10 principal centres in six countries. In February 2012, we announced an acceleration of our R&D transformation originally announced in 2010. This included initiatives to cease R&D activities at our site in Sweden (Södertälje), and close our laboratories in Canada (Montreal), France (Reims) and the US (Mountain View, California) in 2012. These initiatives have impacted a total of approximately 2,200 positions across the R&D organisation.

Our approach to implementing such change is outlined in the Managing change in our organisation section on page 45. Further details are also set out in the Our strategy section from page 20.

Our current R&D geographic footprint includes four main small molecule facilities in: the UK (Alderley Park and Macclesfield); Sweden (MöIndal); and the US (Waltham, Massachusetts). We also have a clinical development facility in Japan (Osaka). Our principal sites for biologics and vaccines are in the US (Gaithersburg, Maryland) and in the UK (Cambridge). Our Wilmington, Delaware site in the US focuses on late-stage development across the entire therapeutic portfolio. Our strategic expansion in Emerging Markets continues and includes the ongoing growth of our research facilities in China (Shanghai) and India (Bangalore).

 

 

32   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

LOGO

In 2012, there was Core R&D expenditure of $4.5 billion in our R&D organisation (2011: $5 billion; 2010: $4.2 billion). In addition, $5,228 million was spent on acquiring product rights (such as in-licensing) (2011: $189 million; 2010: $1,017 million) and we invested approximately $791 million on the implementation of our R&D restructuring strategy. The allocations of spend by early development and late-stage activities are presented in the R&D spend analysis table opposite.

R&D ethics

We want to be recognised for our high quality science and for the impact we can make on serious diseases, and to be trusted for the way we work. Our standards of R&D ethics are global and apply to all AstraZeneca research activity, in all locations, whether conducted by us or on our behalf by third parties.

Clinical trials

Our commitment: to deliver consistently high standards of ethical practice and scientific conduct in all our trials worldwide and to public transparency on registration and results of all clinical trials, whether positive or negative.

Our objective: to be recognised as an industry leader in the publication and sharing of clinical trial information.

We conduct clinical trials at multiple sites in several different countries/regions as shown in the chart above. A broad geographic span helps us to ensure that those taking part in our studies reflect the diversity of patients around the world for whom the new medicine is intended. This approach also helps to identify the types of people for whom the treatment may be most beneficial.

Our global governance process for determining where we place clinical trials provides the framework for ensuring a consistent approach worldwide. We take several factors into account, including the availability of experienced and independent ethics committees and a robust regulatory regime, as well as sufficient numbers of trained healthcare professionals and patients willing to participate in a trial.

Before a trial begins, we work to make sure that those taking part understand the nature and purpose of the research and that proper procedure for gaining informed consent is followed (including managing any special circumstances, such as different levels of literacy). Protecting participants throughout the trial process is a core priority and we have strict procedures in place to ensure that they are not exposed to any unnecessary risks.

All our clinical studies are conceptually designed and finally interpreted in-house but a percentage of them are run for us by contract research organisations (CROs). In 2012, around 31% of patients in our small molecule studies and around 87% of patients in our biologics studies were monitored by CROs on our behalf. We contractually require CROs to work to our global standards and we conduct risk-based audits to monitor compliance.

Animal research

Our commitment: to embrace, promote and embed scientific and technical best practice in animal research.

Our objective : to drive continuous improvement internally and engage with external providers on the implementation of AstraZeneca global standards for non-human primate housing and care. These include the following targets:

 

> roll-out of AstraZeneca Good Statistical Practice (GSP) global standard and associated compliance monitoring
> more than 80% of external providers of AstraZeneca non-human primate research studies are operating to AstraZeneca standards.

We remain committed to minimising our use of animals in our research without compromising the quality of the research data. Wherever possible, we use non-animal methods, such as computer modelling, that eliminate the need to use animals early in drug development or reduce the number required. We also work to refine our existing methods. This replacement, reduction and refinement of animal studies is known as ‘the 3Rs’. To support our drive for

continuous improvement, we work both within AstraZeneca and the wider scientific community to share the 3Rs knowledge and learning.

The number of animals we use will continue to vary because it depends on a number of factors, including the amount of pre-clinical research we are doing, the complexity of the diseases under investigation and regulatory requirements. We believe that, without our active commitment to the 3Rs, our animal use would be much greater. In 2012, we used approximately 304,000 animals in-house (2011: 381,000). In addition, approximately 14,000 animals were used by external CROs on our behalf (2011: 17,000). Against our 2012 target of more than 80%, 85% of our externally-placed non-human primate studies met AstraZeneca standards in 2012. We will continue to progress towards our 2013 target of 100% of our studies being conducted in facilities meeting AstraZeneca required standards.

The welfare of the animals we use continues to be a top priority and our Bioethics Policy applies worldwide. We routinely have inspections by government authorities of our internal animal research facilities. External CROs that conduct animal studies on our behalf are required to comply with our global standards and we undertake audits to ensure our expectations are being met.

During 2012, we developed, launched and began implementation of standard operating procedures and guidance documents to underpin our new GSP global standard, developed in 2011. These apply to our internal animal research and the launch included extensive training programmes for relevant scientists, technical staff and managers across the organisation.

 

Extract from 2012 Responsible Business Plan.

 

   Further information on AstraZeneca’s approach to responsible business can be found in the Responsible Business section from page 48 and on our website, astrazeneca.com/responsibility.
 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   33

Table of Contents

Performance | Business Review

 

LOGO

 

Patient safety

Our commitment: the safety of the patients who take our medicines is of fundamental importance to us.

Our objective: to enhance pharmacovigilance awareness – including the use of collaborative programmes to share and use our knowledge and best practice in order to improve reporting and patient safety in developing countries.

All drugs have potential side effects and we aim to minimise the risks and maximise the benefits of each of our medicines throughout the whole life-cycle of a medicine. We continually monitor the use of all our medicines to ensure that we become aware of any side effects not identified during the development process. This is known as pharmacovigilance and is core to our ongoing responsibility to patients. We have comprehensive and rigorous systems in place for detecting and rapidly evaluating such effects,

including mechanisms for highlighting those that require immediate attention. We also work to ensure that accurate, well-informed and up-to-date information concerning the safety profile of our drugs is provided to regulators, doctors, other healthcare professionals and, where appropriate, patients.

A pharmacovigilance awareness programme was developed in 2012 and circulated to marketing companies, together with guidance about how the information should be shared with regulatory authorities in readiness for external enquiry. One such opportunity arose when SFDA (the Chinese health authority) met UMC (WHO Uppsala Monitoring Centre) and we were able to share our experience and thoughts around signal management.

We have an experienced, in-house team of clinical patient safety professionals dedicated to the task of ensuring that we meet our commitment to patient safety.

At a global level, every medicine in development and on the market is allocated a Global Safety Physician and a team of patient safety scientists. In each of our markets we also have dedicated safety managers with responsibility for patient safety at a local level.

Our Chief Medical Officer has overall accountability for the benefit/risk profiles of the products we have in development and those on the market. He provides medical oversight and ensures that appropriate risk assessment processes are in place to enable informed decisions to be made about safety as quickly as possible.

 

Extract from 2012 Responsible Business Plan.

 

   Further information on AstraZeneca’s approach to responsible business can be found in the Responsible Business section from page 48 and on our website, astrazeneca.com/responsibility.
 

 

Clinical trial transparency

AstraZeneca has a long-standing commitment to making information about our clinical research publicly available to enhance the scientific understanding of how our medicines work and in the medical interest of patients. By the end of 2012, we had registered 2,050 clinical trials and posted the results of 1,360 trials on a range of public websites including our own dedicated clinical trials website, astrazenecaclinicaltrials.com.

We publish information on the registration and results of all new and ongoing AstraZeneca-sponsored clinical trials for all products in all phases, including marketed medicines, drugs in development and drugs whose further development has been discontinued. We post results, irrespective of whether they are favourable or unfavourable to AstraZeneca.

 

 

> Our disclosure policy goes beyond legal requirements, which currently require publication for Phase II studies onwards only.
> From 15 January 2013, we are voluntarily disclosing the research protocol for our clinical trials on astrazenecaclinicaltrials.com once a manuscript relating to an investigational or approved product is published in a peer-reviewed medical journal.

These disclosure requirements are set out in our Bioethics Policy and compliance is mandatory across the Group.

We consider requests for patient-level data from other parties on a case-by-case basis, following consistent criteria to establish if, and how, the information provided will be used for valid scientific purposes and to benefit patients.

 

Calls for ‘open access’ to clinical data raise complex practical, legal and ethical issues around full disclosure of patient information. Decision makers, as well as academia and industry, have a duty to consider all the implications that could arise from such proposals. These include ensuring scientific rigour, safeguarding patient privacy and protecting innovation and medical progress. We are engaging with regulators, legislators, industry, and medical and scientific bodies to discuss the issues raised by the proposals to routinely publish full clinical trial and patient data so we can collectively identify practicable solutions that deliver real benefits to medical science and patients.

 

 

34   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

LOGO

“A period of patent protection is essential in allowing us to achieve a return on our investment in innovation. Our challenge is to refresh our portfolio of patented products and offset the impact when that protection is lost.”

Jeff Pott General Counsel

 

The discovery and development of a new medicine requires a significant investment of resources by research-based pharmaceutical companies over a period of 10 or more years. For this to be a viable investment, the results, new medicines, must be safeguarded from being copied with a reasonable amount of certainty for a reasonable period of time.

The principal economic safeguard in our industry is a well-functioning patent system that recognises our effort and rewards our innovation with appropriate protection, allowing time to generate the revenue we need to reinvest in new pharmaceutical innovation. Patent rights are limited by territory and duration, yet a significant period of this time can be spent on R&D of our products before product launch. Therefore, we commit significant resources to establishing and defending our patent and related IP protections for these inventions.

Patent process

We file applications for patent protection for our inventions to safeguard the large subsequent investment required to obtain approval of potential new drugs for marketing. Further innovation means that we may seek additional patent protection as we develop a product and its uses. We apply for patents via patent offices around the world which assess whether our inventions meet the strict legal requirements for a patent to be granted. In some countries, our competitors can challenge our patents in the patent offices, and, in all countries, competitors can challenge our patents in the courts. We can face challenges early in the patent application process and throughout the life of the patent. These challenges can

be to the validity of a patent and/or to the effective scope of a patent and are based on ever-evolving legal precedents. There can be no guarantee of success for either party in patent proceedings. For information about third party challenges to the patents protecting our products, see Note 25 to the Financial Statements from page 184.

The basic term of a patent is typically 20 years from the filing of the patent application with the relevant government patent office. However, the product protected by a pharmaceutical patent may not be marketed for several years after patent filing due to the time required for clinical trials and the regulatory approval process necessary to obtain marketing approval for the product. Patent Term Extensions (PTE) are available in certain major markets including the EU and US to compensate for these delays. The term of the PTE can vary from zero to five years depending on the time taken to obtain any marketing approval. The maximum patent term, when including PTE, cannot exceed 15 years (EU) or 14 years (US) from the first marketing authorisation.

The generic industry is increasingly challenging innovators’ patents at earlier stages and almost all leading pharmaceutical products in the US have faced or are facing patent challenges from generic manufacturers. The result of patent challenges experienced by our competitors’ products may lead to the availability of generics in the same product class as patented products we currently supply, which may materially impact our business. We are also experiencing increased challenges elsewhere in the world, for example in Europe, Canada, Asia and Latin America. Further information about

the risks relating to patent litigation and early loss and expiry of patents is contained in the Principal risks and uncertainties section from page 75.

Patent expiries

The tables overleaf set out certain patent expiry dates and sales for our key marketed products. The expiry dates relate to the basic substance patent relevant to that product unless indicated otherwise. The expiry dates shown include any PTE and Paediatric Exclusivity periods.

Data exclusivity

In addition to patent protection, Regulatory Data Protection (RDP or ‘data exclusivity’) is an important IP right which arises in respect of data which is required to be submitted to regulatory authorities in order to obtain marketing approvals for our medicines. Significant investment is required to generate such data (for example, through conducting global clinical trials) and the use of this proprietary data is protected from use by third parties (such as generic manufacturers) for a number of years in a limited number of countries. The period of such protection and the extent to which the right is respected differs significantly between these countries. We believe in enforcing our rights to RDP and consider it an important protection for our products, particularly as patent rights are increasingly being challenged.

The period of RDP starts from the date of the first marketing approval from the relevant health authority and runs in parallel to any pending patent protection. RDP would generally be expected to expire prior to patent expiry in all major markets. If a product takes an unusually long time

 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   35

Table of Contents

Performance | Business Review

 

LOGO

 

to secure marketing approval or if patent protection has not been secured, has expired or has been lost, then RDP may be the sole IP right protecting a product from copying, as generics should not be allowed to rely on AstraZeneca’s data to support the generic product’s approval or marketing until the RDP right has expired.

Compulsory licensing

Compulsory licensing (the over-ruling of patent rights to allow patented medicines to be manufactured and sold by other parties) is increasingly being included in the access to medicines debate. We recognise the right of developing countries to use the flexibilities in the World Trade Organization’s Agreement on Trade-Related Aspects of

Intellectual Property Rights (TRIPS) (including the Doha amendment) in certain circumstances, such as a public health emergency. We believe that this should apply only when all other ways of meeting the emergency needs have been considered and where healthcare frameworks and safeguards are in place to ensure that the medicines reach those who need them.

 

 

Patent expiries for our key marketed products

 

             

US revenue ($m)

 

Key marketed products *#

  

US patent expiry

  

             2012

    

        2011

    

          2010

 

Atacand

   Expired          150         182         216   

Crestor

   2016          3,164         3,074         2,640   

Losec/Prilosec

   Expired          30         38         47   

Nexium

   2015 1          2,272         2,397         2,695   

Pulmicort

   2019 2   (Respules)      233         279         305   
   2018   ( Turbuhaler formulation)         
     2019   ( Turbuhaler device)                           

Seloken/Toprol-XL

   Expired          320         404         689   

Seroquel IR

   Expired          697         3,344         3,107   

Seroquel XR

   2017   (formulation) 3      811         779         640   

Symbicort

   2014   (combination), 2023 (formulation), 2026 (pMDI device)      1,003         846         721   

Synagis

   2015   (composition), 2023 (formulation)      611         570         646   

Zoladex

   2021   (safety syringe)      24         39         46   

 

                   

EU, Canada and Japan revenue  ($m) 4

 

Key marketed products *#

   EU patent expiry 5    Canadian patent expiry    Japanese patent expiry                2012              2011                2010  

Atacand

   Expired    Expired    n/a      463         799         837   

Crestor 6

   2017 7    Expired    2017      2,090         2,534         2,201   

Losec/Prilosec

   Expired    Expired    Expired      484         660         660   

Nexium

   2014    2014    2018 8      648         1,042         1,422   

Pulmicort

   2018 ( Respules )    2018 ( Respules )    2018 ( Respules )      300         344         353   
     2018 ( Turbuhaler formulation)    2018 ( Turbuhaler formulation)    2018 ( Turbuhaler formulation)                           

Seloken/Toprol-XL

   Expired    Expired    Expired      139         163         169   

Seroquel IR

   Expired    Expired    Expired      357         651         705   

Seroquel XR

   2017 (formulation) 9    2017 (formulation)    n/a      527         562         401   

Symbicort

   2018 (formulation)    2018 (formulation)    2017 (combination)      1,728         1,822         1,621   
   2019 ( Turbuhaler device)    2019 ( Turbuhaler device)    2018 (formulation)         
               2019 ( Turbuhaler device)                           

Synagis

   2015 (composition)    2015 (composition)    2015 (composition)      427         405         392   

Zoladex

   2021 (safety syringe)    2021 (safety syringe)    2021 (safety syringe)      638         733         718   

 

*   Patents are or may be challenged by third parties. Generic products may be launched ‘at risk’ and our patents may be revoked, circumvented or found not to be infringed. See the Principal risks and uncertainties section from page 75. Many of our products are subject to challenges by third parties. Details of material challenges by third parties can be found in Note 25 to the Financial Statements from page 184.
#   Additional patents relating to the stated products may have terms extending beyond the quoted dates.
1   Licence agreements with Teva and Ranbaxy Pharmaceuticals Inc. allow each to launch a generic version in the US from May 2014, subject to regulatory approval.
2   Date includes Paediatric Exclusivity. A licence agreement with Teva permits their ongoing sale in the US of a generic version from December 2009.
3   Licence agreements with various generics companies allow launches of generic versions of Seroquel XR in the US from 1 November 2016 or earlier upon certain circumstances, subject to regulatory approval.
4   Aggregate revenue for the EU, Canada and Japan.
5   Expiry in major EU markets.
6   Crestor is covered by a range of patents, including substance, formulation and use patents. Crestor patent coverage is not uniform across countries. Granted PTEs mean that a Crestor substance patent remains in force in several major markets after the standard patent term expired in 2012. However, this substance patent is not in force in a number of countries, such as Australia, Brazil, Mexico, Russia and China.
7   A substance patent and PTE with expiry in 2017 is in force in most major EU markets.
8   Includes PTE. Re-examination period (similar to data exclusivity) ends July 2019.
9   AstraZeneca is engaged in numerous patent revocation proceedings regarding Seroquel XR patents and further adverse court rulings, in addition to those seen in Germany and the UK, are possible.

 

36   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

 

LOGO

 

$4.5bn

Some $4.5 billion of revenue decline was related to loss of exclusivity on several brands in the portfolio, with the largest impact from Seroquel IR

$600m

Symbicort , Faslodex , Onglyza , Iressa , Brilinta/Brilique and Seroquel XR accounted for more than $600 million revenue growth

4%

Emerging Markets revenue rose by 4% and included 17% revenue growth in China, offset by weak performance in Mexico, Brazil, Turkey and India

 

 

 

If we are to improve the health of patients around the world, we need to ensure that the right medicines are available and help improve access to them. To that end, our global sales and marketing organisation is active in over 100 countries. At the end of 2012, it comprised approximately 30,200 employees. As well as building on our leading positions in commercialising our medicines in the US and Other Established Markets, we continue to increase our ability to serve customers in Emerging Markets including China, Brazil, Mexico and Russia.

We work to ensure success in serving customers in individual markets by having highly accountable local leaders who understand their markets and have a strong focus on business growth. This extensive network is supported by our Global Sales and Marketing Organisation that develops global product strategies and drives commercial excellence, ensuring a strong customer focus and commercial direction in the management of our pipeline and marketed products. All our efforts are underpinned by a commitment to conducting our sales and marketing activity in accordance with our values and driving commercial success responsibly.

Driving commercial success

Driving commercial success requires us to maximise the value of our portfolio across the whole life-cycle of a medicine. We do so by connecting our science with our customers’ needs. From an early stage in the medicine discovery process we embed customer insights into our R&D strategy based on our interactions with healthcare providers, patients, regulators and payers. We build on this with our local market expertise and knowledge. This approach helps us to prioritise resources

and optimise our portfolio, thereby delivering medicines that customers value and which meet their needs.

For an overview of this process, see the Life-cycle of a medicine diagram on page 14.

Activities in 2012 focused on ensuring continued commercial excellence of key products in our established patented portfolio, such as Crestor, Seroquel XR and Symbicort , driving growth in developing markets and accelerating the commercialisation of recently launched products. Brilinta/Brilique has now been approved for use in hospitalised ACS patients in 88 countries, is reimbursed in 29, available in 33 patient pay markets and commercially launched in 82. Other recently launched products include Caprelsa, Zinforo and Forxiga . In the US, we also started promotion of Bydureon , Byetta and Symlin , the Amylin diabetes products that are part of our expanded diabetes alliance with BMS.

Working in partnership

Our commitment to collaboration is outlined in the Partnering to improve health section from page 31. This approach is further evidenced by our global collaboration agreement, announced in April 2012, with The Medicines Company, which has a strong network in interventional cardiology. In May, their salesforce began supporting Brilinta in the US, complementing our own efforts.

In August, we entered into an agreement with Pfizer pursuant to which Pfizer acquired the exclusive global rights to market Nexium for approved OTC indications. We will continue to manufacture and market the prescription product, as well as supply Pfizer with the OTC product.

 

 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   37

Table of Contents

Performance | Business Review

 

LOGO

 

Global strategies tailored to meet local needs

We focus on developing global strategies tailored to meet local needs and recognise that our commercial capabilities must evolve to meet future market requirements. The pace and degree of change in global economies and intensifying regulatory and access challenges have led us to look at ways of better and more efficiently addressing the changing needs and preferences of payers, prescribers and patients. In 2012, this effort included completing the regional consolidation of our Commercial organisation announced in 2011. Our streamlined operating model includes integrating our smaller local marketing companies into area clusters, allowing them to benefit from global resources while staying local and concentrating on meeting local customer needs.

All our markets have a role to play in delivering our commercial strategy. We continue to prioritise investment and allocate our resources in the most cost-effective way. This allows us to identify those markets of major significance to us, those that will become more important drivers of our business in the future and highlight those Established Markets where we need to refocus our approach to deliver sustained success. Our footprint continues to evolve to reflect declining sales in Established Markets and increasing sales in Emerging Markets. For example, in 2012 we enhanced our presence in Asia with the opening of the Zhangjiang Park Regional Hub Headquarters in Shanghai.

Changing customer needs

In most countries, our sales are made through wholly-owned local marketing companies. In other countries, we sell through distributors or local representative offices. Our products are marketed primarily to primary care and specialist doctors. Our efforts are directed towards explaining the therapeutic as well as the economic benefits of our products to doctors, governments and others who pay for healthcare.

Historically, our commercial model has been based on the use of face-to-face marketing techniques. This is now changing to reflect the changing profile of the prescribers of our medicines. For example, primary care physicians tend to be younger on average than previously, a greater proportion is female, and more work part-time. Primary care physicians want to interact with pharmaceutical companies in different ways. Driven by experience from innovative approaches piloted and implemented in North America and Europe, we have changed the way we work. Improvements include the introduction of office-based sales teams, which include physicians and dedicated customer service staff, and expanded use of digital channels. These selling channels have now been rolled out in more than 30 countries and across a range of products. Evidence to date suggests these channels are appreciated by those who use them and are an efficient and effective way of driving value for our business. We are accelerating the roll-out and adoption of the new model in the majority of markets in which we operate.

Pricing our medicines

Our challenge is to deliver innovative medicines that improve health for patients, bring benefits to society and provide an appropriate return on our investment. Our global pricing policy provides the framework to ensure appropriate patient access while optimising the profitability of all our products in a sustainable way. When setting the price of a medicine, we take into consideration its full value to patients, to those who pay for healthcare and to society in general. We also pursue a flexible approach to the pricing of our medicines. For example, we support the concept of differential pricing, provided that appropriate safeguards are in place to ensure that differentially priced products are not diverted from patients who need them to be sold and used in more affluent markets.

Delivering value for payers

Our medicines play an important role in treating unmet medical need. In doing so, they bring economic as well as therapeutic benefits. Effective treatments can help to lower healthcare costs by reducing the need for more expensive care, such as hospital stays or surgery, or through preventing patients from developing more serious or debilitating diseases that are costly to treat. They also contribute to increased productivity by reducing or preventing the incidence of diseases that keep people away from work.

As outlined in the Pricing pressure section on page 18, there is continued downward pressure on drug pricing and, in the current difficult economic environment, payers expect us to be able to define the value our medicines create. We are acutely aware of the challenges facing those who pay for healthcare and are committed to delivering value, which will allow us to bring our medicines to the patients that need them. Therefore, we work with payers and healthcare providers to understand their priorities and requirements and generate evidence regarding how our products offer value and support cost-effective healthcare delivery.

Increasing access to healthcare

Our commitment: to increase access to healthcare for under-served patient populations in a sustainable way.

Our objective: to roll-out our access to healthcare strategy within the business and further develop the framework for implementation, including non-financial performance indicators for monitoring our performance across all our initiatives.

Sales of medicines in our Established Markets enable us to generate the revenue we need to provide our shareholders with a return, invest in continued innovation and pursue other opportunities to expand the availability of our medicines. Increasing that availability and increasing access to healthcare for under-served patient

 

 

38   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

 

LOGO

 

populations in a sustainable way is a significant global challenge and, in March 2012, we announced our access to healthcare strategy to help in that process. The strategy framework is explained on our website, astrazeneca.com/responsibility. It seeks to take account of the different barriers to healthcare around the world and is tailored locally to meet the needs of different patient populations. We are pursuing a range of initiatives, including broadening affordability of our medicines, across these populations to understand what works best and in what context.

During the year, we rolled out our access to healthcare framework within our Global Sales and Marketing Organisation to support further development of our existing approach and to enable us to capture ongoing ‘broadening affordability’ commercial initiatives. For example, our work to expand patient access to healthcare in countries such as Brazil, Romania and Ukraine continues with a range of different commercial approaches being adopted. In China, we are pursuing our strategy to reach patients in the broader market, beyond the big hospitals in the big cities, by developing new commercial channels for reaching emerging hospitals and community health centres. Best practice will be shared and replicated. In addition, in 2012, we acquired Guangdong BeiKang Pharmaceutical Company Limited, a generics manufacturing company in China which gave us access to a portfolio of injectable medicines used to treat infections. First launches are planned for 2013 and underscore our intention to serve the health needs of Chinese patients through our innovative medicines and, increasingly, high quality branded generic treatments that are locally produced to global standards. You can read more about our strategy and the access initiatives we have under way on our website, astrazeneca.com.

We are making progress on the development of non-financial indicators for monitoring our performance and these are included in our 2013 Responsible Business Plan.

Sales and marketing ethics

Our commitment: to deliver consistently high ethical standards of sales and marketing practice worldwide.

Our objective: to focus on ensuring compliance with our Ethical Interactions Policy and report on the:

 

> number of confirmed breaches of external sales and marketing codes
> number of instances of failure to meet our standards in the Global Commercial Organisation, including contract staff
> number of corrective actions for breaches of our Code of Conduct or supporting policies by Commercial employees, including contract staff.

During 2012, we continued to provide training for employees on our global standards that govern the way that we conduct our business around the world. We have comprehensive processes in place for monitoring compliance with our Code of Conduct and global policies, including dedicated compliance professionals who support our line managers locally in monitoring their staff activities. We also have a network of nominated signatories who review our promotional materials against all applicable requirements. Additionally, in 2012, audit professionals have conducted compliance audits of a selection of our marketing companies.

As shown in the Global KPI: Disciplinary actions chart opposite, we identified a total of 10 confirmed breaches of external sales and marketing regulations or codes globally in 2012 (17 in 2011). There were 1,932 instances, including contract staff, of failure to comply with AstraZeneca’s Code of Conduct and global policies in our Global Commercial Organisation, the majority of which were minor (1,292 in 2011, including external breaches). We believe that the movement in both numbers reflects our enhanced management oversight and compliance monitoring.

As shown in the Corrective actions table above, in relation to these breaches (and it is important to note that a single breach can involve more than one person failing to meet the standards required), we removed 188 people from their role, formally warned 685 people and provided further guidance or coaching on our policies for 1,808 people. The most serious breaches are raised with the Audit Committee.

US Corporate Integrity Agreement reporting

In April 2010, AstraZeneca signed an agreement with the US Department of Justice to settle an investigation relating to the sales and marketing of Seroquel IR . The requirements of the associated Corporate Integrity Agreement between AstraZeneca and the Office of the Inspector General of the US Department of Health and Human Services (OIG) include a number of active monitoring and self-reporting obligations that differ from self-reporting required by authorities in the rest of the world. To meet these obligations, AstraZeneca provides notices to the OIG describing the outcomes of particular investigations potentially relating to violations of certain laws, as well as a separate annual report to the OIG summarising monitoring and investigation outcomes relevant to Corporate Integrity Agreement requirements.

 

Extract from 2012 Responsible Business Plan.

 

   Further information on AstraZeneca’s approach to responsible business can be found in the Responsible Business section from page 48 and on our website, astrazeneca.com/responsibility.
 

 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   39

Table of Contents

Performance | Business Review

 

LOGO

 

81.2%

Sustained Core gross margin in excess of 80%

$566m

Procurement savings of $566 million, representing a 7% reduction

$417m

Capital investment of $417 million in supply and manufacturing facilities

 

 

 

 

Our strategy is to balance innovative and efficient in-house manufacturing capabilities with external manufacturing resources, particularly in relation to the early stages of our production process. Where efficiencies can be achieved, we continue to consider using outsourced production but our strategy is to retain the final stages of the production cycle in-house. This balance is designed to give us product integrity and quality assurance while affording us cost efficiency and volume flexibility.

We progressed two key production facilities during 2012 in China (Taizhou) and Russia (Vorsino), which will enable us to supply our products to both markets locally. These sites are intended to commence phased commercial production in 2014. The work is led by our global engineering group who put a strong focus on carrying out these projects fully in line with our ethical and safety standards. This work was recognised externally in 2012 with the Shell health, safety, security and environment (HSSE) award for embedding an HSSE culture in our Emerging Markets projects.

Product quality and supply chain

We are committed to delivering product quality that underpins the safety and efficacy of our medicines. We have a comprehensive quality management system in place designed to assure the quality of our products in compliance with relevant regulations.

Notwithstanding our efforts, during 2012 we experienced disruptions to our supply chain resulting from the implementation in February 2012 of an enterprise resource planning IT system in our facilities in Sweden (Södertälje and Gärtuna). This change was

necessary, due to the legacy systems reaching the end of their life-cycle. At launch the implementation encountered some unexpected difficulties and we put in place a team with representatives from different parts of the organisation to manage the situation so that impact on patients would be minimised and markets were kept informed. The underlying problems have now been resolved and production levels returned to normal in September. We estimate that the negative revenue impact for the year resulting from this disruption was approximately 1%.

Supply from our site in India (Bangalore) was also disrupted for a period of time following a voluntary recall of products that we determined did not meet our global quality standards. Remediation actions have been implemented.

Continuous improvement

Lessons learned from the supply chain disruptions in 2012 have been shared across the Group as part of our continuous improvement programme. This programme allows us to improve our systems and minimise the impact of our activities on the environment. We focus on what adds value to our customers and patients, as well as waste elimination. The programme has delivered significant benefits in recent years, including reduced manufacturing lead times and lower average stock levels, both of which improve our ability to respond to customer needs and reduce inventory costs. All improvements are designed to ensure we maintain product quality, safety and customer service.

 

 

40   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

 

LOGO

 

We have applied Lean production business improvement tools and ways of working to improve the efficiency of our manufacturing plants for a number of years and, in recent years, have applied them to the whole of our supply chain. This has led to improvements in quality, lead times and overall equipment effectiveness. In 2012, we continued to establish more efficient processes, with experts from our global supply chain organisation providing cross-functional support throughout the business.

Regulation and compliance

Facilities and processes for manufacturing medicines must observe rigorous standards of quality. They are subject to inspections by regulatory authorities to ensure compliance with prescribed standards. Regulatory authorities have the power to require improvements to facilities and processes, halt production and impose conditions that must be satisfied before production can resume. Regulatory standards are not harmonised globally and evolve over time.

We hosted 44 independent inspections from 22 different regulatory authorities in 2012. All observations from such inspections are reviewed along with the outcomes of internal inspections and subsequent improvement actions are put in place as required to ensure ongoing compliance. The knowledge obtained from all inspections is shared across the Group.

We are actively involved in providing input into new product manufacturing regulations and approaches to product registration, both at national and international levels, through our membership of industry associations. For example, in the EU we continue to provide input into the Falsified Medicines Directive, which came into force in January 2013 and starts to take effect in stages from July 2013. We have taken steps to ensure that our supply chains can comply with the Falsified Medicines Directive. In the US, we contributed to debates concerning Supply Chain Security and the prevention of Drug Shortages.

Our supply and manufacturing strategy is based on our commitment to maintaining the highest ethical standards while complying with internal policies, and laws and regulations. We achieve this by placing compliance responsibility with line managers who are supported by dedicated compliance teams. Independent assurance is provided by our GIA function.

Managing risk

Given our strategy to outsource all API manufacturing, we place particular importance on our global procurement policies and integrated risk management processes to ensure uninterrupted supply of high quality raw materials. Supplies are purchased from a range of suppliers. We factor in a wide range of potential risks to global supply, such as disasters that remove supply capability or the unavailability of key raw materials, and work to ensure that these risks are effectively mitigated. Contingency plans include the appropriate use of dual or multiple suppliers and maintaining appropriate stock levels. Although the price of raw materials may fluctuate, our global purchasing policies seek to avoid such fluctuations becoming material to our business.

We also take into account reputational risk associated with our use of suppliers and are committed to working only with suppliers that embrace standards of ethical behaviour that are consistent with our own.

As part of our overall risk management, we carefully consider the timing of investment with a view to ensuring that secure supply chains are in place for our products. We also have a programme in place to provide appropriate supply capabilities for our new products.

Our resources

Capital expenditure on supply and manufacturing facilities totalled approximately $417 million in 2012 (2011: $388 million; 2010: $333 million). This included expenditure on two production facilities, in China (Taizhou) and Russia (Vorsino), which will enable us to supply

our products to both markets locally. In addition to these two facilities, our principal small molecule manufacturing facilities are in the UK (Avlon and Macclesfield), Sweden (Snäckviken, Gärtuna, Södertälje), the US (Newark, Delaware and Westborough, Massachusetts), France (Reims and Dunkerque), Japan (Maihara), Australia (North Ryde), China (Wuxi), Indonesia (Jakarta), Egypt (Cairo), India (Bangalore), Puerto Rico (Canovanas), Germany (Wedel), Mexico (Lomas Verdes), Brazil (Cotia) and Argentina (Buenos Aires). We currently operate sites for the manufacture of APIs in the UK and Sweden complemented by the efficient use of external sourcing. Our principal tablet and capsule formulation sites are in the UK, Sweden, Puerto Rico and the US. We also have major formulation sites for the global supply of parenteral and/or inhalation products in Sweden, France, Australia and the UK.

At the end of 2012, approximately 10,300 people at 22 sites in 16 countries were working on the manufacture and supply of our products. This total includes some 770 permanent and 110 seasonal people who are employed at our four principal biologics commercial manufacturing facilities in the US (Frederick, Maryland and Philadelphia, Pennsylvania), the UK (Speke), and the Netherlands (Nijmegen) with capabilities in process development, manufacturing and distribution of biologics, including worldwide supply of MAbs and influenza vaccines. Our biologics capabilities are scalable, which enables efficient management of our combined small molecule and biologics pipeline.

 

 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   41

Table of Contents

Performance | Business Review

 

LOGO

 

Working with suppliers

Our commitment: to integrate AstraZeneca ethical standards into our procurement activities and decisions worldwide.

Our objective: to monitor compliance through our ongoing assessment and programmes with focus on areas experiencing highest challenges; to address challenges with our suppliers and promote improvement through collaboration.

Our Global Responsible Procurement Standard defines one of the key business processes for integrating our ethical standards into our procurement activity and decision making worldwide. It includes detailed expectations of suppliers. The process is based on an escalating set of risk-based due diligence activities, applied in a pragmatic way. The same initial assessment process is used for all suppliers and more detailed, focused assessments are then made, relevant to the service provided. Since the programme began in 2009, we have completed 5,661 assessments of new and existing suppliers, which accounts for approximately two-thirds of our spend on suppliers.

We categorise suppliers as high, medium or low risk. We focus our auditing efforts on high and medium risk rated suppliers but we also audit some suppliers that we consider to be lower risk, to confirm our performance expectations across all suppliers we do business with. In 2012, we continued our audit activity with 482 audits across 52 countries (751 audits in 2011) as set out in the table on the previous page.

Forty-three percent of suppliers audited demonstrated standards that met our expectations, with a further 53% implementing improvements to address minor non-compliances. We monitor progress across all corrective actions and 4% of suppliers audited this year will require significant follow up to confirm they will make the improvements we require. We will not use suppliers who are unable or unwilling to meet our expectations in a timely way. During 2012, we removed eight suppliers from our supply chain.

Environmental impact

Our commitment: to minimise the environmental impact of our operations by reducing the carbon footprint and natural resource demands of our own and our suppliers’ business activities.

Our targets for 2012 included reducing:

> operational greenhouse gas footprint to 890 kilo tonnes CO 2 e/yr
> hazardous waste to 0.70 tonnes/$m sales and non-hazardous waste to 0.52 tonnes/employee
> water use to 4.0 million m 3 .

Our SHE strategy and associated objectives and targets for 2011 to 2015 provide the framework for driving our environmental sustainability going forward. This section includes summary information about certain key areas of the framework. Full details of our strategy, objectives and targets are available on our website, astrazeneca.com/responsibility.

We work to reduce our greenhouse gas emissions by, among other things, improving our energy efficiency and pursuing lower-carbon alternatives to fossil fuels at our sites. We strive to ensure that our travel and transport activities are as efficient as possible. Our carbon footprint is also affected by some of our respiratory therapies, specifically our pressurised metered-dose inhalers that rely on hydrofluoroalkane (HFA) propellants to deliver the medicine to a patient’s airways. While HFAs have no ozone depletion potential and a third or less of the global warming potential than the chlorofluorocarbons (CFCs) they replace, they are still greenhouse gases. Our target is to reduce our operational greenhouse gas footprint (excluding emissions from patient use of our inhaler therapies) by 20% from our 2011 levels by 2015. In 2012, our gross greenhouse gas emissions (from all sources) totalled 1.15 million tonnes (41 tonnes/$m indexed to Group revenue).

The management of waste is another key aspect of our commitment and we have a 2015 target of a 15% reduction in hazardous and non-hazardous waste from our 2011 levels. Our primary focus is waste prevention, but where this is not practical, we concentrate on waste minimisation and appropriate treatment or disposal to maximise the reuse and recycling of materials and minimise disposal to landfill. In 2012, our total waste was 47,000 tonnes with a tonnes/$m index of 1.7.

We recognise the need to use water responsibly and, where possible, to minimise the use of water in our facilities. To support the delivery of our target to reduce water use by 25% from our 2011 levels by 2015, we now have water conservation plans at our largest sites. In 2012, our water use was 3.6 million m 3 with a m 3 /$m index of 130.

We are also working to ensure that we measure and report the impact of our external manufacturing activity on the environment, and that our suppliers have appropriate environmental improvement targets.

Our continued commitment to product stewardship is underpinned by our ongoing work to integrate environmental considerations into a medicine’s complete life-cycle, from discovery and development, through manufacturing, marketing and to its ultimate disposal. Further information is available on our website, astrazeneca.com/ responsibility, including environmental risk assessment data for our medicines.

 

Extract from 2012 Responsible Business Plan.

 

   Further information on AstraZeneca’s approach to responsible business can be found in the Responsible Business section from page 48 and on our website, astrazeneca.com/responsibility.

 

The following figures have been revised from those previously published to incorporate our biologics capabilities into our targets.
 

 

42   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

 

LOGO

 

81%

Engagement score fell by three percentage points to 81%

Employees by geographical area (%)

 

LOGO

 

 

 

With approximately 51,700 people in over 100 countries worldwide, we value the talents, skills and capabilities that a global workforce brings to our business. Our people strategy, which defines our approach to managing our workforce and supports the delivery of our business strategy, is built around four key priorities that we believe are critical: acquiring and retaining key capabilities and talent; further developing leadership and management capabilities; further improving the strength and diversity of the talent pipeline; and managing employee engagement while building a high performance culture. Managing significant change in the organisation’s workforce is also something to which considerable management attention continues to be directed. We use a range of metrics to track progress against these priorities, many of which are reported regularly to the SET.

Acquiring and retaining key capabilities and talent

During 2012, we hired approximately 5,700 permanent employees to fuel the expansion of our business in Emerging Markets, to continue to build the new capabilities required to implement our strategy successfully and to replace leavers. We have successfully attracted key talent to supplement critical capabilities across the business and to refresh our leadership pipeline in key areas.

With our focus on business growth in Emerging Markets, the composition of our global workforce continued to change, as shown in the Sales and Marketing

workforce composition figure overleaf. For example, in 2012,1,800 of the new recruits joined AstraZeneca in China. We continue to deploy a range of innovative approaches to help us achieve our ambitious growth plans in these markets and to ensure that we have an attractive employer brand and strong reputation globally.

Compared with a level of 6.7% in 2011, the level of voluntary employee turnover across AstraZeneca increased to 7.3% in 2012 and now stands at the average for the pharmaceutical sector. We have continued to invest significant management time to minimise the risks to the business posed by employee turnover, particularly in markets where conditions are most volatile. This has included regular reporting to the SET of resignation rates in total, by SET area and by key markets using the global HR platform being deployed across all markets as part of a transformation of the HR function. In addition, specific steps have been taken to retain key people and talent within our business. For example, regular risk assessments and retention plans are in place in respect of key individuals.

 

 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   43

Table of Contents

Performance | Business Review

 

LOGO

 

Further developing leadership and management capabilities

We encourage and support our people in achieving their full potential by providing a range of learning and development (L&D) programmes. These are designed to build the capabilities and encourage the behaviours needed to deliver our business strategy.

We have a global approach, supported by the creation of our global talent and development organisation, to ensure that high standards of L&D practice are applied across AstraZeneca. We continue to develop and deploy instructor-led and online development resources, which we aim to make available to all employees to increase access to learning and to support self-development.

We recognise the importance of good leadership and its critical role in stimulating high levels of performance and engagement. Our leadership development frameworks are focused on the core capabilities that we believe are essential for strong and effective leadership. These capabilities are defined for each level in the organisation and apply to all our employees. We complement our leadership capabilities with a set of manager accountabilities, which define what we expect from our managers. These manager accountabilities are further enabled across all markets through the deployment of our global HR platform.

Alongside judicious hiring of new leaders into critical senior roles, the development of an internal pipeline of future global leaders is a high priority. We identify individuals with the potential for more senior and complex roles. These talent pools provide succession candidates for a range of leadership roles across AstraZeneca. We regard these individuals as key assets to the organisation and we proactively support them to reach their potential through, for example, global talent development programmes and targeted development opportunities.

Changes to the Senior Executive Team announced in January 2013 included the promotion of six internal candidates and demonstrate our commitment to the development of senior leaders.

We remain committed to making full use of the talents and resource of all our people. We have policies in place to avoid discrimination, including on the grounds of disability. Our policies cover recruitment and selection, performance management, career development and promotion, transfer, and training (including re-training, if needed, for people who have become disabled) and reward.

Improving the strength and diversity of the talent pipeline

Our commitment: to build an inclusive, open and trusting organisation embracing the skills, knowledge and unique ability of our employees.

Our objective: to accelerate diversity and inclusion appropriately throughout the business, build accountability and track progress. Our target for 2015 is to improve female representation:

 

> at senior manager level and above from 38% (2010) to 43% (2015)
> in the global talent pool from 33% (2010) to 38% (2015).

Our global workforce provides a diversity of skills, capabilities and creativity, and we value the benefits that such diversity brings to our business. We aim to foster a culture of respect and fairness where individual success depends solely on ability, behaviour, work performance and demonstrated potential. As we continue to reshape our organisation and geographic footprint, our challenge is to ensure that diversity in its broadest sense is reflected in our workforce and leadership, and integrated into our business and people strategies. Within this context, we support the representation of women at the highest

levels in our business. Women make up 50% of our global workforce, giving us a real opportunity to develop female leaders. Indeed, there are currently three women on our Board (25%) and, below Board level, women account for 40% of senior management.

Under the leadership of a global Diversity & Inclusion steering group chaired by a member of the SET and comprising senior leaders from across the business and geographies, we are driving change in three key areas: ‘leadership & management capability’; ‘transparency in talent management & career progression’; and ‘work-life challenges’. In March 2012, we launched our Global Insight Exchange programme as a direct result of the work of the steering group. This programme, which consists of peer-to-peer mentoring of over 30 ‘learning pairs’ of identified talent from different functional areas and geographies within our organisation, is designed to accelerate the development of our leadership culture and talent pipeline through the exchange of diversity of thought and experience. In addition, we track gender representation at different levels of the organisation and country of origin representation of our senior leaders to measure progress over the medium term.

Driving employee engagement

We use a variety of global leadership communication channels to engage employees in our business strategy. These include face-to-face meetings, video conferencing and Yammer (a social media tool) to encourage two-way dialogue to take place. For the third year in a row our annual global employee survey (FOCUS) included an open text feedback mechanism, with around 25,000 comments made on a variety of topics.

 

 

44   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

 

LOGO

 

In 2012, 91% of our employees participated in the survey, which measures levels of employee engagement and considers the effectiveness of our organisational, leadership and management capabilities, and satisfaction in terms of employees’ working environment. Our employee engagement score decreased by three percentage points this year and our leadership communications and work-life balance scores also decreased. The survey took place at a challenging time for the Group and the scores were disappointing. We remained ahead of external pharmaceutical industry norms in areas such as motivation, willingness to put in more effort than would normally be expected, line management, and operating with integrity and ethics. However, we recognise that we have more work to do in important areas, such as strategic understanding and reducing organisational complexity, to ensure AstraZeneca is a great place to work. Local leadership teams have also identified actions designed to target any concerns specific to their organisational area.

A key element of our people strategy is the continued development of a performance culture across the organisation. By strengthening our focus on setting high quality objectives aligned to our business strategy, and ongoing coaching and feedback, we strive to ensure that performance at all levels of the organisation delivers value. The Board is responsible for setting our high-level strategic objectives and monitoring performance against them (see the Operation of the Board section on page 111). Managers across AstraZeneca are accountable for working with their teams to develop individual and team performance targets, and for ensuring that employees understand how they contribute to overall business objectives.

We will continue to empower our leaders to drive performance, to hold our managers accountable for understanding and delivering against the standards required, and to provide the tools necessary to reward outstanding contributions.

Our focus on optimising performance is reinforced by performance-related bonus and incentive plans. AstraZeneca also encourages employee share ownership by offering the opportunity to participate in various employee share plans, some of which are described in the Directors’ Remuneration Report from page 122 and also in Note 24 to the Financial Statements from page 179.

Human rights

Our commitment: to respect and promote international human rights in our operations and our sphere of influence.

Our objective: to ensure that human rights considerations are appropriately integrated into our policies, processes and practices.

As reported in 2011, we have carried out labour reviews in 106 countries in which we have employees. The reviews focused on International Labour Organization (ILO) core areas, including freedom of association and collective bargaining, child labour, discrimination, working hours and wages. The framework for the review was provided by an adaptation of the employment section of the Danish Institute for Human Rights assessment tool for pharmaceutical companies, which was developed with our industry’s help and launched in 2010. Results showed that our practices are generally consistent across all countries, based on our mandate that our global standards are applied when external national standards do not meet our minimum requirements. Some gaps to ILO standards have been identified and are being addressed as part of the review of our Global People Policy, which is planned for 2014.

Managing change

Recruitment in our Emerging Markets continues to be accompanied by headcount reductions in our Established Markets as a result of our continuing strategic drive to improve efficiency and effectiveness. Reductions have come about through restructuring in R&D, supply and manufacturing, support functions and our sales and marketing workforce. The net effect of these changes since the end of 2006 has been to reduce our total headcount by some 15,100 from 66,800 to 51,700. This decrease includes a reduction of 2,600 positions in 2010, 5,000 in 2011 and a further 6,300 in 2012, which resulted from our business change plans announced since 2010.

We are committed to ensuring that AstraZeneca’s core values, robust people policies, consultation infrastructure and prior experience were integrated into this multi-faceted business transformation. Trade unions and employee representative groups were involved throughout the restructuring process. With significant investment in outplacement support, high levels of success have been achieved in finding employees alternative opportunities outside AstraZeneca. Further details are set out in the Our strategy section from page 20.

 

Extract from 2012 Responsible Business Plan.

 

   Further information on AstraZeneca’s approach to responsible business can be found in the Responsible Business section from page 48 and on our website, astrazeneca.com/responsibility.
 

 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   45

Table of Contents

Performance | Business Review

 

LOGO

 

Managing employee relations

We work to ensure a level of global consistency in managing employee relations, while allowing enough flexibility to support the local markets in building good relations with their workforces, taking into account local laws and circumstances. To that end, relations with trade unions are nationally determined and managed locally in line with the applicable legal framework and standards of good practice. However, each change programme has its unique challenges and a standard solution may not always be appropriate. Where this is the case, the appropriate solution is developed through consultation with employee representatives or, where applicable, trade unions, with the aim of retaining key skills and mitigating job losses.

Early in 2012, we implemented our Global Employment Standards, which are linked to our Global People Policy. Our Global Employment Standards serve to provide common and consistent expectations concerning the way in which our employees will be managed globally and cover matters including attendance, employee concerns, flexible working, leaving AstraZeneca, misconduct, performance improvement, redeployment and redundancy, and work-life balance.

Safety, health and wellbeing

Our commitment: to promote a safe, healthy and energising work environment in which our people, and those from third parties working closely with us, are able to express their talents, drive innovation and improve business performance.

Our targets for 2012 included:

> 0 fatalities
> combined lost time injury/illness rate per million hours worked of 2.38
> 7.1 collisions per million kilometres driven.

Driver safety remains our highest priority for improvement and our focus is on promoting driver safety among our sales forces, collectively the single largest group of employees who drive on AstraZeneca business. Driver safety targets are included in regional and local scorecards. Performance is monitored centrally to assess progress and identify areas for improvement. In 2012, we missed our annual target for collisions per million kilometres driven. We remain on track to achieve our 2015 target.

We regret that during 2012, two members of the public were killed in two separate road traffic accidents involving AstraZeneca drivers in Russia and Turkey. Detailed investigations into both accidents have been carried out. For the Russian accident, an action plan was formulated to respond to the findings of the investigation and those actions are being tracked. The investigation report for the Turkish accident, which occurred in October, has not yet been finalised. Learning from the investigations into both accidents will be shared widely across the Group.

In 2012, the lost time injury/illness rate increased by 3% from 2011. However, we remain on track to achieve our 2015 target of a 25% reduction in the lost time injury/illness rate from the 2010 baseline, with an overall 21% reduction achieved so far.

Work-related stress has been a particular focus for us in recent years; in 2012 we achieved a significant (59%) reduction in the number of reportable cases compared to 2011. We are continuing our efforts in this area, using a risk-based approach, including wellbeing risk assessment tools, to identify high-risk areas and target interventions effectively.

 

Extract from 2012 Responsible Business Plan.

 

   Further information on AstraZeneca’s approach to responsible business can be found in the Responsible Business section from page 48 and on our website, astrazeneca.com/ responsibility.

 

 

 

46   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

 

LOGO

 

Our Global Compliance function has been established to drive and embed a culture of ethics and integrity within our organisation.

Our key compliance priorities include:

 

> focusing our efforts on important compliance risk areas
> communicating clear policies to employees
> improving compliance behaviours through effective training and support
> ensuring employees can raise concerns and that those concerns will be properly addressed
> ensuring fair and objective investigations of possible policy breaches
> monitoring and auditing compliance with policies
> providing key stakeholders with assurance and effective reporting of material issues.

These priorities are closely aligned to the Group’s strategy and reflect our drive to strengthen our efforts for oversight at all levels of our business, including risk management relating to external parties and anti-bribery/anti-corruption. GIA and Global Compliance work closely with one another and both separately provide assurance reporting to the Audit Committee. Our Global Compliance function also works together with a range of specialist compliance functions throughout our organisation to ensure ongoing legal and regulatory compliance. In March 2012, we created a Group Compliance Council, with membership drawn from Global Compliance and from the other specialist compliance functions, whose purpose is to co-ordinate our compliance activities.

When a potential compliance breach is identified, an internal investigation is undertaken by appropriate staff from our Global Compliance, HR and/or Legal teams. When appropriate, external advisers are engaged to conduct and/or advise on investigations. Should the investigation conclude that an actual breach has occurred, management, in consultation with our Legal function, will consider whether the Company needs to make a disclosure and/or to report the findings to a regulatory or governmental authority. More information on GIA and our overall risk management and control framework can be found in the Corporate Governance Report from page 110.

Code of Conduct

Our Code of Conduct (the Code) is at the core of our compliance programme and applies worldwide to all full- and part-time AstraZeneca Directors, officers, employees and temporary staff. It has been translated into over 40 languages and each employee has access to an electronic copy. It provides clear direction as to how our commitment to honesty and integrity is to be realised in consistent actions across all areas of the business. Compliance with the Code is mandatory and every employee receives training on it. Every employee is required to comply with local laws and regulations, as well as applicable national and international codes. We always seek to operate at the highest of these various standards. The Code is regularly reviewed and updated to take account of changing legal and regulatory obligations.

The Code includes information on how to report possible violations of the Code, including through the AZethics telephone lines and AZethics.com. Anyone who raises a possible breach in good faith is fully supported by management. We take all alleged compliance breaches and concerns extremely seriously and investigate them and report the outcome of such investigations to the Audit Committee, as appropriate.

In 2012, 194 reports of alleged compliance breaches or other ethical concerns were made via telephone, the AZethics.com website, or the Global Compliance email or postal addresses described in the Code. In 2011, the number of reports through equivalent channels was 222. This decrease is in the context of a significant increase in management and self-reporting of compliance incidents, which can be seen as an indication that employees are more comfortable in raising their concerns with line managers, local HR, Legal or Compliance, as recommended in the Code and reinforced in the 2012 Code training.

As with the Code, our Global Policies apply to all companies within our Group. They provide clear and comprehensive guidance, in plain language, to all managers and employees as to their accountabilities in key ethical, compliance and corporate responsibility risk areas.

 

 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   47

Table of Contents

Performance | Business Review

 

LOGO

 

In this section, we describe our approach to delivering business success responsibly. Summary information about our commitment and performance in key areas is integrated into the relevant sections of this Annual Report, while further information about these and other areas is available on our website, astrazeneca.com/responsibility.

Introduction

At AstraZeneca, we are dedicated to the discovery, development and commercialisation of prescription medicines that make a difference in healthcare. For us, this is at the core of our responsibility to our stakeholders and to society. Successful pharmaceutical innovation, delivered responsibly, improves health for patients, brings benefits to stakeholders and delivers long-term shareholder value.

In the Strategy section from page 12, we describe our approach to creating value across the life-cycle of a medicine, our distinctive capabilities and our strategy.

All these efforts are underpinned by our commitment to being a responsible company, working with integrity and delivering sustainable business development that adds value for our stakeholders. To that end, our responsible business objectives are aligned to, and support delivery of, our business strategy. Our Responsible Business Plan is our framework for managing our commitments and includes objectives, targets and KPIs that are agreed across the Group, taking account of external stakeholder insights and internal reputational risk assessment. The Responsible Business Plan puts at the top of the agenda those areas most impacted by our business strategy, which are as follows:

> R&D: Underpinning our accelerated drive for innovation with sound R&D ethics worldwide (see page 33).
> Patient safety: Maintaining a strong focus on patient safety in everything we do, minimising the risks and maximising the benefits of all our medicines throughout R&D, and after launch (see page 34).
> Access to healthcare: As we expand our geographic footprint, exploring ways of increasing access to healthcare for more people, tailored locally to different patient needs (see page 38).
> Sales and marketing: Working to consistent global standards of ethical sales and marketing practices in all our markets as we work to restore growth (see page 39).
> Diversity and inclusion: Working to ensure that diversity in its broadest sense is reflected in our leadership and people strategies (see page 44).
> Human rights: Continuing to develop and embed a consistent approach to human rights across all our worldwide activities (see page 45).
> Employee safety, health and wellbeing: Promoting the safety, health and wellbeing of all our people worldwide as we continue to drive a high performance culture and achievement of our business goals (see page 46).
> Working with suppliers: Only working with suppliers who have standards consistent with our own as we increase our outsourcing to drive business efficiency (see page 42).
> The environment: Managing our impact on the environment, across all our operations, with a particular focus on carbon emissions, waste and water use (see page 42).
> Community investment: Making a positive contribution to our local communities around the world, through community support programmes consistent with improving health and promoting science (see page opposite).

A core element of our business strategy is value-creating business development activity that strengthens our pipeline and accelerates growth. This includes targeted acquisitions. When we acquire companies we aim to work with them to align standards of responsible business and incorporate the companies into the setting of targets and measurement of performance. This process can take time. Thus, for example, responsible business data relating to Ardea, acquired in June, is not incorporated in this Annual Report.

Benchmarking

As expectations of stakeholders evolve, we continue to engage with them and use the feedback to inform the development of our responsible business strategy and risk management planning.

We also use the insights we gain from external surveys to develop our approach in line with global best practice. A member of the Dow Jones Sustainability Index since 2001, we were once again listed in the 2012 World Index (the top 10% of the largest 2,500 companies). We also retained our listing on the DJSI STOXX – European index (the top 20% of the 600 largest European companies) for the fifth year running (one of only four pharmaceutical companies to do so out of 14 assessed). We achieved a total score of 83% (2011: 85%) compared with a sector best score of 87% (2011: 87%). We increased individual scores for nine out of 22 criteria for 2012 (compared to 14 out

 

 

48   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

 

LOGO

 

of 23 criteria in 2011) including marketing practices, supply chain management and human capital development. While these scores are encouraging, we lost ground in some areas including innovation management and health outcomes contribution. To better understand these lower scores, we commissioned an in-depth external benchmark survey and the analysis will be used to inform our improvement planning.

Responsible business governance

The Board is responsible for our responsible business framework and Non-Executive Director, Nancy Rothwell, oversees implementation and reporting to the Board.

The SET and senior managers throughout the Group are accountable for operating responsibly within their areas taking into account national, functional and site issues and priorities. Line managers are accountable for ensuring that their teams understand the requirements and that people are clear about what is expected of them as they work to achieve AstraZeneca’s business goals.

Our Responsible Business Council (the Council) is chaired by our Executive Vice-President of Human Resources & Corporate Affairs, and members include senior leaders from each relevant SET area. Its agenda is focused on driving long-term value creation by agreeing, among other things:

 

> responsible business priorities for the Group in line with strategic business objectives
> managing and monitoring the annual process of setting responsible business objectives and targets recorded in the Responsible Business Plan, as well as reviewing performance against KPIs
> appropriate policy positions to support AstraZeneca’s business objectives and reputation management.

The Council is supported by a Responsible Business Working Group (the Working Group) of SET area representatives. Among other things, the Working Group continuously reviews external issues with the potential to impact AstraZeneca and, as appropriate, prepares management and measurement proposals for the Council’s consideration.

External assurance

Bureau Veritas has provided external assurance on the responsible business information contained within this Annual Report on pages 33-34, 38-39, 42, 44-46 and below, and of the performance related content of the Responsibility section of our website. Based on the evidence provided and subject to the scope, objectives and limitations defined in the full assurance statement, nothing has come to the attention of Bureau Veritas causing them to believe that the responsible business information included within this Annual Report is materially misstated. The full assurance statement, which contains detailed scope, methodology, overall opinion and recommendations can be found on our website, astrazeneca.com/responsibility. Bureau Veritas is an independent professional services company that specialises in quality, health, safety, social and environmental management with a long history of providing independent assurance services.

Community investment

Our commitment: to meet our responsibility as a global corporation to support the wider community, maximising the benefit of our investment for all stakeholders, through focused investment and by embracing current best practice.

Our objective: to extend the geographic reach of our Young Health Programme (YHP). Our target was to have 15 YHP country programmes running by the end of 2012 with a total target reach of 500,000 adolescents by 2015.

In 2012, we spent a total of $1.18 billion (2011: $1.06 billion*) on community investment sponsorships, partnerships and charitable donations worldwide, including our product donation and patient assistance programmes which make our medicines available free of charge or at reduced prices. Through our three patient assistance programmes in the US we donated products valued at an average wholesale price of over $1.12 billion (2011: $938 million). We also donated products worth over $5.8 million, valued at average wholesale price, to charitable organisations Americares and Direct Relief International.

Our global community investment strategy focuses on two key areas, healthcare in the community and science in education. In 2012, we continued to expand our YHP country programme. This is designed to help young people in need around the world deal with the health issues they face so they can improve their chances of living a better life. We currently have 15 country programmes under way around the world.

Through YHP, we have reached over 250,000 young people in communities across five continents with health information. Over 3,000 of these young people have been trained to share this health information with their peers and with the community, and over 2,700 frontline health providers have completed training programmes in adolescent health. We are on track to meet our Clinton Global Initiative commitment to reach 500,000 young people by the end of 2015. Initial findings from the Wellbeing of Adolescents in Vulnerable Environments study being undertaken by Johns Hopkins Bloomberg School of Public Health as part of YHP were presented at the World Health Summit in Berlin, Germany in October. As part of our best practice sharing, our dedicated online resource (younghealthprogrammeYHP.com) enables those working with young people to access information and resources created by the YHP partners.

Our support for science education takes a number of forms. For example, in 2011, we entered a three year partnership with Career Academies UK to support increased participation by 16 to 19-year-olds in Science, Technology, Engineering and Maths (STEM) subjects, with a target that one-third of Career Academies have a STEM theme by the 2014/15 academic year. By the 2012/13 academic year, the proportion was almost one-quarter, representing 48 Career Academies. Our work with Career Academies UK complements the involvement we have had since 2003 with the STEM ambassador programme.

 

Extract from 2012 Responsible Business Plan.

 

   Further information on AstraZeneca’s approach to responsible business can be found above and on our website, astrazeneca.com/responsibility.

 

* Figures re-stated to correct product donation data capture error in 2011.
 

 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   49

Table of Contents

Performance | Therapy Area Review

 

LOGO

 

This process is summarised in the Life-cycle of a medicine diagram on page 14, and in the subsequent Business Review section from page 30, we explore how we apply our resources, skills and capabilities to the various elements of that process in furtherance of our business strategy.

This Therapy Area Review contains information about the six Therapy Areas in which our efforts are focused: Cardiovascular, Gastrointestinal, Infection, Neuroscience, Oncology, and Respiratory & Inflammation. For each research area we review our pipeline from early projects through to launched brands. We describe the business environment, trends and other factors that have influenced our decision to focus on diseases in these six areas, our strategic objectives for each and our progress towards achieving these objectives. We include information about our 2012 focus and key developments relating to our marketed medicines and how they are designed to make a meaningful difference for patients. We also report on the potential new products and product life-cycle developments in our pipeline that reflect our commitment to maintaining a flow of innovation that adds value for our shareholders and to society.

This Therapy Area Review reflects the range of our activities. This includes the work of our small molecule and biologics groups, responsible for discovery and development projects up to and including Proof of Concept, as well as our Global Medicines Development (GMD) organisation, which progresses products through late-stage development, registration and post-launch development activities. This Therapy Area Review also draws on the expertise of our Commercial organisation which ensures our science is connected with our customers’ needs. We embed customer insights into our R&D strategy based on our interactions with healthcare providers, patients, regulators and payers. This approach helps us to prioritise resources and optimise our portfolio, thereby delivering medicines that customers value and which meet their needs. While the focus of this Therapy Area Review is on our key marketed products, many of our other established products are key to certain markets within Emerging Markets and, taken together, represent an important part of AstraZeneca’s business.

For a list of all our potential new products and product life-cycle developments, see the Pipeline by Therapy Area table opposite and the Development Pipeline table from page 199. For details of patent expiries of our key marketed products, see the Patent expiries section on page 36.

Indications for each product described in this Therapy Area Review may vary from country to country and local prescribing information should be referred to for country-specific indications for any particular product.

Many of our products are subject to litigation. Information about material legal proceedings can be found in Note 25 to the Financial Statements from page 184. Details of relevant risks are set out in the Principal risks and uncertainties section from page 75.

 

 

Sales by Therapy Area

 

                                                                                                        
     2012     2011     2010  
    

Sales

$m

    

Reported

growth

%

    CER
growth
% 		   

Sales

$m

    

Reported

growth

%

   

CER

growth

%

   

Sales

$m

 

Cardiovascular

     9,531         (7     (4     10,212         9        5        9,403   

Gastrointestinal

     4,852         (12     (11     5,536         (9     (11     6,088   

Infection and other*

     1,715         (8     (7     1,856         (15     (15     2,176   

Neuroscience

     3,923         (46     (44     7,204         7        5        6,704   

Oncology

     3,489         (6     (3     3,705         (8     (12     4,045   

Respiratory & Inflammation

     4,415         (1     2        4,468         9        6        4,099   

Other businesses**

     48         n/m        n/m        610         (19     (22     754   

Total

     27,973         (17     (15     33,591         1        (2     33,269   

 

* Represents all other pharmaceutical product sales that are not in our six Therapy Areas.
** Represents sales by Aptium Oncology of $48m (2011: $224m; 2010: $219m) and Astra Tech of $nil (2011: $386m; 2010: $535m). The last portion of Aptium was sold in July. Astra Tech was sold to DENTSPLY International Inc. on 31 August 2011.

 

50   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

 

LOGO

 

  

 

  

 

  

 

   Phase I    Phase II    Phase III/ Registration    Line extensions

 

  

 

  

 

  

 

Cardiovascular    > AZD1722 # v      

> Brilinta/Brilique ¿

> Forxiga ¿

    (dapagliflozin) #

> metreleptin # v

  

> Axanum p

Brilinta/Brilique  EUCLID v > Brilinta/Brilique

    PEGASUS-TIMI 54 p

> Bydureon EXSCEL # v

> Bydureon Dual

    Chamber Pen # v

> Forxiga #

    (dapagliflozin)/

    metformin FDC »

> Forxiga #

    (dapagliflozin)

    DPP-4 »

  

> Forxiga #

    (dapagliflozin)

    insulin add on »

> Forxiga #

    (dapagliflozin)

    high CV risk p

> Forxiga #

    (dapagliflozin)

    triple therapy v

Kombiglyze XR/

     Komboglyze  FDC   # * ¿

> SaxaDapa FDC # v

> Onglyza

    SAVOR-TIMI 53 # p

 

  

 

  

 

  

 

Gastrointestinal       > tralokinumab Ë      

> Entocort p

> Nexium p

    (peptic-ulcer bleeding)

  

 

  

 

  

 

  

 

Infection   

> ATM AVI v

> MEDI-550 p

> MEDI-557 p

> MEDI-559 p

  

> AZD5847 Ë

> CXL # p

  

> CAZ AVI # p

    (CAZ104)

> Q-LAIV Flu

     Vaccination ¿

> Zinforo # ¿

    (ceftaroline)

     

 

  

 

  

 

  

 

Neuroscience   

> AZD1446 # p

> AZD3293 # v

> MEDI5117 v

  

> AZD3241 Ë

> AZD3480 # p

> AZD5213 Ë

> AZD6765 p

  

> naloxegol # p

    (NKTR-118)

   > Diprivan # p   

 

  

 

  

 

  

 

Oncology   

> AZD1208 v

> AZD2014 p

> AZD5363 # p

> AZD8330 # p

    (ARRY 424704)

> AZD9150 v

> MEDI0639 # v

> MEDI3617 # p

> MEDI4736 # v

> MEDI-565 # p

> MEDI6469 # v

> moxetumomab pasudotox # p > volitinib # v

  

> AZD4547 p

> fostamatinib # p

> MEDI-551 # Ë

> MEDI-573 # Ë

> MEDI-575 # p

> olaparib Ë

> selumetinib # p

    (AZD6244)

    (ARRY-142886)

> tremelimumab p

     

> Faslodex p

    (1 st line advanced breast cancer)

> Iressa p

    (treatment beyond progression)

 

  

 

  

 

  

 

Respiratory & Inflammation   

> AZD8848 # v

> AZD7594 # v

> MEDI2070 # v

> MEDI4212 v

> MEDI-551 # p

> MEDI5872 # v

> MEDI7814 v

> MEDI9929 # v

> RDEA3170 v

  

> AZD2115 # Ë

> AZD5069 p

> AZD5423 # p

> benralizumab # p

> mavrilimumab # p

> MEDI-546 # Ë

> MEDI7183 # v

> MEDI8968 # p

> sifalimumab # p

> tralokinumab p

  

> brodalumab # v

> fostamatinib # p

> lesinurad v

  

> Symbicort BAI p

    (asthma/COPD)

  

 

  

 

  

 

  

 

#   Partnered product.

   Key – showing movements in 2012

*   Kombiglyze XR in the US; Komboglyze FDC in the EU.

  

v Addition

  
           

p No change

  
           

Ë Progression

  
           

» New filing

  
           

¿ Approved/launched

  

 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   51

Table of Contents

Performance | Therapy Area Review

 

LOGO

 

LOGO

LOGO

LOGO

 

Therapy area world market

(MAT/Q3/12) ($bn)

 

LOGO

 

 

LOGO

Our marketed products

Cardiovascular diseases

  > Crestor 1 (rosuvastatin calcium) is a statin used for the treatment of dyslipidaemia and hypercholesterolemia. In some markets it is also indicated to slow the progression of atherosclerosis and to reduce the risk of first cardiovascular (CV) events.
  > Atacand 2 (candesartan cilexetil) is an angiotensin II antagonist used for the 1 st line treatment of hypertension and symptomatic heart failure.
  > Seloken/Toprol-XL (metoprolol succinate) is a beta-blocker once daily tablet used for 24-hour control of hypertension and for use in heart failure and angina.
  > Tenormin (atenolol) is a cardioselective beta-blocker used for hypertension, angina pectoris and other CV disorders.
  > Plendil (felodipine) is a calcium antagonist used for the treatment of hypertension and angina.
  > Zestril 3 (lisinopril dihydrate) is an angiotensin-converting enzyme inhibitor used for the treatment of a wide range of CV diseases, including hypertension.
  > Axanum (acetylsalicylic acid (ASA) and esomeprazole) is a fixed-dose combination indicated for prevention of CV events in high-risk CV patients in need of daily low-dose ASA treatment and who are at risk of gastric ulcers.
  > Brilinta/Brilique (ticagrelor) is an oral antiplatelet for the treatment of acute coronary syndromes (ACS).

 

 

LOGO

Diabetes

  > Forxiga 4 (dapagliflozin) is a selective and reversible inhibitor of human sodium-glucose co-transporter 2 (SGLT2 inhibitor) indicated as an adjunct to diet and exercise as a once daily oral medication to improve glycaemic control in adult patients with Type 2 diabetes mellitus as add on combination therapy or as monotherapy in metformin-intolerant patients.
  > Komboglyze 4 (saxagliptin and metformin HCl) is an immediate release fixed-dose combination indicated as an adjunct to diet and exercise to improve glycaemic control in adult patients with Type 2 diabetes mellitus inadequately controlled on their maximally tolerated dose of metformin alone or those already being treated with the combination of saxagliptin and metformin as separate tablets.
  > Kombiglyze XR 4 (saxagliptin and metformin XR) is an extended release fixed-dose combination indicated as an adjunct to diet and exercise to improve glycaemic control in adults with Type 2 diabetes mellitus when treatment with both saxagliptin and metformin is appropriate.
  > Onglyza 4 (saxagliptin) is a DPP-IV inhibitor used for the treatment of Type 2 diabetes.
  > Byetta 4 (exenatide injection) is an injectable medicine indicated to improve blood sugar (glucose) control along with diet and exercise in adults with Type 2 diabetes mellitus.
  > Bydureon 4 (exenatide extended release injectable suspension) is an injectable medicine indicated to improve blood sugar (glucose) along with diet and exercise in adults with Type 2 diabetes mellitus.
  > Symlin 4 (pramlintide acetate) is an injected amylin analogue for the treatment of Type 1 and Type 2 diabetes in patients with inadequate glycaemic control on meal-time insulin.

 

  1   Licensed from Shionogi & Co. Ltd.
  2   Licensed from Takeda Chemicals Industries Ltd.
  3   Licensed from Merck.
  4   Co-developed and co-commercialised with BMS.
 

 

52   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

LOGO

 

    World     US     Western Europe     Established ROW     Emerging Markets     Prior year  

2012

 

Sales
$m

   

Reported
growth
%

   

CER
growth
%

   

Sales
$m

   

Reported
growth
%

   

Sales
$m

   

Reported
growth
%

   

CER
growth
%

   

Sales
$m

   

Reported
growth
%

   

CER
growth
%

   

Sales
$m

   

Reported
growth
%

   

CER
growth
%

   

World
sales

$m

 

Crestor

    6,253        (6     (4     3,164        3        1,156        (6     2        1,269        (24     (23     664               4        6,622   

Atacand

    1,009        (30     (27     150        (18     422        (42     (39     142        (33     (33     295        (9     (3     1,450   

Seloken/
Toprol–XL

    918        (7     (4     320        (21     70        (18     (12     30        (21     (21     498        8        13        986   

Onglyza

    323        53        53        237        52        47        38        38        13        86        86        26        86        86        211   

Plendil

    252        (2     (2     4        (50     18        (22     (17     12        (14     (14     218        3        2        256   

Tenormin

    229        (15     (13     10        (9     50        (15     (8     106        (15     (15     63        (16     (12     270   

Brilinta/
Brilique

    89        324        348        19        73        55        n/m        n/m        3        n/m        n/m        12        n/m        n/m        21   

Byetta

    74        n/m        n/m        74        n/m                                                                         

Bydureon

    37        n/m        n/m        37        n/m                                                                         

Others*

    347        (12     (8     25        150        157        (17     (12     32        (15     (15     133        (15     (12     396   

Total

    9,531        (7     (4     4,040        5        1,975        (16     (10     1,607        (23     (23     1,909               4        10,212   
                             

2011

                                                                                         

Crestor

    6,622        16        13        3,074        16        1,225        10        5        1,662        25        15        661        9        8        5,691   

Atacand

    1,450        (2     (6     182        (16     731        (1     (6     213        (5     (13     324        6        7        1,483   

Seloken/
Toprol–XL

    986        (19     (20     404        (41     85        (7     (12     38        (3     (13     459        17        15        1,210   

Onglyza

    211        206        206        156        189        34        240        240        7        250        250        14        367        367        69   

Plendil

    256               (4     8        (47     23        (15     (19     14               (7     211        6        2        255   

Tenormin

    270        (2     (8     11        (15     59        (3     (8     125        (2     (10     75               (1     276   

Brilinta/
Brilique

    21        n/m        n/m        11        n/m        9        n/m        n/m                             1        n/m        n/m          

Zestril

    144        (8     (11     10               71        (12     (16     14        (18     (24     49               (2     157   

Others

    252        (4     (7            (100     119        5               25        (4     (15     108                      262   

Total

    10,212        9        5        3,856        6        2,356        6        1        2,098        18        9        1,902        9        8        9,403   

 

* Includes Zestril

For a detailed narrative explanation of the financial performance of our products please see the Geographical Review from page 70.

 

AstraZeneca is one of the world leaders in cardiovascular (CV) medicines, working to improve the treatment of diseases that cause 17 million deaths each year.

We aim to build on our strong position, with a particular focus on thrombosis (blood clotting), atherosclerosis (hardening of the arteries), metabolic diseases, and diabetes and its complications. Despite improvements in the quality of diagnosis and treatment, the unmet medical need remains high and these disease areas, and their complications, continue to grow worldwide (both in Established Markets and Emerging Markets) as a consequence of the spread of a westernised lifestyle.

We are developing potential new therapies using a variety of approaches, including small molecules, antibodies, peptides and proteins, to address unmet medical need in the treatment of obesity, diabetes and heart disease.

Cardiovascular diseases

Hypertension (high blood pressure) and dyslipidaemia (abnormal levels of blood cholesterol) damage the arterial wall which may lead to atherosclerosis. CV events driven by atherosclerotic disease remain the leading cause of death in the western world. Lipid-modifying therapy, primarily statins, is a cornerstone for the treatment of atherosclerosis.

Acute coronary syndromes (ACS) is an umbrella term for sudden chest pain and other symptoms due to insufficient blood supply (ischaemia) to the heart muscle. ACS is the acute culmination of ischaemic heart disease. There remains a significant need to improve outcomes and reduce the costs of treating ACS.

Our 2012 focus

Globally, Crestor has continued to gain market share (by value) since its launch in 2003, with its differentiated profile in managing cholesterol levels and its more recent label indications for slowing the progression of atherosclerosis and reducing the risk of CV events in some markets.

Crestor is the only statin with an atherosclerosis indication in the US which is not limited by disease severity or restricted to patients with coronary heart disease. A competitor to Crestor , atorvastatin ( Lipitor ), was available in generic form in the US from late 2011, and from May several generic atorvastatin products have become available in the market.

Fewer than half the people thought to have high levels of low-density lipoprotein cholesterol (LDL-C) (so-called ‘bad cholesterol’) are diagnosed and treated. Of treated patients, only about half reach their doctors’ recommended cholesterol targets using existing treatments. Study data has shown that the usual 10mg starting dose of Crestor is more effective at lowering LDL-C and produces greater achievement of LDL-C goals than commonly prescribed doses of other statins. Crestor also produces an increase in high-density lipoprotein cholesterol (HDL-C) (so-called ‘good cholesterol’) across the dose range and has again been shown to reduce atherosclerotic plaque in the SATURN study published in 2011.

 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   53

Table of Contents

Performance | Therapy Area Review

 

LOGO

 

Crestor continues to face increasing challenges from generic products. Patents protecting Crestor have been subject to a number of challenges in different jurisdictions. Details of these matters are included in Note 25 to the Financial Statements from page 184.

Atacand continues to be an important treatment option for patients with hypertension and symptomatic heart failure. Atacand is approved for the treatment of hypertension in over 125 countries and for symptomatic heart failure in more than 70 countries. Most patients with hypertension fail to reach their treatment goals with the use of a single anti-hypertensive treatment and fixed-dose combinations of two or more anti-hypertensives are commonly prescribed for patients to improve efficacy and attainment of treatment goals. Atacand Plus (candesartan cilexetil/hydrochlorothiazide) is a fixed-dose combination of Atacand and the diuretic hydrochlorothiazide, indicated for the treatment of hypertension in patients who require more than one anti-hypertensive therapy. Atacand Plus is approved in 99 countries.

Axanum is a single capsule of low-dose ASA and esomeprazole (the active ingredient in Nexium ). It is indicated for prevention of CV events in high-risk CV patients in need of daily low-dose ASA treatment and who are at risk of gastric ulcers. Low-dose ASA is a mainstay of therapy for patients at high risk of having a CV event such as a heart attack or stroke. Up to 30% of high-risk CV patients identified as being at gastrointestinal (GI) risk discontinue or take deliberate breaks from their low-dose ASA and one of the main reasons is GI problems, placing them at risk of a CV event after discontinuation. Following the first national approval in the EU in August 2011, Axanum is now approved in 27 countries and has been launched in 11 countries.

Brilinta/Brilique is an oral antiplatelet treatment for ACS in a new chemical class called cyclo-pentyl-triazolo-pyrimidines which are selective adenosine diphospate (ADP) receptor antagonists that act on the P2Y12 ADP-receptor. Brilinta/Brilique remains under regulatory review in 23

countries. It has been approved in 88 countries, including the US, Canada and Brazil under the trade name Brilinta and in the EU, Iceland and Norway under the trade name Brilique . Additional marketing authorisations and regulatory submissions are planned for 2013.

Clinical studies

GALAXY, is our long-term global clinical research programme for Crestor investigating links between optimal lipid control, atherosclerosis and CV morbidity and mortality. The programme has completed over 29 studies involving approximately 64,000 patients in over 57 countries. The ongoing studies in GALAXY and our investigator sponsored studies programme aim to complete our understanding of the product profile for Crestor .

PEGASUS-TIMI 54, a 21,000 patient study, is ongoing in over 30 countries. The study examines the ability of Brilinta/Brilique plus aspirin to prevent adverse CV events safely compared with aspirin alone in higher-risk patients one to three years after a heart attack.

In July, AstraZeneca announced plans to conduct the EUCLID study, a global clinical trial involving 11,500 patients with peripheral artery disease (PAD), a condition affecting approximately 27 million people in Europe and North America. EUCLID, which began enrolling patients in early 2013, is a randomised, double-blind, parallel group, multi-centre study evaluating the efficacy of Brilinta/Brilique (monotherapy) compared to clopidogrel (monotherapy) in reducing the primary endpoint – a composite of CV death, myocardial infarction or ischaemic stroke – in patients with PAD.

Both PEGASUS-TIMI 54 and EUCLID are part of the PARTHENON programme, an AstraZeneca-funded comprehensive, long-term and evolving global research initiative designed to address unanswered questions in atherothrombotic disease and to investigate the impact of Brilinta/ Brilique on reducing CV events and death. The PARTHENON programme is part of AstraZeneca’s commitment to understand and advance treatments for CV diseases in an effort to improve

patient health. The benefit of Brilinta/Brilique on CV thrombotic events, including CV mortality, observed in patients who have had an ACS event supports continued study in other areas of CV disease. The current PARTHENON programme is designed to include more than 51,000 patients worldwide.

Diabetes

Type 2 diabetes is a chronic progressive disease and patients often require multiple medications to control their condition. The disease continues to grow as a consequence of western lifestyles and it increasingly affects people at a younger age. There are a number of established oral generic and branded classes, such as biguanides and sulfonylureas. However, newer classes such as oral dipeptidyl peptidase IV (DPP-IV) inhibitors and GLP-1 agonists are successfully entering the market by offering effective blood sugar control and improved tolerability. Several new classes of drugs are in development in this area, including sodium-glucose co-transporter 2 (SGLT2). CV safety of these new classes has been given particular emphasis in recent regulatory reviews and guidance documents provided by the FDA and other regulatory authorities.

Our 2012 focus

AstraZeneca continues its worldwide diabetes alliance with BMS to co-develop and co-commercialise two compounds discovered by BMS: Onglyza and Forxiga for the treatment of Type 2 diabetes.

Onglyza is a DPP-IV inhibitor used for the treatment of Type 2 diabetes and has been submitted for regulatory review in 94 countries and approved in 81, including the US, Canada, Mexico, the EU, India, Brazil and China.

Forxiga is a first-in-class SGLT2 inhibitor developed with BMS as a once daily oral therapy for the treatment of adult patients with Type 2 diabetes. In November, Forxiga was approved in the EU to improve glycaemic control in adult patients with Type 2 diabetes. Forxiga is intended to be used as an adjunct to diet and exercise in combination with other glucose-lowering medicinal products, including insulin, or

 

 

54   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

LOGO

 

as a monotherapy in metformin-intolerant patients. With the European approval, Forxiga is now approved in 31 countries with six additional countries under regulatory review. Additional submissions are planned for 2013.

 

In January 2012, AstraZeneca and BMS received a Complete Response Letter from the FDA requesting additional clinical data to allow a better assessment of the benefit/ risk profile for Forxiga . AstraZeneca and BMS have since had discussions with the FDA, which have resulted in a path forward for NDA resubmission. Additional data from ongoing clinical studies will be submitted to further support the benefit/risk profile of Forxiga with resubmission targeted for mid-2013.

 

Komboglyze , an immediate release fixed-dose combination indicated as an adjunct to diet and exercise to improve glycaemic control in adult patients with Type 2 diabetes mellitus inadequately controlled on their maximally tolerated dose of metformin alone or those already being treated with the combination of saxagliptin and metformin as separate tablets, has been submitted for regulatory review in 34 countries and is approved in the EU plus Norway, Iceland, Liechtenstein, Switzerland and Canada.

 

Kombiglyze XR, an extended release fixed-dose combination indicated as an adjunct to diet and exercise to improve glycaemic control in adults with Type 2 diabetes mellitus when treatment with both saxagliptin and metformin is appropriate, has been submitted for regulatory review in 38 countries and is approved in 17 countries, including the US, Brazil, Mexico and India.

 

In August, AstraZeneca and BMS confirmed that, following the completion of BMS’s acquisition of Amylin, AstraZeneca and BMS had expanded their worldwide diabetes alliance to include the co-development and co-commercialisation of Amylin’s portfolio of products related to diabetes (and other metabolic diseases) with a primary focus on a franchise of GLP-1 agonists for the treatment of Type 2 diabetes. The products include Byetta, Bydureon and Symlin .

  

Byetta, a twice daily injectable medicine indicated to improve blood sugar (glucose) control along with diet and exercise in adults with Type 2 diabetes mellitus, has been submitted for regulatory review in 92 countries and approved in 88, including the US, the EU and Japan.

 

Bydureon, which is a weekly injectable medicine indicated to improve blood sugar (glucose), along with diet and exercise, in adults with Type 2 diabetes mellitus, has been submitted for regulatory review in 51 countries and approved in 39, including the US, the EU and Japan.

 

Symlin, an injected amylin analogue for the treatment of Type 1 and Type 2 diabetes in patients with inadequate glycaemic control on meal-time insulin, is approved in the US.

 

During the year, our research activities on anti-arrhythmics to treat atrial fibrillation were terminated.

 

In the pipeline

We expanded our CV research to include End Stage Renal Disease (ESRD) and Chronic Kidney Disease (CKD), with the licensing of an NHE3 inhibitor from Ardelyx. The NHE3 inhibitor is a novel approach to treating sodium and fluid retention in patients with renal impairment.

 

Metreleptin is a leptin analogue under development for the treatment of rare forms of inherited or acquired lipodystrophy, an orphan disease characterised by the deterioration or loss of the body’s adipose tissue. This compound is part of the Amylin portfolio that AstraZeneca and BMS are co-developing. Completion of the Biologics Licence Application submission to the FDA is anticipated in the first half of 2013.

  

Clinical studies

The SAVOR-TIMI 53 (saxagliptin assessment of vascular outcomes recorded in patients with diabetes mellitus) trial, which has completed recruitment, is designed to determine whether treatment with Onglyza when added to a patient’s current standard of care will result in a reduction in a composite CV endpoint (CV death, non-fatal myocardial infarction, non-fatal ischaemic stroke) compared to placebo. This trial, involving 16,500 adult patients with Type 2 diabetes with a history of established CV disease or multiple risk factors, is also designed to fulfil a post-marketing requirement for the FDA.

 

In June, AstraZeneca and BMS announced results from a Phase III clinical study that showed that Forxiga 10mg demonstrated significant reductions in blood sugar levels (glycosylated haemoglobin levels, or HbA1c) compared with placebo at 24 weeks when either agent was added to existing sitagliptin therapy (with or without metformin) in adult patients with Type 2 diabetes. The results were maintained over a 24 week extension and similar results were observed when the data was analysed by subjects’ background therapy. The study also demonstrated significant reductions in total body weight and fasting plasma glucose levels in patients taking Forxiga added to sitagliptin (with or without metformin), with results maintained throughout the duration of the study extension.

 

EXSCEL (EXenatide Study of Cardiovascular Event Lowering) is designed to determine if there are favourable CV effects of exenatide treatment, using Bydureon (exenatide extended release injectable suspension). The EXSCEL study started in 2010 and is planned to run until 2017. The study has enrolled patients during 2012 and is designed for 9,500 patients.

 

   LOGO

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   55

Table of Contents

Performance | Therapy Area Review

 

LOGO

 

LOGO

Therapy area world market

(MAT/Q3/12) ($bn)

 

LOGO

For a detailed narrative explanation of the financial performance of our products please see the Geographical Review from page 70.

LOGO

 

LOGO

 

LOGO

Our marketed products

  > Nexium (esomeprazole magnesium) is the first proton pump inhibitor (PPI) used for the treatment of acid-related diseases to offer clinical improvements over other PPIs and other treatments.
  > Losec/Prilosec (omeprazole) is used for the short-term and long-term treatment of acid-related diseases.
  > Entocort (budesonide) is a locally acting corticosteroid used for the treatment of inflammatory bowel disease.

 

LOGO

 

 

Our financial performance

 

    World     US     Western Europe     Established ROW     Emerging Markets     Prior year  

2012

  Sales
$m 		    Reported
growth
% 		    CER
growth
% 		    Sales
$m 		    Reported
growth
% 		    Sales
$m 		    Reported
growth
% 		    CER
growth
% 		    Sales
$m 		    Reported
growth
% 		    CER
growth
% 		    Sales
$m 		    Reported
growth
% 		    CER
growth
% 		   

World
sales

$m

 

Nexium

    3,944        (11     (10     2,272        (5     417        (45     (41     476        (12     (11     779        7        11        4,429   

Losec/Prilosec

    710        (25     (24     30        (21     188        (22     (17     316        (29     (29     176        (20     (20     946   

Others

    198        24        25        145        44        38        (17     (11     6                      9        29        29        161   

Total

    4,852        (12     (11     2,447        (4     643        (39     (34     798        (20     (19     964        1        4        5,536   
                             

2011

                                                                                         

Nexium

    4,429        (11     (12     2,397        (11     762        (37     (39     540        19        10        730        18        20        4,969   

Losec/Prilosec

    946        (4     (11     38        (21     242        (4     (10     447        2        (7     219        (12     (15     986   

Others

    161        21        19        101        33        46        2        (2     7        17        17        7        17               133   

Total

    5,536        (9     (11     2,536        (10     1,050        (30     (33     994        11        2        956        9        10        6,088   

 

56   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

LOGO

 

We aim to develop our position in gastrointestinal (GI) treatments by continuing to focus on our existing proton pump inhibitors (PPIs) and the development of new therapies for irritable bowel syndrome (IBS) and inflammatory bowel disease (IBD).

Our 2012 focus

Nexium is marketed in more than 125 countries and is available in oral (tablet, capsule and sachet for oral suspension) and intravenous (i.v.) dosage forms, for the treatment of acid-related diseases. Nexium is also approved for use in children from the age of one month in the US and from the age of one year in Europe and other markets. Nexium capsules were launched in Japan in September 2011 after a Japan-specific development programme.

Nexium is an effective short-term and long-term therapy for patients with gastroesophageal reflux disease (GERD). Nexium is also approved for the healing and prevention of ulcers associated with NSAID therapy and for the treatment of patients with the rare gastric disorder, Zollinger-Ellison syndrome. Nexium , in combination with antibiotics, is also approved for use for the treatment of duodenal ulcers caused by Helicobacter pylori infection in the US, Europe and other markets. Nexium is also approved for this use in children from the age of four years (approvals vary between countries).

Nexium i.v. is used as an alternative dosage form when oral administration is not suitable. Nexium i.v. is approved for this use in children from the age of one month in the US and from the age of one year in Europe and other markets. In addition, it is approved in Europe and other markets for the prevention of peptic-ulcer bleeding.

In August, AstraZeneca announced that it had entered into an agreement with Pfizer for the OTC rights for Nexium . Under the terms of the agreement, Pfizer will acquire the exclusive global rights to market Nexium for OTC indications worldwide.

Nexium continues to face increasing challenges from generic products. Patents protecting Nexium have been subject to a number of challenges in different jurisdictions. Details of these matters are included in Note 25 to the Financial Statements from page 184.

Losec/Prilosec , used for the short-term and long-term treatment of acid-related diseases, was first launched in 1988 and is approved for the treatment of GERD and other indications. We continue to maintain certain patent property covering Losec/Prilosec. Losec/Prilosec is available both as a prescription-only medication and, in some countries, as an OTC medication where it offers consumers a more effective self-medication option for the treatment of heartburn compared with antacids and H 2 -receptor antagonists.

In October, AstraZeneca and Ironwood announced an agreement to co-develop and co-commercialise in China Ironwood’s product linaclotide, a guanylate cyclase-C (GC-C) agonist used for the treatment of irritable bowel syndrome with constipation (IBS-C) and chronic idiopathic constipation (CIC) in China. Ironwood markets the product under the name Linzess in the US. Clinical trial applications for linaclotide have been filed with the SFDA.

In the pipeline

Our activities in the field of inflammatory bowel disease include clinical stage testing of two antibodies in collaboration with Amgen that target IL-13 and a4b7. In addition, we have expanded our GI research to include IBS and IBD with the NHE3 inhibitor programme, including the lead compound RDX5791 which we licensed from Ardelyx in October.

 

 

LOGO

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   57

Table of Contents

Performance | Therapy Area Review

 

LOGO

 

LOGO

Therapy area world market

(MAT/Q3/12) ($bn)

 

LOGO

LOGO

 

LOGO

Our marketed products

Respiratory syncytial virus (RSV)

  > Synagis (palivizumab) is a humanised MAb used for the prevention of serious lower respiratory tract disease caused by RSV in paediatric patients at high risk of acquiring RSV disease.

Serious bacterial infections

  > Zinforo 1 (ceftaroline fosamil) is a novel injectable cephalosporin used in community-acquired pneumonia (CAP) and complicated skin and soft tissue infections (CSSTI).
  > Cubicin 2 (daptomycin) is a cyclic lipopeptide anti-bacterial used for the treatment of serious infections in hospitalised patients.
  > Merrem/Meronem 3 (meropenem) is a carbapenem anti-bacterial used for the treatment of serious infections in hospitalised patients.

Influenza virus

  > FluMist/Fluenz (influenza vaccine live, intra-nasal) is an intra-nasal live, attenuated, trivalent influenza vaccine.

 

  1   Licensed from Forest.
  2   Licensed from Cubist Pharmaceuticals, Inc.
  3   Licensed from Dainippon Sumitomo.

 

LOGO

 

 

Our financial performance

 

    World     US     Western Europe     Established ROW     Emerging Markets     Prior year  

2012

  Sales
$m 		   

Reported

growth
%

   

CER

growth
%

    Sales
$m 		   

Reported

growth
%

    Sales
$m 		   

Reported

growth
%

   

CER

growth
%

   

Sales

$m

   

Reported

growth

%

   

CER

growth

%

    Sales
$m 		   

Reported

growth
%

   

CER

growth
%

   

World
sales

$m

 

Synagis

    1,038        6        6        611        7        427        5        5                                                  975   

Merrem/Meronem

    396        (32     (29     38        (7     64        (64     (62     18        (66     (66     276        (11     (6     583   

FluMist

    181        12        12        174        9        3        n/m        n/m        3        n/m        n/m        1                      161   

Others

    100        (31     (28     58        (25     6        (33     (11     16        (20     (20     20        (35     (32     137   

Total

    1,715        (8     (7     881        4        500        (16     (15     37        (49     (49     297        (13     (8     1,856   
                             

2011

                                                                                         

Synagis

    975        (6     (6     570        (12     404        3        3                             1                      1,038   

Merrem/Meronem

    583        (29     (30     41        (68     179        (45     (48     53        (7     (14     310        2               817   

FluMist

    161        (7     (7     160        (8                                               1                      174   

Non Seasonal Flu

    7        (82     (82     7        (82                                                                    39   

Others

    130        19        17        70        3        10        n/m        n/m        20               (25     30        55        90        108   

Total

    1,856        (15     (15     848        (19     593        (18     (19     73        (5     (17     342        5        6        2,176   

For a detailed narrative explanation of the financial performance of our products please see the Geographical Review from page 70.

 

58   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

LOGO

 

We aim to build a leading franchise in the treatment of infectious diseases through continued commercialisation of brands such as Synagis, Merrem/ Meronem, FluMist/Fluenz and Cubicin, the registration and launch of Zinforo in the EU, and through our other ongoing development programmes.

We also aim to make effective use of our structural and genomic-based discovery technologies and antibody platforms, vaccines and continued small molecule and biologics research into novel approaches in areas of unmet medical need. Complementing our biologics capabilities, we are building a small molecule anti-viral platform based on in-house capabilities and external collaborations, focused on respiratory viruses, such as respiratory syncytial virus (RSV) and human rhinovirus.

Respiratory syncytial virus

Approximately half of all infants are infected with RSV during the first year of life and nearly all children in the US have been infected by the time they reach their second birthday. RSV is the most common virus that causes lung and airway infections in infants and young children. It is the leading cause of hospitalisations and admissions to paediatric intensive care units in the first year of life. Premature babies (earlier than 36 weeks gestational age, especially those less than 32 weeks) and babies with chronic lung disease or congenital heart disease are at increased risk of contracting serious RSV disease than full-term healthy babies.

Our 2012 focus

Synagis is used for the prevention of serious lower respiratory tract disease caused by RSV in children at high risk of the disease. It was the first MAb approved in the US for an infectious disease and has become the global standard of care for RSV prevention. Approved in 83 countries worldwide, Synagis remains the only

immunoprophylaxis in the marketplace indicated for the prevention of RSV in paediatric patients at high risk of serious RSV disease. Synagis is administered by intra-muscular injection.

In the pipeline

We are developing a live intranasal vaccine for the prevention of lower respiratory tract illness caused by RSV in otherwise healthy infants. The lead vaccine candidate in clinical development is in Phase I.

Serious bacterial infections

World demand for antibiotics and novel therapeutic approaches remains high and will continue to grow due to escalating resistance and the increased risk of serious infections in both immuno-suppressed patients and ageing populations. Many bacterial infections currently have few satisfactory treatment options, prompting demand for new and better therapies. Our discovery and early development platforms focus on the identification of pathogen-directed approaches, with a particular emphasis on multi-drug resistant gram-negatives and methicillin resistant staphylococcus aureus (MRSA).

Our 2012 focus

Zinforo is a novel injectable cephalosporin, developed in collaboration with Forest, which is approved for use in the EU. Zinforo provides broad coverage against common causative pathogens, such as staphylococcus aureus, including MRSA, a cause of serious and difficult to treat complicated skin infections, streptococci in complicated skin infections, and streptococcus pneumoniae and methicillin-sensitive staphylococcus aureus (MSSA) in community acquired pneumonia. Forest markets ceftaroline in the US under the brand name Teflaro . In August, the European Commission granted marketing authorisation for Zinforo . This makes Zinforo the only approved cephalosporin monotherapy in the EU with demonstrated clinical efficacy against MRSA in difficult to treat complicated skin infections.

Cubicin is used for the treatment of serious gram-positive infections in hospitalised patients and is sold by AstraZeneca in selected territories in Asia, Europe and the Middle East. Cubicin was submitted for marketing approval by the SFDA in China in September for the additional indication of complicated skin and skin structure infections.

Merrem/Meronem remains the leading carbapenem anti-bacterial which is approved in most countries outside Japan.

AZD9773 (formerly known as CytoFab), was a potential treatment for severe sepsis licensed from Protherics Inc. (now part of the BTG plc group). In August, further development of AZD9773 was halted after negative Phase llb study results.

In the pipeline

Following the acquisition of Novexel in 2010, we are working with Forest on future joint global development programmes, including CAZ AVI (a combination of ceftazidime and avibactam), CXL (a combination of ceftaroline and avibactam) and ATM AVI (a combination of aztreonam and avibactam). The CAZ AVI Phase III programme was initiated in 2011 and includes seven trials to confirm the efficacy and tolerability of CAZ AVI in adult patients with complicated intra-abdominal infections, complicated urinary tract infections or nosocomial pneumonia. Patients with infections which are resistant to commonly used antibiotics will also be included in the Phase III programme. CXL is in Phase II development for serious infections where coverage against MRSA and streptococci as well as common gram-negative resistant strains is required.

Our early research and development efforts aim to address multi-resistant bacterial strains expressing metallo-betalactamases, for which very few, if any, treatment options exist. We are collaborating with regulatory authorities to design the clinical trials for these programmes.

 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   59

Table of Contents

Performance | Therapy Area Review

 

LOGO

 

Influenza virus

Influenza is the most common vaccine-preventable disease in the developed world. According to WHO estimates, seasonal influenza results in three to five million cases of severe illness and up to half a million deaths globally each year, primarily among the elderly. Rates of infection are highest among children.

Our 2012 focus

FluMist is a trivalent live, attenuated nasally delivered vaccine approved for the prevention of disease caused by influenza virus subtypes A and B in eligible children and adults. FluMist is approved for eligible individuals in seven countries including the US, Canada and Brazil.

In February 2012, AstraZeneca received approval from the FDA for FluMist Quadrivalent (influenza vaccine live, intra-nasal), formerly known as MEDI3250, in the prevention of influenza. This marks the first four-strain influenza vaccine, and the only intra-nasal four-strain vaccine, approved by the FDA. Most other approved seasonal influenza vaccines currently available in the US are trivalent, containing three strains (two strains of type A influenza (A/H1N1 and A/H3N2) and one B lineage strain). FluMist Quadrivalent contains four strains (two type A strains and two type B lineages) to help provide broad protection against circulating influenza A and B.

In the pipeline

The MAA for the quadrivalent live attenuated influenza vaccine (formerly known as MEDI3250) was submitted in September in the EU.

Neglected tropical diseases

As part of our commitment to make a contribution to improving health in the developing world, we are working to find new, improved treatments for neglected tropical diseases. Our strategy is collaborative and seeks to leverage internal investment and expertise in tuberculosis (TB) and malaria. For other neglected tropical diseases, we participate in open innovation and knowledge-sharing platforms, enabling the use of AstraZeneca assets and infrastructure by external partners.

TB remains a complex research area in which collaborations play an important role. Our discovery collaboration with the Global Alliance for TB Drug Development continues to work towards progressing suitable compounds through to the lead optimisation stage. Research funded by a Wellcome Trust grant under the ‘R&D for Affordable Healthcare in India’ initiative, which will be used to identify novel lead molecules for the treatment of TB, continues. Our most advanced programme, AZD5847

(a novel anti-tubercular oxazolidinone antibiotic), progressed to Phase IIa trials in South Africa, with support from The National Institute of Allergy and Infectious Diseases.

Malaria is another disease for which there remains a tremendous medical need. Our collaboration with Medicines for Malaria Ventures has progressed during 2012 according to plan, and is currently focused on the discovery of a new class of malaria medicines. We anticipate that this collaboration will continue to progress through discovery stages in 2013.

In 2012, we extended our range of external collaborations with new screening agreements with the Liverpool School of Tropical Medicine and the Drugs for Neglected Diseases Initiative. In these collaborations, AstraZeneca shares compounds with external partners with a view to identifying new leads against a variety of diseases of the developing world, including leishmaniasis, sleeping sickness, river blindness and Chagas disease. We also actively participated in the WIPO Re:Search initiative, promoting open innovation for the discovery of novel treatments.

 

 

LOGO

 

60   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

LOGO

LOGO

Therapy area world market

(MAT/Q3/12) ($bn)

 

LOGO

LOGO

 

Our marketed products

Psychiatry

  > Seroquel IR (quetiapine fumarate) is an atypical anti-psychotic drug generally approved for the treatment of schizophrenia and bipolar disorder (mania, depression and maintenance).
  > Seroquel XR (an extended release formulation of quetiapine fumarate) is generally approved for the treatment of schizophrenia, bipolar disorder, major depressive disorder (MDD) and, in some countries, for generalised anxiety disorder (GAD).

Analgesia and anaesthesia

  > Zomig (zolmitriptan) is used for the acute treatment of migraines with or without aura and Zomig Nasal Spray is indicated for the acute treatment of cluster headache in some territories.
  > Diprivan (propofol) is an intravenous general anaesthetic used in the induction and maintenance of general anaesthesia,

 

LOGO

 

for use in intensive care sedation and conscious sedation for surgical as well as diagnostic procedures.

  > Vimovo 1 (naproxen/esomeprazole magnesium) 375/20-500/20mg delayed-release tablet is generally approved for symptomatic relief in the treatment of rheumatoid arthritis, osteoarthritis and ankylosing spondylitis in patients at risk of developing NSAID-associated gastric and/or duodenal ulcers.
  > Naropin (ropivacaine) is used as a long-acting local anaesthetic for surgical anaesthesia and acute pain management.
  > Xylocaine (lidocaine) is a widely used, short-acting local anaesthetic for topical and regional anaesthesia.
  > EMLA (lidocaine and prilocaine) is used as a local anaesthetic for topical application to prevent pain associated with injections and superficial surgical procedures.

 

  1   Licensed from Pozen.
 

 

Our financial performance

 

    World     US     Western Europe     Established ROW     Emerging Markets     Prior year  

2012

  Sales
$m 		    Reported
growth
% 		    CER
growth
% 		    Sales
$m 		    Reported
growth
% 		    Sales
$m 		    Reported
growth
% 		    CER
growth
% 		    Sales
$m 		    Reported
growth
% 		    CER
growth
% 		    Sales
$m 		    Reported
growth
% 		    CER
growth
% 		   

World
Sales

$m

 

Seroquel XR

    1,509        1        4        811        4        446        (9     (2     97        9        10        155        17        27        1,490   

Seroquel IR

    1,294        (70     (70     697        (79     226        (59     (56     202        (11     (12     169        (23     (20     4,338   

Local Anaesthetics

    540        (10     (7            (100     201        (17     (11     206                      133        (8     (4     602   

Diprivan

    291        (1     2               (100     32        (24     (19     78        (6     (6     181        15        19        294   

Zomig

    182        (56     (54     12        (92     103        (41     (37     55        (19     (19     12        (8     8        413   

Vimovo

    65        91        97        25        19        19        217        233        14        133        133        7        n/m        n/m        34   

Others

    42        30        36        16        n/m        11        (35     (29     1        (33     (33     14        17        25        33   

Total

    3,923        (46     (44     1,561        (64     1,038        (32     (27     653        (4     (4     671        (1     4        7,204   
                             

2011

                                                                                         

Seroquel XR

    1,490        29        27        779        22        490        36        30        89        46        34        132        40        41        1,154   

Seroquel IR

    4,338        5        3        3,344        8        546        (3     (8     228        2        (8     220        (15     (17     4,148   

Local Anaesthetics

    602               (6     10        (66     242        (9     (13     205        10               145        16        13        605   

Diprivan

    294        (9     (13     12        (73     42        (16     (20     83        9        1        157        4        (1     322   

Zomig

    413        (4     (7     158        (10     174        1        (4     68        (1     (9     13        18        9        428   

Vimovo

    34        n/m        n/m        21        n/m        6        n/m        n/m        6        n/m        n/m        1        n/m        n/m        5   

Others

    33        (21     (24     1               17        (37     (41     3                      12        9        9        42   

Total

    7,204        7        5        4,325        8        1,517        6        1        682        10        1        680        5        2        6,704   

For a detailed narrative explanation of the financial performance of our products please see the Geographical Review from page 70.

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   61

Table of Contents

Performance | Therapy Area Review

 

 

LOGO

 

There is still significant unmet medical need in the areas of chronic pain, cognitive disorders and other serious central nervous system disorders.

Our aim is to strengthen our position in neuroscience through our experience with Seroquel XR and to discover and develop new drug candidates with meaningful therapeutic advantages, primarily in Alzheimer’s disease, neuropathic pain control and depression. Many of these débilitating illnesses have no effective treatments and, for others, current therapies are poorly effective, leaving major unmet medical need.

Rapid progress is being made in understanding diseases of the brain, driven by technological advances in fields including genetics, cell biology, imaging and informatics. However, despite these advances there have been very few novel treatments delivered during the last 10 to 15 years and it is clear that a new way of working is required which captures advances in neuroscience and harnesses them through the drug development life-cycle.

AstraZeneca responded in 2012 by creating a new neuroscience Innovative Medicines Unit (Virtual iMed) made up of a team of approximately 40 scientists conducting discovery and development externally, through a network of partners in academia and industry. The team is based in Cambridge, Massachusetts, US and Cambridge, UK. The locations are strongly associated with neuroscience research and the team works closely with partners such as the Karolinska Institute in Sweden. The Virtual iMed is designed to be flexible, independent and lean in its structure. Scientists are empowered to make decisions quickly.

The team is focused on target identification to Proof of Concept studies, with high level focus on personalised medicine and innovative approaches to early clinical development. The Virtual iMed is designed to bring together scientific advances of the biotechnology and academic world and to develop their potential through the scientific, commercial and geographical reach of AstraZeneca.

We will consider any treatments for psychiatric, neurological or analgesic disorders affecting the central or peripheral nervous system which have a solid scientific basis, a high probability to deliver meaningful new medicines to patients, and will provide an acceptable return on investment. We will be looking at indications that affect smaller numbers of patients. We will focus on selected populations of patients whose disease biology makes them ideally suited for a particular treatment and we will test our therapeutic candidates in those populations first. Where treatments show promise in such selected patient groups, we will include a broader range of patients with the same disease or other disease states that might benefit from the approach. For example, a treatment that works on a fundamental disease process in neurons that eventually causes neurodegeneration might be best examined initially in patients with Huntington’s disease. That same therapy could be as well suited for Parkinson’s disease, amyotrophic lateral sclerosis (ALS) or other disorders.

Neurology

Alzheimer’s disease remains one of the largest areas of unmet medical need. Product development in this therapy area is particularly difficult due in part to the challenges of establishing efficacy in clinical studies. Current treatments, which doctors consider inadequate, target the symptoms, not the underlying cause, of the disease. Most, if not all, marketed treatments will face patent expiry by 2015. Disease modification, delivered through biologics and/or small molecule treatments, is clearly the hope for Alzheimer’s disease patients and for patients with other neurodegenerative disorders such as Parkinson’s disease. Combined with better diagnostics, disease modifiers in both areas are expected to allow for earlier intervention and better clinical outcomes. Unfortunately, the first wave of disease modifiers is still several years away.

In the pipeline

Alzheimer’s disease is defined and characterised by the presence of the protein amyloid beta (Abeta) deposits in the brain. Present understanding of the pathophysiology of Alzheimer’s disease suggests that alterations in Abeta production, distribution or aggregation lead to Abeta deposition which in turn impacts neuronal viability and function. A second protein altered in Alzheimer’s disease is tau. Our portfolio comprises small molecule and biologic projects addressing both tau and amyloid, as well as exploring new mechanisms based on the developments in disease understanding.

Our research pipeline is also exploiting opportunities presented by emerging biologic therapies and contains projects directed at modulating protein accumulation and signalling for a number of neurodegenerative diseases. In addition, the continued progress of technology platforms directed at facilitating the transport of macromolecules into the central nervous system compartment may provide benefits to patient health.

 

 

62   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

 

LOGO

 

Through our collaborations with the Karolinska Institute in Sweden, the Banner Alzheimer’s Institute in the US, the National Institute of Radiological Sciences in Japan and others, our R&D capabilities in positron emission tomography (PET) imaging of the human brain continues to progress. AstraZeneca’s amyloid PET ligands may enable us to detect Alzheimer’s disease early and to assess drug effects in Alzheimer’s disease. We have discovered and taken into patient studies one F-18 and two C-11 amyloid PET ligands which are being developed as research biomarkers.

A new alliance involving several academic centres, named A5, is a novel, open-architecture alliance with four leading academicians that was launched in July to investigate potential new Alzheimer’s disease treatments. The initiative is focused on the role of apoliprotein E (ApoE) in Alzheimer’s disease. ApoE is considered second only to age as a risk factor for the development of Alzheimer’s disease. Drug discovery efforts involving ApoE have been hampered by challenging biology and a lack of suitable in vivo models. In addition to ApoE, the A5 alliance will focus on identification, validation and risk reduction of other drug targets for treatment of Alzheimer’s disease.

Psychiatry

Globally, more than 350 million people of all ages suffer from depression (WHO 2012). Despite this, psychiatric illness remains under-detected, under-diagnosed and under-treated, and current treatments leave substantial unmet medical need. Three National Institute of Mental Health sponsored effectiveness studies in the US have reported treatment response rates in depression, bipolar disorder and schizophrenia to be less than 50%, with low (around 30%) rates of remission and poor compliance. Clear opportunities exist for novel approaches targeting defined patient sub-groups not adequately treated with current generic broad spectrum agents.

Our 2012 focus

Seroquel XR has been approved in 85 countries for schizophrenia, 81 countries for bipolar mania, 72 countries for bipolar depression, 61 countries for bipolar maintenance, 65 countries for major depressive disorder (MDD) and nine countries for generalised anxiety disorder.

Patents protecting Seroquel XR have been subject to a number of challenges in different jurisdictions. In some cases, the patents have been found to be invalid. Details of these matters are included in Note 25 to the Financial Statements from page 184.

In March 2012, top-line results from the remaining Phase III studies investigating efficacy, tolerability and safety of TC-5214, as an adjunct therapy to an anti-depressant in patients with MDD who did not respond adequately to initial anti-depressant treatment, were released. RENAISSANCE 4 and RENAISSANCE 5, both of which are efficacy and tolerability studies, did not meet the primary endpoint of change on the Montgomery-Asberg Depression Rating Scale total score after eight weeks of adjunct treatment with TC-5214 as compared to placebo. These studies conclude the RENAISSANCE programme for TC-5214. Based on the totality of the results, AstraZeneca and Targacept decided not to pursue a regulatory filing for TC-5214 as an adjunct treatment for patients with MDD. We terminated the TC-5214 collaboration with Targacept, with all rights and licences granted under the licence agreement reverting to Targacept.

In the pipeline

AZD6765, a low-trapping NMDA (N-methyl-D-aspartate) channel blocker to address the needs of patients with severe treatment-refractory depression, has progressed into Phase IIb development. Phase IIa results presented in December demonstrated anti-depressant efficacy following single and repeated intravenous infusions in patients who have shown inadequate response to multiple oral therapies. An ongoing Phase IIb study is designed to establish a chronic treatment regimen in this difficult to treat patient population. Additional early-stage research programmes are also focusing on this area.

Analgesia and anaesthesia

The small number of currently approved products in the neuropathic pain market will come off patent between 2014 and 2017. However, few new products are in development and the unmet medical need for improvements in both efficacy and tolerability is such that the market remains highly attractive. In Asia, neuropathic pain drugs are gaining approval, shifting cultural and medical treatment barriers. The chronic nociceptive pain market, including osteoarthritis and chronic low back pain, is steadily growing due to ageing populations combined with longer life expectancy across all regions, including Asia.

Opioids are considered the gold standard for efficacy for moderate to severe pain across pain segments. However, opioid pain control comes with unwanted side effects such as bowel dysfunction. There remains a high unmet medical need for products that enable continued opioid pain control by reducing or eliminating side effects.

 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   63

Table of Contents

Performance | Therapy Area Review

 

 

LOGO

 

Biologics are an emerging treatment option for pain control and this is an area in which we have an active interest.

It is believed that advances in the understanding of the mechanisms which lead to neuropathic pain will allow for improved patient segmentation and potential increases in the success rate of drug development. We are exploring smaller treatments in focused pain areas where patients can be selected on the basis of symptomatic characteristics within the overall development and regulatory approach.

Our 2012 focus

Vimovo , 375/20-500/20mg delayed-release tablets, co-developed by AstraZeneca and Pozen, is a fixed-dose combination of enteric-coated naproxen (an NSAID), and immediate-release esomeprazole, a stomach acid-reducing proton pump inhibitor (PPI). Vimovo is generally approved for symptomatic relief in the treatment of rheumatoid arthritis, osteoarthritis and ankylosing spondylitis in patients at risk of developing NSAID-associated gastric and/or duodenal ulcers. Vimovo is also indicated for treatment in patients where lower doses of naproxen or of other NSAIDs are not considered sufficient.

Following FDA approval in April 2010, Vimovo launched in the US in July 2010. In October, Vimovo received positive agreement for approval in 23 European member states.

In the pipeline

Naloxegol (formerly NKTR-118), licensed from Nektar Therapeutics, is a once daily, oral, peripherally acting opioid receptor antagonist under investigation for treatment of opioid-induced constipation (OIC) as a side effect of prescription opioid pain medication. Positive top-line results from two Phase III trials and one safety extension trial in patients with non-cancer related pain and OIC, a common side effect of prescription opioids, were announced in November. Additional analyses and regulatory consultations are ongoing.

Our research pipeline is exploring biologic therapies and contains projects directed at modulating afferent signalling, inflammation associated with pain, and the interplay between the immune and nervous systems. Projects are directed at targeting well-defined patient segments, with subset selection based on, for example, an increase in particular inflammatory markers in osteoarthritis and pancreatitis. We continue to focus on areas of high unmet medical need, and thus, in addition to osteoarthritis, we are also active in researching novel therapies for neuropathic pain. Efforts to access targets in the central nervous system compartment, such as the spinal cord and the brain, continue to be facilitated by solid progression of technology platforms designed to transport biologics from the periphery to the central nervous system compartment.

 

 

 

LOGO

 

64   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

LOGO

 

 

LOGO

Therapy area world market

(MAT/Q3/12) ($bn)

 

LOGO

LOGO

 

LOGO

Our marketed products

  > Arimidex (anastrozole) is an aromatase inhibitor used for the treatment of breast cancer.
  > Zoladex (goserelin acetate implant), in one and three month depots 1 , is a luteinising hormone-releasing hormone (LHRH) agonist used for the treatment of prostate cancer, breast cancer and certain benign gynaecological disorders.
  > Casodex (bicalutamide) is an anti-androgen therapy used for the treatment of prostate cancer.
  > Iressa (gefitinib) is used as an epidermal growth factor receptor-tyrosine kinase (EGFR-TK) inhibitor that acts to block signals for cancer cell growth and survival in advanced non-small cell lung cancer.
  > Faslodex (fulvestrant) is an injectable oestrogen receptor antagonist used for the treatment of hormone receptor-positive metastatic breast cancer for post-menopausal women whose disease has progressed following treatment with prior endocrine therapy.
  > Nolvadex (tamoxifen citrate) remains a widely used breast cancer treatment outside the US.
  > Caprelsa (vandetanib) is a kinase inhibitor indicated for the treatment of symptomatic or progressive medullary thyroid cancer (MTC) in patients with unresectable (non-operable) locally advanced or metastatic disease.

 

  1 Depots are subcutaneous or intra-muscular injections.
 

 

Our financial performance

 

    World     US     Western Europe     Established ROW     Emerging Markets     Prior year  

2012

  Sales
$m 		    Reported
growth
% 		    CER
growth
% 		    Sales
$m 		   

Reported

growth

%

    Sales
$m 		    Reported
growth
% 		    CER
growth
% 		    Sales
$m 		   

Reported

growth

%

   

CER

growth

%

    Sales
$m 		   

Reported

growth

%

   

CER

growth

%

   

World
sales

$m

 

Zoladex

    1,093        (7     (5     24        (38     221        (16     (12     448        (9     (9     400        4        9        1,179   

Faslodex

    654        20        24        310        17        186        (4     4        62        n/m        n/m        96        16        27        546   

Iressa

    611        10        12               (100     142        12        20        222        9        9        247        12        12        554   

Arimidex

    543        (28     (26     21        (50     124        (52     (49     279        (9     (9     119        (18     (16     756   

Casodex

    454        (17     (16     (3     n/m        51        (36     (31     301        (17     (17     105        (6     (4     550   

Others

    134        13        15        25        108        17        31        46        63                      29        (6     (3     120   

Total

    3,489        (6     (3     377        7        741        (21     (15     1,375        (4     (4     996        2        6        3,705   
                             

2011

                                                                                         

Zoladex

    1,179        6        3        39        (15     262        (5     (9     494        10               384        12        18        1,115   

Faslodex

    546        58        55        264        71        193        56        48        6        n/m        n/m        83        30        28        345   

Iressa

    554        41        32        2        (50     127        159        147        204        12        2        221        40        34        393   

Arimidex

    756        (50     (53     42        (91     260        (55     (56     308        7        (2     146        (3     (6     1,512   

Casodex

    550        (5     (12     (6     (138     80        (29     (33     364        5        (5     112        9        7        579   

Others

    120        19        12        12        71        13        18        18        64        10               31        24        20        101   

Total

    3,705        (8     (12     353        (51     935        (19     (22     1,440        8        (1     977        16        16        4,045   

For a detailed narrative explanation of the financial performance of our products please see the Geographical Review from page 70.

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   65

Table of Contents

Performance | Therapy Area Review

 

LOGO

 

We aim to build on our position as one of the world leaders in cancer treatment with established brands such as Zoladex and Arimidex and growing brands such as Faslodex and Iressa.

 

Our future growth will be driven through targeting the right treatments, both small molecules and biologics, to the right patients, using companion diagnostics where appropriate. This approach is driving the growth of Iressa and is a key focus in the development of our early stage portfolio.

 

Our 2012 focus

Arimidex , first launched in 1995, remains a leading global hormonal therapy for patients with early breast cancer. This success is largely based on the extensive long-term efficacy and safety results of the ATAC study, which showed Arimidex to be significantly superior to tamoxifen at preventing breast cancer recurrence during and beyond the five year treatment course.

 

Zoladex , a luteinising hormone-releasing hormone (LHRH) agonist, is approved in 120 countries for the treatment of prostate cancer, breast cancer and certain benign gynaecological disorders. In non-metastatic prostate cancer, Zoladex has been shown to improve overall survival, both when used in addition to radical prostatectomy and when used in addition to radiotherapy. In breast cancer, Zoladex is widely approved for use in advanced breast cancer in pre-menopausal women. In a number of countries, Zoladex is also approved for the adjuvant treatment of early stage pre-menopausal breast cancer as an alternative to and/or in addition to chemotherapy. Zoladex offers proven survival benefits for breast cancer patients with a favourable tolerability profile.

 

Casodex and Zoladex are both leading endocrine therapies for the treatment of prostate cancer. Casodex is used as a 50mg tablet for the treatment of advanced prostate cancer and as a 150mg tablet for the treatment of locally advanced prostate cancer.

 

Iressa is approved in 89 countries and is one of the leading epidermal growth factor receptor-tyrosine kinase (EGFR-TK) inhibitors in Japan and the Asia Pacific region where it is marketed for pre-treated advanced non-small cell lung cancer

 

(NSCLC). Outside the EU, indications are being sought or expanded from the pre-treated setting to include 1 st line patients whose tumours harbour activating mutations of the epidermal growth factor receptor (EGFR). In the EU, Iressa is the first personalised medicine for the treatment of adults with locally advanced or metastatic NSCLC with activating mutations.

 

Faslodex 500mg is now approved in 65 countries including the member states of the EU, the US and Japan. It offers an additional, efficacious, hormonal therapy option for patients with hormone-receptor positive advanced breast cancer. It is given by once monthly injections and is approved for the treatment of hormone-receptor positive advanced breast cancer in post-menopausal women whose disease has progressed following treatment with a prior endocrine therapy. We are now exploring the efficacy and safety of Faslodex 500mg compared to Arimidex in the 1 st line advanced breast cancer setting (hormone-naïve patients) in the Phase III FALCON trial.

 

Caprelsa fights cancer through two proven mechanisms: blocking the development of tumour blood supply by inhibition of the vascular endothelial growth factor pathway and by inhibiting the growth and survival of the tumour through EGFR and rearranged during transfection (RET) pathways. Caprelsa was approved by the FDA and granted Orphan Drug status in April 2011, and was approved in the EU in February 2012 for the treatment of medullary thyroid cancer (MTC) in patients with unresectable locally advanced or metastatic disease. Caprelsa is also approved in Canada and remains under review by other regulatory agencies around the world.

 

In the pipeline

Our early oncology pipeline includes a range of novel compounds that target signalling pathways believed to be pivotal in cancer cell growth and survival as well as DNA repair mechanisms. Despite set-backs in earlier Phase II trials, olaparib, a poly ADP-ribose polymerase (PARP) inhibitor, continues in Phase II trials in relapsed ovarian cancer, gastric cancer and germline BRCA mutation positive cancers. Olaparib has been approved to begin Phase III in 2013 pending the results of ongoing trials.

 

Selumetinib, a potent mitogen-activated protein kinase (MEK) inhibitor licensed from Array BioPharma, Inc., continues in Phase II development.

 

We are also developing potential new cancer drugs using a variety of biologics approaches. Our investigational biologics are directed towards molecular targets with a strong role in cancer progression and incorporate innovative technologies, providing the potential to eliminate cancer cells in more effective ways. Within biologics, we continue to progress a discovery and clinical pipeline that is balanced across different anti-tumour approaches, including disrupting cancer cells’ ability to grow or communicate (growth factor and survival signalling), modulating the blood supply that tumours need to grow (vascular modulation) and activating a patient’s own immune system to eliminate cancer cells (immune-mediated therapy).

 

We currently have five investigational biologics in Phase I clinical trials and four in Phase II clinical trials. Additional drug candidates are expected to progress into clinical trials in 2013. Moxetumomab is a monoclonal antibody approved to begin Phase III testing in hairy cell leukemia in 2013.

 

  LOGO

 

 

66   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

LOGO

LOGO

Therapy area world market

(MAT/Q3/12) ($bn)

 

LOGO

 

LOGO

 

LOGO

Our marketed products

  > Symbicort pMDI (budesonide/formoterol in a pressurised metered-dose inhaler) is a combination of an inhaled corticosteroid and a fast onset, long-acting beta 2 -agonist used for maintenance treatment of asthma and chronic obstructive pulmonary disease (COPD), including chronic bronchitis and emphysema in the US.
  > Symbicort Turbuhaler (budesonide/ formoterol in a dry powder inhaler) is a combination of an inhaled corticosteroid and a fast onset, long-acting beta 2 -agonist used for maintenance treatment of asthma and COPD. In asthma, it is also approved for Maintenance And Reliever Therapy (SMART). Symbicort Turbuhaler is used in most parts of the world outside the US.
  > Pulmicort Turbuhaler (budesonide in a dry powder inhaler) is an inhaled corticosteroid used for maintenance treatment of asthma.
  > Pulmicort Respules (budesonide inhalation suspension) is a corticosteroid administered via a nebuliser for the treatment of asthma in both children and adults.
  > Rhinocort (budesonide) is a nasal steroid used as a treatment for allergic rhinitis (hay fever), perennial rhinitis and nasal polyps.
  > Oxis Turbuhaler (formoterol in a dry powder inhaler) is a fast onset, long-acting beta 2 -agonist used for the treatment of bronchial-obstructive symptoms in asthma and COPD.
  > Accolate (zafirlukast) is an oral leukotriene receptor antagonist used for the treatment of asthma.
 

 

Our financial performance

 

    World     US     Western Europe     Established ROW     Emerging Markets     Prior year  

2012

  Sales
$m 		    Reported
growth
% 		    CER
growth
% 		    Sales
$m 		    Reported
growth
% 		    Sales
$m 		    Reported
growth
%% 		   

CER

growth

    Sales
$m 		    Reported
growth
% 		    CER
growth
% 		    Sales
$m 		    Reported
growth
% 		    CER
growth
% 		   

World
sales

$m

 

Symbicort

    3,194        1        5        1,003        19        1,313        (8     (3     443        6        7        435        (3     3        3,148   

Pulmicort

    866        (3     (1     233        (16     156        (17     (12     127        1        1        350        17        19        892   

Rhinocort

    177        (17     (14     55        (26     28        (24     (19     17        (15     (15     77        (5     (1     212   

Others

    178        (17     (14     10        25        92        (16     (11     23        4        4        53        (30     (28     216   

Total

    4,415        (1     2        1,301        8        1,589        (10     (5     610        4        5        915        1        5        4,468   
                             

2011

                                                                                         

Symbicort

    3,148        15        11        846        17        1,434        5               418        46        35        450        21        19        2,746   

Pulmicort

    892        2               279        (9     189        (12     (16     126        11        2        298        25        23        872   

Rhinocort

    212        (7     (9     74        (20     37        (5     (10     20        25        13        81        3               227   

Others

    216        (15     (19     8        (80     109        (8     (13     23        5               76        4        1        254   

Total

    4,468        9        6        1,207        4        1,769        2        (3     587        34        24        905        19        17        4,099   

For a detailed narrative explanation of the financial performance of our products please see the Geographical Review from page 70.

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   67

Table of Contents

Performance | Therapy Area Review

 

LOGO

 

We aim to build on our strong position in the respiratory and inflammation area through the growth of key products, with new indications and market launches, including chronic obstructive pulmonary disease (COPD), as well as through developing a strong pipeline of novel small molecule and biologics approaches to COPD and asthma.

We aspire to enter the rheumatology market through our biologics pipeline and targeted small molecule approaches such as fostamatinib. With our acquisition of Ardea we have expanded our inflammation focus to include gout.

COPD and asthma

According to WHO, COPD, a serious lung disease that includes chronic bronchitis and/or emphysema, is currently the fourth leading cause of death worldwide, with future increases anticipated. Current treatment has recently demonstrated the potential for some survival benefit but the impact of medication on the course of the disease is small and the prognosis of the COPD patient remains poor. In asthma, unmet medical need for patients whose asthma is inadequately controlled by current treatments remains an important issue and disease normalisation is currently not optimally achieved by any approved treatment.

The typical treatment for both COPD and asthma is a fixed-dose combination of an inhaled corticosteroid (ICS) with a long-acting beta 2 -agonist (LABA) (for example Symbicort ) or for COPD specifically, an inhaled long-acting muscarinic antagonist as either monotherapy or adjunctive to ICS/LABA treatment. Other major asthma treatments include monotherapy ICSs, oral leukotriene receptor antagonists and/or oral steroids for severe disease and (in combination with antibiotics) for exacerbations, as well as a MAb targeting allergic asthma for moderate to severe asthma patients. Over recent years, studies employing patient-centric tools, such as the asthma control questionnaire, have revealed surprisingly low asthma control at all severities, highlighting an underestimated medical need.

Our 2012 focus

Symbicort improves symptoms and provides a clinically important improvement in the health of many patients with either asthma or COPD by providing effective and rapid control of the symptoms.

Symbicort pMDI is indicated in the US for the treatment of asthma in patients 12 years of age and older. The COPD indication was approved and launched in the US in early 2009. In June 2010, the US Prescribing Information was updated to include the FDA’s new recommendations for appropriate use of asthma medications containing LABAs. The class label changes for all LABA-containing products are specific to the treatment of asthma and do not apply to the treatment of COPD.

Symbicort Turbuhaler was originally launched in markets outside the US in 2000 and in Japan in 2010 for the treatment of adult asthma and is co-promoted in Japan with Astellas Pharma, Inc. The COPD indication and the SMART treatment regimen were approved in Japan in 2012.

Symbicort SMART (Symbicort Maintenance And Reliever Therapy) provides improved asthma control including less risk for exacerbations relative to comparators and simplifies asthma management through the use of only one inhaler for both maintenance and relief of asthma symptoms. As well as being a cost-effective treatment, the Symbicort SMART approach reduces the usage of both inhaled and oral corticosteroids compared to other treatment options.

Pulmicort is one of the world’s leading inhaled corticosteroids for the treatment of asthma and is available in several forms. Teva has had an exclusive licence to sell a generic version of Pulmicort Respules in the US since 2009. Pulmicort continues to face increasing challenge from generic products. Patents protecting Pulmicort have been subject to a number of challenges in different jurisdictions. Details of these matters are included in Note 25 to the Financial Statements from page 184.

Clinical studies

In April 2012, the FDA provided AstraZeneca with a Post-marketing Requirement for a Symbicort LABA safety study, designed to be pooled with similar studies with other

LABA products. AstraZeneca is required to conduct a trial comparing Symbicort Inhalation Aerosol with Pulmicort to evaluate the risk of serious asthma outcomes (hospitalisations, intubation, death) in 11,700 adult and adolescent patients. Recruitment in the trial is ongoing.

In the pipeline

Building on our capabilities in combinations and inhaler device development demonstrated through our experience with Symbicort , we are aiming to further improve the mainstay of treatment for COPD patients by combining bronchodilators, being developed in collaboration with Pulmagen Therapeutics (Synergy) Limited, with inhaled anti-inflammatory compounds such as inhaled selective glucocorticoid receptor agonists (AZD5423, which continues in Phase II), being developed in collaboration with Bayer Schering Pharma AG. Additionally, we are targeting inflammation in COPD using oral routes of administration with AZD5069, a CXCR2 antagonist that targets neutrophils which is in Phase II. MEDI8968, an anti-interleukin-IL-1 receptor MAb, and benralizumab, an anti-interleukin-5 receptor MAb, are both in Phase II development for severe to very severe COPD.

We are targeting uncontrolled asthma focusing on reducing the rate of annual asthma exacerbations through small molecule approaches such as a CRTh2 receptor antagonist and toll-like receptor 7 agonists (being developed in collaboration with Dainippon Sumitomo). Biological treatments in Phase IIb include benralizumab and tralokinumab, a MAb that targets interleukin-13. Also, in Phase II, brodalumab is an anti-interleukin-17 receptor MAb (being developed in collaboration with Amgen) for asthma.

In April 2012, AstraZeneca and Amgen agreed to jointly develop and commercialise five MAbs from Amgen’s clinical inflammation portfolio including brodalumab. The collaboration will provide Amgen with additional resources to optimally progress its portfolio, and Amgen will benefit from the strong respiratory, inflammation and asthma development expertise of AstraZeneca’s biologics capabilities. The collaboration will also capitalise on AstraZeneca’s global commercial reach in respiratory and gastrointestinal diseases.

 

 

68   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

LOGO

 

Rheumatology and

gout     

 

Rheumatoid arthritis is currently treated with generic disease-modifying anti-rheumatic agents and, where the relevant criteria are met, biologic disease-modifiers. There remains a need for novel effective treatments since only about a third of patients treated with biologics achieve their treatment goals. We anticipate that the rheumatoid arthritis market will experience modest annual growth over the next decade. Sales of the biologic tumour necrosis factor (TNF) alpha blockers accounted for 72% of major market rheumatoid arthritis sales in 2012. Use of other biologic approaches is expected to increase due to new entrants, new subcutaneous formulations and use earlier in the treatment pathway. Novel oral drugs targeting intra-cellular signalling pathways may provide anti-TNF-like levels of efficacy and potentially more convenient dosing, especially in patients who currently are not taking or are ineligible to take injectable biologic agents.

 

Current treatment of systemic lupus erythematosus (SLE) focuses on suppressing symptoms and controlling disease flares, and in the case of lupus nephritis preventing renal failure. Although a biologic has recently been launched for SLE, significant unmet medical need remains. Most emerging biologic agents are likely to be used initially after failure of standard therapies (including corticosteroids and immunosuppressants) or in combination in order to provide incremental benefit, prevent flares and allow reduction of high-dose chronic steroid use.

 

Gout is a chronic, painful, debilitating arthritis caused by elevated serum uric acid due to overproduction and/or under excretion of uric acid. Gout is the second most common arthritis after osteoarthritis and is the most common form of arthritis in men over 40.

 

In the pipeline

Fostamatinib was in-licensed from Rigel Pharmaceuticals, Inc. in 2010. Fostamatinib is a potential first-in-class oral spleen tyrosine kinase (SYK) inhibitor being evaluated for a rheumatoid arthritis indication. It is thought to block reversible signalling in multiple cell types involved in inflammation and tissue degradation

   in rheumatoid arthritis. The
ongoing Phase III programme,
called OSKIRA, commenced in
September 2010. In the Phase
IIb dose finding study
OSKIRA-4, fostamatinib as a
monotherapy met the first
primary objective showing a
statistically significant superior
DAS28 score change from
baseline compared to placebo
at six weeks at the 100mg twice
daily dose and the 100mg twice
daily for a month followed by
150mg once daily dose, but not
at the 100mg twice daily for a
month followed by 100mg once
daily dose. The OSKIRA-4
study did not meet its second
primary objective as all
fostamatinib monotherapy
doses were inferior to
adalimumab monotherapy at
week 24 based on DAS28. The
safety and tolerability findings
for fostamatinib as reported in
the OSKIRA-4 study were
generally consistent with those
previously observed in the
TASKi Phase II programme.
Results from the ongoing Phase
III OSKIRA programme are
anticipated in the first half of
2013 and would form the basis
of regulatory submissions.

 

In June, AstraZeneca acquired
Ardea, a San Diego, California-
based biotechnology company
focused on the development of
small molecule therapeutics.
Ardea’s clinically most
advanced product candidate,
lesinurad (formerly known as
RDEA594), is currently in Phase
III development. Lesinurad is a
selective inhibitor of URAT1, a
transporter in the proximal
tubule cells of the kidney that
regulates uric acid excretion
from the body. The Phase III
programme is exploring
lesinurad as an oral, once daily
treatment for the chronic
management of hyperuricaemia
in patients with gout. Regulatory
filings are planned in the US
and Europe for the first half of
2014. We also plan to develop
and commercialise lesinurad in
China and Japan.

 

 

 

   In 2012, we continued to invest in
several novel multi-functional MAbs in
inflammatory and autoimmune
conditions. Sifalimumab, which targets
interferon-alpha, continued clinical
development with an ongoing Phase IIb
study in patients with SLE. MEDI-546,
which targets the Type I IFN receptor,
continued in a Phase IIb study in
patients with SLE. Mavrilimumab, which
targets the alpha sub-unit of the
granulocyte-macrophage colony
stimulating factor receptor, continues in
Phase IIb for patients with rheumatoid
arthritis.

 

Dermatology

 

Psoriasis is a chronic disease in which
the immune system causes the skin
cells to grow at an accelerated rate.
Instead of being shed, the skin cells
pile up, causing painful and itchy, red,
scaly patches that can bleed. Up to
12 million patients are diagnosed with
psoriasis across the US and Europe
each year. Despite various treatment
options for moderate to severe plaque
psoriasis, many patients do not meet
their therapeutic goals including
resolution of underlying inflammation,
clearing of symptoms and improving
quality of life. Biologics are currently
used in moderate to severe patients
who are candidates for, or are
unresponsive to, phototherapy or
systemic therapy.

 

In the pipeline

As mentioned previously, in 2012
AstraZeneca and Amgen entered into
an agreement to jointly develop
brodalumab, which has commenced
Phase III development in patients with
moderate to severe plaque psoriasis. In
addition, brodalumab is being
considered in a Phase IIb development
programme in psoriatic arthritis.

   LOGO  

 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   69

Table of Contents

Performance | Geographical Review

 

LOGO

 

2012 in brief

> In the US, sales were down 21% to $10,655 million (2011: $13,426 million; 2010: $13,727 million). Loss of exclusivity on Seroquel IR in March 2012 as well as the impact of increased generic competition experienced by our other mature brands was partially offset by strong performance from our key brands, Brilinta, Crestor, Onglyza, Symbicort and Faslodex .
> AstraZeneca is the fourth largest pharmaceutical company in the US, with a 5% market share of US pharmaceuticals by sales value.
> AstraZeneca is the eighth largest prescription-based pharmaceutical company in Western Europe, with a 3.4% market share of sales by value.
> Sales in Western Europe were down 19% to $6,486 million (2011: $8,501 million; 2010: $9,168 million). Key drivers of the decline were the volume erosion on Atacand, Seroquel IR, Nexium, Arimidex and Meronem , following entry of generic competition and the negative price and volume impact primarily related to government interventions, particularly in Greece, Italy, Portugal and Spain. This development was partially offset by revenue growth from Brilique, Onglyza, Vimovo and Iressa .
> Established ROW sales were down 14%. The entry of generic competition of Crestor in Canada, and Seroquel IR and Arimidex in Australia was partially offset by the successful first full year of launch of Nexium and Faslodex in Japan.
> Emerging Markets sales increased by 4% to $5,752 million (2011: $5,763 million; 2010: $5,198 million) with sales growth in China of 17% and also in Russia of 17%.

2011 in brief

> In the US, sales were down 2% to $13,426 million (2010: $13,727 million). The pricing impact from US healthcare reform measures lowered revenue by around 3.3%. Good growth for Crestor , the Seroquel franchise, Symbicort and Onglyza , broadly offset the impact of generic competition for Arimidex, Toprol-XL and Merrem , and declines in Nexium .
> Sales in Western Europe were down 11% to $8,501 million (2010: $9,168 million), due largely to volume erosion on Nexium, Arimidex and Meronem . This was partially offset by volume growth attributable to Crestor , Seroquel XR , Symbicort , Iressa and Faslodex .
> Established ROW sales were up 4%, driven by continued growth of Symbicort , Crestor , Nexium and the Seroquel franchise. In 2011, AstraZeneca became the largest research-based pharmaceutical company in Canada by sales value.
> Emerging Markets sales increased by 10% to $5,763 million (2010: $5,198 million), with sales growth in China of 15% and Russia of 19%. Sales in Brazil were down as a result of generic competition for Crestor and Seroquel IR .

For more information regarding our products, see the Therapy Area Review from page 50. Details of material legal proceedings can be found in Note 25 to the Financial Statements from page 184

 

and details of relevant risks are set out in the Principal risks and uncertainties section from page 75. See the Market definitions table on page 209 for information about AstraZeneca’s market definitions. Sales figures in this Geographical Review are with reference to the customers’ location.

US

AstraZeneca is the fourth largest pharmaceutical company in the US, with a 5% market share of US pharmaceuticals by sales value.

Sales in the US decreased by 21% to $10,655 million (2011: $13,426 million; 2010: $13,727 million), as strong performance from our key brands, Brilinta , Crestor , Onglyza , Symbicort and Faslodex , was offset by loss of exclusivity on Seroquel IR in March 2012 as well as the impact of increased generic competition experienced by our other mature brands. Combined sales of our key brands, Brilinta , Crestor , Onglyza , Symbicort and Faslodex , were up by 9% to $4,733 million (2011: $4,351 million; 2010: $3,569 million). Other drivers of the sales decline include the reduction of sales for Zomig following the licensing of Zomig to Impax Pharmaceuticals Inc. in February 2012 down to $12 million (2011: $158 million; 2010: $176 million), additional generic competition affecting sales of Toprol-XL down to $320 million (2011: $404 million; 2010: $689 million), and loss of exclusivity of Atacand down to $150 million (2011: $182 million; 2010: $216 million).

Brilinta achieved sales of $19 million. Commercial preferred unrestricted managed markets access was 54%

 

 

Our financial performance

 

     2012     2011     2010  
    

Sales

$m

     Reported
growth
% 		    CER
growth
% 		    Sales
$m 		     Reported
growth
% 		    CER
growth
% 		    Sales
$m 		 

US

     10,655         (21     (21     13,426         (2     (2     13,727   

Western Europe

     6,486         (24     (19     8,501         (7     (11     9,168   

Canada

     1,090         (32     (31     1,604         6        1        1,510   

Japan

     2,904         (5     (5     3,064         17        6        2,617   

Other Established ROW

     1,086         (12     (12     1,233         18        4        1,049   

Established ROW

     5,080         (14     (14     5,901         14        4        5,176   

Emerging Europe

     1,165         (6     2        1,244         7        7        1,165   

China

     1,512         20        17        1,261         20        15        1,047   

Emerging Asia Pacific

     923         (5     (3     968         9        5        890   

Other Emerging ROW

     2,152         (6            2,290         9        12        2,096   

Emerging Markets

     5,752                4        5,763         11        10        5,198   

Total

       27,973         (17     (15       33,591         1        (2       33,269   

 

70   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

LOGO

 

and trial among target interventional cardiologist initiators was 39% at the end of 2012. Crestor demonstrated resilience in the face of the November 2011 market entry of a generic version and, from May, multiple generic versions of atorvastatin, all competitors of Crestor. Crestor’s performance volume showed resilience in two of the largest and most profitable segments of the market, Commercial and Medicare. Crestor’s existing patient base remained solid, and continuing patients represented 94% of Crestor’s volume. Crestor achieved sales of $3,164 million (2011: $3,074 million; 2010: $2,640 million) and a total prescription share of 11.8% within the statin market. In 2012, Crestor became the most prescribed branded pharmaceutical in the US.

Symbicort pMDI continued to deliver steady growth in the US with sales up 19% to $1,003 million (2011: $846 million; 2010: $721 million) and prescription growth of 12.5%. It achieved a 21.3% total prescription share and a 22.5% new prescription share of the inhaled corticosteroid/long-acting beta 2 -agonist market.

Following the completion of BMS’s acquisition of Amylin, AstraZeneca and BMS have been developing and commercialising Amylin’s portfolio of products related to diabetes (and other metabolic diseases). Sales of GLP-1 agonists for the treatment of diabetes were $74 million for Byetta , $37 million for Bydureon and $17 million for Symlin.

Onglyza/Kombiglyze XR captured more than one in five new DPP-IV patient treatment decisions and achieved a 2.8% total prescription market share gain in 2012, ending the year with a total prescription market share of 17.1% of the rapidly growing DPP-IV inhibitor market. Onglyza revenues in the US were $237 million (2011: $156 million; 2010: $54 million).

The loss of exclusivity for Seroquel IR in March 2012 resulted in a decrease in sales of 79% to $697 million (2011: $3,344 million; 2010: $3,107 million). In 2012, generics accounted for 58.5% of quetiapine prescriptions in the US. The presence of generic competition impacted the prescription volume of Seroquel XR in 2012. However, sales of Seroquel XR were up 4% to $811 million (2011: $779 million; 2010: $640 million) because of higher prices.

Nexium was the third most prescribed branded pharmaceutical in the US. In the face of continuing generic, OTC and pricing pressures, Nexium sales declined 5% to $2,272 million (2011: $2,397 million; 2010: $2,695 million). Nexium remains the branded market leader retaining significant market share and volume within the proton pump inhibitor class.

In 2012, sales of Synagis were up 7% to $611 million (2011: $570 million; 2010: $646 million). Sales in the 2011 to 2012 RSV season experienced payer pressure, which was offset by heightened awareness efforts surrounding the RSV burden of disease, appropriate patient identification and enhanced efforts to ensure continuity of care for patients from the hospital to the paediatrician’s office.

In March 2010, the Affordable Care Act came into force. It has had, and is expected to continue to have, a significant impact on our US sales and the US healthcare industry as a whole. In 2012, the overall reduction in our profit before tax for the year due to higher minimum Medicaid rebates on prescription drugs, discounts on branded pharmaceutical sales to Medicare Part D beneficiaries and an industry-wide excise fee was $858 million. This amount reflects only those effects of the Affordable Care Act that we know have had or will have a direct impact on our financial condition or results of operations and which we are therefore able to quantify based on known and isolatable resulting changes in individual financial items within our Financial Statements. There are other potential indirect or associated consequences of these legislative developments, which continue to evolve and which cannot be estimated but could have similar impacts. These include broader changes in access to or eligibility for coverage under Medicare, Medicaid or similar governmental programmes, such as the recent proposals to limit Medicare benefits. These could indirectly impact our pricing or sales of prescription products within the private sector. By their nature and the fact that these potentially numerous consequences are not directly linked to a corresponding and quantifiable impact on our Financial Statements, it is not possible to accurately estimate the financial impact of these

potential consequences of the Affordable Care Act or related legislative changes when taken together with the number of other market and industry-related factors that can also result in similar impacts. Further details on the impact of the Affordable Care Act are contained in the Pricing pressure section from page 18 and the Principal risks and uncertainties section from page 75.

Currently, there is no direct governmental control of prices for commercial prescription drug sales in the US. However, some publicly funded programmes, such as Medicaid and TRICARE (Department of Veterans Affairs), have statutorily mandated rebates and discounts that have the effect of price controls for these programmes. Additionally, pressure on pricing, availability and utilisation of prescription drugs for both commercial and public payers continues to increase. This is driven by, among other things, an increased focus on generic alternatives. Primary drivers of increased generic use are budgetary policies within healthcare systems and providers, including the use of ‘generics only’ formularies, and increases in patient co-insurance or co-payments. In 2012, 84% of the prescriptions dispensed in the US were generic. While it is unlikely that there will be widespread adoption of a broad national price control scheme in the near future, there will continue to be increased attention to pharmaceutical prices and their impact on healthcare costs for the foreseeable future.

Rest of World

Sales performance outside the US in 2012 was down by 11% to $17,318 million (2011: $20,165 million; 2010: $19,542 million), due to loss of exclusivity, competition from generic products and the continuing challenging economic environment. Combined sales of key products ( Arimidex, Crestor, Nexium, Seroquel IR and Seroquel XR , and Symbicort ) were down 11% with sales of $8,769 million (2011: $10,301 million; 2010: $9,923 million). Emerging Markets delivered strong sales, up 4% with sales of $5,752 million (2011: $5,763 million; 2010: $5,198 million).

Western Europe

AstraZeneca is the eighth largest pharmaceutical company in Western Europe, with a 3.4% market share of prescription sales by value.

 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   71

Table of Contents

Performance  | Geographical Review

 

LOGO

 

The macro-economic situation has deteriorated, particularly in Greece, Italy, Portugal and Spain which have seen the implementation of new austerity measures, leading to increased pressure on healthcare budgets. Most governments in Europe intervene directly to control the price, volume and reimbursement of medicines. Several governments have imposed price reductions and increased the use of generic medicines as part of healthcare expenditure control. A number of countries are applying strict criteria for cost-effectiveness evaluations of medicines, which has delayed and reduced access to medicines for patients in areas of important unmet medical need. These and other measures all contribute to an increasingly difficult environment for branded pharmaceuticals in Europe.

Total sales in Western Europe were down 19% to $6,486 million (2011: $8,501 million; 2010: $9,168 million) due largely to volume erosion on Seroquel IR, Nexium, Arimidex and Meronem following generic entrants and the negative price and volume impact primarily related to government interventions, particularly in Greece, Italy, Portugal and Spain. The loss of exclusivity for Atacand in April 2012 resulted in a decrease in sales of 39% to $422 million (2011: $731 million; 2010: $736 million). Generics now account for 9.7% of candesartan prescriptions in Western Europe. This development was partially offset by revenue growth attributable to Brilique, Onglyza, Vimovo and Iressa.

Crestor outperformed the statin class with strong 2% sales growth. Generic versions of Seroquel IR are now available in Western Europe, with overall sales down 56% to $226 million (2011: $546 million; 2010: $560 million).

Brilique has been launched in all markets in Western Europe and sales reached $55 million in 2012 (2011: $9 million).

In Germany, sales fell by 30% to $775 million (2011: $1,189 million; 2010: $1,235 million), mainly driven by market entries of generic versions of Atacand (sales declined to $141 million; 2011: $255 million; 2010: $252 million), Seroquel IR (sales declined to $31 million; 2011: $127 million; 2010: $113 million) and Seroquel XR (sales declined to $93 million; 2011: $151 million; 2010: $100 million).

In the UK, a 22% decrease in sales to $668 million (2011: $866 million; 2010: $1,022 million) reflected strong volume erosion on Seroquel IR and Seroquel XR (sales declined to $58 million; 2011: $120 million; 2010: $124 million), following generic entrants. Sales of Nexium decreased by 59% to $17 million (2011: $41 million; 2010: $89 million) and sales of Arimidex decreased by 85% to $4 million (2011: $28 million; 2010: $114 million), both following the impact of a full year of generic penetration. The decrease in UK sales was partially offset by the solid performance of Symbicort , up 6% to $328 million (2011: $312 million; 2010: $272 million).

Sales in France decreased by 18% to $1,314 million (2011: $1,740 million; 2010: $1,889 million), driven largely by volume erosion on Nexium, Atacand, Zomig and Arimidex , following generic entrants, and the impact from the disposal of Astra Tech, which was not entirely offset by the strong growth of Crestor and the successful launch of Seroquel XR , which had sales of $37 million. Sales in Spain and Italy were down by 22% to $510 million (2011: $708 million; 2010: $788 million) and by 15% to $876 million (2011: $1,113 million; 2010: $1,198 million), respectively, mainly driven by generic entrants and the implementation of price and prescription controls associated with existing and new austerity measures.

Established ROW

Sales in Established ROW decreased by 14%. The key products with sales growth in 2012 were Symbicort, Seroquel XR, Onglyza, Faslodex and Iressa .

Canada

The trend in Canada indicates that provinces will continue to introduce policy changes that drive cost savings and exert pricing pressure on new and existing medicines (for example, conditional listings, product listing agreements and bulk purchasing), while providing reasonable patient access to innovative medicines.

Due to the loss of exclusivity for Crestor in Canada in April 2012, and the continued impact of the ‘at risk’ launch of a generic version of Nexium by a competitor in 2011, total Canadian sales decreased by 31% to $1,090 million (2011: $1,604 million; 2010: $1,510 million). Combined sales of Crestor ,

Nexium, Symbicort, Seroquel IR and Seroquel XR were $742 million (2011: $1,171 million; 2010: $1,055 million).

Japan

Sales in Japan decreased by 5% to $2,904 million (2011: $3,064 million; 2010: $2,617 million). Strong performance from Crestor, Symbicort, Faslodex and Iressa was largely offset by biennial price cuts imposed in April 2012.

Crestor sales grew by 4%, becoming the number one brand in the statin market in Japan. Symbicort sales grew 12%, backed by additional therapeutic indications for SMART and COPD.

Nexium achieved sales of $78 million in its first full year after launch, with sales accelerating following the lifting in October of the two week prescription limit imposed by the Japanese Ministry of Health, Labour and Welfare on new medicines during the first year from launch.

Our oncology business remains one of the leaders in Japan based on the performance of established brands including Iressa, Arimidex, Zoladex and Casodex. Faslodex, launched in November 2011, achieved sales of $58 million in its first full year in the market.

Other Established ROW

Our sales in Other Established ROW showed a decline of 12% to $1,086 million (2011: $1,233 million; 2010: $1,049 million). Australian sales were impacted by price cuts triggered by loss of exclusivity of Seroquel IR and Arimidex in April 2012, as well as by price reductions due to the Australian government’s therapeutic group policy, which impacted Crestor and Atacand. Price reductions were partially offset by performance of Crestor, Nexium and Symbicort , which all gained market share. Crestor achieved a 28.1% volume share in the statin class and became the number one drug in the statin market in Australia following loss of exclusivity of atorvastatin. Brilinta was successfully launched in Australia with reimbursement through the Australian pharmaceutical benefits scheme becoming available from August. Brilinta achieved formulary listing in the vast majority of hospitals in Australia in 2012. Marketing authorisation was obtained for Symbicort pMDI in Australia.

 

 

72   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

LOGO

 

Crestor continues to face challenges from generic competitors. The patent protecting Crestor in Australia has been challenged. Details of this matter are included in Note 25 to the Financial Statements from page 184.

Emerging Markets

In Emerging Markets, our sales increased by 4% to $5,752 million (2011: $5,763 million; 2010: $5,198 million), which was principally driven by growth in China and Russia.

In many of the larger markets, such as Brazil and Mexico, patients tend to pay directly for prescription medicines and consequently these markets are at less risk of direct government interventions on pricing and reimbursement. In other markets such as South Korea, Taiwan and Turkey, where governments pay for medicines, we are seeing continued efforts to reduce the cost of prescriptions in line with the systems in Western Europe, Canada and Australia. Some strong growth markets such as Vietnam are also implementing price and volume controls in an attempt to control government spending.

Emerging Europe

Sales in Emerging Europe grew by 2% to $1,165 million (2011: $1,244 million; 2010: $1,165 million) driven by increased sales in Russia and Romania, which more than offset reduced sales in Turkey.

We have continued to build our presence in Russia, where sales increased by 17% to $314 million (2011: $284 million; 2010: $232 million) mainly due to increased sales of Symbicort by 24%, Nexium by 93%, Crestor by 14% and Seroquel XR by 154%, driven by growth in the retail segment. We have also consolidated our position among the growth leaders in the hospital and regional reimbursement segments.

In Romania, we delivered a strong performance with sales up 19% to $161 million (2011: $154 million; 2010: $119 million), largely as a result of sales of Atacand increasing by 34%, Seroquel XR increasing by 41%, Crestor increasing by 10% and Symbicort increasing by 4%. In Turkey, a decrease in sales to $252 million (2011: $297 million; 2010: $304 million) reflected the additional price and prescription controls imposed by the Turkish government in late 2011.

China

Our sales in China (excluding Hong Kong) increased by 17% to $1,512 million (2011: $1,261 million; 2010: $1,047 million). Sales of products in our Cardiovascular and Respiratory & Inflammation Therapy Areas continue to grow ahead of the market, driven by strong performances of Crestor, Betaloc Zok and Pulmicort Respules . Sales of Nexium and Symbicort grew strongly by 27% and 50% respectively, while our mature gastrointestinal and oncology brands experienced challenges from government pricing reductions. In 2012, we saw Zoladex 10.8mg successfully launched in China, the expansion of our co-promotion with BMS to achieve listing of Onglyza into key hospitals, and a new collaboration formed between AstraZeneca and Ironwood to co-develop and co-commercialise linaclotide in China. We continue to be one of the leading multinational pharmaceutical companies in China.

Emerging Asia Pacific

Sales in Emerging Asia Pacific decreased by 3% to $923 million (2011: $968 million; 2010: $890 million). This decline was driven by India, where sales decreased by 29% to $67 million (2011: $110 million; 2010: $92 million), due primarily to supply issues; continued government interventions on pricing in countries such as Thailand, where sales decreased by 7% to $97 million (2011: $106 million; 2010: $114 million); and by Vietnam, where sales decreased by 4% to $45 million (2011: $47 million; 2010: $37 million). This was partially offset by sales growth in Indonesia, up 7% to $39 million (2011: $39 million; 2010: $34 million); South Korea, up 4% to $239 million (2011: $235 million; 2010: $213 million); and Malaysia, up 6% to $73 million (2011: $70 million; 2010: $66 million).

Other Emerging ROW

Sales in Other Emerging ROW were flat at $2,152 million (2011: $2,290 million; 2010: $2,096 million), with increased sales in Latin America, Egypt, Maghreb, Saudi Arabia and the Gulf States balanced by reduced sales in South Africa and Israel.

The Latin American pharmaceutical market continues to grow, underpinned by a reasonably stable political and economic climate. However, in many of the countries, the majority of the growth in the market is being captured by generics, branded generics and private label product offerings, often from local, non-multinational, companies.

In Latin America, our sales were down 1% to $1,331 million (2011: $1,455 million; 2010: $1,392 million). This was driven by declines in Mexico, down 22%, and Brazil, down 5%. Brazil continued to feel the effects of the loss of exclusivity on Seroquel IR and Crestor with year-on-year declines of 54% and 39% respectively. Growth of Seloken, Faslodex and older products such as Diprivan and Meronem helped to compensate for this development. In Mexico, challenging market conditions and the impact of an ‘at risk’ generic version of Crestor , resulted in weak performance with sales in Mexico declining by 22%. This was partially offset by sales growth in Venezuela (up 41%) and Argentina (up 24%). All key brands achieved double digit growth in Argentina ( Nexium, Crestor, Atacand, Symbicort and Seroquel XR ) and growth of more than 40% in Venezuela ( Crestor, Symbicort, Seroquel XR, Atacand, Zoladex and Arimidex ).

Successful product launches in the year included Brilinta and Kombiglyze XR in Mexico, Colombia and Argentina, and Vimovo in Brazil, Colombia and Argentina. Faslodex 500mg was launched in the fourth quarter of 2012 in Argentina, and is expected to launch in the first half of 2013 in Brazil and Venezuela.

In the Middle East and Africa, despite political challenges arising from the ‘Arab Spring’ revolutions, we further accelerated our growth with sales up 3%. Our largest markets were South Africa, Saudi Arabia and the Gulf States.

 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   73

Table of Contents

Performance | Risk

 

  

LOGO

 

In this section we describe our key risk management and assurance mechanisms and the principal risks and uncertainties which we consider to be material to our business as they may have a significant effect on our financial condition, results of operations and/or reputation. Specific risks and uncertainties are also discussed in the Business Review from page 30, where relevant.

Managing risk

As an innovation-driven, global, prescription-based biopharmaceutical business, we face a diverse range of risks and uncertainties that may adversely affect our business. Our approach to risk management is designed to encourage clear decision making as to which risks we take and how these are managed, based on an understanding of the potential strategic, commercial, financial, compliance, legal and reputational implications of these risks.

We work continuously to ensure that we have effective risk management processes in place to support the delivery of our strategic objectives, the material needs of our stakeholders and our core values. We monitor our business activities and external and internal environments for new, emerging and changing risks to ensure that these are managed appropriately as they arise.

The Board believes that the processes and accountabilities which are in place (described below) provide it with adequate information on the key risks and uncertainties we face. Further information about these risks and uncertainties is set out in the Principal risks and uncertainties section from page 75.

Embedded in business processes

We strive to ensure that sound risk management is embedded within our strategy, planning, budgeting and performance management processes. The Board has defined the Group’s risk appetite expressing the acceptable levels of risk for the Group using three key dimensions. These are (i) earnings and cash flow (ii) return on investment and (iii) potential impact on our reputation. This definition provides a clear statement by the Board of its position on risk which enables the Group, in both quantitative and qualitative terms, to judge the level of risk it is prepared to take so as to achieve its overall objectives.

Annually, the Group develops a long-term business plan to support the delivery of its strategy, which the Board reviews to ensure that it conforms to its risk appetite. Line managers are accountable for identifying and managing risks, and for delivering business objectives in accordance with the Group’s risk appetite. Each area for which a SET member is responsible (a SET function) is required to provide a comprehensive assessment of its risks as part of the annual business planning process. Identified risks are mapped to AstraZeneca’s risk ‘taxonomy’, providing a structured disaggregation of the various potential risks facing the Group.

The CEO and the CFO undertake quarterly business reviews (QBRs) with each SET function, where the key risks are reviewed. Business managers within each SET function are required to provide quarterly updates on their key risks, which are then consolidated to create a list of key risks for

that SET function to review at QBRs. The key risks for each SET function are then aggregated into a Group risk register. The purpose of the risk review is to identify and measure risks, and to define and review risk management and mitigation plans. Supporting tools are in place to assist the managers in this process and we continue to work on developing our risk management standards and guidelines.

We develop business resilience plans to provide for situations where specific risks have the potential to severely impact our business. Global business resilience plans covering crisis management, business continuity and emergency responses are in place. These plans are supported by the provision of training and crisis simulation activities for business managers.

Key responsibilities

Management of risk

Day-to-day risk management is delegated from the Board to the CEO and through the SET to line managers. SET functions are accountable for establishing an appropriate line management-led process and for providing the resources for supporting effective risk management.

Line and project managers have primary responsibility, within the context of their functional area, for identifying and managing risk as well as for putting in place appropriate controls and procedures to monitor effectiveness.

 

 

74   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

LOGO

 

Oversight and monitoring

The SET is responsible for overseeing and monitoring the effectiveness of the risk management processes implemented by management. The Compliance and Finance functions, together with the GIA, support the SET by advising on policy and standard setting, monitoring and auditing, communication and training, as well as reporting on the adequacy of line management processes as they apply to managing our risk. Our compliance organisation is comprised of the Global Compliance function together with a wide range of specialist compliance functions. Further information about Global Compliance and the Code of Conduct can be found in the Compliance section on page 47.

Management reporting and assurance

We provide quarterly risk reports to the SET and to the Board. Among other things, these summarise our current assessment of the principal risks facing the Group, including environmental, social and governance risks, senior management accountability and our expected plans in order to address these risks, to the extent possible.

The Audit Committee comprises five Non-Executive Directors. It reviews and reports to the Board following each Audit Committee meeting on the overall framework of risk management and internal controls, and is responsible for promptly bringing to the Board’s attention any significant concerns about the conduct, results or outcomes of internal audits and other compliance matters. The Audit Committee receives regular reports from our external auditor and the following business functions:

> GIA: independent assurance reports on the Group’s risk management and control framework
> Global Compliance: compliance programme reports on key compliance risks, updates on key compliance initiatives, reports on performance against the Global Compliance scorecard, and summaries of compliance incidents and investigations including contact made by employees with AZethics via our helplines
> Financial Control and Compliance Group: reports on Sarbanes-Oxley Act compliance and the financial control framework
> Management: the Group-level risk summary from the annual business planning process and QBRs and reports on the performance management and monitoring processes.

For further information on the Audit Committee, see the Audit Committee section from page 115.

GIA is an independent assurance and advisory function that reports to, and is accountable to, the Audit Committee. GIA’s budget, resources and programme of audits are approved by the Audit Committee annually and the findings from its audit work are reported to, and discussed at, each Audit Committee meeting. A core part of the audit work carried out by GIA includes assessing how we are managing risk and reviewing the effectiveness of selected aspects of our risk control framework, including the effectiveness of other assurance and compliance functions within the business.

Principal risks and uncertainties

The pharmaceutical sector is inherently risky and a variety of risks and uncertainties may affect our business. In the remainder of this section we describe the principal risks and uncertainties which we consider to be material to our business in that they may have a significant effect on our financial condition, results of operations and/or reputation.

These risks are not listed in any particular order of priority. Other risks, unknown or not currently considered material, could have a similar effect. We believe that the forward-looking statements about AstraZeneca in this Annual Report, identified by words such as ‘anticipates’, ‘believes’, ‘expects’ and ‘intends’, are based on reasonable assumptions. However, forward-looking statements involve inherent risks and uncertainties such as those summarised below. They relate to events that may occur in the future, that may be influenced by factors beyond our control and that may have actual outcomes materially different from our expectations.

 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   75

Table of Contents

Performance | Risk

Product pipeline risks

 

Failure to meet development targets

 

    

Impact

 

The development of any pharmaceutical product candidate is a complex, risky and lengthy process involving significant financial, R&D and other resources, which may fail at any stage of the process due to a number of factors. These include: failure to obtain the required regulatory or marketing approvals for the product candidate or its manufacturing facilities, unfavourable clinical efficacy data, safety concerns, failure of R&D to develop new product candidates, failure to demonstrate adequate cost-effective benefits to regulators and the emergence of competing products.

 

Production and release schedules for biologics may be more significantly impacted by regulatory processes than other products. This is due to more complex and stringent regulation on the manufacturing of biologics and their supply chain.

 

     A succession of negative drug project results and a failure to reduce development timelines effectively, or produce new products that achieve commercial success, could adversely affect the reputation of our R&D capabilities, and is likely to materially adversely affect our business or results of operations.

 

Difficulties of obtaining and maintaining

regulatory approvals for new products

 

    

 

Impact

 

We are subject to strict controls on the commercialisation processes for our pharmaceutical products, including their development, manufacture, distribution and marketing. The requirements to obtain regulatory approval based on a product’s safety, efficacy and quality before it can be marketed for an indication in a particular country, as well as to maintain and comply with licences and other regulations relating to its manufacture and marketing, are particularly important. The submission of an application to regulatory authorities (which vary, with different requirements, in each region or country) may or may not lead to the grant of marketing approval. Regulators can refuse to grant approval or may require additional data before approval is given, even though the medicine may already be launched in other countries. The approval of a product is required by the relevant regulatory authority in each country, although a single pan-EU MAA can be obtained through a centralised procedure.

 

In recent years, companies sponsoring NDAs and regulatory authorities have been under increased public pressure to apply more conservative benefit/risk criteria. In some instances, regulatory authorities require a company to develop plans to ensure safe use of a marketed product before a pharmaceutical product is approved, or after approval, if a new and significant safety issue is established. In addition, third party interpretation of publicly available data on our marketed products has the potential to influence the approval status or labelling of a currently approved and marketed product.

 

    

The predictability of the outcome and timing of review processes remains challenging, particularly in the US, due to competing regulatory priorities and a continuing sentiment of risk aversion on the part of regulatory reviewers and management.

 

Delays in regulatory reviews and approvals could impact the timing of a new product launch. In addition, the drive for public transparency of the review processes through the more extensive use of public advisory committees, increase the unpredictability of the process.

 

Failure to obtain and enforce effective IP protection

 

    

 

Impact

 

Our ability to obtain and enforce patents and other IP rights in relation to our products is an important element of our ability to protect our investment in R&D and create long-term value for the business. A number of the countries in which we operate are still developing their IP laws or may even be limiting the applicability of these laws to pharmaceutical inventions. Adverse political perspectives on the desirability of strong IP protection for pharmaceuticals in certain emerging and even developed markets may limit the scope for us to obtain effective IP protection for our products. As a result, certain countries may seek to limit or deny effective IP protection for pharmaceuticals.

 

     Limitations on the availability of patent protection or the use of compulsory licensing in certain countries in which we operate could have a material adverse effect on the pricing and sales of our products and, consequently, could materially adversely affect our revenues from those products. More information about protecting our IP is contained in the Intellectual Property section on page 35. Information about the risk of patent litigation and the early loss of IP rights is contained in the Expiry or loss of, or limitations on, IP rights risk on page 78.

 

Delay to new product launches

 

    

 

Impact

 

Our continued success depends on the development and successful launch of innovative new drugs. The anticipated launch dates of major new products have a significant impact on a number of areas of our business, including investment in large clinical studies, the manufacture of pre-launch product stocks, investment in marketing materials pre-launch, sales force training and the timing of anticipated future revenue streams from new product sales. These launch dates are primarily driven by the development programmes that we run and the demands of the regulatory authorities in the approvals process, as well as pricing negotiations. Delays to anticipated launch dates can result from a number of factors including adverse findings in pre-clinical or clinical studies, regulatory demands, price negotiation, competitor activity and technology transfer.

 

 

     Significant delays to anticipated launch dates of new products could have a material adverse effect on our financial condition and results of operations. For example, for the launch of products that are seasonal in nature, delays in regulatory approvals or manufacturing difficulties may delay launch to the next season which, in turn, may significantly reduce the return on costs incurred in preparing for the launch for that season. In addition, a delay in the launch may lead to increased costs if, for example, marketing and sales efforts need to be rescheduled or protracted for longer than expected.

 

76   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

Strategic alliances and acquisitions may be unsuccessful

 

    

Impact

 

We seek technology licensing arrangements and strategic collaborations to expand our product portfolio and geographical presence as part of our business strategy.

 

Such licensing arrangements and strategic collaborations are key, enabling us to grow and strengthen the business. The success of such arrangements is largely dependent on the technology and other IP we acquire rights to, and the resources, efforts and skills of our partners. Also, under many of our strategic alliances, we make milestone payments well in advance of the commercialisation of the products, with no assurance that we will recoup these payments.

 

Furthermore, we experience strong competition from other pharmaceutical companies in respect of licensing arrangements and strategic collaborations, and therefore we may be unsuccessful in establishing some of our intended projects.

 

We may also seek to acquire complementary businesses as part of our business strategy. The integration of an acquired business could involve incurring significant debt and unknown or contingent liabilities, as well as having a negative effect on our reported results of operations from acquisition related charges, amortisation of expenses related to intangibles and charges for the implementation of long-term assets. We may also experience difficulties in integrating geographically separated organisations, systems and facilities, and personnel with different organisational cultures.

 

    

If we fail to complete these types of collaborative projects in a timely manner, on a cost-effective basis, or at all, this may limit our ability to access a greater portfolio of products, IP technology and shared expertise.

 

Additionally, disputes or difficulties in our relationship with our collaborators or partners may arise, often due to conflicting priorities or conflicts of interest between parties, which may erode or eliminate the benefits of these alliances.

 

The incurrence of significant debt or liabilities as a result of integration of an acquired business could cause deterioration in our credit rating and result in increased borrowing costs and interest expense.

 

Further, if, following an acquisition, liabilities are uncovered in the acquired business, the Group may suffer losses and may not have remedies against the seller or third parties. The integration process may also result in business disruption, diversion of management resources, the loss of key employees and other issues, such as a failure to integrate IT and other systems.

Commercialisation and business execution risks

 

Challenges to achieving commercial success of new products

 

    

Impact

 

The successful launch of a new pharmaceutical product involves substantial investment in sales and marketing activities, launch stocks and other items. The commercial success of our new medicines is of particular importance to us in order to replace lost sales following patent expiry. We may ultimately be unable to achieve commercial success for any number of reasons. These include difficulties in manufacturing sufficient quantities of the product candidate for development or commercialisation in a timely manner, the impact of price control measures imposed by governments and healthcare authorities, erosion of IP rights, including infringement by third parties and failure to show a differentiated product profile.

 

As a result, we cannot be certain that compounds currently under development will achieve success, and our ability to accurately assess, prior to launch, the eventual efficacy or safety of a new product once in broader clinical use can only be based on data available at that time, which is inherently limited due to relatively short periods of product testing and relatively small clinical study patient samples.

 

The commercialisation of biologics is often more complex than for small molecule pharmaceutical products, primarily due to differences in the mode of administration, technical aspects of the product and rapidly changing distribution and reimbursement environments.

 

    

If a new product does not succeed as anticipated or its rate of sales growth is slower than anticipated, there is a risk that we are unable to fully recoup the costs incurred in launching it, which could materially adversely affect our business or results of operations.

 

Due to the complexity of the commercialisation process for biologics, the methods of distributing and marketing biologics could materially adversely impact our revenues from the sales of products such as Synagis and FluMist/Fluenz.

 

Illegal trade in our products

 

    

 

Impact

 

Illegal trade covers the theft, illegal diversion and counterfeiting of our products. Illegal trade in pharmaceutical products is estimated to exceed $75 billion per year and is generally considered by the industry, non-governmental organisations and governmental authorities to be increasing. We suffer a commensurate financial exposure to illegal trade and there is also a risk to public health. Regulators and the public expect us to secure the integrity of our supply chain and to co-operate actively in the reduction of illegal trade in AstraZeneca products, through surveillance, investigation and legal action against others engaged in illegal trade.

 

    

Public loss of confidence in the integrity of pharmaceutical products as a result of counterfeiting could materially adversely affect our reputation and financial performance. In addition, undue or misplaced concern about the issue may induce some patients to stop taking their medicines, with consequential risks to their health. There is also a direct financial loss where counterfeit medicines replace sales of genuine products and where genuine products are recalled following discovery of counterfeit, stolen and/or illegally traded products in an effort to regain control of the integrity of the supply chain.

 

 

Developing our business in Emerging Markets

 

    

 

Impact

 

The development of our business in Emerging Markets is a critical factor in determining our future ability to sustain or increase our global product revenues. This poses various challenges including: more volatile economic conditions; competition from companies with existing market presence; the need to identify correctly and to leverage appropriate opportunities for sales and marketing; poor IP protection; inadequate protection against crime (including counterfeiting, corruption and fraud); the need to impose developed market compliance standards; inadvertent breaches of local and international law; not being able to recruit appropriately skilled and experienced personnel; identification of the most effective sales channels and route to market; and interventions by national governments or regulators restricting access to market and/or introducing adverse price controls.

 

     The failure to exploit potential opportunities appropriately in Emerging Markets may materially adversely affect our reputation, business or results of operations.

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   77

Table of Contents

Performance | Risk

 

Expiry or loss of, or limitations on, IP rights

 

    

Impact

 

Pharmaceutical products are only protected from being copied during the limited period of protection under patent rights and/or related IP rights such as Regulatory Data Protection or Orphan Drug status. Expiry or loss of these rights typically leads to the immediate launch of generic copies of the product in the country where the rights have expired or been lost. See the Intellectual Property section on page 35 which contains a table of certain patent expiry dates for our key marketed products.

 

Additionally, the expiry or loss of patents covering other innovator companies’ products may also lead to increased competition for our own, still-patented, products in the same product class due to the availability of generic products in that product class. Further, there may be increased pricing pressure on our still-patented products as a result of the lower prices of generic entrants.

 

     Products under patent protection or within the period of Regulatory Data Protection typically generate significantly higher revenues than those not protected by such rights. Our revenues, financial condition and results of operations may be materially adversely affected upon expiry or early loss of our IP rights, due to generic entrants into the market for the applicable product. Additionally, the loss of patent rights covering major products of other pharmaceutical companies, such as Plavix in May, may adversely affect the growth of our still-patented products in the same product class ( eg Brilinta/ Brilique ) in that market.

Pressures resulting from generic competition

 

    

Impact

 

Our products compete not only with other products approved for the same condition, marketed by research-based pharmaceutical companies, but also with generic drugs marketed by generic pharmaceutical manufacturers. These competitors may invest more of their resources into the marketing of their products than we do depending on the relative priority of these competitor products within their company’s portfolio. Generic versions of products are often sold at lower prices than branded products as the manufacturer does not have to recoup the significant cost of R&D investment and market development. The majority of our patented products, including Nexium, Crestor and Seroquel XR , are subject to price pressures as a result of competition from generic copies of these products and from generic forms of other drugs in the same product class (for example, generic forms of Lipitor and Plavix and generic forms of Seroquel IR ).

 

As well as facing generic competition upon expiry or loss of IP rights, we also face the risk that generic drug manufacturers seek to market generic versions of our products prior to expiries of our patents and/or the Regulatory Exclusivity periods. For example, we are currently facing challenges in the US from numerous generic drug manufacturers regarding our patents for Seroquel XR , Nexium , Crestor and Pulmicort , four of our key products. Generic manufacturers may also take advantage of the failure of certain countries to properly enforce Regulatory Data Protection and may launch generics during this protected period. This is a particular risk in some Emerging Markets where appropriate patent protection may be difficult to obtain or enforce.

 

     If challenges to our patents by generic drug manufacturers succeed and generic products are launched, or generic products are launched ‘at risk’ on the expectation that challenges to our IP will be successful, this may materially adversely affect our financial condition and results of operations. In 2012, US sales for Seroquel XR , Nexium and Crestor were $811 million, $2,272 million and $3,164 million respectively. Furthermore, if limitations on the availability, scope or enforceability of patent protection are implemented in jurisdictions in which we operate, generic manufacturers in these countries may be increasingly able to introduce competing products to the market earlier than they would have been able to, had more robust patent or Regulatory Data Protection been available.

Effects of patent litigation in respect of IP rights

 

    

Impact

 

Any of the IP rights protecting our products may be asserted or challenged in IP litigation initiated against or by external parties. Such IP rights may also be the subject of validity challenges in patent offices. We expect our most valuable products to receive the greater number of challenges. Despite our efforts to establish and defend robust patent protection for our products, we may not succeed in protecting our patents from such litigation or other challenges.

 

Where we assert our IP rights and allege infringement, we bear the risk that courts may decide that third parties do not infringe our IP rights. This may result in AstraZeneca losing exclusivity and/or erosion of revenues. Non-infringement defences are typically filed by third parties in response to patent infringement lawsuits including in so-called 505(b)(2) cases in the US. Details of 505(b)(2) actions can be found in Note 25 to the Financial Statements from page 184.

 

We also bear the risk that we may be found to infringe patents owned or licensed exclusively by third parties, including research-based and generic pharmaceutical companies and individuals. Infringement accusations may implicate, for example, our manufacturing processes, product intermediates or use of research tools. Details of significant infringement claims against us by third parties enforcing IP rights can be found in Note 25 to the Financial Statements from page 184.

 

    

If we are not successful in maintaining exclusive rights to market one or more of our major products, particularly in the US where we achieve our highest revenue, our revenue and margins could be materially adversely affected.

 

Managing or litigating infringement disputes over so-called ‘freedom to operate’ can be costly. We may be subject to injunctions against our products or processes and be liable for damages or royalties. We may need to obtain costly licences. These risks may be greater in relation to biologics and vaccines, where patent infringement claims may relate to discovery or research tools, and manufacturing methods and/or biological materials. While we seek to manage such risks by, for example, acquiring licences, foregoing certain activities or uses, or modifying processes to avoid infringement claims and permit commercialisation of our products, such steps can entail significant cost and there is no guarantee that they will be successful.

 

78   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

Price controls and reductions

 

    

Impact

 

Most of our key markets have experienced the implementation of various cost control or reimbursement mechanisms in respect of pharmaceutical products.

 

For example, in the US, realised prices are being depressed through restrictive reimbursement policies and cost-control tools such as restricted lists and formularies, which employ ‘generic first’ strategies and require physicians to obtain prior approval for the use of a branded medicine where a generic alternative exists. These mechanisms can be used by payers to limit the use of branded products and put pressure on manufacturers to reduce net prices. Many of these mechanisms shift a greater proportion of the cost of medicines to the patient via out-of-pocket payments at the pharmacy counter. The patient out-of-pocket spend is generally in the form of a co-payment or, in some cases, a co-insurance, which is designed, principally, to encourage patients to use generic medicines.

 

A summary of the principal aspects of price regulation and how price pressures are affecting our business in our most important markets is set out in the Pricing pressure section from page 18 and these economic pressures are also further discussed below in the following risk factor.

 

    

Due to these pressures on the pricing of our products, there can be no certainty that we will be able to charge prices for a product that, in a particular country or in the aggregate, enable us to earn an adequate return on our product investment. These pressures, including the increasingly restrictive reimbursement policies to which we are subject and the potential adoption of new legislation expanding the scope of permitted commercial importation of medicines into the US, could materially adversely affect our business or results of operations.

 

We expect that these pressures on pricing will continue, and may increase.

Economic, regulatory and political pressures

 

    

Impact

 

We face continued economic, regulatory and political pressures to limit or reduce the cost of our products.

 

In 2010, the US passed the Affordable Care Act, a comprehensive health reform package with provisions taking effect between 2010 and 2014. The law expands insurance coverage, establishes health insurance exchanges and establishes new national entities focused on health system reforms. In terms of specific provisions impacting our industry, the law mandates higher rebates and discounts on branded drugs for certain Medicare and Medicaid patients as well as an industry-wide excise fee. Implementation of several health system delivery reforms included in the law has commenced and will continue over the next two years. For example, a new comparative effectiveness research organisation, the Patient-Centered Outcomes Research Institute, has been established and an Independent Payment Advisory Board, with broad authority to propose to cut Medicare expenditures, is scheduled to commence in 2014.

 

The Affordable Care Act expands the patient population eligible for Medicaid and will provide new insurance coverage for individuals through state-operated and federal-operated health insurance exchanges from 2014. Large employers have typically offered generous health insurance benefits, but many are struggling with increasing health insurance premiums and may, therefore, opt to shift employee coverage into the health insurance exchanges, which will be operational by 2014. The pharmaceutical industry could be adversely impacted by such shifts if the health insurance exchanges do not offer a prescription drug benefit that is as robust as benefits historically provided by large employers.

 

We anticipate further government intervention in the US in connection with the recent initiative to contain federal spending. For more information see the Regulatory requirements and Pricing pressure sections from page 17 and 18, respectively.

 

In the EU, efforts by the European Commission to reduce inconsistencies and to improve standards in the disparate national regulatory systems have met with little immediate success. The industry continues to be exposed in Europe to a range of disparate pricing systems, ad hoc cost-containment measures and reference pricing mechanisms, which impact prices.

 

Concurrently, many markets are adopting the use of Health Technology Assessment (HTA) to provide a rigorous evaluation of the clinical efficacy of a product, at or post launch. HTA evaluations are also increasingly being used to assess the clinical as well as cost-effectiveness of products in a particular health system. This comes as payers and policymakers attempt to drive increased efficiencies in the use and choice of pharmaceutical products.

 

Further information regarding these pressures is contained in the Regulatory requirements and Pricing pressure sections from page 17 and page 18, respectively.

 

    

It is not possible to accurately estimate the financial impact of the potential consequences resulting from the Affordable Care Act or related legislative changes when taken together with the number of other market-related and industry-related factors that can also result in similar impacts. While the overall reduction in our profit before tax for the year due to higher minimum Medicaid rebates on prescription drugs, discounts on branded pharmaceutical sales to Medicare Part D beneficiaries and an industry-wide excise fee was $858 million, this reflects only the limited number of known, quantifiable and isolatable effects of these legislative developments. Other potential indirect or associated consequences of these legislative developments, which continue to evolve and which cannot be estimated, could have similar impacts. These include broader changes in access to, or eligibility for, coverage under Medicare, Medicaid or similar governmental programmes, such as the recent proposals to limit Medicare benefits, which could indirectly impact our pricing or sales of prescription products within the private sector.

 

These continued disparities in pricing systems could lead to marked price differentials between markets, which, by way of the implementation of existing or new reference pricing mechanisms, increases the pricing pressure affecting the industry. The importation of pharmaceutical products from countries where prices are low due to government price controls, or other market dynamics, to countries where prices for those products are higher, is already prevalent and may increase. In particular, as discussed in the Pricing pressure section on page 18, Greece, Portugal and Spain have all introduced measures to lower healthcare spending, including mandatory discounts, clawbacks and price referencing rules, which could have a material adverse effect on our business or results of operations.

 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   79

Table of Contents

Performance | Risk

 

Biosimilars

 

    

Impact

 

While no application for a biosimilar has been made in relation to an AstraZeneca biologic, various regulatory authorities are implementing or considering abbreviated approval processes for biosimilars that would compete with patented biologics.

 

For example, in 2010, the US enacted the Biologics Price Competition and Innovation Act within the Affordable Care Act, which contains general directives for biosimilar applications. The FDA issued draft guidance in February 2012 on implementing an abbreviated biosimilar approval pathway. However, significant questions remain, including standards for designation of interchangeability. In 2012, the FDA also implemented user fee programmes to support biosimilar product review and policy development. In Europe, the EMA published final guidelines on similar biological medicinal products containing MAbs and in May, the first MAb biosimilar application was made. Notably, a number of jurisdictions have adopted either the EMA guidelines or those recently set forth by the WHO to enable biosimilars to enter the market after discrete periods of data exclusivity.

    

The extent to which biosimilars would be differentiated from patented biologics on price is unclear. However, due to their complex nature, it is uncertain whether biosimilars would have the same impact on patented biologics that generic products have had on patented small molecule products.

 

In addition, it is uncertain when any such abbreviated approval processes may be fully realised, particularly for more complex protein molecules such as MAbs. Any such processes may materially adversely affect the future commercial prospects for patented biologics, such as the ones that we produce.

Increasing implementation and enforcement of more stringent anti-bribery and anti-corruption legislation

 

    

Impact

 

There is an increasing global focus on the implementation and enforcement of anti-bribery and anti-corruption legislation.

 

For example, the UK Bribery Act 2010 came into force in July 2011. This act has extensive extra-territorial application, implements significant changes to existing UK anti-bribery legislation and broadens the scope of statutory offences and the potential applicable penalties, including, organisational liability for any bribe paid by persons or entities associated with an organisation where the organisation failed to have adequate preventative procedures in place at the time of the offence. There is also an increase in the maximum applicable penalties for bribery, including up to 10 years imprisonment and unlimited fines. There have also been increased enforcement efforts in the UK by the Serious Fraud Office and, in the US, there has been significant enforcement activity in respect of the Foreign Corrupt Practices Act by the SEC and US Department of Justice against US companies and non-US companies listed in the US.

 

We are the subject of current anti-corruption investigations and there can be no assurance that we will not, from time to time, continue to be subject to informal inquiries and formal investigations from governmental agencies. In the context of our business, governmental officials interact with us in a variety of roles that are important to our operations, such as in the capacity of a regulator, partner or healthcare payer, reimburser or prescriber, among others. Details of these matters are included in Note 25 to the Financial Statements from page 184.

 

     We devote significant resources to the considerable challenge of compliance with this legislation, including in emerging and developing markets, at considerable cost. Investigations from governmental agencies require additional resources. Despite taking significant measures to prevent breaches of applicable anti-bribery and anti-corruption laws by our personnel, breaches may result in the imposition of significant penalties, such as fines, the requirement to comply with monitoring or self-reporting obligations, or debarment or exclusion from government sales or reimbursement programmes, any of which could materially adversely affect our reputation, business or results of operations.

Any expected gains from productivity initiatives are uncertain

 

    

Impact

 

We continue to implement various productivity initiatives and restructuring programmes with the aim of enhancing the long-term efficiency of the business. However, anticipated cost savings and other benefits from these programmes are based on estimates and the actual savings may vary significantly. In particular, these cost reduction measures are often based on current conditions and cannot always take into account any future changes to the pharmaceutical industry or our operations, including new business developments, wage or price increases.     

If inappropriately managed, the expected value of these initiatives could be lost through low employee engagement and hence productivity, increased absence and attrition levels, and industrial action.

 

Our failure to successfully implement these planned cost reduction measures, either through the successful conclusion of employee relations processes (including consultation, engagement, talent management, recruitment and retention), or the possibility that these efforts do not generate the level of cost savings we anticipate, could materially adversely affect our business or results of operations.

 

 

80   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

Changes in senior management, failure to attract and retain key personnel and failure to successfully engage with our employees

 

    

Impact

 

The success of our business is guided by our SET and their direct reports. The departure of senior leaders can introduce uncertainty in the business.

 

We rely heavily on recruiting and retaining talented employees with a diverse range of skills and capabilities to meet our strategic objectives. For example, the success of our R&D activities is particularly dependent on our ability to attract and retain sufficient numbers of high-quality researchers and development specialists. We face intense competition for qualified individuals, as the supply of people with specific skills and significant leadership potential or in specific geographic regions may be limited.

 

Our ability to achieve high levels of employee engagement in the workforce, and hence benefit from strong commitment and motivation, is key to the successful delivery of our business objectives.

    

In 2012, we appointed a new CEO and in January 2013, we changed the composition of our SET. Senior management transitions can introduce uncertainty and could materially adversely impact our business or results of operations.

 

The inability to attract and/or retain highly skilled personnel, in particular those in key scientific and leadership positions, may weaken our succession plans for critical positions in the medium term, may materially adversely affect the implementation of our strategic objectives and could ultimately impact our business or results of operations.

 

Failure to engage effectively with our employees could lead to business disruption in our day-to-day operations, reduce levels of productivity and/or increase levels of voluntary turnover, all of which could ultimately adversely impact our business or results of operations.

 

While we are committed to working on improving drivers of engagement, such as increasing our employees’ understanding of our new management, strategy and our ongoing efforts to reduce organisational complexity, our efforts may be unsuccessful.

 

Failure of information technology

 

    

Impact

 

We are dependent on effective IT systems. These systems support key business functions such as our R&D, manufacturing, supply chain and sales capabilities, and are an important means of safeguarding and communicating data.     

Any significant disruption to these IT systems, including breaches of data centre security or cybersecurity, or failure to integrate new and existing IT systems, could harm our reputation and materially adversely affect our financial condition or results of operations.

 

While we have invested heavily in the protection of our data and IT, we may be unable to prevent breakdowns or breaches in our systems that could adversely affect our business.

 

For example, in 2012, the failure of the implementation of an IT interface in an enterprise resource planning IT system in our facility in Sweden (Södertälje) caused a disruption to our supply chain resulting in an estimated negative revenue impact of 1%.

 

As previously disclosed, we terminated our previous outsourcing relationship for the provision of IT infrastructure services. We continue to migrate applications and servers to equipment and facilities managed by AstraZeneca and our current providers of IT infrastructure services. This migration activity may not be completed on time and within budget, which could adversely impact our business or results of operations.

 

Failure of outsourcing

 

    

Impact

 

We have outsourced a number of business critical operations to third party providers. This includes certain R&D processes, IT systems, HR, and finance and accounting services.     

A failure to successfully manage and implement the integration of IT infrastructure services provided by our outsourcing providers could create disruption, which could materially adversely affect our business or results of operations.

 

Failure of outsource providers to deliver timely services, and to the required level of quality, and failure of outsource providers to co-operate with each other, could materially adversely affect our financial condition or results of operations. In addition, such failures could adversely impact our ability to meet business targets, maintain a good reputation within the industry and with stakeholders, and result in non-compliance with applicable laws and regulations.

 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   81

Table of Contents

Performance | Risk

Supply chain and delivery risks

 

Manufacturing biologics

 

    

Impact

 

Manufacturing biologics, especially in large quantities, is complex and may require the use of innovative technologies to handle living micro-organisms and facilities specifically designed and validated for this purpose, with sophisticated quality assurance and control procedures.

 

     Slight deviations in any part of the manufacturing process may result in lot failure, product recalls or spoilage, for example due to contamination.

Difficulties and delays in the manufacturing, distribution and sale of our products

 

    

Impact

 

We may experience difficulties and delays in manufacturing our products, such as (i) supply chain continuity, including as a result of disruptions such as a natural or man-made disaster at one of our facilities or at a critical supplier or vendor; (ii) delays related to the construction of new facilities or the expansion of existing facilities, including those intended to support future demand for our products; (iii) seizure or recalls of products or shutdown of manufacturing plants; and (iv) other manufacturing or distribution problems including changes in manufacturing production sites, limits to manufacturing capacity due to regulatory requirements, changes in the types of products produced, or physical limitations or other business interruptions that could impact continuous supply.

 

    

Manufacturing distribution and sale difficulties may result in product shortages and significant delays, which may lead to lost sales.

 

In 2012, supply from our site in India was disrupted for a period of time, following a voluntary recall of products that we determined did not meet our global quality standards.

 

In 2012, the failure of the implementation of an IT interface in an enterprise resource planning IT system in our facility in Sweden (Södertälje) caused a disruption to our supply chain resulting in an estimated negative revenue impact of 1%.

Reliance on third parties for goods

 

    

Impact

 

We increasingly rely on third parties for the timely supply of goods, such as raw materials (for example, the API in some of our medicines), equipment, formulated drugs and packaging, all of which are key to our operations.

 

Unexpected events and/or events beyond our control could result in the failure of the supply of goods. For example, suppliers of key goods we rely on may cease to trade. In addition, we may experience limited supply of biological materials, such as cells, animal products or by-products. Furthermore, government regulations in multiple jurisdictions could result in restricted access to, use or transport of such materials.

 

    

Third party supply failure could materially adversely affect our financial condition or results of operations. This may lead to significant delays and/or difficulties in obtaining goods and services on commercially acceptable terms.

 

Loss of access to sufficient sources of key goods and biological materials may interrupt or prevent our research activities as planned and/or increase our costs. Further information is contained in the Managing risk section on page 74.

Legal, regulatory and compliance risks

 

Adverse outcome of litigation and/or governmental investigations

 

    

Impact

 

We may be subject to legal proceedings and governmental investigations. Litigation, particularly in the US, is inherently unpredictable and unexpectedly high awards for damages can result from an adverse verdict. In many cases, plaintiffs may claim compensatory, punitive and statutory damages in extremely high amounts. In particular, the marketing, promotional, clinical and pricing practices of pharmaceutical manufacturers, as well as the manner in which manufacturers interact with purchasers, prescribers and patients, are subject to extensive regulation, litigation and governmental investigation. Many companies, including AstraZeneca, have been subject to claims related to these practices asserted by federal and state governmental authorities and private payers and consumers, which have resulted in substantial expense and other significant consequences. Note 25 to the Financial Statements from page 184 describes the material legal proceedings in which we are currently involved.

 

     Investigations or legal proceedings, regardless of their outcome, could be costly, divert management attention, or damage our reputation and demand for our products. Unfavourable resolution of current and similar future proceedings against us could subject us to criminal liability, fines, penalties or other monetary or non-monetary remedies, require us to make significant provisions in our accounts relating to legal proceedings and could materially adversely affect our business or results of operations.

Substantial product liability claims

 

    

Impact

 

Pharmaceutical companies have, historically, been subject to large product liability damages claims, settlements and awards for injuries allegedly caused by the use of their products. Adverse publicity relating to the safety of a product or of other competing products may increase the risk of product liability claims.     

Substantial product liability claims that result in court decisions against us or in the settlement of proceedings could materially adversely affect our financial condition or results of operations, particularly where such circumstances are not covered by insurance. Furthermore, in the past we incurred substantial costs relating to product liability litigation involving Seroquel IR . For more information, see the Limited third party insurance coverage risk on page 84.

 

 

82   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

Failure to adhere to applicable laws, rules and regulations

 

     

Impact

 

Any failure to comply with applicable laws, rules and regulations may result in civil and/or criminal legal proceedings being filed against us, or in us becoming subject to regulatory sanctions. Regulatory authorities have wide-ranging administrative powers to deal with any failure to comply with continuing regulatory oversight and this could affect us, whether such failure is our own or that of our contractors or external partners.      

Failure to comply with applicable laws, including ongoing control and regulation, could materially adversely affect our business or results of operations. For example, once a product has been approved for marketing by the regulatory authorities, it is subject to continuing control and regulation, such as the manner of its manufacture, distribution, marketing and safety surveillance. In addition, any changes that are made to the manufacturing, distribution, marketing and safety surveillance processes of our products may require additional regulatory approvals, which could result in significant additional costs and/or disruption to these processes. Such changes may be imposed on us by regulatory authorities as a result of continuing inspections to which we are subject or may be made at our own discretion. For example, if regulatory issues concerning compliance with current Good Manufacturing Practice or safety monitoring regulations for pharmaceutical products (often referred to as pharmacovigilance) arise, this could lead to loss of product approvals, product recalls and seizures, and interruption of production, which could create product shortages and delays in new product approvals.

 

Failure to adhere to laws, rules and regulations relating to anti-competitive behaviour

 

     

Impact

 

Any failure to comply with laws, rules and regulations relating to anti-competitive behaviour may expose us to regulatory sanctions or lawsuits from private, non-governmental entities.

 

Certain of our commercial arrangements with generics companies, which have sought to settle patent challenges on terms acceptable to both innovator and generics manufacturer, may be subject to challenge by competition authorities. An example of such a challenge is the Federal Trade Commission inquiry. See Note 25 to the Financial Statements from page 184 for more details.

     

Where a government authority investigates our adherence to competition laws, or we become subject to private party lawsuits, this may result in inspections of our sites or requests for documents and other information. Competition investigations or legal proceedings could be costly, divert management attention, or damage our reputation.

 

Unfavourable resolution of such challenges, investigations or legal proceedings against us could require us to make changes to our commercial practice and could subject us to fines and penalties and other sanctions. These could materially adversely affect our business or results of operations.

 

Environmental and occupational health and safety liabilities

 

     

Impact

 

We have environmental and/or occupational health and safety-related liabilities at some currently or formerly owned, leased and third party sites, the most significant of which are detailed in Note 25 to the Financial Statements from page 183.      

While we carefully manage these liabilities, if a significant non-compliance issue, environmental, occupational health or safety incident for which we are responsible were to arise, this could result in us being liable to pay compensation, fines or remediation costs. In some circumstances, such liability could materially adversely affect our business or results of operations. In addition, our financial provisions for any obligations that we may have relating to environmental or occupational health and safety liabilities may be insufficient if the assumptions underlying the provisions, including our assumptions regarding the portion of waste at a site for which we are responsible, prove incorrect or if we are held responsible for additional contamination or occupational health and safety-related claims.

 

Misuse of social media platforms and new technology

 

     

Impact

 

We increasingly use the internet, social media, mobile applications and other forms of new technology to communicate internally and externally. The accessibility and instantaneous nature of interactions with such media may facilitate or exacerbate the risk of data leakages from within AstraZeneca or false or misleading statements being made about AstraZeneca, which may be damaging to our reputation. As social media platforms expand, it becomes increasingly challenging to identify new points of entry and to put structures in place to secure and protect information.      

Inappropriate use of certain media vehicles could lead to misuse including public disclosure of sensitive information (such as personally identifiable information on employees, healthcare professionals or patients, for example, those enrolled in our clinical trials), which may damage our reputation and expose us to legal risks as well as additional legal obligations. Similarly, the involuntary public disclosure of commercially sensitive information such as trade secrets through external media channels, or an information loss, could materially adversely affect our business or results of operations. In addition, negative posts or comments on social media websites about us or, for example, the safety of any of our products, could harm our reputation.

 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   83

Table of Contents

Performance | Risk

Economic and financial risks

 

Adverse impact of a sustained economic downturn

 

    

Impact

 

A variety of significant risks may arise from a sustained global economic downturn. Additional pressure from governments and other healthcare payers on medicine prices and volumes of sales in response to recessionary pressures on budgets may cause a slowdown or a decline in growth in some markets. In some cases, those governments most severely impacted by the economic downturn may seek alternative ways to settle their debts through, for example, the issuance of government bonds which might trade at a discount to the face value of the debt.

 

In addition, our customers may cease to trade, which may result in losses from writing off debts. We are highly dependent on being able to access a sustainable flow of liquid funds due to the high fixed costs of operating our business and the long and uncertain development cycles of our products. In a sustained economic downturn, financial institutions with whom we deal may cease to trade and there can be no guarantee that we will be able to access monies owed to us without a protracted, expensive and uncertain process, if at all.

 

More than 95% of our cash investments are managed centrally and are invested in AAA credit rated institutional money market funds backed by institutions in the US and the EU, which, in turn, invest in other funds, including sovereign funds. This means our credit exposure is a mix of US sovereign default risk and financial institution default risk.

 

     While we have adopted cash management and treasury policies to manage this risk (see Financial risk management policies section on page 99), we cannot be certain that these will be as effective as they are intended to be, in particular in the event of a global liquidity crisis. In addition, open positions where we are owed money and investments we have made in financial institution money market funds cannot be guaranteed to be recoverable. Additionally, if we need access to external sources of financing to sustain and/or grow our business, such as the debt or equity capital financial markets, this may not be available on commercially acceptable terms, if at all, in the event of a severe and/or sustained economic downturn. This may, for instance, be the case in the event of any default by the Group on its debt obligations, which may materially adversely affect our ability to secure debt funding in the future or our financial condition in general. Further information on debt funding arrangements is contained in the Financial risk management policies section on page 99.

Political and socio-economic conditions

 

    

Impact

 

We operate in over 100 countries across the world, some of which may be subject to political and social instability. There may be disruption to our business if there is instability in a particular geographic region, including as a result of war, terrorism, riot, unstable governments, civil insurrection or social unrest.     

Deterioration of, or failure to improve, socio-economic conditions, and situations and/or events resulting therefrom, depending on their severity, could adversely affect our supply and/or distribution chain in the affected countries and the ability of customers or ultimate payers to purchase our medicines. This could materially adversely affect our business or results of operations.

 

Impact of fluctuations in exchange rates

 

    

Impact

 

As a global business, currency fluctuations can significantly affect our results of operations, which are reported in US dollars. Approximately 38% of our global 2012 sales were in the US, which is expected to remain our largest single market for the foreseeable future. Sales in other countries are predominantly in currencies other than the US dollar, including the euro, Japanese yen, Australian dollar and Canadian dollar. We have a growing exposure to emerging market currencies, where some have exchange controls in place, but for others the exchange rates are also linked to the US dollar. Major components of our cost base are located in the UK and Sweden, where an aggregate of approximately 25.9% of our employees are based.

 

     Movements in the exchange rates used to translate foreign currencies into US dollars may materially adversely affect our financial condition or results of operations. Additionally, some of our subsidiaries import and export goods and services in currencies other than their own functional currency and so the financial results of such subsidiaries could be affected by currency fluctuations arising between the transaction dates and the settlement dates for these transactions. In addition, there are foreign exchange differences arising on the translation of equity investments in subsidiaries. See Note 23 to the Financial Statements from page 175.

Limited third party insurance coverage

 

    

Impact

 

In recent years, the costs associated with product liability litigation have increased the cost of, and narrowed the coverage afforded by, pharmaceutical companies’ product liability insurance. To contain insurance costs in recent years, we have continued to adjust our coverage profile, accepting a greater degree of uninsured exposure. The Group has not held any material product liability insurance since February 2006. In addition, where claims are made under insurance policies, insurers may reserve the right to deny coverage on various grounds. For example, product liability litigation cases relating to Crestor and ( Nexium ) in the US are not covered by third party product liability insurance. See Note 25 to the Financial Statements from page 183 for details.

 

    

If we are found to have a financial liability as a result of product liability or other litigation, in respect of which we do not have appropriate insurance, or if an insurer’s denial of coverage is ultimately upheld, this could materially adversely affect our business or results of operations. For details about litigation with a number of insurers with respect to the Seroquel IR liability claim, see Note 25 to the Financial Statements from page 184.

 

For more information, see the Substantial product liability claims risk on page 82.

 

84   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

Taxation

 

    

Impact

 

The integrated nature of our worldwide operations can produce conflicting claims from revenue authorities as to the profits to be taxed in individual countries. The majority of the jurisdictions in which we operate have double tax treaties with other foreign jurisdictions, which provide a framework for mitigating the incidence of double taxation on our revenues and capital gains.     

The resolution of these disputes can result in a reallocation of profits between jurisdictions and an increase or decrease in related tax costs, and has the potential to affect our cash flows and EPS. Claims, regardless of their merits or their outcome, are costly, divert management attention and may adversely affect our reputation.

 

If any of these double tax treaties should be withdrawn or amended, especially in a territory where a member of the Group is involved in a taxation dispute with a tax authority in relation to cross-border transactions, such withdrawal or amendment could materially adversely affect our business or results of operations, as could a negative outcome of a tax dispute or a failure by the tax authorities to agree through competent authority proceedings. See the Financial risk management policies section on page 99 for tax risk management policies and Note 25 to the Financial Statements on page 189 for details of current tax disputes.

 

Pensions

 

    

Impact

 

Our pension obligations are backed by assets invested across the broad investment market. Our most significant obligations relate to the UK pension fund.     

Sustained falls in these asset values will put a strain on funding, which may result in requirements for additional cash, restricting cash available for strategic business growth. Similarly, if the liabilities increase as a result of a sustained low interest rate environment, there will be a strain on funding from the business. The likely increase in the IAS 19 accounting deficit generated by any of these factors may cause the ratings agencies to review our credit rating, with the potential to negatively affect our ability to raise debt. See Note 18 to the Financial Statements from page 167 for further details of the Group’s pension obligations.

 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   85

Table of Contents

Performance | Financial Review

 

LOGO

 

     Contents
  86    Introduction
  86    2012 Business background and results overview
  88    Measuring performance
     2012
  89    Results of operations – summary analysis of year to 31 December
  91    Cash flow and liquidity
  92    Financial position
  94    Capitalisation and shareholder return
  94    Future prospects
     2011
  95    Results of operations – summary analysis of year to 31 December
  96    Cash flow and liquidity
  97    Financial position
  97    Revised Core financial measures
  99    Financial risk management
  99    Critical accounting policies and estimates
  103    Sarbanes-Oxley Act Section 404

 

 

The financial performance for the full year 2012 was defined by the significant revenue decline associated with the loss of exclusivity for several products, with revenue down 15% in constant currency terms.

Spending discipline and restructuring benefits only partially mitigated the impact of the revenue decline on Core profits and margins, particularly as we remain committed to investment to drive future growth and value. Core earnings per share, which benefited from the favourable impact of two tax related matters and the sale of Nexium OTC rights, were down 9%.

Productivity and efficiency programmes continue to deliver their target levels of savings, providing the headroom to invest behind key growth platforms and in progressing the pipeline. Our cash generation remains strong, funding these investments for future growth and value whilst providing $5.9 billion in net cash distributions to shareholders through net share repurchases of $2.2 billion and $3.7 billion from payment of the second interim dividend from 2011 and the first interim dividend from 2012. The Company’s commitment to its progressive dividend policy was confirmed with the full year 2012 results announcement.

Simon Lowth

Chief Financial Officer

The purpose of this Financial Review is to provide a balanced and comprehensive analysis of the financial performance of the business during 2012, the financial position as at the end of the year and the main business factors and trends which could affect the future financial performance of the business.

All growth rates in this Financial Review are expressed at CER unless noted otherwise.

2012 Business background and results overview

The business background is covered in the Our industry section from page 16, the Therapy Area Review from page 50 and the Geographical Review from page 70, and describes in detail the developments in both our products and geographical regions.

As described earlier in this Annual Report, sales of our products are directly influenced by medical need and are generally paid for by health insurance schemes or national healthcare budgets. Our operating results can be affected by a number of factors other than the delivery of operating plans and normal competition, such as:

 

>

The risk of generic competition following loss of patent protection or patent expiry of one of our products or an ‘at risk’ launch by a competitor or the launch of a generic competitor in the same class as one of our products, with the potential adverse effects on sales volumes and prices. For example, in 2012, our performance was affected by generic competition in the US for Seroquel IR and, again in the US, there has been

 

 

86   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

LOGO

 

   some volume decline of Crestor following the introduction of a large number of generic atorvastatin products. Further details of patent expiries for our key marketed products are included in the Patent expiries section on page 35.
> The adverse impact on pharmaceutical prices as a result of the macroeconomic and regulatory environment. For instance, although there is no direct governmental control on prices in the US, action from federal and individual state programmes and health insurance bodies is leading to downward pressures on realised prices. In other parts of the world, there are a variety of price and volume control mechanisms and retrospective rebates based on sales levels that are imposed by governments.
> The timings of new product launches, which can be influenced by national regulators, and the risk that such new products do not succeed as anticipated, together with the rate of sales growth and costs following new product launches.
> Currency fluctuations. Our functional and reporting currency is the US dollar, but we have substantial exposures to other currencies, in particular the euro, Japanese yen, pound sterling and Swedish krona.
> Macro factors such as greater demand from an ageing population and increasing requirements of Emerging Markets.

Over the longer term, the success of our R&D is crucial and we devote substantial resources to this area. The benefits of this investment are expected to emerge over the long term and there is considerable inherent uncertainty as to whether and when it will generate future products.

The most significant features of our financial results in 2012 are:

 

> Revenue was down 15% to $27,973 million (Reported: 17%).
> Loss of exclusivity on several brands, most notably Seroquel IR , and the disposals of Astra Tech and Aptium were the key drivers of the revenue decline.
> Symbicort, Faslodex, Onglyza, Iressa, Brilinta/Brilique and Seroquel XR delivered aggregate CER revenue growth of $600 million for the full year.
> Emerging Markets revenue increased by 4% (Reported: unchanged).
> Core operating profit was down 18% (Reported: 21%) to $10,430 million, driven by lower revenues and lower Core gross margin, partially offset by reduced Core R&D and SG&A expenses.
> Reported operating profit was down 34% (Reported: 36%) to $8,148 million.
> Core operating margin of 37.3% of revenue was down 1.6 percentage points at CER. Reported operating margin was 29.1% of revenue.
> Core EPS decreased by 9% (Reported: 12%) to $6.41. Basic EPS was down 29% (Reported: 32%) to $4.99. Basic and Core EPS benefited by $0.37 from two separate tax-related matters during the year. Proceeds from the sale of Nexium OTC rights contributed $0.16 to Basic and Core EPS. The larger decline in Basic EPS reflects the $1.08 per share benefit in 2011 from the sale of Astra Tech and higher restructuring costs in 2012, neither of which are included in Core earnings.
> Dividends paid decreased to $3,665 million (2011: $3,764 million). Net share repurchases totalled $2,206 million (2011: $5,606 million). On 1 October, the Group announced the suspension of its share repurchase programme.
> Total restructuring costs associated with the global programme to reshape the cost base of the business were $1,558 million in 2012. Total costs to date for this third phase of restructuring, comprised of initiatives across the supply chain, SG&A and R&D, amount to $1,819 million. This brings the total restructuring costs charged to 31 December, since the start of our restructuring programme in 2007, to $6,427 million. Most of the remaining costs of approximately $300 million for the third phase of our restructuring will be taken in 2013.
 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   87

Table of Contents

Performance | Financial Review

Measuring performance

 

 

 

The following measures are referred to in this Financial Review when reporting on our performance both in absolute terms but more often in comparison to earlier years:

 

> Reported performance. Reported performance takes into account all the factors (including those which we cannot influence, principally currency exchange rates) that have affected the results of our business as reflected in our Group Financial Statements prepared in accordance with IFRSs as adopted by the EU and as issued by the IASB.
> Core financial measures. These are non-GAAP measures because, unlike Reported performance, they cannot be derived directly from the information in the Group’s Financial Statements. These measures are adjusted to exclude certain significant items, such as charges and provisions related to our global restructuring programmes, amortisation and impairment of the significant intangibles relating to the acquisition of MedImmune in 2007, the amortisation and impairment of the significant intangibles relating to our exit arrangements with Merck in the US and other specified items. In determining the adjustments to arrive at the Core result, we use a set of established principles relating to the nature and materiality of individual items or groups of items, excluding, for example, events which (i) are outside of the normal course of business, (ii) are incurred in a pattern that is unrelated to the trends in the underlying financial performance of our ongoing business, or (iii) are related to major acquisitions, to ensure that investors’ ability to evaluate and analyse the underlying financial performance of our ongoing business is enhanced. See the 2012 Reconciliation of Reported results to Core results table on the page opposite for a reconciliation of Reported to Core performance.
> Constant exchange rate (CER) growth rates. These are also non-GAAP measures. These measures remove the effects of currency movements (by retranslating the current year’s performance at previous year’s exchange rates and adjusting for other exchange effects, including hedging). A reconciliation of the Reported results adjusted for the impact of currency movements is provided in the 2012 Reported operating profit table on the page opposite.
> Gross and operating profit margin percentages, and Core pre-R&D operating margin. These measures set out the progression of key performance margins and illustrate the overall
  quality of the business. Core pre-R&D operating margin is a non-GAAP measure of our Core financial performance. A reconciliation of Core pre-R&D operating margin to our operating profit is provided on the page opposite and page 95.
> Prescription volumes and trends for key products. These measures can represent the real business growth and the progress of individual products better and more immediately than invoiced sales.
> Net funds/debt. This represents our cash and cash equivalents, current investments and derivative financial instruments less interest-bearing loans and borrowings.

CER measures allow us to focus on the changes in sales and expenses driven by volume, prices and cost levels relative to the prior period. Sales and cost growth expressed in CER allows management to understand the true local movement in sales and costs, in order to compare recent trends and relative return on investment. CER growth rates can be used to analyse sales in a number of ways but, most often, we consider CER growth by products and groups of products, and by countries and regions. CER sales growth can be further analysed into the impact of sales volumes and selling price. Similarly, CER cost growth helps us to focus on the real local change in costs so that we can manage the cost base effectively.

We believe that disclosing Core financial and growth measures in addition to our Reported financial information enhances investors’ ability to evaluate and analyse the underlying financial performance of our ongoing business and the related key business drivers. The adjustments made to our Reported financial information in order to show Core financial measures illustrate clearly, and on a year-on-year or period-by-period basis, the impact upon our performance caused by factors such as changes in sales and expenses driven by volume, prices and cost levels relative to such prior years or periods.

As shown in the 2012 Reconciliation of Reported results to Core results table on the page opposite, our reconciliation of Reported financial information to Core financial measures includes a breakdown of the items for which our Reported financial information is adjusted and a further breakdown by specific line item as such items are reflected in our Reported income statement. This illustrates the significant items that are excluded from Core financial measures and their impact

on our Reported financial information, both as a whole and in respect of specific line items.

Core pre-R&D operating margin is our Core operating margin before Core R&D costs recorded in the year. This measure reflects Core operating performance before reinvestment in internal R&D.

Management presents these results externally to meet investors’ requirements for transparency and clarity. Core financial measures are also used internally in the management of our business performance, in our budgeting process and when determining compensation.

Core financial measures are non-GAAP adjusted measures. All items for which Core financial measures are adjusted are included in our Reported financial information as they represent actual costs of our business in the periods presented. As a result, Core financial measures merely allow investors to differentiate between different kinds of costs and they should not be used in isolation. You should also refer to our Reported financial information in the 2012 Reported operating profit table on the page opposite, our reconciliation of Core financial measures to Reported financial information in the Reconciliation of Reported results to Core results table on the page opposite, and to the Results of operations – summary analysis of year to 31 December 2011 section from page 95 for our discussion of comparative Reported growth measures that reflect all factors that affect our business. Our determination of non-GAAP measures, and our presentation of them within this financial information, may differ from similarly titled non-GAAP measures of other companies.

With effect from the first quarter results of 2013, we will update our definition of Core financial measures to exclude all intangible asset amortisation charges and impairments, except those for IS-related intangibles. Further details of this change are included in the Revised Core financial measures section of this Financial Review from page 97. With the exception of the numbers detailed on page 98, all other references to Core in this Annual Report are calculated using our current definition of Core.

The SET retains strategic management of the costs excluded from Reported financial information in arriving at Core financial measures, tracking their impact on Reported operating profit and EPS, with operational management being delegated on a case-by-case basis to ensure clear accountability and consistency for each cost category.

 

 

88   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

     Results of operations – summary analysis of year to 31 December 2012

    2012 Reported operating profit

 

        2012     2011     Percentage of sales     2012 compared with 2011    

 

       

Reported

$m

   

CER

growth

$m

   

Growth

due to

exchange

effects

$m

   

Reported

$m

   

Reported

2012

%

   

Reported

2011

%

   

CER

growth

%

   

Reported

growth

%

     
 

Revenue

    27,973        (4,965     (653     33,591                        (15     (17  
 

Cost of sales

    (5,393     528        105        (6,026     (19.3     (17.9     (9     (11  
 

Gross profit

    22,580        (4,437     (548     27,565        80.7        82.1        (16     (18  
 

Distribution costs

    (320     16        10        (346     (1.1     (1.0     (5     (8  
 

Research and development

    (5,243     208        72        (5,523     (18.8     (16.5     (4     (5  
 

Selling, general and administrative costs

    (9,839     1,134        188        (11,161     (35.2     (33.2     (10     (12  
 

Profit on disposal of Astra Tech

           (1,483            1,483               4.4        n/a        n/a     
 

Other operating income and expense

    970        211        (18     777        3.5        2.3        27        25     
 

Operating profit

    8,148        (4,351     (296     12,795        29.1        38.1        (34     (36  
 

Net finance expense

    (430                     (428                                  
 

Profit before tax

    7,718                        12,367                                     
 

Taxation

    (1,391                     (2,351                                  
 

Profit for the period

    6,327                        10,016                                     
 

    

                                                                 
 

Basic earnings per share ($)

    4.99                        7.33                                     
 

2012 Core operating results

 

  

             
                    2012     2011     2012 compared with  2011    

 

                   

Core

$m

   

CER

growth

$m

   

Growth

due to

exchange

effects

$m

   

Core

$m

   

CER

growth

%

   

Total

Core

growth

%

     
 

Gross profit

        22,716        (4,355     (548     27,619        (16     (18  
 

Gross margin %

                    (81.2%                     82.2%                     
 

Distribution costs

                    (320     16        10        (346     (5     (8  
 

Research and development

                    (4,452     533        48        (5,033     (11     (12  
 

Selling, general and administrative costs

  

            (8,541     1,207        170        (9,918     (12     (14  
 

Other operating income and expense

  

            1,027        200        (18     845        24        22     
 

Operating profit

        10,430        (2,399     (338     13,167        (18     (21  
 

Operating margin %

                    (37.3%                     39.2%                     
 

Net finance expense

                    (430                     (428                  
 

Profit before tax

                    10,000                        12,739                     
 

Taxation

                    (1,885                     (2,797                  
 

Profit for the period

                    8,115                        9,942                     
 

    

                                                                 
 

Basic earnings per share ($)

                    6.41                        7.28                     
 

2012 Reconciliation of Reported results to Core results

 

  

       
                                Merck & MedImmune     Legal            
                   

2012

Reported

$m

   

Restructuring

costs

$m

   

Amortisation

$m

   

Intangible

impairments

$m

   

provisions

and other

$m

   

2012

Core

$m

     
 

Gross profit

                    22,580        136                             22,716     
 

Distribution costs

                    (320                                 (320  
 

Research and development

                    (5,243     791                             (4,452  
 

Selling, general and administrative costs

  

            (9,839     631        534               133        (8,541  
 

Other operating income and expense

  

            970               57                      1,027     
 

Operating profit

        8,148        1,558        591               133        10,430     
   

Add back: Research and development

  

            5,243        (791                          4,452       
   

Pre-R&D operating profit

        13,391        767        591               133        14,882       
   

Pre-R&D operating margin %

                    47.9%                                        53.2%       
 

Net finance expense

                    (430                                 (430  
 

Profit before tax

                    7,718        1,558        591               133        10,000     
 

Taxation

                    (1,391     (375     (87            (32     (1,885  
 

Profit for the period

                    6,327        1,183        504               101        8,115     
 

    

                                                                 
 

Basic earnings per share ($)

                    4.99        0.94        0.40               0.08        6.41     

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   89

Table of Contents

Performance | Financial Review

 

Revenue decreased by 15% on a CER basis and 17% on a Reported basis. More than 13 percentage points of the decline at CER (approximately $4.5 billion) was related to loss of exclusivity on several brands in the portfolio. Seroquel IR revenues declined by $3 billion and regional losses of exclusivity for Atacand, Nexium and Crestor combined for a further negative impact of more than $1 billion. The disposals of Astra Tech and Aptium accounted for a further decrease of $562 million, or approximately 1.7 percentage points of the year-on-year revenue change at CER. Disruptions to our supply chain, from the implementation of an enterprise resource planning IT system in our plant in Sweden early in the year, negatively impacted revenues by approximately 1%.

Revenue in the US was down 21% (Reported: 21%) with revenue in the Rest of World down 11% (Reported: 14%). Emerging Markets sales increased by 4% (Reported: flat). Further details of our sales performance are contained in the Therapy Area Review from page 50 and the Geographical Review from page 70.

Core gross margin of 81.2% decreased 0.9 percentage points (Reported: 1.0 percentage points). In 2012, benefits from the absence of the lower margin businesses of Astra Tech and Aptium, and from lower net expense related to our accounting for the amendments to the Merck exit arrangements (as detailed in Note 9 to the Financial Statements from page 159), were more than offset by an unfavourable impact from product mix. Core gross margin in 2011 benefited from a $131 million settlement of a royalty dispute with PDL Biopharma Inc.

Core R&D expenditure was $4,452 million, 11% lower than last year (Reported: 12%). Higher costs from new spending on in-licensed, acquired or partnered projects, including $151 million relating to Amylin, Ardea and Amgen, were more than offset by lower intangible impairments in 2012 of $186 million compared with 2011 impairments of $527 million, a reduction of $341 million, and reduced spend on projects.

Core SG&A costs of $8,541 million were 12% lower than in 2011 (Reported: 14%), as a result of spending discipline, partially offset by amortisation expense related to the expansion of our diabetes alliance with BMS and increased promotional costs in Emerging Markets. The excise fee imposed by the enactment of US healthcare reform measures amounted to 2.8% (2011: 2.1%) of Core SG&A expense for the year.

Core other income of $1,027 million was $182 million higher (Reported growth) than the previous year principally as a result of $250 million income from an agreement with Pfizer for OTC rights for Nexium .

Core pre-R&D operating margin was 53.2%, down 0.9 percentage points (Reported: 1.0 percentage points), as the benefit from higher Core other income was more than offset by higher Core cost of sales and Core SG&A costs as a percentage of revenue.

Core operating profit was $10,430 million, a decrease of 18% (Reported: 21%). Core operating margin declined by 1.6 percentage points (Reported: 1.9 percentage points) to 37.3% as a result of an unfavourable impact from lower Core gross margin combined with higher Core R&D and SG&A costs as a percentage of revenue, being only partially mitigated by the increased Core other income for the year.

Core EPS was $6.41, down 9% (Reported: 12%), lower than the decline in Core operating profit as a result of the benefits from net share repurchases and a lower tax rate.

Pre-tax adjustments to arrive at Core amounted to $2,282 million in 2012 (2011: $372 million). Excluded from Core results were:

 

> Restructuring costs totalling $1,558 million (2011: $1,161 million), incurred as the Group commenced the third phase of restructuring announced in February 2012.
> Amortisation totalling $591 million (2011: $537 million) relating to assets capitalised as part of the MedImmune acquisition and the Merck exit arrangements, the increase driven by the additional amortisation arising from the amendment to the Merck exit arrangements during 2012, as detailed in Note 9 to the Financial Statements from page 159.
> $72 million (2011: $135 million) of legal provision charges in respect of ongoing Seroquel franchise legal matters, Average Wholesale Price litigation in the US, the Toprol-XL anti-trust litigation and Nexium commercial litigation. In line with prior years these have been excluded from our Core performance and full details of these matters are included in Note 25 to the Financial Statements from page 184.
> $61 million (2011: $nil) of acquisition- and transaction-related expenses in relation to our Ardea and new BMS collaboration arrangements. Further details of these transactions are included in Note 9 and Note 22 to the Financial Statements.
> In 2011, the profit on sale of our subsidiary Astra Tech of $1,483 million was also excluded from Core results. Further details of this disposal are included in Note 22 to the Financial Statements on page 173.

Reported operating profit was down 34% (Reported: 36%) at $8,148 million. Reported EPS was $4.99, down 29% (Reported:

32%). The larger declines compared with the respective Core financial measures are the result of the $1,483 million benefit to Reported other income in 2011 from the sale of Astra Tech, together with higher restructuring and amortisation costs in 2012 compared with the prior year.

Net finance expense was $430 million, in line with the $428 million expense recorded in 2011. Net fair value losses on long-term debt and derivatives were $10 million for the year, versus $4 million gains in 2011. This was partially offset by reduced net finance cost on the Group’s pension schemes.

The Reported taxation charge of $1,391 million (2011: $2,351 million) consists of a current tax charge of $1,682 million (2011: $2,578 million) and a credit arising from movements on deferred tax of $291 million (2011: $227 million). The current year tax charge includes a prior period current tax credit of $79 million (2011: $102 million).

The Reported tax rate for the year was 18.0% (2011: 19.0%). The Reported tax rate for the year benefited from a $230 million adjustment to deferred tax balances following substantive enactment in 2012 of a reduction in the Swedish corporation tax rate from 26.3% to 22%, which is effective 1 January 2013, and a $240 million adjustment in respect of prior periods following the favourable settlement of a transfer pricing matter. Excluding these items, the Reported tax rate for the year would have been 24.1%; this tax rate is applied to the taxable Core adjustments to operating profit, resulting in a Core tax rate for the year of 18.9%. The Reported tax rate for last year benefited from a non-taxable gain on the disposal of Astra Tech and a favourable adjustment to tax provisions of $520 million following the announcement in March 2011 that HM Revenue & Customs in the UK and the US Internal Revenue Service had agreed the terms of an Advance Pricing Agreement regarding transfer pricing arrangements for AstraZeneca’s US business for the period from 2002 to the end of 2014 and a related valuation matter. Excluding these benefits, the Reported tax rate for 2011 was 26.4%.

Total comprehensive income for the year decreased by $3,065 million from 2011 to $6,405 million. This was driven by the decrease in profit for the year of $3,689 million, partially offset by an increase of $624 million in other comprehensive income, which was principally due to the non-recurrence in 2012 of $741 million of actuarial losses recorded in 2011 on our defined benefit schemes, arising from lower discount rates applied to our long-term pension obligations reflecting external market conditions.

 

 

90   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

Cash flow and liquidity – 2012

All data in this section is on a Reported basis.

Summary cash flows

 

      

2012

$m

    2011
$m 		    2010
$m 		 

Net funds brought forward at 1 January

     2,849        3,653        535   

Earnings before interest, tax, depreciation, amortisation and impairment (EBITDA)

     10,666        15,345        14,235   

Profit on disposal of Astra Tech

            (1,483       

EBITDA before profit on disposal of Astra Tech

     10,666        13,862        14,235   

Movement in working capital and short-term provisions

     (706     (897     82   

Tax paid

     (2,043     (3,999     (2,533

Interest paid

     (545     (548     (641

Non-cash and other movements

     (424     (597     (463

Net cash available from operating activities

     6,948        7,821        10,680   

Purchase of intangibles (net)

     (3,947     (458     (1,180

Other capital expenditure (net)

     (473     (737     (708

Acquisitions of business operations

     (1,187            (348

Net cash received on disposal of Astra Tech

            1,772          

Investments

     (5,607     577        (2,236

Dividends

     (3,665     (3,764     (3,361

Net share repurchases

     (2,206     (5,606     (2,110

Distributions

     (5,871     (9,370     (5,471

Other movements

     312        168        145   

Net (debt)/funds carried forward at 31 December

     (1,369     2,849        3,653   

Net debt/funds reconciliation

 

    

2012

$m

    2011
$m 		    2010
$m 		 

Cash and cash equivalents

     7,701        7,571        11,068   

Short-term investments

     823        4,248        1,482   

Net derivative financial instruments

     417        358        325   

Cash, short-term investments and derivatives

     8,941        12,177        12,875   

Overdraft and short-term borrowings

     (879     (221     (125

Finance leases

     (84              

Current instalments of loan

            (1,769       

Loans due after one year

     (9,347     (7,338     (9,097

Loans and borrowings

     (10,310     (9,328     (9,222

Net (debt)/funds

     (1,369     2,849        3,653   

 

Cash generated from operating activities was $6,948 million in the year to 31 December 2012, compared with $7,821 million in 2011. The decrease of $873 million is primarily driven by lower operating profits, offset by lower tax payments.

Investment cash outflows of $5,607 million include the purchases of Ardea ($1,187 million) and intangible assets associated with our collaboration with BMS on Amylin ($3,358 million). The 2011 investment cash inflow of $577 million benefited from the sale of Astra Tech ($1,772 million). Further details of the Ardea acquisition and Astra Tech disposal are included in Note 22 to the Financial Statements from page 173. Our Amylin transaction is detailed in Note 9 to the Financial Statements on page 161.

Net cash distributions to shareholders decreased from $9,370 million in 2011 to $5,871 million in 2012, the reduction being driven by the suspension of our share repurchase programme in October. Included in net cash distributions to shareholders are dividend payments of $3,665 million (2011: $3,764 million).

At 31 December 2012, outstanding gross debt (interest-bearing loans and borrowings) was $10,310 million (2011: $9,328 million). Of this gross debt, $901 million is due within one year, including $774 million of commercial paper borrowings (2011: $nil) with various short-term maturities all within 90 days. In 2011, amounts due within one year included $1,769 million relating to current instalments of loans.

During September, the Company issued $2 billion of new long-term debt in two

tranches; $1 billion maturing in 2019 with a coupon of 1.95% and $1 billion maturing in 2042 with a coupon of 4.00%. Net proceeds of $1,980 million from the issue were used to repay a $1.75 billion bond with a coupon of 5.40% maturing in September 2012 and for general corporate purposes.

Net debt was $1,369 million at the end of the year, a decrease from net funds of $2,849 million at the end of 2011, a movement of $4,218 million during the year as a result of the net cash outflow described above.

Off-balance sheet transactions and commitments

We have no off-balance sheet arrangements and our derivative activities are non-speculative. The table below sets out our minimum contractual obligations at the year end.

 

 

Payments due by period

 

     Less than
1 year
$m 		     1-3 years
$m 		     3-5 years
$m 		     Over
5 years
$m 		     2012
Total
$m 		     2011
Total
$m 		 

Bank loans and other borrowings 1

     1,365         2,649         2,536         10,766         17,316         15,515   

Finance leases

     23         46         32                 101           

Operating leases

     102         140         83         109         434         392   

Contracted capital expenditure

     245                                 245         190   

Total

     1,735         2,835         2,651         10,875         18,096         16,097   

 

1   Bank loans and other borrowings include interest charges payable in the period, as detailed in Note 23 to the Financial Statements on page 175.

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   91

Table of Contents

Performance | Financial Review

Financial position – 2012

All data in this section is on a Reported basis.

Summary statement of financial position

 

     2012
$m 		    Movement
$m 		    2011
$m 		    Movement
$m 		    2010
$m 		 

Property, plant and equipment

     6,089        (336     6,425        (532     6,957   

Goodwill and intangible assets

     26,346        5,504        20,842        (1,187     22,029   

    

                                        

Inventories

     2,061        209        1,852        170        1,682   

Trade and other receivables

     7,981        (773     8,754        907        7,847   

Trade and other payables

     (10,222     (862     (9,360     (326     (9,034

Provisions

     (1,344     518        (1,862     76        (1,938

    

                                        

Net income tax payable

     (2,059     275        (2,334     1,521        (3,855

Net deferred tax liabilities

     (1,465     (244     (1,221     449        (1,670

    

                                        

Retirement benefit obligations

     (2,265     409        (2,674     (202     (2,472

    

                                        

Non-current other investments

     199        (2     201        (10     211   

Net (debt)/funds

     (1,369     (4,218     2,849        (804     3,653   

    

                                        

Net assets

     23,952        480        23,472        62        23,410   

 

In 2012, net assets increased by $480 million to $23,952 million. The increase in net assets is broadly as a result of the Group profit of $6,327 million, offset by dividends of $3,619 million and net share repurchases of $2,206 million.

Property, plant and equipment

Property, plant and equipment decreased by $336 million to $6,089 million. Additions of $772 million (2011: $807 million) were offset by depreciation of $1,023 million (2011: $1,086 million) and disposals of $224 million (2011: $233 million).

Goodwill and intangible assets

The Group’s goodwill of $9,898 million (2011: $9,862 million) principally arose on the acquisition of MedImmune in 2007 and the restructuring of our US joint venture with Merck in 1998. Goodwill of $30 million arising on our acquisition of Ardea, as detailed in Note 22 to the Financial Statements on page 173, was capitalised in 2012.

Intangible assets amounted to $16,448 million at 31 December 2012 (2011: $10,980 million). Intangible asset additions were $6,916 million in 2012 (2011: $442 million), including $1,464 million arising on the acquisition of Ardea, $3,358 million arising from the expansion of our diabetes alliance with BMS and $1,475 million in connection with our Merck arrangements. Amortisation in the year was $1,296 million (2011: $911 million) and impairments totalled $199 million (2011: $553 million). Further details of our additions to intangible assets, and impairments recorded, are included in Note 9 to the Financial Statements from page 159.

 

Receivables, payables and provisions

Trade receivables decreased by $934 million to $5,696 million in line with lower revenues in 2012.

Included within trade receivables is approximately $420 million of net receivables, representing 7% of our trade receivables, due from customers in the eurozone countries of Spain, Italy, Portugal and Greece (Spain: $120 million; Italy: $205 million; Portugal: $30 million; and Greece: $65 million). Within this balance is approximately $130 million of overdue government trade receivables. In light of current market conditions, debts within these eurozone countries have been subject to enhanced monitoring and scrutiny by the Group. Our bad debt provisioning against these debts reflects our current estimate of the recoverability of these balances based on consideration of a number of factors such as the status of current negotiations, past payment history and the budget constraints of individual countries. In 2012, our revenue from these four countries was $876 million (Italy), $510 million (Spain), $241 million (Greece) and $168 million (Portugal).

Other receivables decreased by $402 million to $835 million as a result of monies being released from externally held settlement funds in relation to Seroquel franchise legal matters. Prepayments and accrued income increased by $563 million driven, principally, by an increase in prepayments related to our Amylin transaction (see Note 9 to the Financial Statements on page 161).

Trade and other payables increased by $862 million in 2012 to $10,222 million, with increases in accruals of $1,323 million due to our Merck exit commitments, as detailed in Note 9 to the Financial Statements from page 161, being offset by a decrease

in rebates and chargeback accruals of $799 million. The decrease in rebates and chargebacks is principally driven by the reduction in US revenues recorded in 2012. Further details of the movements on rebates and chargebacks are included from page 99.

The reduction in provisions of $518 million in 2012 includes $1,096 million of additional charges recorded in the year, offset by $1,476 million of cash payments. Included within the $1,096 million of charges for the year is $873 million for our global restructuring initiative and $90 million in respect of legal charges. Cash payments of $1,476 million include a reduction in our Seroquel franchise-related provisions of $427 million, following release of monies from our settlement funds as detailed above, and $853 million for our global restructuring programme. Further details of the charges made against our provisions are contained in Notes 17 and 25 to the Financial Statements.

Tax payable and receivable

Net income tax payable has decreased by $275 million to $2,059 million, principally due to the settlement of a transfer pricing matter as detailed in Note 4 to the Financial Statements from page 152. Our tax receivable balance of $803 million comprises tax owing to AstraZeneca from certain governments expected to be received on settlements of transfer pricing audits and disputes (see Note 25 to the Financial Statements on page 189) and cash tax timing differences. Net deferred tax liabilities increased by $244 million in the year.

Retirement benefit obligations

Net retirement benefit obligations decreased by $409 million, driven by an additional lump sum payment made into the UK defined benefit scheme in 2012.

 

 

92   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

In recent years the Group has undertaken several initiatives to reduce its net pension obligation exposure. For the UK defined benefit pension scheme, which represents AstraZeneca’s largest defined benefit scheme, these initiatives have included agreeing funding principles for cash contributions to be paid to the UK pension scheme to target a level of assets in excess of the current expected cost of providing benefits, and, in 2010, amendments to the scheme to freeze pensionable pay at 30 June 2010 levels. In addition to the cash contributions to be paid into the UK pension scheme, AstraZeneca makes contributions to an escrow account which is held outside the pension scheme. The escrow account assets are payable to the fund in agreed circumstances, for example, in the event of AstraZeneca and the pension fund trustee agreeing on a change to the current long-term investment strategy.

AstraZeneca has agreed to fund the UK defined benefit scheme shortfall by making lump sum payments totalling £715 million ($1,103 million). The first of these lump sum payments of £180 million ($278 million) was paid into the pension scheme from the escrow account in December 2011. A further £300 million ($463 million) was paid into the pension scheme during January 2012 and the balance will be paid in due course. In 2011, £132 million ($213 million) was paid into the escrow account and a further £230 million ($355 million) was paid in during January 2012. At 31 December 2012, £462 million ($748 million) escrow fund assets are included within other investments (as detailed in Note 10 to the Financial Statements on page 163).

In 2012, approximately 97% of the Group’s obligations were concentrated in the UK, the US, Sweden and Germany. Further details of the Group’s pension schemes are included in Note 18 to the Financial Statements from page 167.

Commitments and contingencies

The Group has commitments and contingencies which are accounted for in accordance with the accounting policies described in the Financial Statements in the Group Accounting Policies section from page 146. The Group also has taxation contingencies. These are described in the Taxation section in the Critical accounting policies and estimates section on page 99 and in Note 25 to the Financial Statements from page 189.

Research and development collaboration payments

Details of future potential R&D collaboration payments are also included in Note 25 to the Financial Statements from page 183. As detailed in Note 25 to the Financial Statements, payments to our collaboration

partners may not become payable due to the inherent uncertainty in achieving the development and revenue milestones linked to the future payments. As part of our overall externalisation strategy, we may enter into further collaboration projects in the future that may include milestone payments and, therefore, as certain milestone payments fail to crystallise due to, for example, development not proceeding, they may be replaced by potential payments under new collaborations.

Investments, divestments and capital expenditure

As detailed earlier in the Research and Development section from page 30, AstraZeneca views collaborations, including externalisation arrangements in the field of R&D, as a crucial element of the development of our business.

The Group has completed over 130 major externalisation transactions over the past three years, two of which were accounted for as business acquisitions under IFRS 3 ‘Business Combinations’, being the acquisition of Ardea in 2012 for $1.3 billion and Novexel in 2010 for $0.5 billion, and all others were strategic alliances and collaborations. Further details of our business acquisitions and disposals in the past three years are contained in Note 22 to the Financial Statements from page 173. Details of our significant externalisation transactions are given below:

 

> In January 2007, AstraZeneca signed an exclusive co-development and co-promotion agreement with BMS for the development and commercialisation of Onglyza , a DPP-IV and Forxiga , a selective sodium-glucose co-transporter 2 (SGLT2) inhibitor, both for the treatment of Type 2 diabetes. The agreement is global with the exception of Japan for Onglyza . Under each agreement, the two companies jointly develop the clinical and marketing strategy and share development and commercialisation expenses on a global basis. To date, AstraZeneca has made upfront and milestone payments totalling $300 million for Onglyza and $170 million for Forxiga , will make a further payment of $80 million for Forxiga in early 2013, and may make future milestone payments of up to $150 million on Forxiga contingent on achievement of regulatory milestones and launch in key markets. Following launch, profits and losses globally are shared equally and an additional $300 million of sales-related payments for each product may be triggered based on worldwide sales success.
> In August, AstraZeneca expanded its diabetes alliance with BMS to incorporate the development and marketing of
  Amylin’s portfolio of diabetes products. Amylin, a wholly owned subsidiary of BMS, is a biopharmaceutical company dedicated to the discovery, development and commercialisation of innovative medicines for patients with diabetes and other metabolic diseases. Amylin’s primary focus is on the research, development and commercialisation of a franchise of GLP-1 agonists for the treatment of Type 2 diabetes. The portfolio of collaboration products includes Byetta (exenatide) injection and Bydureon (exenatide extended-release for injectable suspension/exenatide 2mg powder and solvent for prolonged release suspension for injection) that are approved for use in both the US and Europe, Symlin (pramlinitide acetate) injection that is approved for use in the US, and metreleptin, a leptin analogue currently under review at the FDA for the treatment of diabetes and/or hypertriglyceridaemia in patients with rare forms of inherited or acquired lipodystrophy. AstraZeneca has expanded the alliance for a total consideration of $3.7 billion. This includes an amount of $135 million relating to an option of AstraZeneca contained in the collaboration agreement to acquire certain additional governance rights in respect of the collaboration. The Group notified BMS of its decision to exercise the option in August and the balance of $135 million will be payable once applicable anti-trust and competition approvals are received by AstraZeneca. The Group expects to make this payment in the first half of 2013. Profits and losses arising from the collaboration will be shared equally. Further details of this collaboration and our accounting treatment for this arrangement are included in Note 9 to the Financial Statements on page 161.
> In April 2012, AstraZeneca announced an agreement to jointly develop and commercialise five monoclonal antibodies from Amgen’s clinical inflammation portfolio: AMG 139, AMG 157, AMG 181, AMG 557 and brodalumab (AMG 827). Under the terms of the agreement, AstraZeneca made a $50 million upfront payment and the companies share both costs and profits. Approximately 65% of costs for the 2012 to 2014 period will be funded by AstraZeneca. Thereafter, the companies will split costs equally. In addition, AstraZeneca will make milestone payments to a maximum of $30 million up to launch. On commercialisation, Amgen will retain a low single-digit royalty for brodalumab and a mid-single-digit royalty for the rest of the portfolio after which the companies will share profits equally.
 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   93

Table of Contents

Performance | Financial Review

Capitalisation and shareholder return

Dividend for 2012

 

     $      Pence      SEK      Payment date  

First interim dividend

     0.90         58.1         6.26         10 September 2012   

Second interim dividend

     1.90         120.5         12.08         18 March 2013   

Total

     2.80         178.6         18.34            

Summary of shareholder distributions

 

             
     Shares
repurchased
(million) 		     Cost
$m 		    

Dividend per
share

$

    

Dividend
cost

$m

    Shareholder
distributions
$m 		 

2000

     9.4         352         0.70         1,236        1,588   

2001

     23.5         1,080         0.70         1,225        2,305   

2002

     28.3         1,190         0.70         1,206        2,396   

2003

     27.2         1,154         0.795         1,350        2,504   

2004

     50.1         2,212         0.94         1,555        3,767   

2005

     67.7         3,001         1.30         2,068        5,069   

2006

     72.2         4,147         1.72         2,649        6,796   

2007

     79.9         4,170         1.87         2,740        6,910   

2008

     13.6         610         2.05         2,971        3,581   

2009

                     2.30         3,339        3,339   

2010

     53.7         2,604         2.55         3,604        6,208   

2011

     127.4         6,015         2.80         3,653        9,668   

2012

     57.8         2,635         2.80         3,493 1       6,128   

Total

     610.8         29,170         21.225         31,089        60,259   

 

1   Total dividend cost estimated based upon number of shares in issue at 31 December 2012.

 

The Group determines the above externalisation transactions to be significant using a range of factors. We look at the specific circumstances of the individual externalisation arrangement and apply several quantitative and qualitative criteria. Because we consider our externalisation strategy to be an extension of our R&D strategy, the expected total value of development payments under the transaction and its proportion of our annual R&D spend, both of which are proxies for overall R&D effort and cost, are important elements of the significance determination. Other quantitative criteria we apply include, without limitation, expected levels of future sales, the possible value of milestone payments and the resources used for commercialisation activities (for example, the number of staff). Qualitative factors we consider include, without limitation, new market developments, new territories, new areas of research and strategic implications.

In aggregate, payments capitalised under the Group’s externalisation arrangements, other than those detailed above, amounted to $156 million in 2012, $123 million in 2011 and $337 million in 2010. The Group recognised other income in respect of other externalisation arrangements totalling $255 million in 2012, including $250 million of income from an agreement with Pfizer for OTC rights for Nexium , $18 million in 2011 and $82 million in 2010.

 

Capitalisation

The total number of shares in issue at 31 December 2012 was 1,247 million. 12.2 million Ordinary Shares were issued in consideration of share option exercises for a total of $429 million. Share repurchases amounted to 57.8 million Ordinary Shares at a cost of $2,635 million. Shareholders’ equity increased by $491 million to $23,737 million at the year end. Non-controlling interests decreased to $215 million (2011: $226 million).

Dividend and share repurchases

The Board has recommended a second interim dividend of $1.90 (120.5 pence, 12.08 SEK) to be paid on 18 March 2013. This brings the full year dividend to $2.80 (178.6 pence, 18.34 SEK).

This dividend is consistent with the progressive dividend policy, by which the Board intends to maintain or grow the dividend each year. In adopting this policy, the Board recognised that some earnings fluctuations are to be expected as the Group’s revenue base transitions through this period of exclusivity losses and new product launches. The Board’s view is that the annual dividend will not just reflect the financial performance of a single year taken in isolation, but reflect its view of the earnings prospects for the Group over the entirety of the investment cycle.

The Company has revised the basis by which it assesses dividend cover. The previous basis was a dividend cover target of two times (ie a payout ratio of 50%) based on Reported earnings (before restructuring

costs). With the adoption of new definitions of Core financial measures, as detailed from page 97, the dividend cover target is now two times based on Core earnings under the new definition. In the context of the earnings fluctuations that are to be expected as the Group’s revenue base transitions through this period of exclusivity losses and new product launches, the Board recognises that dividend cover in any year is likely to vary from the two times target level through the investment cycle.

In setting the distribution policy and the overall financial strategy, the Board’s aim is to continue to strike a balance between the interests of the business, our financial creditors and our shareholders. After providing for business investment, funding the progressive dividend policy and meeting our debt service obligations, the Board will keep under review the opportunity to return cash in excess of these requirements to shareholders through periodic share repurchases.

Future prospects

We believe challenging market conditions will persist in 2013, including continued government interventions in price. The revenue impact from the loss of exclusivity will also continue to affect our performance. In the context of the ongoing update to our strategy, we have withdrawn the planning assumptions for revenue and margin evolution for the period 2010 to 2014 we outlined in January 2010. We plan to hold a Capital Markets Day in March 2013 to provide a more detailed exposition of our strategic priorities.

 

 

94   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

    Results of operations – summary analysis of year to 31 December 2011

    2011 Reported operating profit

 

        2011     2010     Percentage of sales     2011 compared with 2010    

 

       

Reported

$m

   

CER

growth

$m

   

Growth

due to

exchange

effects

$m

   

Reported

$m

   

Reported

2011

%

   

Reported

2010

%

   

CER

growth

%

   

Reported

growth

%

     
 

Revenue

    33,591        (601     923        33,269                        (2     1     
 

Cost of sales

    (6,026     625        (262     (6,389     (17.9     (19.2     (10     (6  
 

Gross profit

    27,565        24        661        26,880        82.1        80.8               3     
 

Distribution costs

    (346     3        (14     (335     (1.0     (1.0     (1     3     
 

Research and development

    (5,523     (15     (190     (5,318     (16.5     (16.0            4     
 

Selling, general and administrative costs

    (11,161     (409     (307     (10,445     (33.2     (31.4     4        7     
 

Profit on disposal of Astra Tech

    1,483        1,483                      4.4               n/a        n/a     
 

Other operating income and expense

    777        59        6        712        2.3        2.1        8        9     
 

Operating profit

    12,795        1,145        156        11,494        38.1        34.5        10        11     
 

Net finance expense

    (428                     (517                                  
 

Profit before tax

    12,367                        10,977                                     
 

Taxation

    (2,351                     (2,896                                  
 

Profit for the period

    10,016                        8,081                                     
 

    

                                                                 
 

Basic earnings per share ($)

    7.33                        5.60                                     
 

2011 Core operating results

 

  

           
                    2011     2010     2011 compared with 2010    

 

                   

Core

$m

   

CER

growth

$m

   

Growth

due to

exchange

effects

$m

   

Core

$m

   

CER

growth

%

   

Total

Core

growth

%

     
 

Gross profit

        27,619        (63     658        27,024               2     
 

Gross margin %

                    82.2%                        81.2%                     
 

Distribution costs

                    (346     3        (14     (335     (1     3     
 

Research and development

                    (5,033     (639     (175     (4,219     15        19     
 

Selling, general and administrative costs

  

            (9,918     160        (301     (9,777     (2     1     
 

Other operating income and expense

                    845        (71     6        910        (8     (7  
 

Operating profit

        13,167        (610     174        13,603        (4     (3  
 

Operating margin %

                    39.2%                        40.8%                     
 

Net finance expense

                    (428                     (517                  
 

Profit before tax

                    12,739                        13,086                     
 

Taxation

                    (2,797                     (3,416                  
 

Profit for the period

                    9,942                        9,670                     
 

    

                                                                 
 

Basic earnings per share ($)

                    7.28                        6.71                     
 

2011 Reconciliation of Reported results to Core results

 

  

       
                          Merck & MedImmune           Profit on            
             

2011

Reported

$m

   

Restructuring

costs

$m

   

Amortisation

$m

   

Intangible

impairments

$m

   

Legal

settlements

$m

   

disposal of

Astra Tech

$m

   

2011

Core

$m

     
 

Gross profit

            27,565        54                                    27,619     
 

Distribution costs

            (346                                        (346  
 

Research and development

            (5,523     468               22                      (5,033  
 

Selling, general and administrative costs

  

    (11,161     639        469               135               (9,918  
 

Profit on disposal of Astra Tech

            1,483                                    (1,483         
 

Other operating income and expense

            777               68                             845     
 

Operating profit

      12,795        1,161        537        22        135        (1,483     13,167     
   

Add back: Research and development

  

    5,523        (468            (22                   5,033       
   

Pre-R&D operating profit

      18,318        693        537               135        (1,483     18,200       
   

Pre-R&D operating margin %

            54.5%                                                54.2%       
 

Net finance expense

            (428                                        (428  
 

Profit before tax

            12,367        1,161        537        22        135        (1,483     12,739     
 

Taxation

            (2,351     (306     (98     (6     (36            (2,797  
 

Profit for the period

            10,016        855        439        16        99        (1,483     9,942     
 

    

                                                                 
 

Basic earnings per share ($)

            7.33        0.63        0.32        0.01        0.07        (1.08     7.28     

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   95

Table of Contents

Performance | Financial Review

 

2011 revenue increased by 1% on a Reported basis but decreased by 2% on a CER basis. As in 2010, revenue benefited from strong growth of Crestor, Symbicort and the Seroquel franchise but was offset by lower revenues for Nexium, Arimidex and Seloken/Toprol-XL . Emerging Markets sales growth of 10% in 2011 (Reported: 11%) and Established ROW 4% (Reported: 14%) was offset by a decline in 2011 US sales of 2% (Reported: 2%) and Western Europe of 11% (Reported: 7%). Further details of our sales performance are contained in the Therapy Area Review from page 50 and the Geographical Review from page 70.

Core gross margin in 2011 of 82.2% increased 1.3 percentage points (Reported: 1.0 percentage points). The 2011 year-on-year improvement in the margin was largely due to the impact of the intangible impairment related to lesogaberan on 2010 gross margin and a $131 million benefit from the settlement of a royalty dispute with PDL Biopharma Inc. in 2011.

Core R&D expenditure in 2011 was $5,033 million, 15% higher than 2010 (Reported: 19%), driven by higher intangible impairments charged to R&D expenditure in 2011, including $285 million for olaparib and $150 million for TC-5214, and late-stage project spend.

2011 Core SG&A costs of $9,918 million were 2% lower than in 2010 (Reported: 1% higher). Investment in Emerging Markets and recently launched brands, as well as the impact of the US healthcare reform excise tax were more than offset by operational efficiencies across Established Markets.

Core other income in 2011 of $845 million was $65 million less than the previous year, principally as a result of a higher level of disposal gains in 2010.

Core pre-R&D operating margin was 54.2% in 2011, up 1.0 percentage points (Reported: 0.7 percentage points), as the higher 2011 gross margin was only slightly offset by lower Core other income and higher SG&A costs as a percentage of revenue.

2011 Core operating profit was $13,167 million, a decrease of 4% from 2010 (Reported: 3%). Core operating margin declined by 1.2 percentage points (Reported: 1.6 percentage points) to 39.2% in 2011 as a result of the higher R&D spend and lower Core other operating income.

 

Core EPS was $7.28 in 2011, up 7% (Reported: 9%), with the lower operating profit offset by a lower tax rate, lower net interest as well as the benefit of a lower average number of shares outstanding.

Within Core adjustments for 2011, restructuring costs and amortisation were broadly in line with 2010. Non-core intangible impairments and legal provisions were significantly reduced from 2010. In 2011, Core adjustments also included the profit on the sale of our dental and healthcare subsidiary Astra Tech. Excluded from 2011 Core results were:

 

> Impairment charges of $22 million (2010: $568 million), arising from impairments of assets capitalised as part of the MedImmune acquisition.
> $135 million (2010: $612 million) of legal provision charges in respect of the ongoing Seroquel IR product liability litigation, Average Wholesale Price litigation in the US and the Toprol-XL anti-trust litigation.
> Restructuring costs totalling $1,161 million in 2011 (2010: $1,202 million), incurred as the Group continued its previously announced efficiency programmes.
> Amortisation totalling $537 million (2010: $518 million) relating to assets capitalised in 2011 as part of the MedImmune acquisition and the Merck exit arrangements.
> Profit on sale of our subsidiary Astra Tech of $1,483 million. On 31 August 2011, we completed the sale of Astra Tech to DENTSPLY International Inc. for a net cash consideration of $1,772 million. Further details of this disposal are included in Note 22 to the Financial Statements on page 173.

2011 Reported operating profit was up 10% at CER (Reported: 11%) at $12,795 million, largely as a result of the impact of the profit on the disposal of Astra Tech. Reported EPS was $7.33 in 2011, up 29% (Reported: 31%), as a result of the same factors affecting Core EPS along with the profit recognised on the disposal of Astra Tech.

Net finance expense was $428 million in 2011, against $517 million in 2010, due to reduced interest payable on lower debt balances ($46 million) and a lower net pension interest expense of $55 million principally due to increased pension assets held by our defined benefit schemes.

 

The 2011 Reported taxation charge of $2,351 million (2010: $2,896 million) consisted of a current tax charge of $2,578 million (2010: $3,435 million) and a credit arising from movements on deferred tax of $227 million (2010: $539 million). The 2011 current year tax charge included a prior period current tax credit of $102 million (2010: charge of $370 million). The Reported tax rate for 2011 was 19.0% (2010: 26.4%). The 2011 Reported tax rate benefited from the non-taxable gain on the disposal of Astra Tech and an adjustment in respect of prior periods following the announcement in March 2011 that HM Revenue & Customs in the UK and the US Internal Revenue Service had agreed the terms of an Advance Pricing Agreement regarding transfer pricing arrangements for AstraZeneca’s US business for the period from 2002 to the end of 2014 and a related valuation matter. Excluding these benefits, the Reported tax rate for 2011 was 26.4%.

Total comprehensive income for 2011 increased by $1,364 million to $9,470 million. This was driven by the increase in profit in 2011 of $1,935 million, offset by a decrease of $571 million in other comprehensive income, principally due to $741 million of actuarial losses on our defined benefit schemes arising from lower discount rates being applied in 2011 to our long-term pension obligations reflecting external market conditions.

Cash flow and liquidity – 2011

All data in this section is on a Reported basis.

Cash generated from operating activities was $7,821 million in the year to 31 December 2011, compared with $10,680 million in 2010. The decrease of $2,859 million was primarily driven by higher tax payments made in 2011, including a net amount of $1.1 billion in relation to the Advance Pricing Agreement between the UK and US governments’ tax authorities and the settlement of a related valuation matter, an increase in trade and other receivables and higher contributions made to our UK defined benefit pension fund.

Investment cash inflows of $577 million in 2011 included the sale of Astra Tech ($1,772 million). Cash outflows on the purchase of tangible fixed assets amounted to $839 million in 2011, in line with the previous year.

Net cash distributions to shareholders increased from $5,471 million in 2010 to $9,370 million in 2011 through dividend payments of $3,764 million and net share repurchases of $5,606 million.

 

 

96   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

At 31 December 2011, outstanding gross debt (interest-bearing loans and borrowings) was $9,328 million (2010: $9,222 million). Of this gross debt, $1,990 million was due within one year (2010: $125 million).

Financial position – 2011

All data in this section is on a Reported basis.

In 2011, net assets increased by $62 million to $23,472 million. The increase in net assets as a result of the 2011 Group profit of $10,016 million was offset by dividends of $3,752 million and share repurchases of $6,015 million.

Property, plant and equipment

Property, plant and equipment decreased by $532 million to $6,425 million in 2011. Additions of $807 million (2010: $808 million) were offset by depreciation of $1,068 million (2010: $1,076 million) and disposals of $233 million (2010: $73 million), including $151 million of assets on the sale of Astra Tech.

Goodwill and intangible assets

Our goodwill of $9,862 million at 31 December 2011 (2010: $9,871 million) principally arose on the acquisition of MedImmune and the restructuring of our US joint venture with Merck in 1998. No goodwill was capitalised in 2011.

Intangible assets amounted to $10,980 million at 31 December 2011 (2010: $12,158 million). Intangible asset additions were $442 million in 2011 (2010: $1,791 million), amortisation was $911 million (2010: $810 million) and impairments totalled $553 million (2010: $833 million). $113 million of intangible assets were disposed of on the sale of Astra Tech in 2011.

Intangible asset impairment charges recorded in 2011 included $285 million following the termination of development of olaparib for the maintenance treatment of serous ovarian cancer and an impairment of $150 million reflecting a lower probability of success assessment for TC-5214, based on the results of the first two of four Phase III efficacy and tolerability studies.

Receivables, payables and provisions

In 2011, trade receivables increased by $383 million to $6,630 million driven, principally, by higher gross sales in the US in December 2011 and the way calendar working days fell at the 2011 year end. Other receivables increased by $566 million to $1,237 million at 31 December 2011 driven by an increase in our Seroquel IR -related settlement funds.

 

Trade and other payables increased by $326 million in 2011, driven by increases in accruals of $177 million and rebates and chargebacks of $446 million, offset by a decrease in other payables of $215 million. The increase in rebates and chargebacks arose principally from increased managed-care and group purchasing organisation rebates. Further details of the movements on rebates and chargebacks are included from page 99.

The movement in provisions of $76 million in 2011 included $716 million of additional charges recorded in the year, offset by $657 million of cash payments. Included within the $716 million of charges in 2011 was $135 million in respect of legal charges and $450 million for our global restructuring initiative. 2011 cash payments of $657 million included $377 million against our ongoing global restructuring initiative and $153 million related to legal matters.

Tax payable and receivable

Net income tax payable in 2011 decreased by $1,521 million to $2,334 million, principally due to the payment of a net amount of $1.1 billion in relation to the Advance Pricing Agreement between the UK and US governments’ tax authorities and the settlement of a related valuation matter. The tax receivable balance of $1,056 million largely comprised tax owing to AstraZeneca from certain governments expected to be received on settlements of transfer pricing audits and disputes. Net deferred tax liabilities reduced by $449 million in 2011.

Retirement benefit obligations

Net retirement benefit obligations increased by $202 million in 2011, due to an increase in post-retirement scheme obligations of $954 million driven by a reduction in the discount rate applied to long-term scheme obligations, reflecting present market conditions for corporate bonds, offset by pension fund employer contributions made in the year of $733 million (2010: $469 million).

Revised Core financial measures

As detailed in our announcement of 12 November 2012, with effect from our first quarter results in 2013, the Group will update its definition of Core financial measures to exclude all intangible asset amortisation charges and impairments, except those for IS-related intangibles. As intangible assets acquired as a result of externalisation become an increasing proportion of the Group’s asset base,

the new definition has been extended to provide better clarity of the impact from amortisation and impairment charges included in Reported results and, in addition, while recognising that non-GAAP measures differ between companies, it will aid comparability of our results versus our peers.

The items excluded from Core results under the existing definition, as disclosed in detail on page 88, remain a constituent part of the new definition. The existing definition excludes from our Core numbers certain significant items, such as charges and provisions related to our global restructuring programmes, amortisation and impairment of the significant intangibles relating to our acquisition of MedImmune in 2007 and our exit arrangements with Merck in the US, and other specified items. In determining the adjustments to arrive at the Core result, we use a set of established principles relating to the nature and materiality of individual items or groups of items, excluding, for example, events which (i) are outside of the normal course of business, (ii) are incurred in a pattern that is unrelated to the trends in the underlying financial performance of our ongoing business, or (iii) are related to major acquisitions, to ensure that investors’ ability to evaluate and analyse the underlying financial performance of our ongoing business is enhanced.

Adjustments between Reported and revised Core performance measures

Under the revised definition of Core, our Reported performance will be adjusted for:

 

> Amortisation and impairments of intangible assets. The definition of this item will be updated to include all amortisation and impairment charges for intangible assets except for those arising on IS-related assets. Adjusting for these items removes the volatility when impairments are booked on such assets and is intended to provide a better measure of underlying business performance. It will be extended to cover all amortisation and impairments relating to product marketing and distribution rights and other intangibles, incorporating those already excluded under the current definition relating to our acquisition of MedImmune and our exit arrangements with Merck. The amortisation and impairment of IS-related intangibles
 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   97

Table of Contents

Performance | Financial Review

 

   are not included in the adjustment, and will remain in Core.
> Restructuring costs. The definition for this item has not been changed. These charges arise from the major restructuring programmes announced by the Group.
> Legal charges and other charges. The definition for this item has not been changed. Legal payments, charges and expenses related to settlements, judgments and fines in the context of product liability litigation, anti-trust litigation, patent litigation and government
  investigations will be excluded from the Core measures and the adjustment will be stated net of related insurance recoveries. In the ordinary course of business, external legal professional fees, including those relating to IP protection costs, and the costs of AstraZeneca’s in-house legal function will remain in Core. Professional fees directly attributable to AstraZeneca’s significant acquisitions and other significant business combination activity will continue to be excluded from Core. Other specified items deemed not
  to be in the ordinary course of business will continue to be excluded from Core.
> Tax on adjustments. The definition for this item has not been changed. The Group’s Reported tax rate, adjusted for significant one-off items embedded within that rate, is applied to all taxable Core adjustments.

Reconciliations of Existing Core to Revised Core

The adjustments that will be made to our existing Core definition to arrive at our revised Core definition for use from 2013 onwards are detailed in the tables below.

 

 

2012 Reconciliation of Existing Core results to Revised Core results

 

    

 

    Revised Core additional
adjustments 		   

 

    Revised Core
2012 compared with 2011 		 
    

2012 Existing

Core

$m (page 89)

    Amortisation     Impairments    

2012 Revised

Core

$m

   

CER growth

%

   

Total growth

%

 

Revenue

     27,973                      27,973        (15     (17

Cost of sales

     (5,257     325               (4,932                

Gross profit

     22,716        325               23,041        (15     (17

Distribution costs

     (320                   (320     (5     (8

Research and development

     (4,452     25        186        (4,241     (4     (5

Selling, general and administrative costs

     (8,541     152               (8,389     (13     (15

Other operating income and expense

     1,027        41               1,068        29        26   

Operating profit

     10,430        543        186        11,159        (17     (20

Net finance expense

     (430                   (430                

Profit before tax

     10,000        543        186        10,729        (18     (20

Taxation

     (1,885     (107     (45     (2,037                

Profit for the period

     8,115        436        141        8,692        (15     (17

    

                                                

Basic earnings per share ($)

     6.41        0.35        0.11        6.87        (8     (11

2011 Reconciliation of Existing Core results to Revised Core results

 

  

   
    

 

    Revised Core  additional
adjustments 		   

 

    Revised Core
2011 compared with 2010 		 
    

2011 Existing

Core

$m (page 95)

    Amortisation     Impairments    

2011 Revised

Core

$m

   

CER growth

%

   

Total growth

%

 

Revenue

     33,591                      33,591        (2     1   

Cost of sales

     (5,972     129               (5,843                

Gross profit

     27,619        129               27,748        (1     2   

Distribution costs

     (346                   (346     (1     3   

Research and development

     (5,033     27        527        (4,479     6        10   

Selling, general and administrative costs

     (9,918     78        4        (9,836     (2     1   

Other operating income and expense

     845                      845        (8     (7

Operating profit

     13,167        234        531        13,932        (2     (1

Net finance expense

     (428                   (428                

Profit before tax

     12,739        234        531        13,504        (1       

Taxation

     (2,797     (28     (140     (2,965                

Profit for the period

     9,942        206        391        10,539        4        5   

    

                                                

Basic earnings per share ($)

     7.28        0.15        0.29        7.72        10        11   

 

98   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

Financial risk management

Financial risk management policies

Insurance

Our risk management processes are described in the Managing risk section from page 74. These processes enable us to identify risks that can be partly or entirely mitigated through the use of insurance. We negotiate best available premium rates with insurance providers on the basis of our extensive risk management procedures. In the current insurance market, the level of cover is decreasing while premium rates are increasing. Rather than simply paying higher premiums for lower cover, we focus our insurance resources on the most critical areas, or where there is a legal requirement, and where we can get best value for money. Risks to which we pay particular attention include business interruption, Directors’ and Officers’ liability and property damage. Insurance for product liability has not been available on commercially acceptable terms for several years and the Group has not held product liability insurance since February 2006.

Taxation

Tax risk management forms an integrated part of the Group’s risk management processes. Our tax strategy is to manage tax risks and tax costs in a manner consistent with shareholders’ best long-term interests, taking into account both economic and reputational factors. We draw a distinction between tax planning using artificial structures and optimising tax treatment of business transactions, and we engage only in the latter.

Treasury

The principal financial risks to which the Group is exposed are those arising from liquidity, interest rate, foreign currency and credit. The Group has a centralised treasury function to manage these risks in accordance with Board-approved policies. Specifically, liquidity risk is managed through maintaining access to a number of sources of funding to meet anticipated funding requirements, including committed bank facilities and cash resources. Interest rate risk is managed through maintaining a debt portfolio that is weighted towards fixed rates of interest. Accordingly, the Group’s net interest charge is not significantly affected by movements in floating rates of interest. We do not currently hedge the impact on earnings and cash flow of changes in exchange rates, with the exception of the currency exposure that arises between the booking and settlement dates on non-local currency purchases and sales by subsidiaries and the external dividend. Credit risk is managed through setting and monitoring credit limits appropriate for the assessed risk of the counterparty.

Our capital and risk management objectives and policies are described in further detail in Note 23 to the Financial Statements from page 175 and in the Risk section from page 74.

Sensitivity analysis of the Group’s exposure to exchange rate and interest rate movements is also detailed in Note 23 to the Financial Statements from page 175.

Critical accounting policies and estimates

Our Financial Statements are prepared in accordance with IFRSs as adopted by the EU (adopted IFRS) and as issued by the IASB, and the accounting policies employed are set out in the Group Accounting Policies section in the Financial Statements from page 146. In applying these policies, we make estimates and assumptions that affect the reported amounts of assets and liabilities and disclosure of contingent assets and liabilities. The actual outcome could differ from those estimates. Some of these policies require a high level of judgement because the areas are especially subjective or complex. We believe that the most critical accounting policies and significant areas of judgement and estimation are in:

 

> revenue recognition
> research and development
> impairment testing of goodwill and intangible assets
> litigation
> post-retirement benefits
> taxation.

Revenue recognition

Revenue is recorded at the invoiced amount (excluding inter-company sales and value added taxes) less movements in estimated accruals for rebates and chargebacks given to managed-care and other customers and product returns – a particular feature in the US. The impact in the rest of the world is not significant. It is the Group’s policy to offer a credit note for all returns and to destroy all returned stock in all markets. Cash discounts for prompt payment are also deducted from sales. Revenue is recognised at the point of delivery, which is usually when title passes to the customer either on shipment or on receipt of goods by the customer depending on local trading terms. Income from royalties and from disposals of IP, brands and product lines is included in other operating income.

Rebates, chargebacks and returns in the US

When invoicing sales in the US, we estimate the rebates and chargebacks that we expect to pay. These rebates typically arise from sales contracts with third party managed-care organisations, hospitals, long-term care facilities, group purchasing organisations and various federal or state programmes (Medicaid ‘best price’ contracts, supplemental rebates etc). They can be classified as follows:

 

> Chargebacks, where we enter into arrangements under which certain parties, typically hospitals, the Department of Veterans Affairs, Public Health Service Covered Entities and the Department of Defense, are able to buy products from wholesalers at the lower prices we have contracted with them. The chargeback is the difference between the price we invoice to the wholesaler and the contracted price charged by the wholesaler. Chargebacks are paid directly to the wholesalers.
> Regulatory, including Medicaid and other federal and state programmes, where we pay rebates based on the specific terms of agreements with the US Department of Health and Human Services and with individual states, which include product usage and information on best prices and average market prices benchmarks.
> Contractual, under which entities such as third party managed-care organisations, long-term care facilities and group purchasing organisations are entitled to rebates depending on specified performance provisions, which vary from contract to contract.

The effects of these deductions on our US pharmaceuticals revenue and the movements on US pharmaceuticals revenue provisions are set out overleaf.

Accrual assumptions are built up on a product-by-product and customer-by-customer basis, taking into account specific contract provisions coupled with expected performance, and are then aggregated into a weighted average rebate accrual rate for each of our products. Accrual rates are reviewed and adjusted on a monthly basis. There may be further adjustments when actual rebates are invoiced based on utilisation information submitted to us (in the case of contractual rebates) and claims/invoices are received (in the case of regulatory rebates and chargebacks). We believe that we have made reasonable estimates for future rebates using a similar methodology to that of previous years. Inevitably, however, such estimates involve judgements on aggregate future sales levels, segment mix and the customers’ contractual performance.

The large increase in managed-care and group purchasing organisation rebates in 2011 was principally driven by the impacts of the Affordable Care Act. See page 71 of the Geographical Review for more information. The 2012 adjustment in respect of prior years includes refinements of the provisions recorded for the Affordable Care Act.

Cash discounts are offered to customers to encourage prompt payment. Accruals are calculated based on historical experience and are adjusted to reflect actual experience.

 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   99

Table of Contents

Performance | Financial Review

Gross to net sales – US Pharmaceuticals

 

    

2012

$m

   

2011

$m

   

2010

$m

 

Gross sales

     20,747        23,613        22,909   

Chargebacks

     (2,261     (1,958     (2,075

Regulatory – US government and state programmes

     (1,426     (2,293     (1,949

Contractual – Managed-care and group purchasing organisation rebates

     (5,597     (5,437     (4,755

Cash and other discounts

     (401     (452     (437

Customer returns

     (182     (72     (21

Other

     (273     (276     (265

Net sales

     10,607        13,125        13,407   

Movement in provisions – US Pharmaceuticals

 

    

Brought

forward at

1 January

2012

$m

    

Provision for

current year

$m

    

Adjustment in

respect of

prior years

$m

   

Returns and

payments

$m

   

Carried

forward at

31 December

2012

$m

 

Chargebacks

     395         2,296         (35     (2,343     313   

Regulatory – US government and state programmes

     1,290         1,585         (159     (1,891     825   

Contractual – Managed-care and group purchasing organisation rebates

     1,600         5,578         19        (5,849     1,348   

Cash and other discounts

     41         401                (409     33   

Customer returns

     121         117         65        (92     211   

Other

     80         273                (308     45   

Total

     3,527         10,250         (110     (10,892     2,775   

    

            
    

Brought

forward at

1 January

2011

$m

    

Provision for

current year

$m

    

Adjustment in

respect of

prior years

$m

   

Returns and

payments

$m

   

Carried

forward at

31 December

2011

$m

 

Chargebacks

     523         2,012         (54     (2,086     395   

Regulatory – US government and state programmes

     1,122         2,364         (71     (2,125     1,290   

Contractual – Managed-care and group purchasing organisation rebates

     1,194         5,452         (15     (5,031     1,600   

Cash and other discounts

     41         452                (452     41   

Customer returns

     133         75         (3     (84     121   

Other

     64         276                (260     80   

Total

     3,077         10,631         (143     (10,038     3,527   

    

            
    

Brought

forward at

1 January

2010

$m

    

Provision for

current year

$m

    

Adjustment in

respect of

prior years

$m

   

Returns and

payments

$m

   

Carried

forward at

31 December

2010

$m

 

Chargebacks

     396         2,107         (32     (1,948     523   

Regulatory – US government and state programmes

     775         1,984         (35     (1,602     1,122   

Contractual – Managed-care and group purchasing organisation rebates

     1,447         4,826         (71     (5,008     1,194   

Cash and other discounts

     41         438         (1     (437     41   

Customer returns

     177         22         (1     (65     133   

Other

     59         269         (4     (260     64   

Total

     2,895         9,646         (144     (9,320     3,077   

 

100   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

Industry practice in the US allows wholesalers and pharmacies to return unused stocks within six months of, and up to 12 months after, shelf-life expiry. The customer is credited for the returned product by the issuance of a credit note. Returned products are not exchanged for products from inventory and once a return claim has been determined to be valid and a credit note has been issued to the customer, the returned products are destroyed. At the point of sale in the US, we estimate the quantity and value of products which may ultimately be returned. Our returns accruals in the US are based on actual experience. Our estimate is based on the preceding 12 months for established products together with market-related information, such as estimated stock levels at wholesalers and competitor activity, which we receive via third party information services. For newly launched products, we use rates based on our experience with similar products or a pre-determined percentage.

For products facing generic competition (such as Seroquel IR in the US) our experience is that we usually lose the ability to estimate the levels of returns from wholesalers with the same degree of precision that we can for products still subject to patent protection. This is because we have limited or no insight into a number of areas: the actual timing of the generic launch (for example, a generic manufacturer may or may not have produced adequate pre-launch inventory); the pricing and marketing strategy of the competitor; the take-up of the generic; and (in cases where a generic manufacturer has approval to launch only one dose size in a market of several dose sizes) the likely level of switching from one dose to another. Under our accounting policy, revenue is recognised only when the amount of the revenue can be measured reliably. Our approach in meeting this condition for products facing generic competition will vary from product to product depending on the specific circumstances.

The closing adjustment in respect of prior years benefited 2012 net US pharmaceuticals revenue by 1.0% (2011: increased revenue by 1.1%; 2010: increased revenue by 1.1%). However, taking into account the adjustments affecting both the current and the prior year, 2011 revenue was reduced by 0.3%, and 2010 revenue was not impacted, by adjustments between years.

 

We have distribution service agreements with major wholesaler buyers which serve to reduce the speculative purchasing behaviour of the wholesalers and reduce short-term fluctuations in the level of inventory they hold. We do not offer any incentives to encourage wholesaler speculative buying and attempt, where possible, to restrict shipments to underlying demand when such speculation occurs.

Sales of intangible assets

A consequence of charging all internal R&D expenditure to the income statement in the year in which it is incurred (which is normal practice in the pharmaceutical industry) is that we own valuable intangible assets which are not recorded on the balance sheet. We also own acquired intangible assets which are included on the balance sheet. As a consequence of regular reviews of product strategy, from time to time we sell such assets and generate income. Sales of product lines are often accompanied by an agreement on our part to continue manufacturing the relevant product for a reasonable period (often about two years) while the purchaser constructs its own manufacturing facilities. The contracts typically involve the receipt of an upfront payment, which the contract attributes to the sale of the intangible assets, and ongoing receipts, which the contract attributes to the sale of the product we manufacture. In cases where the transaction has two or more components, we account for the delivered item (for example, the transfer of title to the intangible asset) as a separate unit of accounting and record revenue on delivery of that component provided that we can make a reasonable estimate of the fair value of the undelivered component. Where the fair market value of the undelivered component (for example, a manufacturing agreement) exceeds the contracted price for that component, we defer an appropriate element of the upfront consideration and amortise this over the performance period. However, where the fair market value of the undelivered component is equal to or lower than the contracted price for that component, we treat the whole of the upfront amount as being attributable to the delivered intangible assets and recognise that part of the revenue upon delivery. No element of the contracted revenue related to the undelivered component is allocated to the sale of the intangible asset. This is because the contracted revenue relating to the undelivered component is contingent on future events (such as sales) and so cannot be anticipated.

 

Research and development

Our business is underpinned by our marketed products and development portfolio. The R&D expenditure on internal activities to generate these products is generally charged to profit in the year that it is incurred. Purchases of IP and product rights to supplement our R&D portfolio are capitalised as intangible assets. Further details of this policy are included in the Group Accounting Policies section of our Financial Statements from page 146. Such intangible assets are amortised from the launch of the underlying products and are tested for impairment both before and after launch. This policy is in line with practice adopted by major pharmaceutical companies.

Impairment testing of goodwill and intangible assets

We have significant investments in goodwill and intangible assets as a result of acquisitions of businesses and purchases of assets, such as product development and marketing rights.

Details of the estimates and assumptions we make in our annual impairment testing of goodwill are included in Note 8 to the Financial Statements on page 158. No impairment of goodwill was identified.

Impairment reviews have been carried out on all intangible assets that are in development (and not being amortised), all major intangible assets acquired during the year and all intangible assets that have had indications of impairment during the year. Sales forecasts and specific allocated costs (which have both been subject to appropriate senior management sign-off) are discounted using appropriate rates based on AstraZeneca’s risk-adjusted pre-tax weighted average cost of capital. Our weighted average cost of capital reflects factors such as our capital structure and our costs of debt and equity. In building to the range of rates used in our internal investment appraisal of future projects and capital investment decisions, we adjust our weighted average cost of capital for other factors, which reflect, without limitation, local matters such as risk on a case-by-case basis.

 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   101

Table of Contents

Performance | Financial Review

 

The majority of our investments in intangible assets and goodwill arose from the restructuring of the joint venture with Merck in 1998, the acquisition of MedImmune in 2007 and the payments to partially retire Merck’s interests in our products in the US in 2008 and 2010. Additions in 2012 have included intangible assets acquired through our new collaboration with BMS concerning Amylin’s portfolio of products, our acquisition of Ardea and revised arrangements with Merck concerning the final step in our exit arrangements. The Group, including acquisitions, is considered a single cash-generating unit for impairment purposes. We are satisfied that the carrying values at 31 December 2012 are fully justified by estimated future cash flows. The accounting for our arrangements with Merck and our Amylin collaboration with BMS are fully explained in Note 9 to the Financial Statements from page 159. Further details of our acquisition of Ardea are included in Note 22 to the Financial Statements from page 173.

Further details of the estimates and assumptions we make in impairment testing of intangible assets are included in Note 9 to the Financial Statements.

Litigation

In the normal course of business, contingent liabilities may arise from product-specific and general legal proceedings, from guarantees or from environmental liabilities connected with our current or former sites. Where we believe that potential liabilities have a less than 50% probability of crystallising, or where we are unable to make a reasonable estimate of the liability, we treat them as contingent liabilities. These are not provided for but are disclosed in Note 25 to the Financial Statements from page 183.

In cases that have been settled or adjudicated, or where quantifiable fines and penalties have been assessed and which are not subject to appeal (or other similar forms of relief), or where a loss is probable (more than 50% assessed probability) and we are able to make a reasonable estimate of the loss, we indicate the loss absorbed or the amount of the provision accrued.

 

Where it is considered that the Group is more likely than not to prevail, or in the rare circumstances where the amount of the legal liability cannot be estimated reliably, legal costs involved in defending the claim are charged to profit as they are incurred. Where it is considered that the Group has a valid contract which provides the right to reimbursement (from insurance or otherwise) of legal costs and/or all or part of any loss incurred or for which a provision has been established and we consider recovery to be virtually certain, then the best estimate of the amount expected to be received is recognised as an asset.

Assessments as to whether or not to recognise provisions or assets and of the amounts concerned usually involve a series of complex judgements about future events and can rely heavily on estimates and assumptions. AstraZeneca believes that the provisions recorded are adequate based on currently available information and that the insurance recoveries recorded will be received. However, given the inherent uncertainties involved in assessing the outcomes of these cases and in estimating the amount of the potential losses and the associated insurance recoveries, we could in future periods incur judgments or insurance settlements that could have a material adverse effect on our results in any particular period.

The position could change over time, and there can, therefore, be no assurance that any losses that result from the outcome of any legal proceedings will not exceed the amount of the provisions that have been booked in the accounts.

Although there can be no assurance regarding the outcome of legal proceedings, we do not currently expect them to have a material adverse effect on our financial position, but they could significantly affect our financial results in any particular period.

Post-retirement benefits

We offer post-retirement benefit plans which cover many of our employees around the world. In keeping with local terms and conditions, most of these plans are ‘defined contribution’ in nature, where the resulting

income statement charge is fixed at a set level or is a set percentage of employees’ pay. However, several plans, mainly in the UK (which has by far the largest single scheme), the US and Sweden, are defined benefit plans where benefits are based on employees’ length of service and final salary (typically averaged over one, three or five years). The UK and US defined benefit schemes were closed to new entrants in 2000. All new employees in these countries are offered defined contribution schemes.

In applying IAS 19, we recognise all actuarial gains and losses immediately through reserves. This methodology results in a less volatile income statement charge than under the alternative approach of recognising actuarial gains and losses over time. Investment decisions in respect of defined benefit schemes are based on underlying actuarial and economic circumstances with the intention of ensuring that the schemes have sufficient assets to meet liabilities as they fall due, rather than meeting accounting requirements. The trustees follow a strategy of awarding mandates to specialist, active investment managers, which results in a broad diversification of investment styles and asset classes. The investment approach is intended to produce less volatility in the plan asset returns.

In assessing the discount rate applied to the obligations, we have used rates on AA corporate bonds with durations corresponding to the maturities of those obligations, except in Sweden where we have used rates on mortgage bonds as the market in high quality corporate bonds is insufficiently deep.

In all cases, the pension costs recorded in the Financial Statements are assessed in accordance with the advice of independent qualified actuaries but require the exercise of significant judgement in relation to assumptions for future salary and pension increases, long-term price inflation and investment returns.

As detailed in our Accounting Policies section of the Financial Statements on page 146, the Group will adopt the amended IAS 19 from 1 January 2013.

 

 

102   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

Taxation

Accruals for tax contingencies require management to make judgements and estimates in relation to tax audit issues and exposures. Amounts accrued are based on management’s interpretation of country-specific tax law and the likelihood of settlement. Tax benefits are not recognised unless the tax positions are probable of being sustained. Once considered to be probable, management reviews each material tax benefit to assess whether a provision should be taken against full recognition of the benefit on the basis of potential settlement through negotiation and/or litigation. All such provisions are included in current liabilities. Any recorded exposure to interest on tax liabilities is provided for in the tax charge.

AstraZeneca faces a number of transfer pricing audits in jurisdictions around the world and, in some cases, is in dispute with the tax authorities. These disputes usually result in taxable profits being increased in one territory and correspondingly decreased in another. Our balance sheet positions for these matters reflect appropriate corresponding relief in the territories affected.

Further details of the estimates and assumptions we make in determining our recorded liability for transfer pricing audits and other tax contingencies are included in the Tax section of Note 25 to the Financial Statements on page 189.

Sarbanes-Oxley Act Section 404

As a consequence of our NYSE listing, AstraZeneca is required to comply with those provisions of the Sarbanes-Oxley Act applicable to foreign issuers. Section 404 of the Sarbanes-Oxley Act requires companies annually to assess and make public statements about the quality and effectiveness of their internal control over financial reporting.

Our approach to the assessment has been to select key transaction and financial reporting processes in our largest operating units and a number of specialist areas, such as financial consolidation and reporting, treasury operations and taxation, so that,

in aggregate, we have covered a significant proportion of each of the key line items in our Financial Statements. Each of these operating units and specialist areas has ensured that its relevant processes and controls are documented to appropriate standards, taking into account, in particular, the guidance provided by the SEC. We have also reviewed the structure and operation of our ‘entity level’ control environment. This refers to the overarching control environment, including structure of reviews, checks and balances that are essential to the management of a well-controlled business.

The Directors have concluded that our internal control over financial reporting is effective at 31 December 2012 and the assessment is set out in the Directors’ Responsibilities for, and Report on, Internal Control over Financial Reporting on page 140. KPMG Audit Plc has audited the effectiveness of our internal control over financial reporting at 31 December 2012 and, as noted in the Auditor’s Reports on the Financial Statements and on Internal Control over Financial Reporting (Sarbanes-Oxley Act Section 404) on page 141, their report is unqualified.

 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   103

Table of Contents

Corporate Governance | The value of innovation

Innovation means

 

LOGO

 

104   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

We are active in pioneering public/private sector collaborations to identify pragmatic ways of overcoming barriers to healthcare at a global level.

 

LOGO

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   105

Table of Contents

Corporate Governance | Board of Directors

as at 31 January 2013

 

LOGO

 

1 Leif Johansson (61)

Non-Executive Chairman of the Board, Chairman of the Nomination and Governance Committee and member of the Remuneration Committee

Elected as a Director in April 2012 and became Non-Executive Chairman of the Board on 1 June. Leif Johansson is also the Chairman of global telecommunications company, LM Ericsson, a position he has held since April 2011. From 1997 until 2011, he was Chief Executive of AB Volvo, one of the world’s leading manufacturers of trucks, buses, construction equipment, drive systems and aerospace components. He spent a significant part of his early career at AB Electrolux, latterly as Chief Executive from 1994 to 1997. He was a Non-Executive Director of BMS from 1998 to September 2011, serving on the board’s audit committee and compensation and management development committee. He is Chairman of the European Round Table of Industrialists and the International Advisory Board of the Nobel Foundation. He holds board positions at Svenska Cellulosa Aktiebolaget SCA and Ecolean AB. He holds an MSc in engineering from Chalmers University of Technology, Gothenburg, and has been a member of the Royal Swedish Academy of Engineering Sciences since 1994. He became Chairman of the Academy in 2012.

2 Pascal Soriot (53)

Executive Director

and Chief Executive Officer

Pascal Soriot was appointed as a Director and as CEO in October. From 2010 to September 2012, he served as Chief Operating Officer of Roche AG’s pharmaceuticals division. Prior to that, he was CEO of Genentech, a biologics business, and led its successful merger with Roche. He joined the pharmaceutical industry in 1986 and has worked in senior management roles throughout the world in a number of major companies since then. He brings to AstraZeneca a significant breadth of experience in both established and emerging markets, strength of strategic thinking, a successful track record of managing change and putting strategy into operation, as well as the ability to lead a diverse organisation having lived in Australia, Japan,

the US and Europe. He is a doctor of veterinary medicine (École Nationale Vétérinaire d’Alfort, Maisons-Alfort) and holds an MBA from L’Institut Supérieur des Affaires, Jouy-en-Josas.

3 Simon Lowth (51)

Executive Director

and Chief Financial Officer

Appointed as a Director and as CFO in November 2007, and served as Interim CEO from June to September 2012. Simon Lowth is also a Non-Executive Director of Standard Chartered PLC. He was previously at ScottishPower Energy where he was Finance Director, a position he left following completion of the sale of the company to Iberdrola S.A. His move to ScottishPower followed 15 years’ experience with the global management consultancy, McKinsey & Company, where he advised leading multinational companies on a wide range of strategic, financial and operational issues. He has an engineering degree from Cambridge University and an MBA from the London Business School.

4 Geneviève Berger (58)

Non-Executive Director

and member of the Science Committee

Elected as a Director in April 2012. Geneviève Berger is Chief Science Officer at Unilever PLC and a member of the Unilever Leadership Executive. She holds three doctorates – in physics, human biology and a medical doctorate. She was appointed Professor of Medicine at Université Pierre et Marie Curie, Paris in 2006. From 2003 to 2008 she was Professor and Hospital Practitioner at l’Hôpital de la Pitié-Salpêtrière, Paris. Previous positions she has held include Director of the Biotech and Agri-Food Department, then Head of the Technology Directorate at the French Ministry of Research and Technology (1998-2000); Director General, Centre National de la Recherche Scientifique (2000-2003); and Chairman of the Health Advisory Board of the EU Commission (2006-2008). She was a non-executive board member of Unilever from 2007 to 2008 before being appointed to her current position and was a Non-Executive Director of Smith & Nephew plc from 2010 to 2012.

5 Bruce Burlington (64)

Non-Executive Director and member of the Audit Committee and the Science Committee

Appointed as a Director in August 2010. Bruce Burlington is a pharmaceutical product development and regulatory affairs consultant and brings extensive experience in those areas to the Board. He is also a non-executive board member of Cangene Corporation and the International Partnership for Microbicides, and a member of the scientific advisory boards of the International Medical Foundation and H. Lundbeck A/S. Previously he spent 17 years with the FDA, serving as director of the FDA’s Center for Devices and Radiological Health as well as holding a number of senior roles in the Center for Drug Evaluation and Research. After leaving the FDA he served in a series of senior executive positions at Wyeth (now part of Pfizer).

6 Graham Chipchase (50)

Non-Executive Director

and member of the Audit Committee

Elected as a Director in April 2012. Graham Chipchase is the Chief Executive of global consumer packaging company, Rexam PLC. He was appointed to the position in 2010 after previous service at Rexam as Group Director, Plastic Packaging (2005-2009) and Group Finance Director (2003-2005). Prior to joining Rexam, he was Finance Director of Aerospace Services at global engineering group, GKN plc, from 2001 to 2003. After starting his career with Coopers & Lybrand Deloitte, he held a number of finance roles in the industrial gases company, The BOC Group plc (now part of The Linde Group) (1990-2001). He is a Fellow of the Institute of Chartered Accountants in England and Wales and holds an MA (Hons) in chemistry from Oriel College, Oxford.

 

 

106   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

LOGO

 

7 Jean-Philippe Courtois (52)

Non-Executive Director

and member of the Audit Committee

Appointed as a Director in February 2008. Jean-Philippe Courtois has close to 30 years’ experience in the global technology industry. He is President of Microsoft International and a board member of PlaNet Finance. Previously he was Chief Executive Officer and President of Microsoft EMEA and has served as co-chairman of the World Economic Forum’s Global Digital Divide Initiative Task Force and on the European Commission Information and Communication Technology Task Force. In 2009, he also served as an EU Ambassador for the Year of Creativity and Innovation and in 2011 was named as one of ‘Tech’s Top 25’ by The Wall Street Journal Europe.

8 Rudy Markham (66)

Non-Executive Director, Chairman of the Audit Committee, member of the Remuneration Committee and the Nomination and Governance Committee

Appointed as a Director in September 2008. Rudy Markham takes a particular interest on behalf of the Board in SHE assurance. He has significant international business and financial experience, having formerly held a number of senior commercial and financial positions worldwide with Unilever, culminating in his appointment as Chief Financial Officer of Unilever. He is currently Chairman and Non-Executive Director of Moorfields Eye Hospital NHS Foundation Trust and a non-executive member of the boards of United Parcel Services Inc., Standard Chartered PLC and Legal & General plc. He is also a non-executive member of the board of the UK Foreign and Commonwealth Office, a member of the supervisory board of CSM NV, a Fellow of the Chartered Institute of Management Accountants and a Fellow of the Association of Corporate Treasurers. He served as a Non-Executive Director of the UK Financial Reporting Council from 2007 to 2012.

9 Nancy Rothwell (57)

Non-Executive Director, Chairman of the Science Committee, member of the Remuneration Committee and the Nomination and Governance Committee

Appointed as a Director in April 2006. Nancy Rothwell oversees responsible business on behalf of the Board, as is described more fully in the Responsible Business section from page 48. She is a distinguished life scientist and academic and is the President and Vice-Chancellor of the University of Manchester. She is also President of the Society of Biology and Co-Chair of the Prime Minister’s Council for Science and Technology. Previously she has served as President of the British Neuroscience Association and has been on the councils of the Medical Research Council, the Royal Society, the Biotechnology and Biological Sciences Research Council, the Academy of Medical Sciences and Cancer Research UK.

10 Shriti Vadera (50)

Non-Executive Director

and member of the Audit Committee

Appointed as a Director in January 2011. Shriti Vadera has significant experience of emerging markets, and knowledge of global finance and public policy. She is a Non-Executive Director of BHP Billiton Plc and BHP Billiton Limited. She advises funds, governments and companies, and has recently undertaken a number of international assignments including advising the Republic of Korea as Chair of the G20, the government of Dubai on the restructuring of Dubai World, Temasek Holdings, Singapore on strategy and Allied Irish Banks on restructuring and European policy.

She was Minister in the UK government from 2007 to 2009, most latterly in the Cabinet Office and Business Department, working on the government’s response to the financial crisis. From 1999 to 2007, she was on the Council of Economic Advisers, HM Treasury focusing on business and international economic issues. Prior to that she spent 14 years in investment banking with S G Warburg/UBS in banking, project finance and corporate finance specialising in emerging markets.

11 John Varley (56)

Senior independent Non-Executive Director, Chairman of the Remuneration Committee and member of the Nomination and Governance Committee

Appointed as a Director in July 2006. John Varley was formerly Group Chief Executive of the Barclays Group, having held a number of senior positions with the bank during his career, including that of Group Finance Director. He brings additional international, executive business leadership experience to the Board. He is also a Non-Executive Director of BlackRock, Inc., and Rio Tinto plc and Rio Tinto Limited, Chairman of Business Action on Homelessness and of Marie Curie Cancer Care, President of Business Disability Forum, and Honorary President of the UK Drug Policy Commission.

12 Marcus Wallenberg (56)

Non-Executive Director

and member of the Science Committee

Appointed as a Director in April 1999. Marcus Wallenberg has international business experience across a broad range of industry sectors, including the pharmaceutical industry from his directorship with Astra prior to 1999. He is the Chairman of Skandinaviska Enskilda Banken AB, AB Electrolux, Saab AB and LKAB, and a Non-Executive Director of Investor AB, Stora Enso Oyj, Temasek Holdings Limited and the Knut and Alice Wallenberg Foundation.

Other officers of the Company at 31 January 2013 included members of the SET, as set out on pages 108 and 109, and Adrian Kemp, Company Secretary.

 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   107

Table of Contents

Corporate Governance | Senior Executive Team

as at 31 January 2013

 

LOGO

 

1 Pascal Soriot

Chief Executive Officer

See page 106.

2 Simon Lowth

Chief Financial Officer

See page 106.

3 Katarina Ageborg

Chief Compliance Officer

Katarina Ageborg was appointed Chief Compliance Officer in July 2011 and has overall responsibility for the design, delivery and implementation of AstraZeneca’s compliance responsibilities. Since joining AstraZeneca in 1998, she has held a series of senior legal roles supporting Commercial and Regulatory and most recently led the Global IP function from 2008 to 2011. Prior to joining AstraZeneca, she established her own law firm in Sweden and worked as a lawyer practising on both civil and criminal cases.

4 Ruud Dobber

Executive Vice-President, Europe

Ruud Dobber was appointed as Executive Vice-President, Europe in January 2013 and leads AstraZeneca’s commercial operations in Europe. In this capacity, Ruud is responsible for sales, marketing and commercial operations across AstraZeneca’s businesses in the 27 EU member states. Ruud joined AstraZeneca in 1997 and has held a number of senior commercial roles including Regional Vice-President of AstraZeneca’s European, Middle East and African division and Regional Vice-President for the Group’s Asia Pacific region. Since 2012, Ruud has been an Executive Committee Member of EFPIA. In 2011, Ruud was the Chairman of the Asia division of Pharmaceutical Research and Manufacturers of America. Ruud commenced his career as a scientist, researching in the field of immunology and ageing. He holds a doctorate in immunology from the University of Leiden in the Netherlands.

5 Paul Hudson

Executive Vice-President, North America

Paul Hudson was appointed Executive Vice-President, North America in January 2013 and leads AstraZeneca’s commercial operations in North America. In this capacity, he is accountable for driving growth and maximising the contribution of North America to AstraZeneca’s global business. Paul joined AstraZeneca in 2006 as Vice-President and Primary Care Director, UK. Paul’s most recent role with AstraZeneca was President of AstraZeneca’s Japanese business. He has served as a Standing Board Member of Japan Pharmaceuticals Manufacturers Association and EFPIA in Japan. Previously, Paul was President of AstraZeneca’s business in Spain. Before AstraZeneca, Paul worked for Schering-Plough, where he held senior global marketing roles. Paul received a degree in economics from Manchester Metropolitan University and a DipM from the UK’s Chartered Institute of Marketing.

6 Bahija Jallal

Executive Vice-President, MedImmune

Dr Bahija Jallal was appointed Executive Vice-President, MedImmune in January 2013 and is responsible for biologics research, development and clinical activities. Bahija is tasked with advancing the biologic pipeline of drugs. Bahija joined MedImmune as Vice-President, Translational Sciences in 2006 and has held roles of increasing responsibility. Prior to joining AstraZeneca, Bahija worked with Chiron Corporation where she served as Vice-President, Drug Assessment and Development. Bahija received a master’s degree in biology from the Université de Paris VII and her doctorate in physiology from the Université Pierre et Marie Curie, Paris. She conducted her postdoctoral research at the Max-Planck Institute of Biochemistry in Martinsried, Germany. She is a member of the American Association of Cancer Research, the American Association of Science, the Pharmacogenomics Working Group and is a member of the Board of Directors of the Association of Women in Science.

7 Mark Mallon

Executive Vice-President, International

Mark Mallon was appointed as Executive Vice-President, International in January 2013 and is responsible for the growth and performance of AstraZeneca’s commercial businesses in regions including Asia Pacific, Russia, Latin America, the Middle East and Africa. Since joining AstraZeneca in 1994, Mark has held a number of senior sales and marketing roles including Regional Vice-President for Asia Pacific, President of AstraZeneca China and head of marketing, sales and commercial operations for AstraZeneca in Japan. Mark has a degree in chemical engineering from the University of Pennsylvania and an MBA in marketing and finance from the Wharton School of Business.

8 Briggs Morrison

Executive Vice-President,

Global Medicines Development

Dr Briggs Morrison was appointed Executive Vice-President, Global Medicines Development in January 2013 and leads our global late-stage development organisation for both small molecules and biologics. He joined AstraZeneca in 2012 from Pfizer, where he was Head of Medical Excellence, overseeing development, medical affairs, safety and regulatory affairs for Pfizer’s human health businesses. Briggs has a track record of successfully developing novel medicines in roles at both Pfizer and Merck. Briggs has a biology degree from Georgetown University and a medical doctorate from the University of Connecticut. Briggs has also undertaken an internship and residency in internal medicine at the Massachusetts General Hospital, a fellowship in medical oncology at the Dana-Farber Cancer Institute and a post-doctoral research fellowship in genetics at Harvard Medical School.

 

 

108   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

LOGO

 

9 Menelas Pangalos

Executive Vice-President, Innovative Medicines

Menelas (Mene) Pangalos, was appointed Executive Vice-President, Innovative Medicines in January 2013 and leads AstraZeneca’s small molecule discovery research and early development activities. Mene joined AstraZeneca from Pfizer, where he was Senior Vice-President and Chief Scientific Officer of Neuroscience Research. Previously, Mene held senior discovery and neuroscience roles at Wyeth and GSK. He completed his undergraduate degree in biochemistry at the Imperial College of Science and Technology, London and earned a doctorate in neurochemistry from the University of London. He is a Visiting Professor of Neuroscience at King’s College, London. In the UK, Mene sits on the Medical Research Council and the Innovation Board for the Association of the British Pharmaceutical Industry.

10 Jeff Pott

General Counsel

Jeff Pott was appointed General Counsel in January 2009 and has overall responsibility for all aspects of AstraZeneca’s Legal and IP function. He joined AstraZeneca in 1995 and has worked in various litigation roles, where he has had responsibility for IP, anti-trust and product liability litigation. Prior to joining AstraZeneca, he spent five years at the US legal firm Drinker Biddle and Reath LLP, where he specialised in pharmaceutical product liability litigation and anti-trust advice and litigation. He received his bachelor’s degree in political science from Wheaton College and his Juris Doctor Degree from Villanova University School of Law.

11 David Smith

Executive Vice-President, Operations & Information Services

David Smith joined AstraZeneca in 2006 as Executive Vice-President, Operations. He leads AstraZeneca’s global manufacturing and supply organisation and is also responsible for the Safety, Health and Environment, Regulatory Compliance, Procurement and Engineering functions and has overall responsibility for IS. He spent his early career in pharmaceuticals, initially with the Wellcome Foundation in the UK. He subsequently spent nine years in the consumer goods sector working for Estée Lauder Inc. and Timberland LLC in senior supply chain roles. In 2003, he returned to the pharmaceutical sector and joined Novartis in Switzerland.

12 Lynn Tetrault

Executive Vice-President, Human Resources & Corporate Affairs

Lynn Tetrault was appointed Executive Vice-President, Human Resources & Corporate Affairs in 2007, having previously been Vice-President, Corporate Affairs. She has also held the role of Vice-President HR, Global Drug Development and Vice-President, HR in AstraZeneca’s US business following the merger between Astra and Zeneca. She started her career in private law practice where she specialised in general corporate and healthcare law. She joined Astra USA in 1993 as Associate General Counsel in the company’s legal department. She received her bachelor’s degree from Princeton University and her law degree from the University of Virginia Law School.

The SET position of Executive Vice-President, Global Portfolio & Product Strategy is currently vacant, pending the appointment of an individual for this role.

During 2012, Martin Mackay, President, Global R&D (below left) and Tony Zook, Executive Vice-President, Global Commercial Operations (below right) served as SET members. With effect from 15 January 2013, these two roles were eliminated and the newly-constituted SET shown above was appointed. Martin and Tony left the Company at the end of February 2013.

 

LOGO

 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   109

Table of Contents

Corporate Governance | Corporate Governance Report

 

LOGO

 

Since joining the Board and becoming Chairman, I have focused on three main priorities. As Chairman of the Nomination and Governance Committee, my first priority was to lead a thorough search for a new CEO, which started in April 2012. The section on page 117 describing the work of the Nomination and Governance Committee gives more information about this and how the Committee and the Board approach succession planning generally. I am delighted that we were able to recruit Pascal Soriot and appoint him as AstraZeneca’s new CEO with effect from 1 October. Pascal stood out from a strong field of candidates and has a number of attributes that made him the outstanding candidate. Succession planning remains the main focus of the Nomination and Governance Committee’s work.

Alongside the CEO search, I also spent a significant amount of time following my appointment meeting shareholders in the UK, Sweden and the US and listening to their comments and views. I was supported in this by John Varley, who became senior independent Non-Executive Director in April 2012, and Simon Lowth, CFO who acted as Interim CEO for four months at a critical

time for the Company. My thanks go to John and Simon for their work in this regard and for their support during the transition to a new CEO. Since his appointment, Pascal has also met numerous investors. He, Simon and I, supported by John Varley, will work hard to maintain these contacts and a constructive and frank dialogue with our shareholders.

My third priority has been the annual review of AstraZeneca’s strategy. Due to the timing of the CEO succession process, this has run over a longer period than usual to enable Pascal to form his conclusions about AstraZeneca’s strengths, weaknesses and the best strategy for its future success. From a corporate governance perspective, my aim has been to ensure that the review has been thorough; that a good, open and robust discussion about all aspects of the strategy has taken place at the Board table with management being challenged appropriately about their proposals and recommendations; and that all Board members have felt able to and have, in fact, contributed fully to that discussion.

Leif Johansson

Chairman

This Corporte Governance Report describes how the Group is organised, including the overall structure and principal roles and responsibilities of the Board, its Committees and the SET.

Board composition, processes and responsibilities

The Board comprises two Executive Directors (the CEO and the CFO) and 10 Non-Executive Directors. The membership of the Board at 31 January 2013 and information about individual Directors is contained in the Board of Directors section on pages 106 and 107.

All Directors are collectively responsible for the success of the Group. In addition, the Non-Executive Directors are responsible for exercising independent, objective judgement in respect of Board decisions and for scrutinising and challenging management. The Non-Executive Directors also have various responsibilities concerning the integrity of financial information, internal controls and risk management.

Corporate governance

We have prepared this Annual Report with reference to the UK Corporate Governance Code published by the UK Financial

 

 

Length of tenure of   Directors’ nationalities   Gender split
Non-Executive Directors (years)     of Directors

LOGO

 

Leif Johansson, Geneviève Berger and Graham Chipchase have served for less than one year

  LOGO   LOGO

 

110   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

LOGO

 

Reporting Council (FRC) in June 2010. This Corporate Governance Report (together with other sections of this Annual Report) describes how we apply the main principles of good governance in the UK Corporate Governance Code. We have complied throughout the accounting period with the provisions of the UK Corporate Governance Code, which is available on the FRC’s website, frc.co.uk.

Leadership

The roles of Chairman and CEO are split. Leif Johansson, our Non-Executive Chairman, is responsible for leadership of the Board. Our CEO, Pascal Soriot, leads the SET and has executive responsibility for running our business. The Board comprises 10 Non-Executive Directors, including the Chairman, and two Executive Directors – the CEO, Pascal Soriot, and the CFO, Simon Lowth.

All Directors are collectively responsible for our long-term success. In addition, the Non-Executive Directors are responsible for exercising independent, objective judgement in respect of Board decisions and for scrutinising and challenging the actions of executive management.

The Board runs an annual strategy review process. The CEO, the CFO and the SET take the lead in developing our strategy, which is then reviewed, constructively challenged and approved by the Board.

John Varley, who joined the Board as a Non-Executive Director in 2006, was appointed as our senior independent Non-Executive Director in April 2012. The role of the senior independent Non-Executive Director is to provide a sounding board for the Chairman and to serve as an intermediary for the other Directors when necessary. The senior independent Non-Executive Director is also available to shareholders if they have concerns that contact through the normal channels of Chairman or Executive Directors has failed to resolve, or for which such contact is inappropriate.

There are four principal Board Committees: the Audit Committee; the Remuneration Committee; the Nomination and Governance Committee; and the Science Committee.

The membership and work of these Committees is described below. In addition, there may from time to time be constituted ad hoc Board Committees for specific projects or tasks. In these cases, the scope and responsibilities of the Committee are documented. The Board provides adequate resources to enable each Committee to undertake its duties.

Reserved matters and delegation of authority

The Board maintains and periodically reviews a list of matters that are reserved to, and can only be approved by, the Board. These include: the appointment, termination and remuneration of any Director; approval of the annual budget; any item of fixed capital expenditure or any proposal for the acquisition or disposal of an investment or business which exceeds $150 million; the raising of capital or loans by the Company (subject to certain exceptions); the giving of any guarantee in respect of any borrowing of the Company; and allotting shares of the Company. The matters that have not been expressly reserved to the Board are either delegated by the Board to its Committees or to the CEO.

The CEO is responsible to the Board for the management, development and performance of our business in relation to those matters in respect of which he has been delegated authority from the Board.

Although the CEO retains full responsibility for the authority delegated to him by the Board, he is responsible for establishing, and chairs, the SET, which is the vehicle through which he exercises certain of that authority in respect of our business.

The roles of the Board, the Board Committees, the Chairman and the CEO are documented, as are the Board’s delegated authorities and reserved powers.

Operation of the Board

The Board is responsible for setting our strategy and policies, oversight of risk and corporate governance, and also monitors progress towards meeting our objectives and annual plans. The Board discharges these responsibilities through a programme of meetings that includes regular reviews of financial performance and critical business

issues, and the formal annual strategy review day. The Board also aims to ensure that a good dialogue with our shareholders takes place and that their issues and concerns are understood and considered.

The Board held 14 meetings in 2012, which included sessions to cover its usual annual strategy review. Eight of those meetings were telephone meetings, some convened at short notice, at which Board changes and business development transactions were discussed and approved. All of the meetings held in person took place in London, UK. The Board is currently scheduled to meet six times in 2013, and will meet at such other times as may be required to conduct business.

As part of the business of each Board meeting, the CEO typically submits a progress report on each key business area, giving details of progress against the goals the Board has approved. To ensure that the Board has good visibility of the key operating decisions of the business, members of the SET routinely attend Board meetings on a rotational basis and Board members regularly meet other senior executives throughout the year. The Board also receives accounting and other management information about our resources, and presentations from internal and external speakers on legal, governance and regulatory developments. At the end of Board meetings, the Non-Executive Directors meet without the Executive Directors present to review and discuss any matters that have arisen during the meeting and/or such other matters as may appear to the Non-Executive Directors to be relevant in properly discharging their duty to act independently.

Board effectiveness

Composition of the Board, succession planning and diversity

The Nomination and Governance Committee and, where appropriate, the full Board regularly review the composition of the Board and the status of succession to both senior executive management and Board-level positions. Directors have regular contact with, and access to, succession candidates for senior executive management positions.

 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   111

Table of Contents

Corporate Governance | Corporate Governance Report

 

The Board aims to maintain a balance in terms of the range of experience and skills of individual Board members, which includes relevant international business, pharmaceutical industry and financial experience, as well as appropriate scientific and regulatory knowledge. The biographies of Board members set out on pages 106 and 107 give more information about current Directors in this respect. The Board views gender, nationality and cultural diversity among Board members as important considerations when reviewing the composition of the Board. The Board recognises, in particular, the importance of gender diversity. Currently, 30% of the Company’s Non-Executive Directors are women and they make up 25% of the full Board. Since the formation of AstraZeneca in 1999, the proportion of women Board members has been approximately 25%. Although it has not set any specific measurable objectives, the Board intends to continue with its current approach to diversity in all its aspects, while at the same time seeking Board members of the highest calibre and with the necessary experience and skills to meet the needs of the Company and its shareholders. Information about our approach to diversity in the organisation below Board-level can be found in the People section from page 43.

The following changes to the composition of the Board have occurred during the period covered by this Annual Report:

> Louis Schweitzer and David Brennan, formerly Chairman and CEO respectively, retired from the Board on 1 June.
> Leif Johansson was elected as a Non-Executive Director at the AGM on 26 April 2012 and appointed Chairman of the Board with effect from 1 June. He was appointed Chairman of the Nomination and Governance Committee and as a member of the Remuneration Committee with effect from 26 April 2012.
> Pascal Soriot was appointed CEO with effect from 1 October.
> Simon Lowth served as Interim CEO with effect from 1 June and remained in this role until Pascal Soriot’s appointment, following which he reverted to his position as CFO.
> Michele Hooper retired from the Board at the end of the AGM on 26 April 2012.
> John Varley was appointed as senior independent Non-Executive Director with effect from 26 April 2012.
> Rudy Markham was appointed as Chairman of the Audit Committee and as a member of the Nomination and Governance Committee with effect from 26 April 2012. He also remained in his role as a member of the Remuneration Committee.
> Geneviève Berger was elected as a Non-Executive Director and appointed as a member of the Science Committee with effect from 26 April 2012.
> Graham Chipchase was elected as a Non-Executive Director and appointed as a member of the Audit Committee with effect from 26 April 2012.

Independence of the

Non-Executive Directors

During 2012, the Board considered the independence of each Non-Executive Director for the purposes of the UK Corporate Governance Code and the corporate governance listing standards of the NYSE (Listing Standards). With the exception of Marcus Wallenberg, the Board considers that all of the Non-Executive Directors are independent. Leif Johansson was considered by the Board to be independent upon his appointment as Chairman. In accordance with the UK Corporate Governance Code, the test of independence is not appropriate in relation to the Chairman after his appointment.

Marcus Wallenberg was appointed as a Director of Astra in May 1989 and subsequently became a Director of the Company in 1999. He is a Non-Executive Director of Investor AB, which has a 4.13% interest in the issued share capital of the Company as at 31 January 2013. Wallenberg family foundations remain Investor AB’s largest shareholders in terms of votes controlled. For these reasons, the Board does not believe that Marcus Wallenberg can be determined independent under the UK Corporate Governance Code. However, the Board believes that he has brought, and continues to bring, considerable business experience and makes a valuable contribution to the work of the Board. In April 2010, he was appointed as a member of the Science Committee, reflecting his interest in innovation and R&D, knowledge of the

 

 

Board Committee membership

 

Name

   Audit      Remuneration     

Nomination

and
Governance

     Science      Independent 1  

Geneviève Berger

                                ü         ü   

Bruce Burlington

     ü                           ü         ü   

Graham Chipchase

     ü                                    ü   

Jean-Philippe Courtois

     ü                                    ü   

Leif Johansson

              ü         Chair                  ü 2   

Simon Lowth

                                         n/a   

Rudy Markham

     Chair         ü         ü                  ü   

Nancy Rothwell

              ü         ü         Chair         ü   

Pascal Soriot

                                         n/a   

Shriti Vadera

     ü                                    ü   

John Varley

              Chair         ü                  ü   

Marcus Wallenberg

                                ü         x   

 

1   As determined by the Board for UK Corporate Governance Code purposes.
2   Leif Johansson was considered by the Board to be independent upon his appointment as Chairman; in accordance with the UK Corporate Governance Code, the test of independence is not appropriate in relation to the Chairman after his appointment.

 

112   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

history of the Company and its scientific heritage and culture, and his broad experience of other industries and businesses in which innovation and R&D are important determinants of success.

Conflicts of interest

The Articles enable the Directors to authorise any situation in which a Director has an interest that conflicts or has the potential to conflict with the Company’s interests and which would otherwise be a breach of the Director’s duty, under section 175 of the Companies Act 2006. The Board has a formal system in place for Directors to declare such situations to be considered for authorisation by those Directors who have no interest in the matter being considered. In deciding whether to authorise a situation, the non-conflicted Directors must act in the way they consider, in good faith, would be most likely to promote the success of the Company, and they may impose limits or conditions when giving the authorisation, or subsequently, if they think this is appropriate. Situations considered by the Board and authorisations given are recorded in the Board minutes and in a register of conflicts maintained by the Company Secretary and are reviewed annually by the Board. The Board considers that this system continues to operate effectively.

Appointments to the Board

The Nomination and Governance Committee section on page 117 gives information about the appointment process for new Directors.

 

Newly appointed Directors are provided with comprehensive documentation containing information about the Group and their role as Non-Executive Directors. They also typically attend tailored induction programmes that take account of their individual skills and experience.

Time commitment

Our expectation is that Non-Executive Directors should be prepared to commit about 15 days per annum, as a minimum, to the Group’s business. In practice, Board members’ time commitment usually exceeds this minimum expectation when all the work that they undertake for the Group is considered, particularly in the case of the Chairman of the Board and the Chairmen of the Board Committees. As well as their work in relation to formal Board and Board Committee meetings, the Non-Executive Directors also commit time throughout the year to meetings and telephone calls with various levels of executive management, visits to AstraZeneca’s sites throughout the world and, for new Non-Executive Directors, induction sessions and site visits.

On occasions when a Director is unavoidably absent from a Board or Board Committee meeting, for example where a meeting clashes with his or her existing commitments, he or she still receives and reviews the papers for the meeting and typically provides verbal or written input ahead of the meeting, usually through the Chairman of the Board or the Chairman of the Board Committee, so that his or her

views are made known and considered at the meeting. In addition, given the nature of the business to be conducted, some Board meetings are convened at short notice, which can make it difficult for some Directors to attend due to prior commitments.

Information and support

The Compay Secretary is responsible to the Chairman for ensuring that all Board and Board Committee meetings are properly conducted, that the Directors receive appropriate information prior to meetings to enable them to make an effective contribution, and that governance requirements are considered and implemented.

The Company maintained directors’ and officers’ liability insurance cover throughout 2012. The Directors are also able to obtain independent legal advice at the expense of the Company, as necessary, in their capacity as Directors.

The Company has entered into a deed of indemnity in favour of each Board member since 2006. These deeds of indemnity are still in force and provide that the Company shall indemnify the Directors to the fullest extent permitted by law and the Articles, in respect of all losses arising out of, or in connection with, the execution of their powers, duties and responsibilities, as Directors of the Company or any of its subsidiaries. This is in line with current market practice and helps us attract and retain high-quality, skilled Directors.

 

 

Board and Board Committee meeting attendance in 2012

 

Name

   Board
(scheduled) 		   

Board

(unscheduled) 1

    Audit     Remuneration     Nomination
and
Governance 		    Science  

Geneviève Berger 2

     4 (4     2 (5                          7 (7

David Brennan 3

     2 (2     3 (3     2 (2                     

Bruce Burlington

     6 (6     8 (8     7 (7                   7 (7

Graham Chipchase 4

     4 (4     3 (5     4 (4                     

Jean-Philippe Courtois

     5 (6     5 (8     5 (7                     

Michele Hooper 5

     2 (2     3 (3     3 (3            2 (2       

Leif Johansson 6

     4 (4     5 (5            9 (9     4 (4       

Simon Lowth

     6 (6     6 (8 ) 7       7 (7                     

Rudy Markham

     6 (6     6 (8     7 (7     9 (12     4 (4       

Nancy Rothwell

     6 (6     8 (8            7 (12     6 (6     7 (7

Louis Schweitzer 8

     2 (2     3 (3            5 (5     2 (2       

Pascal Soriot 9

     2 (2            2 (2                     

Shriti Vadera

     6 (6     8 (8     7 (7                     

John Varley

     6 (6     8 (8            12 (12     6 (6       

Marcus Wallenberg

     6 (6     6 (8                          5 (7

---------------------------

PagePro

---------------------------

Cannot open the Clipboard

---------------------------

OK

---------------------------

Note: number in brackets denotes number of meetings during the year that Board members were entitled to attend.

 

1   The Board held eight unscheduled meetings by telephone during the year, some convened at short notice, at which Board changes and business development transactions were discussed and approved.
2   Geneviève Berger was elected to the Board on 26 April 2012.
3   David Brennan retired from the Board on 1 June.
4   Graham Chipchase was elected to the Board on 26 April 2012.
5   Michele Hooper retired from the Board on 26 April 2012.
6   Leif Johansson was elected to the Board on 26 April 2012.
7   At the Chairman’s request, Simon Lowth absented himself from two of the eight unscheduled meetings at which Board changes were discussed.
8   Louis Schweitzer retired from the Board on 1 June.
9   Pascal Soriot was appointed to the Board on 1 October.

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   113

Table of Contents

Corporate Governance | Corporate Governance Report

 

Performance evaluation

During the year, the Board conducted the annual evaluation of its own performance and that of its Committees and individual Directors.

The 2012 evaluation was conducted internally and involved a series of web-based questionnaires. A draft report based on responses from the questionnaires was prepared and reviewed by the Chairman and the Company Secretary. The final report was circulated to the full Board and discussed at the Board meeting held in January 2013. The evaluation covered a range of topics, including: the composition of the Board; the effectiveness of its strategic oversight; Board members’ involvement in the affairs of the Company outside Board meetings; decision making and time management; the nature and quality of the information and general support provided to the Board; its approach to risk management and oversight of internal controls; and succession planning and how effectively the Board prioritises matters. Separate questionnaires covered the operation and effectiveness of the Board’s Committees, and relevant Board members (those serving in the period January to April 2012) also responded to a questionnaire dealing specifically with shareholder engagement.

The composition and dynamics of the Board were generally thought to be balanced and appropriate. Information flows to the Board from the management team, and from Board Committees, were usually considered to be good and Board meetings were generally felt to be well-structured. The expanded role of the Science Committee reviewing the R&D aspects of a number of business development and acquisition proposals on behalf of the Board was seen as a positive development. However, a number of areas were identified for improvement. The importance of shareholder engagement and succession planning were highlighted by the performance evaluation. The Board’s visibility of major shareholders’ views will be improved. The engagement of the new Chairman and, more recently, the new CEO with the Company’s largest investors is contributing to this but, in addition, more structured and regular discussion on this topic and greater analyst/broker insight at Board-level will be implemented. In recent years, the Board’s overview of senior executive succession planning work has increased but needs to be further improved by the Board receiving more detailed information about the work of the Nomination and Governance Committee.

As part of the assessment process, each Director had an individual discussion with the Chairman to discuss their contribution to the work of the Board and personal development needs. Each Director continues to perform effectively and to demonstrate commitment to their role.

The Board’s annual performance evaluation was last externally facilitated in 2011. The Board intends to continue to comply with the UK Corporate Governance Code guidance that the evaluation should be externally facilitated at least every three years.

Re-election of Directors

In accordance with Article 66 of the Articles, all Directors retire at each AGM and may offer themselves for re-election by shareholders. Accordingly, all of the Directors will retire at the AGM in April 2013. The Notice of AGM will give details of those Directors seeking re-election.

Accountability

Risk management and internal control

The Non-Executive Directors have various responsibilities concerning the integrity of financial information, internal controls and risk management.

The Board has overall responsibility for our system of internal controls and risk management policies and is also responsible for reviewing their effectiveness. During 2012, the Directors have continued to review the effectiveness of our system of controls, risk management and our high-level internal control processes. These reviews have included an assessment of internal controls, and in particular, financial, operational and compliance controls and risk management and their effectiveness, supported by management assurance of the maintenance of controls reports from GIA, as well as the external auditor on matters identified in the course of its statutory audit work. The system is designed to manage rather than eliminate the risk of failure to achieve business objectives and can only provide reasonable (not necessarily absolute) assurance of effective operation and compliance with laws and regulations.

Underpinning these reviews is an annual ‘letter of assurance’ process by which responsible managers confirm the adequacy of their systems of internal financial and non-financial controls, their compliance with Group policies and relevant laws and regulations (including the industry’s regulatory requirements), and that they have reported any control weaknesses through our ‘continuous assurance’ process.

The internal control framework has been in operation throughout 2012 and continues to operate up to the date of the approval of this Annual Report. The Directors believe that the Group maintains an effective, embedded system of internal controls and complies with the Turnbull Report guidance and, in the view of the Directors, no significant deficiencies have been identified in the system.

Further information about the ways in which we manage our business risks is set out in the Risk section from page 74, which also contains a list of the principal risks and uncertainties that we face.

Remuneration

Information about our approach to remuneration and the role and work of the Remuneration Committee, including our policy on executive remuneration, is set out in the Directors’ Remuneration Report from page 122.

Relations with shareholders

In our financial and business reporting to shareholders and other interested parties by means of quarterly, half-yearly and annual reports, we aim to present a balanced and understandable assessment of our strategy, financial position and prospects.

We make information about the Group available to shareholders through a range of media, including a fully integrated html corporate website, astrazeneca.com, containing a wide range of data of interest to institutional and private investors. We consider our website to be an important means of communication with our shareholders.

The Company has been authorised by shareholders to place shareholder communications (such as the Notice of AGM and this Annual Report) on the corporate website in lieu of sending paper copies to shareholders (unless specifically requested by shareholders). While recognising and respecting the fact that some of our shareholders may have different preferences about how they receive information from us, we will continue to promote the benefits of electronic communication given the advantages that this has over traditional paper-based communications, both in terms of the configurability and accessibility of the information provided and the consequent cost savings and reduction in environmental impact associated with reduced printing and distribution costs.

We have frequent discussions with institutional shareholders on a range of issues. These include individual meetings with some of our largest institutional shareholders to seek their views. Board

 

 

114   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

members are kept informed of any issues and receive regular reports and presentations from executive management and our brokers in order to assist them to develop an understanding of major shareholders’ views about the Group. From time to time, we conduct an audit of institutional shareholders to ensure that we are communicating clearly with them and that a high-quality dialogue is being maintained. The results of this audit are reported to, and discussed by, the full Board.

We also respond to individual ad hoc requests for discussions from institutional shareholders and analysts. Our Investor Relations team acts as the main point of contact for investors throughout the year. As discussed above, the senior independent Non-Executive Director, John Varley, is also available to shareholders if they have concerns that contact through the normal channels of Chairman, CEO and/or CFO has failed to resolve, or in relation to which such contact is inappropriate. All shareholders, including private investors, have an opportunity at the AGM to put questions to members of the Board about our operation and performance. Formal notification of the AGM is sent to shareholders at least one month in advance. The Chairmen of the Board Committees ordinarily attend the AGM to answer questions raised by shareholders. In line with the UK Corporate Governance Code, details of proxy voting by shareholders, including votes withheld, are given at the AGM and are posted on our website following the AGM.

Audit Committee

The members of the Audit Committee are Rudy Markham (Chairman of the Audit Committee), Bruce Burlington, Graham Chipchase, Jean-Philippe Courtois and Shriti Vadera (and, until her retirement at the 2012 AGM, Michele Hooper). They are (or in the case of Michele Hooper, were) all Non-Executive Directors. The Board considers each member to be independent under the UK Corporate Governance Code and under the general guidance and specific criteria of the Listing Standards concerning the composition of audit committees applicable to non-US companies listed on the NYSE. In April 2012, we submitted the required annual written affirmation to the NYSE confirming our full compliance with those standards. For the purposes of the UK Corporate Governance Code, the Board remains satisfied that at least one member of the Audit Committee has recent and relevant financial experience. At its meeting in December, the Board determined that Rudy Markham and Graham Chipchase are audit committee financial experts for the purposes of the Sarbanes-Oxley Act.

The Deputy Company Secretary acts as secretary to the Audit Committee.

The core terms of reference of the Audit Committee include, reviewing and reporting to the Board on:

 

> matters relating to the audit plans of the external auditor and GIA as well as oversight of the work of the Global Compliance function
> our overall framework for internal control over financial reporting and for other internal controls and processes
> our overall framework for risk management, particularly financial risks
> our accounting policies and practices
> our annual and quarterly financial reporting, including the critical estimates and judgements contained in our reporting
> our internal control over financial reporting
> our Code of Conduct and whistleblower procedures
> compliance with the Corporate Integrity Agreement (CIA).

The Audit Committee is responsible for notifying the Board of any significant concerns of the external auditor or the Vice-President, GIA arising from their audit work, any matters that may materially affect or impair the independence of the external auditor, any significant deficiencies or material weaknesses in the design or operation of our internal control over financial reporting or other internal controls, any serious issues of non-compliance and how the Audit Committee has discharged its responsibilities. It oversees the establishment, implementation and maintenance of our Code of Conduct and other related policies. It monitors the Company’s response to letters requesting information and investigations initiated by regulatory and governmental authorities such as the SEC and the US Department of Justice and the UK Financial Reporting Council pertaining to matters within the remit of the Audit Committee’s work. It has established procedures for the receipt and handling of complaints concerning accounting or audit matters. It recommends to the Board the appointment of the external auditor, subject to the approval of the Company’s shareholders at a general meeting. Shareholders in a general meeting authorise the Directors to fix the remuneration of the external auditor. The Audit Committee reviews and approves the appointment and dismissal of the Vice-President, GIA.

The Audit Committee maintains policies and procedures for the pre-approval of all audit services and permitted non-audit services undertaken by the external auditor, the principal purpose of which is to ensure that the independence of the external auditor is not impaired. The policies and procedures

cover three categories of work; audit services, audit-related services and tax services. The policies define the type of work that falls within each of these categories and the non-audit services that the external auditor is prohibited from performing under the rules of the SEC and other relevant UK and US professional and regulatory requirements. The pre-approval procedures permit certain audit, audit-related and tax services to be performed by the external auditor during the year, subject to fee limits agreed with the Audit Committee in advance. The CFO (supported by the Vice-President, Group Finance) monitors the status of all services being provided by the external auditor. The procedures also deal with placing non-audit work out for tender, where appropriate. Authority to approve work in excess of the pre-agreed fee limits is delegated to the Chairman of the Audit Committee together with one other Audit Committee member in the first instance. A standing agenda item at Audit Committee meetings covers the operation of the pre-approval procedures and regular reports are provided to the full Audit Committee. Fees paid to the auditor for audit, audit-related and other services are analysed in Note 27 to the Financial Statements on page 190.

The Audit Committee held seven scheduled meetings in 2012. The individual attendance record of members of the Audit Committee is set out in the Board and Board Committee meeting attendance in 2012 table on page 113. Following each Audit Committee meeting, the Chairman of the Audit Committee reported to the Board on the principal matters covered at the meeting and minutes of the meetings were circulated to all Board members. In addition, the Chairman of the Audit Committee held regular scheduled calls between Audit Committee meetings with each of the Vice-President, GIA, the Chief Compliance Officer, the CFO and the lead partner of the external auditor.

During 2012 and January 2013, the Audit Committee considered and discussed the following matters:

 

> The key elements of the financial statements, and estimates and judgements contained in our financial disclosures, which were reviewed and various accounting matters considered. These included the areas described in the Financial Review under the heading ‘Critical Accounting Policies and Estimates’ (with a focus on accounting issues relevant to litigation and taxation matters and goodwill impairment) from page 99 and discussion was supported by papers prepared by management and the external auditor.
 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   115

Table of Contents

Corporate Governance | Corporate Governance Report

 

> The reports received from the external auditor concerning its audit of the Financial Statements of the Group and from management, GIA, Global Compliance and the external auditor on the effectiveness of our system of internal controls and, in particular, our internal control over financial reporting. This included review and discussion of the results of the ‘continuous assurance’ and annual ‘letter of assurance’ processes. The Audit Committee also reviewed quarterly activity reports of audit work carried out by GIA and the status of follow-up actions with management as well as reports from the Global Compliance function.
> The systems and processes that management has developed pertaining to risk identification, classification and mitigation.
> Compliance with the applicable provisions of the Sarbanes-Oxley Act. In particular, the Audit Committee regularly reviewed the status of compliance with the programme of internal controls over financial reporting implemented pursuant to section 404 of the Sarbanes-Oxley Act. The Audit Committee remained focused on IS/IT controls in the context of the changes to the Group’s IS/IT environment, described below. Further information about this is set out in the Sarbanes-Oxley Act Section 404 section on page 103.
> Data about reports made by employees via the AZethics helpline, online facilities and other routes regarding potential breaches of the Code of Conduct together with the results of inquiries into these matters.
> Quarterly reports received from the US Compliance Officer responsible for monitoring the US business’ compliance with the CIA (for more information about the obligations imposed on the Board by the CIA, see below).
> Regular progress updates from IS/IT on the status of the transition from the existing outsource provider to the new providers.
> Reports from the Group Treasury function and, in particular, reports concerning the Group’s liquidity and cash position and the appropriateness of its cash management policies in the context of the current economic situation.
> Going concern assessment and adoption of the going concern basis in preparing this Annual Report and the Financial Statements.
> Other reports concerning the GIA, Global Compliance and Finance functions, including the internal audit plan and progress and plans of the Global Compliance function.
> Reports from the General Counsel on the status of certain litigation matters and governmental investigations.
> The amount of audit and non-audit fees of the external auditor throughout 2012. The Audit Committee was satisfied throughout the year that the objectivity and independence of the external auditor were not in any way impaired by the nature of the non-audit work undertaken by the external auditor during the year, the level of non-audit fees charged for such work or any other facts or circumstances. Further information about the audit and non-audit fees for 2012 is disclosed in Note 27 to the Financial Statements on page 190.
> The rotation of the lead partner of the external auditor. In advance of the expiry of the permitted tenure of the lead audit partner, Jimmy Daboo, at the conclusion of the 2012 audit, the Audit Committee oversaw a process whereby a number of potential successors were considered and Tony Cates was endorsed as his successor. The Audit Committee also considered the external auditor’s proposed arrangements to ensure an effective handover of responsibilities.
> A review and assessment of the Audit Committee’s performance which concluded that such performance was satisfactory.

In line with its normal practice, the Audit Committee also held a number of private meetings, without management present, with the Vice-President, GIA, the Chief Compliance Officer, the General Counsel and the Company’s external auditor. These meetings were held between Audit Committee members and those individuals, separately from the main sessions of the Audit Committee, which were also attended by the CEO, the CFO, the General Counsel and the Vice-President, Group Finance.

In addition to its usual business as described above, during 2012, members of the Audit Committee met individual managers or groups of managers on a number of occasions in order to gain a deeper insight into areas relevant to the Audit Committee’s work and to provide an opportunity to discuss specific areas of interest. These included:

 

> Considering the potential impact of the eurozone crisis on AstraZeneca’s operations, in particular in Greece, Italy and Spain.
> Hearing from the regional finance directors of the Americas, Asia Pacific and EMEA regions on the financial objectives, the local challenges and organisational structures in their respective regions and learning how the Group Finance organisation supports AstraZeneca’s network of local marketing companies.
> Learning about AstraZeneca’s business processing outsourcing centre of excellence and the work it does to support the various outsourcing initiatives currently ongoing in the business as we seek to reduce our cost base.
> Receiving regular updates from the IS/IT team in connection with the transition from the Company’s previous IT infrastructure outsourcing provider to its new providers.
> Considering a presentation on the lessons learnt from the implementation of an enterprise resource planning IT system at our plant in Sweden which led to disruptions in our supply chain during the year.
> Meeting with the Global Compliance Leadership Team which comprises representatives from the second line assurance functions in R&D, Operations, and Sales and Marketing.
> Considering the risks associated with the Group’s pension and other benefit obligations and the steps taken to manage those risks.
> Monitoring the operation of controls and reporting arrangements, cognisant of the additional pressures on management during the tenure of the Interim CFO.

In addition to the quarterly reporting stipulated by the CIA as described above, a number of other obligations required by the CIA were discharged by members of the Board and the Audit Committee during 2012. For example, all members of the Board completed the annual CIA-required training, addressing the Code of Conduct and the elements of the CIA and the US compliance programme. Furthermore, the Board adopted a resolution (signed by each member) in respect of the second 12 month reporting period under the CIA. The resolution summarised the Board’s oversight of the US compliance programme and stated that, to the best of the Board’s knowledge, AstraZeneca Pharmaceuticals, LP and AstraZeneca LP (AstraZeneca’s principal US trading entities) have implemented an effective US compliance programme to meet Federal healthcare programme, FDA and CIA requirements.

In accordance with its normal practice, the Audit Committee considered the performance of our external auditor KPMG Audit Plc (KPMG). It also considered KPMG’s compliance with the independence criteria under the relevant statutory, regulatory and ethical standards applicable to auditors and assessed its objectivity, taking into account the level of challenge provided around the critical estimates and judgements involved in our financial

 

 

116   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

reporting and the quality of our internal control over financial reporting. Having considered all these factors, the Audit Committee unanimously recommended to the Board that a resolution for the re-appointment of KPMG as the Company’s external auditor for the year ending 31 December 2013, be proposed to shareholders at the AGM in April 2013.

Consistent with current market practice, KPMG’s services to the Company are provided pursuant to terms of engagement which are reviewed by the Audit Committee. Neither these terms of engagement nor any other agreement include any contractual obligations under which the Directors would be prevented from appointing a different audit firm were they to consider this to be in the best interests of the Group. The Audit Committee, through management, continues to maintain contact and dialogue with other major audit firms who are familiar with the Group’s business for succession purposes as required. This is reported to the Audit Committee in order to ensure a smooth transition from the current auditor, should this be necessary. In December 2012, the Audit Committee reviewed the changes to the UK Corporate Governance Code with regard to putting the external audit contract out to tender at least every 10 years. It noted that KPMG was first appointed as sole external auditor to AstraZeneca in 2001 following a competitive tender. The Audit Committee concluded that, as the lead audit partner at KPMG is rotating in 2013, then in accordance with the transitional guidance issued by the FRC, the audit would be put out to tender by 2018.

At the January 2013 meeting, the CFO presented to the Audit Committee the conclusions of the CEO and the CFO following the evaluation of the effectiveness of our disclosure controls and procedures required by Item 15(a) of Form 20-F at 31 December 2012. Based on their evaluation, the CEO and the CFO concluded that, as at that date, we maintain an effective system of disclosure controls and procedures.

There was no change in our internal control over financial reporting that occurred during the period covered by this Annual Report that has materially affected, or is reasonably likely to materially affect, our internal control over financial reporting.

The Audit Committee is currently scheduled to meet six times in 2013 and will meet at such other times as may be required.

The Audit Committee’s terms of reference are available on our website, astrazeneca.com.

Code of Conduct

Our Code of Conduct (the Code), which is available on our website, astrazeneca.com, applies worldwide to all full-time and part-time AstraZeneca Directors, officers, employees and temporary staff. Further information relating to the Code can be found in the Compliance section on page 47.

A Group Finance Code of Conduct complements the Code. It applies to the CEO, the CFO, the Group’s principal accounting officers (including key Finance staff in major overseas subsidiaries) and all Finance function employees. This reinforces the importance of the integrity of the Group’s Financial Statements, the reliability of the accounting records on which they are based and the robustness of the relevant controls and processes.

Remuneration Committee

The principal role of the Remuneration Committee is to consider and set, on behalf of the Board, the remuneration (including pension rights and compensation payments) of Executive Directors and other senior executives. It also considers and sets the remuneration of the Chairman, in conjunction with the senior independent Non-Executive Director and in the absence of the Chairman. No Director is involved in deciding his or her own remuneration. More information is set out in the Directors’ Remuneration Report from page 122.

Nomination and Governance Committee

The Nomination and Governance Committee’s role is to recommend to the Board any new Board appointments and to consider, more broadly, succession plans at Board level. It continually reviews the composition of the Board using a matrix that records the skills and experience of current Board members and comparing this with the desired skills and experience it believes are appropriate to the Company’s overall business and strategic needs both now and in the future. Any decisions relating to the appointment of Directors are made by the entire Board based on the merits of the candidates and the relevance of their background and experience, measured against objective criteria, with care taken to ensure that appointees have enough time to devote to our business.

The Nomination and Governance Committee also advises the Board periodically on significant developments in corporate governance and the Company’s compliance with the UK Corporate Governance Code.

During 2012, the members of the Nomination and Governance Committee were Louis Schweitzer (Chairman of the Committee until 26 April 2012 and member until his retirement on 1 June), Leif Johansson (member and Chairman of the Committee from 26 April 2012), John Varley, Rudy Markham (from 26 April 2012) and Michele Hooper (until her retirement on 26 April 2012). Each of them is (and in the case of each of Louis Schweitzer and Michele Hooper, was) a Non-Executive Director and considered independent by the Board. Each of Louis Schweitzer and Leif Johansson was considered by the Board to be independent upon his appointment as Chairman; in accordance with the UK Corporate Governance Code, the test of independence is not appropriate in relation to the Chairman after his appointment. The Company Secretary acts as secretary to the Nomination and Governance Committee.

The Nomination and Governance Committee considers both planned and unplanned (unanticipated) succession scenarios. It was anticipated that Louis Schweitzer would retire from the Board in 2012 and, consequently, a thorough search for a new Chairman was started at the beginning of 2011. Although Mr Schweitzer retired a few months earlier than originally envisaged, succession plans were well-advanced and our new Chairman, Leif Johansson, joined the Board in April 2012 and became Chairman in June. In the fourth quarter of 2010, in anticipation of the likelihood of David Brennan retiring within the next two years, the Nomination and Governance Committee engaged the search firm Spencer Stuart to carry out a desktop exercise to identify potential external candidates for this position. This work, combined with a good overview of potential internal candidates as a result of the Board’s normal work with and exposure to senior executives, put the Nomination and Governance Committee in a position to react quickly to Mr Brennan’s decision in 2012 that he wished to retire. A strong slate of internal and external candidates was identified, who were thoroughly assessed over the summer of 2012, leading to the appointment of Pascal Soriot as CEO with effect from 1 October.

The Nomination and Governance Committee met six times in 2012. Much of its work during the year naturally focused on the recruitment of Mr Soriot. The Committee engaged Spencer Stuart to assist it with the assignment.

 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   117

Table of Contents

Corporate Governance | Corporate Governance Report

 

The ad hoc Board Committee formed for the purpose of appointing a new Chairman of the Board also completed its work during 2012 and the appointment of Leif Johansson was announced by the Company on 1 March 2012. He was elected as a Director at the AGM on 26 April 2012 and became Chairman with effect from 1 June. This work was led by Michele Hooper in her capacity as senior independent Non-Executive Director and the search firm, MWM Consulting, was engaged to assist with the assignment.

The Nomination and Governance Committee also recommended to the Board the appointments of Geneviève Berger and Graham Chipchase during the year as part of routine Board succession planning. Professor Berger and Mr Chipchase were elected to the Board on 26 April 2012 and became members of the Science Committee and the Audit Committee, respectively, from the same date. Professor Berger strengthens the Board’s scientific and R&D knowledge and experience. Mr Chipchase adds to the Board’s international business leadership. The Nomination and Governance Committee engaged MWM Consulting and The Zygos Partnership to assist it with the assignments to appoint Professor Berger and Mr Chipchase respectively.

Neither MWM Consulting nor The Zygos Partnership has any other connection to the Company. Spencer Stuart undertakes executive search assignments for the Company periodically.

The individual attendance record of the Nomination and Governance Committee’s members is set out on page 113. During the year, the Nomination and Governance Committee also reviewed the composition of Board Committees in the light of the Board changes described above and recommended to the Board appropriate changes, which are described in this Annual Report.

The Nomination and Governance Committee’s terms of reference are available on our website, astrazeneca.com.

Science Committee

The Science Committee’s core role continues to be to provide assurance to the Board regarding the quality, competitiveness and integrity of the Group’s R&D activities by way of: meetings and dialogue with our R&D leaders and other scientist employees; visits to our R&D sites throughout the world; and review and assessment of the:

> approaches we adopt in respect of our chosen Therapy Areas
> scientific technology and R&D capabilities deployed
> decision making processes for R&D projects and programmes
> quality of our scientists, career opportunities and talent development
> benchmarking against industry and scientific best practice, where appropriate.

The Science Committee also reviews, from time to time, important bioethical issues that we face, and assists in the formulation of, and agrees on behalf of the Board, appropriate policies in relation to such issues. It may also consider, from time to time, future trends in medical science and technology. The Science Committee does not review individual R&D projects. However, during 2012 the Science Committee did review on behalf of the Board the R&D aspects of a number of specific business development or acquisition proposals and advised the Board on its conclusions.

During 2012, the members of the Science Committee, all of whom have a knowledge of, or an interest in, life sciences, were Nancy Rothwell (Chairman of the Science Committee), Bruce Burlington, Marcus Wallenberg and Geneviève Berger (from 26 April 2012). The President, Global R&D; the Executive Vice-President, Innovative Medicines; the Executive Vice-President, MedImmune; and the Executive Vice-President, Global Medicines Development attended meetings of the Science Committee in 2012. The Vice-President, Strategy, Portfolio & Performance, R&D also attended all meetings and acted as secretary to the Science Committee.

The Science Committee met twice in person in 2012, in Cambridge and London, UK and held five meetings by telephone to review specific business development or acquisition proposals.

The Science Committee’s terms of reference are available on our website, astrazeneca.com.

US corporate governance requirements

Our ADSs are traded on the NYSE and, accordingly, we are subject to the reporting and other requirements of the SEC applicable to foreign private issuers. Section 404 of the Sarbanes-Oxley Act requires companies to include in their annual report on Form 20-F filed with the SEC a report by management stating its responsibility for establishing internal control

over financial reporting and to assess annually the effectiveness of such internal control. We have complied with those provisions of the Sarbanes-Oxley Act applicable to foreign private issuers. The Board continues to believe that the Group has a sound corporate governance framework, good processes for the accurate and timely reporting of its financial position and results of operations, and an effective and robust system of internal controls. We have established a Disclosure Committee, further details of which can be found in the Disclosure Committee section on the page opposite.

The Directors’ assessment of the effectiveness of the internal control over financial reporting is set out in the Directors’ Responsibilities for, and Report on, Internal Control over Financial Reporting section in the Financial Statements on page 140.

We are required to disclose any significant ways in which our corporate governance practices differ from those followed by US companies under the Listing Standards. In addition, we must comply fully with the provisions of the Listing Standards relating to the composition, responsibilities and operation of audit committees, applicable to foreign private issuers. These provisions incorporate the rules concerning audit committees implemented by the SEC under the Sarbanes-Oxley Act. We have reviewed the corporate governance practices required to be followed by US companies under the Listing Standards and our corporate governance practices are generally consistent with those standards.

Business organisation

Senior Executive Team

The CEO is responsible for establishing, and chairs, the SET. The SET normally meets once a month to consider and decide major business issues, or as otherwise required by business needs. Typically, it also reviews, in advance of submission to the Board, those matters that are to be submitted to the Board for review and decision.

In addition to the CEO, the CFO, the General Counsel, and the Chief Compliance Officer, the SET comprises nine Executive Vice-Presidents representing: Innovative Medicines (small molecules); MedImmune (biologics); Global Medicines Development; North America; Europe; International; Global Portfolio & Product Strategy; Operations & Information Services; and Human Resources & Corporate Affairs. The Company Secretary acts as secretary to the SET.

 

 

118   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

Portfolio Investment Board (PIB)

The CEO is responsible for establishing, and chairs, the PIB, a senior-level, cross-functional governance body, which seeks to maximise the value of our internal and external R&D investments through robust, transparent and well-informed decisions that drive business performance and accountability.

Specifically, the PIB has responsibility for:

 

> Reviewing the R&D portfolio, by conducting an objective and transparent review of R&D performance, product launch profile and alignment with corporate strategy. The review is also an important step in reconfirming the R&D three year budget.
> Approving the business plans of the Innovative Medicines groups and the Global Medicines Development demand forecast, by confirming the allocation of resources across early-stage and late-stage elements of R&D as well as assessing licensing and acquisition opportunities.
> Approving late-stage (internal and external) investment decisions.
> Monitoring environmental events that could have a major transformational or disruptive impact on our business.

In addition to the CEO, the PIB’s members in 2012 were: the CFO; the President, Global R&D; the Executive Vice-President, Global Commercial Operations; the Executive Vice-President, Innovative Medicines; the Executive Vice-President, MedImmune; the Executive Vice-President, Global Medicines Development; and the Vice-President, Strategic Partnering & Business Development. The PIB has a permanent secretary and typically meets at around the time of the monthly SET meetings, or as otherwise required by business needs.

Disclosure Committee

Our disclosure policy provides a framework for the handling and disclosure of inside information and other information of interest to shareholders and the investment community. It also defines the role of the Disclosure Committee. The members of the Disclosure Committee in 2012 were: the CEO; the CFO, who chaired the Disclosure Committee; the President, Global R&D; the General Counsel; the Vice-President, Corporate Affairs; the Vice-President, Investor Relations; and

the Vice-President, Group Finance. The Deputy Company Secretary acted as secretary to this Committee. The Disclosure Committee meets regularly to assist and inform the decisions of the CEO concerning inside information and its disclosure. Periodically, it reviews our disclosure controls and procedures and its own operation as part of work carried out to enable management and the Board to assure themselves that appropriate processes are operating for our planned disclosures, such as our quarterly results announcements and scheduled investor relations events.

Disclosure of information to auditors

The Directors who held office at the date of approval of this Annual Report confirm that, so far as they are each aware, there is no relevant audit information of which the Company’s auditors are unaware; and each Director has taken all the steps that he or she ought to have taken as a Director to make himself or herself aware of any relevant audit information and to establish that the Company’s auditors are aware of that information.

Compliance and Group Internal Audit

The role of the Global Compliance function is to manage and maintain the compliance programme infrastructure and to help embed a culture of ethics and integrity in the Group. Global Compliance works closely with GIA, with whom it provides assurance reporting to the Audit Committee. During 2013, the Global Compliance function will continue to focus on ensuring the delivery of an aligned approach to compliance that addresses key risk areas across the business. Further information can be found in the Compliance section from page 47.

Global Compliance provides direct assurance to the Audit Committee on matters concerning compliance issues, including the results of monitoring and auditing conducted by Global Compliance and an analysis of compliance breaches. Complementing this, GIA carries out a range of audits that include compliance-related audits and reviews of the assurance activities of other Group assurance functions. The results from these activities are reported to the Audit Committee.

GIA is an independent appraisal function that derives its authority from the Board through the Audit Committee. Its primary role is to provide reasonable and objective assurance to the Directors regarding the

adequacy and effectiveness of the Group’s risk management and control framework and the internal controls over key business risks, including financial controls and compliance with laws, regulations and policies.

GIA seeks to discharge the responsibilities set down in its charter by reviewing:

 

> the processes for ensuring that key business risks are effectively managed
> the financial and operational controls that help to ensure the Group’s assets are properly safeguarded from losses, including fraud
> the controls that help to ensure the reliability and integrity of management information systems
> the processes for ensuring compliance with policies and procedures, external legislation and regulation.

In addition to fulfilling its primary remit of assurance to the Audit Committee, GIA acts as a source of constructive advice and best practice, assisting senior management to improve governance, control, compliance and risk management.

Other matters

Corporate governance statement under the UK Disclosure and Transparency Rules (DTR)

The disclosures that fulfil the requirements of a corporate governance statement under the DTR can be found in this section and in other parts of this Annual Report as listed below, each of which is incorporated into this section by reference:

 

> Significant holders of the Company’s shares (contained in the Shareholder Information section from page 203).
> Articles (contained in the Corporate Information section on page 208).
> Amendments to the Articles (contained in the Corporate Information section on page 208).

Subsidiaries and principal activities

The Company is the holding company for a group of subsidiaries whose principal activities are described in this Annual Report. Principal subsidiaries and their locations are given in the Principal Subsidiaries section in the Financial Statements on page 191.

 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   119

Table of Contents

Corporate Governance | Corporate Governance Report

 

Branches and countries in which the Group conducts business

In accordance with the Companies Act 2006, we disclose below our subsidiary companies that have representative or scientific branches/offices outside the UK:

 

> AstraZeneca UK Limited: Albania, Algeria (scientific office), Angola, Azerbaijan, Belarus, Bulgaria, Chile, Costa Rica, Croatia, Cuba, Georgia, Ghana (scientific office), Ireland, Jordan, Kazakhstan, Macedonia, Nigeria, Romania, Russia, Saudi Arabia (scientific office), Serbia and Montenegro, Slovenia, Syria and Ukraine.
> AstraZeneca AB: Egypt (scientific office), Slovakia and the United Arab Emirates.
> AstraZeneca Singapore Pte Limited: Vietnam.

Distributions to shareholders and dividends for 2012

Our distribution policy comprises both a regular cash dividend and a share repurchase component, further details of which are set out in the Financial Review on page 94 and Notes 20 and 21 to the Financial Statements on page 173.

The Company’s dividends for 2012 of $2.80 (178.6 pence, SEK 18.34) per Ordinary Share amount to, in aggregate, a total dividend payment to shareholders of $3,665 million. Two of our employee share trusts, AstraZeneca Share Trust Limited and AstraZeneca Quest Limited, waived their right to a dividend on the Ordinary Shares that they hold and instead received a nominal dividend.

A shareholders’ resolution was passed at the 2012 AGM authorising the Company to purchase its own shares. Pursuant to this resolution, the Company repurchased (and subsequently cancelled) 57.8 million Ordinary Shares with a nominal value of $0.25 each, at an aggregate cost of $2,635 million, representing 4.6% of the closing total issued share capital of the Company. The Company suspended its share repurchase programme on 1 October as a prudent step to maintain flexibility while the Board and the newly-appointed CEO completed the Company’s annual strategy update.

During our share repurchase programmes that operated between 1999 and September 2012, a total of 615.2 million Ordinary Shares were repurchased, and subsequently cancelled, at an average price of 2777 pence per share for a consideration, including expenses, of $29,352 million.

Going concern accounting basis

Information on the business environment AstraZeneca operates in, including the factors underpinning the industry’s future growth prospects, is included in the Directors’ Report. Details of the product portfolio of the Group (including patent expiry dates for key marketed products), our approach to product development and our development pipeline are covered in detail with additional information by Therapy Area in the Directors’ Report.

The financial position of the Group, its cash flows, liquidity position and borrowing facilities are described in the Financial Review from page 86. In addition, Note 23 to the Financial Statements from page 175 includes the Group’s objectives, policies and processes for managing its capital, its financial risk management objectives, details of its financial instruments and hedging activities and its exposures to credit, market and liquidity risk. Further details of the Group’s cash balances and borrowings are included in Notes 13 and 14 to the Financial Statements from page 164.

The Group has considerable financial resources available. As at 31 December 2012, the Group had $9.8 billion in financial resources (cash balances of $7.7 billion and undrawn committed bank facilities of $3 billion which are available until April 2017, with only $0.9 billion of debt due within one year). The Group’s revenues are largely derived from sales of products which are covered by patents which provide a relatively high level of resilience and predictability to cash inflows, although our revenue is expected to continue to be significantly impacted by the expiry of patents over the medium term. In addition, recent government price interventions in response to budgetary constraints are expected to continue to adversely affect revenues in many of our mature markets. However, we anticipate new revenue streams from both recently launched medicines and products in development, and the Group has a wide diversity of customers and suppliers across different geographic areas. Consequently, the Directors believe that, overall, the Group is well placed to manage its business risks successfully despite the current uncertain economic outlook.

After making enquiries, the Directors have a reasonable expectation that the Company and the Group have adequate resources to continue in operational existence for the foreseeable future. Accordingly, they continue to adopt the going concern basis in preparing the Annual Report and Financial Statements.

Changes in share capital

Changes in the Company’s Ordinary Share capital during 2012, including details of the allotment of new shares under the Company’s share plans, are given in Note 20 to the Financial Statements from page 172.

Directors’ shareholdings

The Articles require each Director to be the beneficial owner of Ordinary Shares in the Company with an aggregate nominal value of $125 (which currently represents at least 500 shares because each Ordinary Share has a nominal value of $0.25). Such holding must be obtained within two months of the date of the Director’s appointment. At 31 December 2012, all of the Directors complied with this requirement and full details of each Director’s interests in shares of the Company are set out in the Directors’ interests in shares section from page 134. Information about the shareholding expectations of the Remuneration Committee (in respect of Executive Directors and SET members) and the Board (in respect of Non-Executive Directors) is also set out in the Directors’ Remuneration Report from page 122.

Political donations

Neither the Company nor its subsidiaries made any EU political donations or incurred any EU political expenditure in 2012 and they do not intend to do so in the future in respect of which shareholder authority is required, or for which disclosure in this Annual Report is required, under the Companies Act 2006. However, to enable the Company and its subsidiaries to continue to support interest groups or lobbying organisations concerned with the review of government policy or law reform without inadvertently breaching the Companies Act 2006, which defines political donations and other political expenditure in broad terms, a resolution will be put to shareholders at the 2013 AGM, similar to that passed at the 2012

 

 

120   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

AGM, to authorise the Company and its subsidiaries to:

 

> make donations to political parties or independent election candidates
> make donations to political organisations other than political parties
> incur political expenditure, up to an aggregate limit of $250,000.

Corporate political contributions in the US are permitted in defined circumstances under the First Amendment of the US Constitution and are subject to both federal and state laws and regulations. In 2012, the Group’s US legal entities made contributions amounting in aggregate to $1,759,450 (2011: $1,099,450) to national political organisations, state-level political party committees and to campaign committees of various state candidates. No corporate donations were made at the federal level and all contributions were made only where allowed by US federal and state law. We publicly disclose details of our corporate US political contributions, which can be found at astrazeneca-us.com/responsibility/ transparency/. The annual corporate contributions budget is reviewed and approved by the US General Counsel, the US Vice-President, Corporate Affairs and the President of our US business to ensure robust governance and oversight. US citizens or individuals holding valid green cards exercised decision making over the contributions and the funds were not provided or reimbursed by any non-US legal entity. Such contributions do not constitute political donations or political expenditure for the purposes of the Companies Act 2006 and were made without any involvement of persons or entities outside the US.

Significant agreements

There are no significant agreements to which the Company is a party that take effect, alter or terminate on a change of control of the Company following a takeover bid. There are no persons with whom we have contractual or other arrangements, who are deemed by the Directors to be essential to our business.

Use of financial instruments

The Notes to the Financial Statements, including Note 23 (from page 175), include further information on our use of financial instruments.

Creditor payment policy

Our policy is to agree appropriate payment terms with all suppliers when agreeing to the terms of each transaction, to ensure that those suppliers are made aware of the terms of payment and, subject to their compliance, to abide by the terms of payment. A considerable part of the trade creditors’ balance continues to relate to the Merck account in the US, which has particularly long contractual payment terms. On 26 June 2012, AstraZeneca and Merck agreed to amend certain provisions of their ongoing Agreements with respect to the Second Option, as detailed in Note 9 to the Financial Statements from page 161. Our trade creditors’ balance excluding payments to Merck and other items not directly related to trade purchases in the US is our most accurate calculation of balances owed by the Company’s subsidiaries to trade creditors at the balance sheet date. This was equivalent to 56 days’ average purchases (2011: 43 days; 2010: 57 days). Historically, we have also disclosed the total figure including any trade balances payable to Merck. By including these items, an average of 58 days is obtained (2011: 50 days; 2010: 62 days).

The Company has no external trade creditors.

Annual General Meeting

The Company’s AGM will be held on 25 April 2013. The meeting place will be in London, UK. A Notice of AGM will be sent to all registered holders of Ordinary Shares and, where requested, to the beneficial holders of shares.

External auditor

A resolution will be proposed at the AGM on 25 April 2013 for the re-appointment of KPMG as auditor of the Company. The external auditor has undertaken various non-audit work for us during 2012. More information about this work and the audit and non-audit fees that we have paid are set out in Note 27 to the Financial Statements on page 190. The external auditor is not engaged by us to carry out

any non-audit work in respect of which it might, in the future, be required to express an audit opinion. As explained more fully in the Audit Committee section from page 115, the Audit Committee has established pre-approval policies and procedures for audit and non-audit work permitted to be carried out by the external auditor and has carefully monitored the objectivity and independence of the external auditor throughout 2012.

Directors’ Report

The Directors’ Report, which has been prepared in accordance with the requirements of the Companies Act 2006, comprises the following sections:

 

> Strategy
> Performance
> Corporate Governance
> Development Pipeline
> Shareholder Information
> Corporate Information

and has been signed on behalf of the Board.

A C N Kemp

Company Secretary

31 January 2013

 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   121

Table of Contents

Corporate Governance | Directors’ Remuneration Report

 

LOGO

 

The performance of AstraZeneca as set out in this Annual Report was mixed. Revenues and profit were down versus prior year. Although Core earnings per share and cash flow fell versus 2011, they both exceeded targets set at the beginning of the year. Shareholders also had mixed fortunes. Total shareholder return performance was weak. But cash distributions (including buybacks) reflected the strong cash flow generation, which also supported the strengthening of the product pipeline through the acquisition of Ardea, the collaboration with Amgen and the extension of our diabetes alliance with BMS. We know that our shareholders expect pay appropriately to reflect performance. The Remuneration Committee has taken these diverse factors and expectations into account in making its judgements in 2012.

The business environment for the Company will continue to be challenging in 2013, and beyond, in terms of the fiscal pressures on governments, which in most markets have a direct affect on the Company’s business; the need to continue to address R&D productivity; and the need to maintain a level of investment that is right for the future of AstraZeneca but which is also balanced against shareholders’ expectations for return on their investment in the Company. The Remuneration Committee has to take a judicious view of performance stretch and reward. So performance targets must be stretching; but not so stretching as to compromise or weaken incentivisation. For example, we have increased for 2013, many of the revenue targets in priority areas (Emerging Market sales and sales of Brilinta/ Brilique would be two cases in point). But the environmental factors referred to above were also recognised by the Remuneration Committee in setting the free cash flow

threshold under the AstraZeneca Performance Share Plan (PSP) in March 2012 (relating to performance over the period 2012 to 2014 inclusive), which is lower (principally but not solely because of patent expiry) than the equivalent cash flow targets applicable to previous awards (details are set out on pages 129 and 130).

Following Pascal Soriot’s appointment as CEO in October, the Remuneration Committee has been reviewing the Company’s remuneration framework. The Remuneration Committee wishes to ensure that remuneration structures continue to be closely aligned with the Company’s strategy, and that they will support and drive achievement of our business objectives.

The Remuneration Committee is proposing a number of changes to both short-term and long-term incentive arrangements for Executive Directors and other senior executives.

 

> The composition of performance metrics for the annual bonus plan will be adjusted. From 2013, they will be based on an integrated Group scorecard that includes both financial and non-financial performance metrics, as well as reflecting individual performance. No changes are being made to the funding of the bonus pool, the overall quantum at the Group or individual level, or the payout curve. The new integrated Group scorecard will be based on four key priorities: ‘Achieve scientific leadership’, ‘Restore growth’, ‘Achieve Group financial targets’ and ‘Ensure AstraZeneca is a great place to work’, with all but the last scorecard priority forming part of the financial determination of the bonus outcome. Targets for each category have been set for 2013.
> Proposed changes to performance metrics (but not to the rules nor the quantum of compensation opportunity) of the PSP are under consideration. The Remuneration Committee will consult the Group’s largest investors about the PSP proposals and will take those views into account before reaching its final decision. This consultation process will take place in the first quarter of 2013 and before any awards are made under the PSP. The Remuneration Committee’s intention in considering these changes is to ensure that the PSP continues to provide incentives for management to perform successfully against a balance of both financial and non-financial metrics. Further information about the new PSP performance metrics will be made available at the AGM. Shareholders will of course have an opportunity to vote on the new PSP arrangements as part of the vote on remuneration policy to be introduced by the new UK Department for Business, Innovation & Skills’ executive remuneration proposals, which we expect to be implemented with effect from 2014.

Given the Board changes during the year, the Remuneration Committee gave careful consideration to a number of related remuneration matters. In particular, the remuneration package for our new CEO; the arrangements for Simon Lowth’s four months service as Interim CEO and his return to the role of CFO; and the arrangements relating to the retirement of our former CEO, David Brennan. We consulted with our major investors where appropriate on these matters, and related information was provided to the market by way of announcements at the relevant times. The arrangements are described in detail in this Remuneration Report.

 

 

122   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

LOGO

 

There are a number of ways in which we seek to listen and respond to the views of shareholders on remuneration matters during the year, including at the AGM, and via consultation with the Company’s largest investors about specific remuneration matters. In the latter part of each year, the Company usually hosts a meeting to which we invite our largest shareholders and seek their views on executive remuneration and corporate governance more broadly. In previous years, a number of Non-Executive Directors have been available to shareholders at that meeting, including the Chairman of the Board, myself as Chairman of the Remuneration Committee as well as other Board members. Although we cancelled the meeting proposed to be held in December in anticipation of our dialogue with shareholders on remuneration matters in the first quarter of 2013, we intend to continue to hold such meetings annually, with the aim of maintaining a constructive discussion with shareholders on these topics.

Anticipating the coming into effect of the new regulations proposed by the UK Department for Business, Innovation & Skills, we have taken the opportunity to structure this 2012 Directors’ Remuneration Report to incorporate a number of the proposed features. As a result, this Remuneration Report has been prepared with separate sections that set out, first, our remuneration policy (Policy Report) and, second, how that policy has been implemented in 2012 (Implementation Report). We have not yet produced a Remuneration Report that is fully compliant with the proposed new regulations because they are still to be published in their final form. But our 2013 Remuneration Report will fully reflect the new regulations and we will place resolutions before shareholders accordingly at the 2014 AGM.

As last year, we have sought in this Remuneration Report to answer the question: what have we paid our Executive Directors and why? The answer to this question is largely contained in the Implementation Report, which commences on page 127. To simplify the narrative and structure of this year’s Remuneration Report we have placed a lot of detailed disclosure (including pensions, the fees paid to the Chairman and Non-Executive Directors, and facts and figures relating to the long-term incentive plans) in the Appendix from page 131. We have taken into account Group and individual performance in 2012. We are guided in our judgements by our compensation schemes and their rules. But we know that we must exercise appropriate discretion to ensure that reward outcomes at AstraZeneca are appropriately consistent with the protection of your interests as our shareholders.

As ever, we would welcome your feedback.

John Varley

Chairman of the Remuneration Committee

 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   123

Table of Contents

Corporate Governance | Directors’ Remuneration Report

 

Remuneration Committee membership

The Remuneration Committee members are John Varley (Chairman of the Remuneration Committee), Leif Johansson, Rudy Markham and Nancy Rothwell. Leif Johansson was considered by the Board to be independent upon his appointment as Chairman of the Board; in accordance with the UK Corporate Governance Code, the test of independence is not appropriate in relation to the Chairman after his appointment. All other members of the Remuneration Committee are independent Non-Executive Directors. The Deputy Company Secretary acts as the secretary to the Remuneration Committee.

Terms of reference

A copy of the Remuneration Committee’s terms of reference is available on our website, astrazeneca.com. The Remuneration Committee conducted a review of its terms of reference during 2012. A small number of minor changes were recommended to the Board, principally to reflect updated guidance issued by the Association of British Insurers in September. The changes were approved by the Board in January 2013.

Main work of the Remuneration Committee during 2012

The Remuneration Committee met 12 times in 2012. The individual attendance record of Remuneration Committee members is set out on page 113. At the invitation of the Remuneration Committee, except where their own remuneration was being discussed, the CEO; the Executive Vice-President, Human Resources & Corporate Affairs; the Global Head, Reward & Employment; and the Vice-President, Global Compensation attended one or more Remuneration Committee meetings in 2012 and provided advice and services that materially assisted the Remuneration Committee. In addition, all meetings of the Remuneration Committee were attended by Carol Arrowsmith, representing Deloitte LLP (Deloitte), the Remuneration Committee’s independent adviser.

The work of the Remuneration Committee focused on the following principal matters during 2012:

 

> Executive Directors’ remuneration arrangements on appointment, change of role and retirement as described elsewhere in this Remuneration Report.
> The terms of other senior executives’ remuneration packages on appointment, promotion or termination.
> The Non-Executive Chairman’s remuneration arrangements on appointment.
> The assessment of Group and individual performance against performance targets to determine the level of executive bonuses for performance during 2011 and to set executive bonus performance targets for 2012.
> The assessment of performance against targets to determine the level of vesting in 2012 under the PSP, and the setting of PSP and AZIP performance thresholds for awards made in 2012.
> The determination of individual awards made under the Group’s main long-term incentive plans: the PSP, the AZIP and the AstraZeneca Global Restricted Stock Plan to SET members and other participants.
> The determination of restricted share awards to a number of senior executives under the AstraZeneca Restricted Share Plan.
> Proposed changes to certain elements of short-term and long-term incentive arrangements.
> A review of Group reward data, including CEO pay relative to average pay, and average salary data analysed by gender, and bonus data for the direct reports of SET members.
> A review of the sources and robustness of market remuneration data provided to the Remuneration Committee.
> A benchmarking review of the Remuneration Committee’s activities and policies against institutional investor guidelines.
> A review of the shareholding requirements for Executive Directors and the shareholding levels of other SET members.
> A review of the pension entitlements of Executive Directors and other SET members.
> A review of the proportion of Executive Directors’ and SET members’ annual cash bonuses that are deferred into shares with a three year vesting period.
> Consideration of the UK government’s June proposals concerning executive pay.
> A review of the performance of Deloitte, the independent adviser to the Remuneration Committee.
> The annual review of the performance of the Remuneration Committee.
> The preparation, review and approval (in January 2013) of this Remuneration Report.

Adviser to the Remuneration Committee

The Remuneration Committee retains Deloitte, represented by Carol Arrowsmith, who provided independent advice on various matters considered by the Remuneration Committee in 2012. The cost of this service to the Company in 2012 was £229,260 (including VAT). During the year, Deloitte also provided taxation advice and other specific non-audit services to the Group. The Remuneration Committee reviewed the potential for conflicts of interest and judged that there were no conflicts. Deloitte is a member of the Remuneration Consultants’ Group, which is responsible for the stewardship and development of the voluntary code of conduct in relation to executive remuneration consulting in the UK. The principles on which the code is based are transparency, integrity, objectivity, competence, due care and confidentiality. Deloitte adheres to the code.

Shareholder context

At the Company’s AGM in April 2012, the resolution to approve the Directors’ Remuneration Report for the year ended 31 December 2011 was passed with 91.37% of the votes cast for the resolution and 8.63% of the votes cast against the resolution.

Basis of preparation of this Remuneration Report

This Remuneration Report has been prepared in accordance with the Large and Medium-sized Companies and Groups (Accounts and Reports) Regulations 2008 (Regulations) and meets the relevant requirements of the Financial Services Authority’s Listing Rules. As required by the Regulations, a resolution to approve this Remuneration Report will be proposed at the AGM on 25 April 2013.

 

 

124   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

Policy Report

Key elements of remuneration policy

 

     Purpose and link to strategy    Operation    Performance measures
Base salary    Base salary is intended to be sufficient (but no more than necessary) to attract, retain and develop high-calibre talent.   

Based on conditions in the relevant market and recognising the value of an individual’s sustained personal performance and contribution to the business, taking account of the market rate for an individual’s skills and experience.

 

Benchmarked periodically (but not annually) against external comparators.

 

    
Benefits   

Non-cash benefits are designed to be sufficient (but no more generous than necessary) to attract, retain and develop high-calibre talent.

 

   Based on local median market practice.     
Annual bonus    The annual bonus rewards short-term performance against specific Group and individual objectives.   

An annual cash incentive opportunity determined by reference to an integrated Group scorecard and individual performance, measured over a single financial year of the Company relative to targets set at the beginning of each year.

 

The Remuneration Committee requires that certain percentages of the annual bonus are converted into stock to be held for three years before vesting.

 

  

The Group performance measures ensure that all eligible employees receive an element of reward based on the Group’s overall financial and non-financial performance.

 

Individual goals are based on annual objectives.

 

More information about the performance measures for the 2012 annual bonus in respect of the Executive Directors is set out on page 129.

 

AstraZeneca Performance

Share Plan (PSP) 1

As described in the introduction to this Remuneration Report from the Chairman of the Remuneration Committee, changes to performance metrics for the PSP are under consideration. It is planned that consultation with shareholders and implementation of the changes will take place in 2013. The information set out in this table refers to awards made under the PSP, up to and including 2012.

 

   The PSP rewards the outperformance of industry peers in terms of shareholder value creation measured by relative TSR, and the generation of cash at levels to finance investment in the business, debt repayment and the Company’s shareholder distribution policy.   

The PSP was approved by shareholders at the 2005 AGM and provides for the grant of awards over Ordinary Shares or ADSs.

 

The three year performance periods commence on 1 January in the year of the award. The vesting date is the third anniversary of the date of the award.

 

In respect of any financial year of the Company, the maximum market value of shares that may in theory be put under an award under the PSP is 500% of a participant’s base salary (which converts into an expected value of 250%). The actual individual limits that apply under the PSP, subject to this maximum, are set by the Remuneration Committee from time to time.

 

In the event that employment ceases for anything other than a ‘good leaver’ reason, any unvested awards lapse unless the Remuneration Committee decides otherwise.

 

  

Fifty percent based on the relative TSR performance of the Company over the relevant three year performance period against a predetermined peer group of global pharmaceutical companies.

 

Fifty percent based on the achievement of a cumulative free cash flow target over the relevant three year performance period, based on a sliding scale between a threshold target and an upper target.

 

More information about the PSP’s performance measures is set out on page 129.

AstraZeneca Investment Plan (AZIP) 1   

The performance and holding periods of the AZIP are influenced by the Group’s targeted product development cycle, reflecting the long-term investment horizons that are a feature of the industry.

 

Dividend-based performance hurdles motivate the generation of returns for shareholders on a sustainable basis over an extended period of time.

  

The AZIP was approved by shareholders at the 2010 AGM and provides for the grant of awards over Ordinary Shares or ADSs.

 

The AZIP is operated over a four year performance period and a subsequent four year holding period.

 

Performance periods commence on 1 January in the year of the award. Holding periods commence at the end of the performance period and end eight years from 1 January in the year of the award.

 

In respect of any financial year of the Company, the maximum market value of shares that may, in theory, be put under an award under the AZIP is 500% of a participant’s base salary (which converts into an expected value of 500%). The actual individual limits that apply under the AZIP, subject to this maximum, are set by the Remuneration Committee from time to time.

 

Clawback – the Remuneration Committee may claw back some or all of the shares that are the subject of a participant’s award at any time during the performance or the holding period if, in the opinion of the Remuneration Committee (acting fairly and reasonably), this is warranted by underlying Company performance, the occurrence of an event that causes or is very likely to cause reputational damage to the Company or serious misconduct by the participant.

 

  

A combination of dividend and dividend cover hurdles, assessed over the relevant four year performance period.

 

More information about the AZIP’s performance hurdles is set out on page 130.

Pension    Provision of retirement benefits.   

Benchmarked against the relevant local

employment market.

 

    

 

1   In respect of long-term incentive awards, the current distribution between the PSP and the AZIP is in the ratio 75% to 25%.

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   125

Table of Contents

Corporate Governance | Directors’ Remuneration Report

Performance evaluation process

AstraZeneca conducts an annual performance evaluation process for all of its executives. In the case of members of the Senior Executive Team, this is conducted by the CEO. In the case of the CEO, this is conducted by the Chairman of the Board. Recommendations are then made to the Remuneration Committee. Those reviews take place relative to Group and individual objectives which are set at the beginning of each year.

Service contracts

The notice periods and unexpired terms of Executive Directors’ service contracts at 31 December 2012 are shown in the table below.

Subject to the arrangements in respect of the first 12 months of Pascal Soriot’s service, which are described below, either AstraZeneca or the Executive Director may terminate the service contract on 12 months’ notice. It is the Remuneration Committee’s intention that, in the event of early termination of an Executive Director’s employment, any compensation payable under his/her service contract should not exceed the salary and benefits that would have been received had the contractual notice period been worked and this may be further reduced in line with the Executive Director’s duty to mitigate losses.

None of the Executive Directors has any provision in their service contracts giving them a right to liquidated damages or an automatic entitlement to bonus for the duration of their notice period.

 

Executive Director

   Date of service contract    Unexpired term at 31 December 2012    Notice period

Pascal Soriot

   27 August 2012    21 months 1    Reducing to 12 months 1

Simon Lowth

   5 November 2007    12 months    12 months

 

1   The notice period in Mr Soriot’s service contract is 24 months initially, which is reducing by one month for each month of service and will stabilise at a 12 month notice period.

Policy on external appointments and retention of fees

Subject to specific Board approval in each case, Executive Directors and other SET members may accept external appointments as non-executive directors of other companies, and retain any related fees paid to them, provided that such appointments are not considered by the Board to prevent, or reduce, the ability of the executive to perform their role within the Group to the required standard. Simon Lowth is a Non-Executive Director of Standard Chartered PLC. In respect of this position, he received fees of £130,000 for his services in 2012.

Considering the wider employee context

The Remuneration Committee sets overall remuneration policy and makes decisions about specific remuneration arrangements in the broader context of employee remuneration throughout the Group. The Remuneration Committee annually reviews Group remuneration data including ratios of average pay to senior executive pay; bonus data; gender and geographical data in relation to base salaries and variable compensation; and aggregate data about the shareholding levels of senior managers. In reviewing the base salaries of Executive Directors and SET members, the Remuneration Committee considers the overall level of any salary increases being awarded to employees across the Group in the relevant year.

Shareholder and broader context

In all aspects of its work, the Remuneration Committee considers both the external environment in which the Company operates and the guidance issued by organisations representing institutional shareholders. It consults the Company’s largest investors on general and specific remuneration and provides an annual opportunity for representatives of those investors to meet the Chairman of the Remuneration Committee and other Remuneration Committee and Board members. The Remuneration Committee works with the Audit Committee to ensure that the Group’s remuneration policies and practices achieve the right balance between appropriate incentives to reward good performance and managing risk in terms of employee behaviour and how the Company achieves its business objectives. The annual bonus plan, in which all employees participate, contains goals relating to the demonstration of commitment to integrity, with the aim of enhancing the Company’s reputation and avoiding reputational damage.

 

126   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

Implementation Report

Implementation of remuneration policy in 2012

Pascal Soriot

Mr Soriot joined AstraZeneca as CEO on 1 October. In establishing his remuneration arrangements, the Remuneration Committee sought to offer a package that was internationally competitive, but pay no more than was necessary. In doing so, to the extent possible, the Remuneration Committee put in place a framework that maintained broadly the same balance in terms of its constituent elements and overall quantum as for the previous CEO, which the Remuneration Committee considers to be right for AstraZeneca and its shareholders.

At the time of Mr Soriot’s appointment as CEO, certain share awards and payments, which are described below, were negotiated and agreed. They were approved by the Remuneration Committee in order to compensate Mr Soriot for the forfeiture of unvested long-term incentive awards and forfeited 2012 bonus opportunity from his previous employer. The principle governing the decision of the Remuneration Committee was that the buyout should be implemented predominantly in shares of AstraZeneca in circumstances where the vesting and, in the case of the award under the AZIP, the holding period operate over several years. The unvested long-term incentive awards from Mr Soriot’s previous employer were valued with the assistance of an independent third party, using its standard methodology for such work and, where relevant, taking into account the extent to which such awards might have been expected to vest.

General information about annual bonus outcomes for performance in 2012 can be found on page 129. In awarding Mr Soriot’s bonus for 2012, the Remuneration Committee recognised the strong start he had made since becoming CEO and his positive impact on the organisation.

 

     2012    Notes
Base salary    £275,000   

The annual rate of base salary for the CEO in 2012 was £1,100,000.

 

         

Mr Soriot was appointed as CEO with effect from 1 October.

 

Benefits    £1,017,000   

This sum is made up of:

 

         

£991,000 being cash paid to compensate Mr Soriot in respect of his forfeited bonus opportunity for 2012 from his previous employer, paid at his previous employer’s target bonus rate and pro-rated from 1 January 2012 to 30 September. Mr Soriot is required to invest this sum, after payment of income tax, in AstraZeneca shares; and

 

£26,000 being remaining cash following selection of benefits within the Company’s UK flexible benefits programme.

 

Annual bonus    £335,000   

Mr Soriot was awarded a bonus for performance during 2012 of 122% of base salary out of a maximum possible award of 180% of base salary (range 0% – 180% with a target annual bonus of 100%). This award was pro-rated from 1 October to 31 December to reflect the date of Mr Soriot’s appointment as CEO.

 

     

One-third of any pre-tax bonus must be deferred into Ordinary Shares or ADSs. These are held for three years before being released.

 

         

The bonus is not pensionable.

 

Award of restricted shares 1    £2,000,000   

On 26 October, Mr Soriot was granted an award of 69,108 restricted Ordinary Shares at a price of 2894 pence per share by way of compensation for the loss of long-term incentives from his previous employer.

 

     

No performance conditions apply.

 

     

Vesting schedule for this award (subject to Mr Soriot’s continued employment with the Company):

 

      > 40% on 1 October 2013
      > 30% on 1 October 2014
         

> 30% on 1 October 2015.

 

Pension    £66,000   

Cash payment equivalent to 24% of base salary (time pro-rated to take account of Mr Soriot’s joining date in 2012) taken by Mr Soriot as a cash alternative to participation in a defined contribution pension scheme.

 

 

1   In addition to the award of restricted shares, on 26 October, Mr Soriot was also granted an award of 69,108 Ordinary Shares at a price of 2894 pence per share under the AZIP (also by way of compensation for the loss of long-term incentives from his previous employer). This award is subject to a four year performance period (1 January 2012 to 31 December 2015) and a subsequent four year holding period (1 January 2016 to 31 December 2019). The performance hurdles that apply to this award are that the annual dividend per share paid to holders of Ordinary Shares must increase from $2.80 over the four year performance period ($2.80 being the full-year dividend for 2011), and that dividend cover over the same period (based on Reported earnings before restructuring costs) does not fall below 1.5 times.

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   127

Table of Contents

Corporate Governance | Directors’ Remuneration Report

Simon Lowth

During 2012, at a time of considerable change within the Group, Mr Lowth served as Interim CEO for the period 1 June to 30 September, reverting to his previous role as CFO on 1 October.

To reflect his additional responsibilities during his tenure as Interim CEO, he was awarded a temporary increase in base salary. General information about annual bonus outcomes for performance in 2012 can be found on the page opposite. The Remuneration Committee also recognised Mr Lowth’s excellent performance as Interim CEO, and his strong support to Mr Soriot in his new position as CEO, in determining the quantum of his annual bonus award.

 

     2012    Notes
Base salary    £740,000   

Base salary for the CFO in 2012 was £660,000.

 

         

Temporary base salary increase effective from June to September inclusive (period as Interim CEO) was £20,000 gross per month creating an annualised base pay figure of £900,000. This compares with the annualised salary of the outgoing CEO of £997,223. This temporary base salary increase was not pensionable.

 

Benefits    £103,000   

This sum is made up of:

 

     

£47,000 being cash paid in respect of dividends accrued on Ordinary Shares which vested in 2012, having been deferred in 2009 in respect of Mr Lowth’s annual bonus awarded for performance in 2008;

 

         

£50,000 being remaining cash following selection of benefits within the Company’s UK flexible benefits programme; and £6,000 for other benefits, including healthcare insurance.

 

Annual bonus    (a) £554,000   

(a)  Mr Lowth was awarded a bonus for performance during his period as CFO during 2012 of 126% of base salary out of a maximum possible award of 150% of base salary (range 0% – 150% with a target annual bonus of 90%).

 

   (b) £480,000   

(b)  The annual bonus target was increased from 90% to 100% of base salary effective from June to September inclusive (Mr Lowth’s period as Interim CEO), in line with that applicable to the CEO. For this period, Mr Lowth was awarded a bonus of 160% (range 0% – 180% with a target annual bonus of 100%).

 

   Total: £1,034,000   

One-third of any pre-tax bonus must be deferred into Ordinary Shares or ADSs. These are held for three years before being released.

 

         

The bonus is not pensionable.

 

AstraZeneca Performance Share Plan (PSP)    £897,000   

This sum is made up of:

 

£771,000 being the estimated market value1 of Ordinary Shares which will vest in March 2013 in respect of the 2010 PSP award (three year performance period 2010 to 2012); and

 

£126,000 being cash to be paid on the vesting of this award in respect of dividends accrued.

Pension    £158,000   

Cash payment equivalent to 24% of base salary (as CFO) taken by Mr Lowth as a cash alternative to participation in a defined contribution pension scheme.

 

 

1   Estimated market value of 3153 pence per Ordinary Share based on the London Stock Exchange closing price on 30 January 2013.

David Brennan

In April 2012, Mr Brennan informed the Board that he wished to retire. Mr Brennan relinquished his responsibilities as a Director and as CEO on 1 June.

 

     2012    Notes
Base salary    £499,000   

Base salary for the CEO in 2012 was at the rate of £997,223.

 

         

Mr Brennan retired as CEO and as a Director on 1 June. His employment with the Company ended on 30 June.

 

Pay in lieu of
notice 		   £914,000   

On leaving the Company at a date determined by the Board, Mr Brennan received a lump sum payment in lieu of contractual notice, representing 11 months’ base pay.

 

Benefits    £252,000   

This sum is made up of:

 

an allowance of up to £120,000 for relocation costs under Mr Brennan’s contract;

 

     

£86,000 being cash paid in respect of dividends accrued on Ordinary Shares which vested in 2012, having been deferred in 2009 in respect of Mr Brennan’s annual bonus awarded for performance in 2008;

 

     

£17,000 allowance for professional fees (legal and pensions advice in connection with Mr Brennan’s retirement);

 

     

£16,000 for other benefits including healthcare insurance; and

 

         

£13,000 car allowance.

 

Annual bonus    None awarded   

Mr Brennan informed the Remuneration Committee that he did not wish to be considered for a bonus in respect of that part of 2012 during which he was CEO. The Remuneration Committee determined that no such bonus would be awarded and also that there should be no bonus award relating to the contractual notice period.

 

AstraZeneca Performance Share Plan (PSP)    £1,577,000   

This sum is made up of:

 

£1,355,000 being the estimated market value 1 of Ordinary Shares which will vest in March 2013 in respect of the 2010 PSP award (three year performance period 2010 to 2012), and being pro-rated from 7 May 2010 to 30 June 2012 to reflect the period of Mr Brennan’s employment since the award was granted; and

 

£222,000 being cash to be paid on the vesting of this award in respect of dividends accrued.

 

The Remuneration Committee determined that the share awards made to Mr Brennan in 2011 and 2012 under the PSP and the AZIP should be forfeited.

 

Pension        

Mr Brennan’s pension entitlement was provided through a combination of the AstraZeneca US Defined Benefit Pension Plan and US defined contribution arrangements. He had an accrued pension at 30 June of $1,584,000 (£1,000,000) per annum from his defined benefit arrangements. Full details can be found on page 131.

 

 

1   Estimated market value of 3153 pence per Ordinary Share based on the London Stock Exchange closing price on 30 January 2013.

 

128   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

Variable elements of the CEO’s and CFO’s remuneration in 2012 – additional disclosures

Annual bonus outcomes for performance in 2012

For Executive Directors, the principal drivers of annual bonus opportunity are EPS (27% weighting), cash flow (9% weighting), and scorecards (Group and SET area, 64% weighting). For the CEO, the average of all SET area scorecards is used to create an aggregate scorecard weighting. For the CFO, the average of Finance and Strategic Partnering and Business Development scorecards is used. Reward driven by EPS and cash flow performance depends on EPS and cash flow outcomes versus targets set at the beginning of each year. Reward driven by the scorecards depends on performance outcomes relative to goals in the areas of Values, Pipeline and People set at the beginning of each year. At constant exchange rates, there were declines in revenue, Core operating profit and EPS versus prior year. However, the Core EPS outcome and the cash flow outcome both exceeded the target set at the beginning of 2012. That element of the bonus payout which was driven by EPS and cash flow performance therefore exceeded target. In respect of the scorecards, a number of factors were taken into consideration. These include the supply problems described elsewhere in this Remuneration Report and the slower than expected uptake of Brilinta/Brilique . But they also include the strengthening of the pipeline through the acquisition of Ardea, the collaboration with Amgen, and the extension of our diabetes alliance with BMS through the inclusion of the Amylin product portfolio. Both Forxiga and Zinforo were launched in Europe, and we had a successful launch of Nexium in Japan. These factors collectively drove a score relative to scorecard performance of slightly below target.

The outturn is that the total variable short-term compensation of Executive Directors and other SET members in 2012 fell relative to the equivalent number in 2011.

The Remuneration Committee decided that Mr Soriot’s annual bonus should amount to 122% of base salary, representing 68% of the potential maximum. The Remuneration Committee decided that Mr Lowth’s annual bonus should be 140% of base salary, representing 86% of the potential maximum.

Mr Brennan informed the Remuneration Committee that he did not wish to be considered for a bonus in respect of that part of 2012 during which he was CEO and the Remuneration Committee determined that no such bonus would be awarded.

Annual bonus deferral

Part of the annual bonus of Executive Directors and other SET members is deferred into shares, helping to align senior executives’ interests with those of shareholders. The proportion currently deferred into shares is one-third of the pre-tax annual bonus for Executive Directors and one-sixth for other SET members. The shares are acquired on the open market at the prevailing market price and held for a period of three years from the date of acquisition before being delivered to individual Executive Directors and other SET members.

Performance measures under the PSP

The vesting of PSP awards is contingent on performance against specified performance measures over the relevant three year performance period and continued employment with the Group. Equal weighting is given to the two performance measures used: relative TSR and cumulative free cash flow.

Relative TSR – Fifty percent of the award is based on the Group’s relative TSR performance against a predetermined peer group of global pharmaceutical companies. The peer group is: Abbott, BMS, Eli Lilly & Company, GSK, Johnson & Johnson, Merck, Novartis, Pfizer, Hoffmann-La Roche Ltd and Sanofi-Aventis. TSR measures share price growth, and dividends reinvested in respect of a notional number of shares from the beginning of the relevant performance period to the end of it, and ranks the companies in the peer group by reference to their TSR achieved over that period. The rank which the Company’s TSR achieves over the performance period will determine how many shares will vest under the relevant PSP award. Payouts against performance in relation to TSR for PSP awards are expressed as a percentage of the maximum award currently payable, shown within a range of 0% to 100%, as set out in the table below.

 

TSR ranking of the Company

   % of the maximum PSP award that vests  

Below median

     0%   

Median

     25%   

Between median and upper quartile

     Pro rata   

Upper quartile

     75%   

Significantly above upper quartile

     100%   

Although 100% of the maximum award may vest at the Remuneration Committee’s discretion if the Company’s TSR performance is substantially better than that of the upper quartile of the comparator group, the Company would need to have sustained a level of performance significantly in excess of upper quartile over a period of years for the Remuneration Committee to be satisfied that the vesting of awards at this level was warranted.

In addition to the TSR performance target being met for each PSP award, the Remuneration Committee has to satisfy itself that achievement of the TSR performance target is an appropriate reflection of the Group’s underlying financial performance. It has the discretion to prevent PSP awards from vesting or only allow them to vest partially where this, in the judgement of the Remuneration Committee, is warranted.

The TSR graphs on page 134 show, for each PSP award, how the Company’s TSR performance has compared with the TSR for the companies in the comparator group from the first day of the relevant performance period to 31 December 2012, and how the Company ranks against those other peer companies on this basis.

Cumulative free cash flow – Fifty percent of the award vests subject to the achievement of the free cash flow performance measure, which operates as a cumulative cash flow target over the same three year performance period as the TSR performance measure. The measure for the cash flow target is net cash flow (before distributions) (subject to any further adjustments the Remuneration Committee chooses to make at its discretion and thus referred to as ‘adjusted cumulative cash flow’) and the level of vesting is based on a sliding scale between a threshold cash flow target and an upper target. Vesting levels in relation to the threshold target and the upper target are shown in the table overleaf.

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   129

Table of Contents

Corporate Governance | Directors’ Remuneration Report

 

Adjusted cumulative cash flow – all PSP awards made before 2012

   Adjusted cumulative cash flow – PSP awards made in 2012    % of the maximum PSP award that vests  

Less than $16 billion

   Less than $12 billion      0%   

$16 billion

   $12 billion      25%   

Between $16 billion and $23 billion

   Between $12 billion and $18 billion      Pro rata   

$23 billion and above

   $18 billion and above      100%   

Cumulative cash flow is considered to be the most appropriate measure of cash flow performance because it relates to the residual cash available to finance additional investment in specific business needs, debt repayments and our distribution policy. The cash flow measure encompasses a number of important elements of operational and financial performance and helps to align executives’ rewards with shareholder value creation. The level of vesting of this element is based on a sliding scale against a target that is intended to represent a significant challenge for the business. It is intended that the Remuneration Committee should have the discretion to adjust, but on an exceptional basis only, the free cash flow target during the performance period for material factors that might otherwise distort the performance measure in either direction. This allows performance to be assessed against targets that have been set on a consistent basis. For example, adjustments may be required to reflect exchange rate movements, significant acquisitions or divestments, and major legal and taxation settlements. Any major adjustments to the calculation are disclosed to shareholders. There is no retesting of performance.

Vesting of share awards made in 2010 under the PSP

In 2012, the TSR ranking of the Company was below median and therefore none of the award will vest in respect of that element of the performance measure. Fifty percent of the PSP award is based on free cash flow and in 2012 the Company achieved 95% of the free cash flow performance measure. The PSP share awards made in 2010 in respect of the 2010 to 2012 performance period will therefore vest at 47% for SET members, including Simon Lowth but excluding Pascal Soriot who does not hold any 2010 PSP awards. For the former CEO, David Brennan, vesting of his 2010 PSP awards will be pro-rated from 7 May 2010 to 30 June 2012 to reflect the period of his employment since the award was granted.

Performance hurdles under the AZIP

The performance hurdles for the AZIP awards are shown in the table below.

 

Year in which AZIP

award made

 

Relevant four year

performance period

   Dividend hurdle   

Dividend cover hurdle (based on Reported earnings

before restructuring costs)

2010   1 January 2010 to
31 December 2013 		  

That the annual dividend per share paid to holders of Ordinary Shares is increased from $2.30 over the performance period ($2.30 being the full year dividend for 2009)

 

   That dividend cover does not fall below 1.5 times over the performance period
2011   1 January 2011 to
31 December 2014 		  

That the annual dividend per share paid to holders of Ordinary Shares is increased from $2.55 over the performance period ($2.55 being the full year dividend for 2010)

 

   That dividend cover does not fall below 1.5 times over the performance period
2012   1 January 2012 to
31 December 2015 		  

That the annual dividend per share paid to holders of Ordinary Shares is increased from $2.80 over the performance period ($2.80 being the full year dividend for 2011)

 

   That dividend cover does not fall below 1.5 times over the performance period

The AZIP awards made to date remain outstanding other than those made to David Brennan in 2011 and 2012, which the Remuneration Committee determined should be forfeited.

Statement of Executive Directors’ shareholdings

In addition to the shareholding requirements imposed by the Board on Executive Directors and SET members and shown in the table below, under the Articles, all Directors must, within two months of their appointment, acquire a beneficial interest in at least 500 shares.

 

     Pascal Soriot      Simon Lowth  

Shareholding requirement for the CEO and CFO 1

     300% of base salary         200% of base salary   

Total number of shares beneficially owned as at 31 January 2013

     3,500         56,960   
Estimated market value of total number of shares beneficially owned based on the London Stock Exchange closing price of 3153 pence per share on 30 January 2013      £110,000         £1,796,000   

Estimated market value of total number of shares beneficially owned as a percentage of 2012 base salary

     10%         272%   

Total number of shares subject to deferral

     69,108         29,042   

Total number of shares subject to performance conditions

     69,108         205,397   

 

1   The shareholding requirement for all other SET members is 125% of base salary.

Further information about Executive Directors’ shareholdings can be found from page 134.

 

130   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

Appendix – Additional information

Audit

The Executive Directors’ pension arrangements disclosed in the Pension arrangements section below, the Directors’ emoluments disclosed in the Directors’ emoluments in 2012 section from page 132 and the details of the Directors’ interests in Ordinary Shares disclosed in the Directors’ interests in shares section (excluding the Beneficial interests sub-section) from page 134 have been audited by KPMG Audit Plc.

Pension arrangements

Pascal Soriot and Simon Lowth

Pascal Soriot and Simon Lowth are eligible to join the AstraZeneca Group Self Invested Personal Pension (UK Defined Contribution Plan (UK DCP)) at a Company contribution rate of 24% of annual base salary or, alternatively, to take the Company contribution as a cash allowance. Since joining AstraZeneca, Mr Lowth has elected to take the cash allowance in lieu of a pension, which during 2012 amounted to £158,000 ($251,000) (2011: £153,000 ($245,000)). In respect of 2012, Mr Soriot made a similar election, which amounted to £66,000 ($105,000).

In the event of a senior employee in the UK DCP (including one who has taken the alternative cash allowance) becoming incapacitated, permanent health insurance cover provides continuation of a proportion of salary, subject to the satisfaction of certain medical criteria. In the event of death prior to retirement, dependants are entitled to a lump sum secured from a multiple of 10 times salary, capped at £4.3 million.

David Brennan

David Brennan is a member of the AstraZeneca US Defined Benefit Pension Plan (US DBP). Benefits for members of the US DBP are delivered on a tax-qualified basis, with accrued benefits that exceed specific limits under the US DBP’s formula and the US Tax Code being delivered through a supplementary, non-qualified plan. The normal pension age under the US DBP is 65. However, on his retirement in 2012, Mr Brennan was eligible to take a pension or lump sum equivalent based on accrued service and final pensionable pay (ie without actuarial reduction) due to his satisfaction of a condition in the pension plan relating to combined age and service exceeding 85 years.

Mr Brennan’s participation in the US DBP was subject to a service cap at 35 years’ service, which was attained during his tenure as CEO and therefore service beyond 35 years is not shown in the table below. During his tenure as a Director, bonus payments were removed from the calculation of his pensionable pay under the US DBP.

Pension is payable to Mr Brennan in US dollars. For ease of understanding, the table below has been presented in both pounds sterling and US dollars using the exchange rates for 2012 set out on page 133. Transfer values are calculated to be consistent with the value of the lump sum distribution equivalent to his deferred accrued pension annually.

 

           David Brennan  
           £ 000        $000  

Defined benefit arrangements

                           

1.   Accrued pension at 1 January 2012

             988           1,565   

2.   Increase in accrued pension during year as a result of inflation

                         

3.   Adjustment to accrued pension as a result of salary increase relative to inflation

             12           19   

4.   Increase in accrued pension as a result of additional service

                         

5.   Accrued pension at 30 June 2012 1

             1,000           1,584   

6.   Employee contributions during 2012

                         

7.   Transfer value of accrued pension at 31 December 2011

             14,200           22,488   

8.   Transfer value of accrued pension at 30 June 2012 1

             14,776           23,400   

9.   Change in transfer value during the period less employee contributions

             576           912   

10. Age at 30 June 2012 1

     58 10/12                     

11. Pensionable service (years) at 30 June 2012 1

     35                      

 

1   Mr Brennan’s employment with AstraZeneca ended on 30 June 2012.

In addition to the US DBP, Mr Brennan (as a US citizen) was a contributing member of the US 401(k) savings plan. He also participated in AstraZeneca’s Executive Deferred Compensation Plan (EDCP) which is operated as a supplemental non-qualified plan in respect of US employees should annual contributions exceed the limit applicable to contributions under the qualified 401(k) plan. During 2012, total employer matching contributions of $47,000 (£30,000) (2011: $96,000 (£60,000)) were made to his 401(k) plan and EDCP. Member contributions of £224,000 ($355,000) were paid through salary sacrifice into the plans.

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   131

Table of Contents

Corporate Governance | Directors’ Remuneration Report

Summary of other share plans

AstraZeneca Global Restricted Stock Plan

The AstraZeneca Global Restricted Stock Plan (GRSP) was introduced in 2010 and provides for the grant of restricted stock awards over the Company’s Ordinary Shares or ADSs. The GRSP is operated for below SET-level employees only. Typically, awards are made in March each year and, in relation, for example, to new appointments or promotions, in August. Awards under the GRSP do not involve the issue or allotment of new Ordinary Shares or ADSs but rely instead on the market purchase of Ordinary Shares or ADSs.

AstraZeneca Restricted Share Plan

The AstraZeneca Restricted Share Plan (RSP) was introduced in 2008 and provides for the granting of restricted share awards to key employees, excluding Executive Directors. Awards are made on an ad hoc basis with variable vesting dates. The RSP was used in 2012 to make awards (totalling an aggregate of 643,000 Ordinary Shares under the plan for the calendar year 2012) to a number of key senior executives in specific situations considered by the Remuneration Committee. The Remuneration Committee has responsibility for agreeing any awards under the RSP and for setting the policy for the way in which the RSP operates. Awards under the RSP do not involve the issue or allotment of new Ordinary Shares or ADSs but rely instead on the market purchase of Ordinary Shares or ADSs.

AstraZeneca Share Option Plan

The AstraZeneca Share Option Plan (SOP) expired in May 2010. Details of outstanding options granted to Executive Directors are shown in the table on page 137. The Remuneration Committee imposed performance conditions in respect of the exercise of such options by SET members (including the Executive Directors) which, in the view of the Remuneration Committee, were considered appropriately stretching. In order for options to vest, the EPS of the Group must increase at least in line with the UK Retail Prices Index plus 5% per annum on average, over a three year period, the base figure being the EPS for the financial year preceding the date of grant, with no retesting. In addition, since the review of executive remuneration in 2004, the Remuneration Committee has included a condition that, if an event occurs which causes material reputational damage to the Company, such that it is not appropriate for the options to vest and become exercisable, the Remuneration Committee can make a determination to reflect this. No such determination was made in 2012.

Other plans

In addition to the plans described above, the AstraZeneca Savings-Related Share Option Plan and the AstraZeneca All-Employee Share Plan are operated in the UK, both of which are HM Revenue & Customs approved plans. Executive Directors and certain other SET members are eligible to participate in these plans.

Dilution under share plans

Other than the AstraZeneca Savings-Related Share Option Plan and the AstraZeneca All-Employee Share Plan, which operate in the UK only, and the SOP, none of AstraZeneca’s share plans has a dilutive effect because they do not involve the issue or allotment of new Ordinary Shares or ADSs but rely instead on the market purchase of Ordinary Shares or ADSs.

Chairman

The Remuneration Committee determines the terms of service, including remuneration, of the Chairman. The annual Board fees payable to the Chairman are set out in the table below. In addition to the Chairman’s fee, a proportion of the office costs of the Chairman are reimbursed; the sum paid in this respect in 2012 is set out in the Directors’ emoluments section below. The Chairman receives no additional fee or allowance for Remuneration Committee membership. The Chairman does not participate in the Group’s incentive plans or pension or healthcare arrangements.

Non-Executive Directors

None of the Non-Executive Directors has a service contract but all have letters of appointment. In accordance with the Articles, following their appointment, Directors must retire at each AGM and may present themselves for election or re-election. None of the Non-Executive Directors has any provision in their letter of appointment giving them a right to compensation payable upon early termination of their appointment. They are not eligible for performance-related bonuses or the grant of share awards or options. No pension contributions are made on their behalf.

The annual Board fees applicable to Non-Executive Directors are set out below.

Under the Articles, all Directors must, within two months of their appointment, acquire a beneficial interest in at least 500 shares. In addition to this mandatory shareholding requirement, the Board encourages each Non-Executive Director to build up, over time, a shareholding in the Company with a value approximately equivalent to the basic annual fee for a Non-Executive Director (£75,000) or, in the case of the Chairman, approximately equivalent to his annual fee (£500,000).

Non-Executive Directors’ fees

 

     £  

Chairman’s fee

     500,000   

Basic fee

     75,000   

Senior independent Non-Executive Director

     30,000   

Membership of the Audit Committee

     20,000   

Membership of the Remuneration Committee

     15,000   

Chairman of the Audit Committee or the Remuneration Committee 1

     20,000   

Membership of the Science Committee

     10,000   

Chairman of the Science Committee 1

     7,000   

 

1   This fee is in addition to the fee for membership of the relevant Committee.

Directors’ emoluments in 2012

The aggregate remuneration, excluding pension contributions and the value of shares under option and shares subject to share awards, paid to or accrued for all Directors for services in all capacities during the year ended 31 December 2012 was £7,308,000 ($11,572,000). The remuneration of individual Directors is set out in the Directors’ remuneration tables opposite in pounds sterling and US dollars. All salaries, fees, bonus and other benefits for Directors are established in pounds sterling.

 

132   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

Directors’ remuneration – pounds sterling

 

Name

   Salary
and fees
£ 000 		     Bonus
cash
£ 000 		     Bonus
Shares 1
£ 000 		     Taxable
benefits
£ 000 		     Other
payments
and
allowances
£ 000 		     Total
2012
£ 000 		     Total
2011
£ 000 		     Total
2010
£ 000 		 

Leif Johansson

     318 2                                        318                   

Pascal Soriot

     275         223         112                 1,017 3        1,627                   

Simon Lowth

     740         689         345         6         300 4        2,080         1,785         1,642   

Geneviève Berger

     58                                         58                   

Bruce Burlington

     105                                         105         98         33   

Graham Chipchase

     65                                         65                   

Jean-Philippe Courtois

     95                                         95         95         80   

Rudy Markham

     124                                         124         110         90   

Nancy Rothwell

     107                                         107         107         96   

Shriti Vadera

     95                                         95         95           

John Varley

     130                                         130         110         99   

Marcus Wallenberg

     85                                         85         85         71   

Former Directors

                                                                       

Louis Schweitzer

     208 5                                        208         500         456   

David Brennan

     499 6                        11         1,653 7        2,163         3,370         3,044   

Michele Hooper

     48 8                                        48         145         120   

Others

                                                     35         149   

Total

     2,952         912         457         17         2,970           7,308           6,535         5,880   

Directors’ remuneration – US dollars

 

Name

   Salary
and fees
$000 		     Bonus
cash
$000 		     Bonus
Shares 1
$000 		     Taxable
benefits
$000 		     Other
payments
and
allowances
$000 		     Total
2012
$000 		     Total
2011
$000 		     Total
2010
$000 		 

Leif Johansson

     504 2                                        504                   

Pascal Soriot

     436         353         177                 1,611 3        2,577                   

Simon Lowth

     1,172         1,091         546         10         475 4        3,294         2,857         2,537   

Geneviève Berger

     92                                         92                   

Bruce Burlington

     166                                         166         157         51   

Graham Chipchase

     103                                         103                   

Jean-Philippe Courtois

     150                                         150         152         124   

Rudy Markham

     196                                         196         176         139   

Nancy Rothwell

     169                                         169         171         148   

Shriti Vadera

     150                                         150         152           

John Varley

     206                                         206         176         153   

Marcus Wallenberg

     135                                         135         136         110   

Former Directors

                                                                       

Louis Schweitzer

     329 5                                        329         800         705   

David Brennan

     790 6                        17         2,618 7        3,425         5,393         4,705   

Michele Hooper

     76 8                                        76         232         185   

Others

                                                     56         231   

Total

     4,674         1,444         723         27         4,704         11,572         10,458         9,088   

 

1   These figures represent that portion of the 2012 bonuses required to be deferred into shares to be held for a three year period under the Deferred Bonus Plan.
2   Includes office costs of £19,000 ($30,000).
3   Relates to remaining cash following selection of benefits within AstraZeneca’s UK flexible benefits programme and cash of £991,000 ($1,571,000) paid to compensate Mr Soriot in respect of forfeited bonus opportunity for 2012 from his previous employer.
4   Relates to remaining cash following selection of benefits within AstraZeneca’s UK flexible benefits programme and cash of £203,000 ($322,000) on the vesting of a PSP Share Award and £47,000 ($74,000) on the release of shares under the Deferred Bonus Plan, in each case paid in respect of dividends accrued.
5   Part year only as ceased to be a Director on 1 June.
6   This figure includes a sum of £224,000 ($355,000) in respect of member contributions to the 401(k) plan and to the AstraZeneca Executive Deferred Compensation Plan which was paid into the plans by means of a salary sacrifice (see the section relating to David Brennan on page 131 for further details). Part year only as employment ceased on 30 June.
7   Relates to £914,000 ($1,447,000) payment in lieu of notice, other allowances for professional fees, a car allowance and cash of £498,000 ($789,000) on the vesting of a PSP Share Award and £86,000 ($136,000) on the release of shares under the Deferred Bonus Plan, in each case paid in respect of dividends accrued.
8   Part year only as ceased to be a Director on 26 April 2012.

In the tables on this page and on the previous page, salaries have been converted between pounds sterling and US dollars at the average exchange rate for the year in question. These rates were:

 

     GBP/USD  

2012

     0.631   

2011

     0.625   

2010

     0.647   

Details of share options exercised by Directors and the aggregate of gains realised on the exercise of options and of awards under long-term incentive plans in the year are given in the Directors’ interests in shares section on page 134.

No Director has a family relationship with any other Director.

Transactions with Directors

There were no material recorded transactions between the Group and the Directors during 2012 or 2011.

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   133

Table of Contents

Corporate Governance | Directors’ Remuneration Report

 

LOGO

Key: AZ AstraZeneca, AL Abbott Laboratories, BMS Bristol-Myers Squibb, GSK GlaxoSmithKline, J&J Johnson & Johnson, LLY Eli Lilly, MRK Merck, NOV Novartis, PFI Pfizer, RCH Hoffmann-La Roche Ltd, SA Sanofi-Aventis

Total shareholder return

The Regulations require the inclusion of a graph showing TSR over a five year period in respect of a holding of the Company’s shares, plotted against TSR in respect of a hypothetical holding of shares of a similar kind and number by reference to which a broad equity market index is calculated. The Company is a member of the FTSE 100 Index and consequently, for the purposes of this graph, which is set out above, we have selected the FTSE 100 Index as the appropriate index. This graph is re-based to 100 at the start of the rolling five year period. We have also included a ‘Pharmaceutical peers (average)’, which reflects the TSR of the same comparator group used for the PSP graphs above.

The PSP requires that the TSR in respect of a holding of the Company’s shares over the relevant performance period be compared with the TSR of a peer group of pharmaceutical companies (as described on page 129). The graphs above show how the Company’s TSR performance has compared with the TSR for the relevant companies in the comparator group from the first day in the relevant three year performance period in respect of each PSP award to 31 December 2012 and how the Company ranks against those other companies on this basis.

To alleviate any short-term volatility, the return index is averaged in the TSR calculations for each company over the three months prior to the start of the relevant performance period (as stipulated in the PSP) and, for the purposes of the graphs above, over the last three months of 2012.

Directors’ interests in shares

Beneficial interests

The table opposite shows any change in the interests of the Directors (including the interests of their Connected Persons, as such term is defined in the Financial Services and Markets Act 2000) in Ordinary Shares from 1 January 2012 to 31 December 2012 or on the date of resignation of such Director (if earlier). All such interests were beneficial except as otherwise stated. However, interests in Ordinary Shares or ADSs that are the subject of PSP awards and/or AZIP awards, as well as Ordinary Shares or ADSs that are deferred under the annual bonus plan discussed in this Remuneration Report, are not included in the Directors’ interests in shares table opposite but are shown in the relevant tables from page 135. No Director or senior executive beneficially owns, or has options over, 1% or more of the issued share capital of the Company, nor do they have different voting rights from other shareholders. None of the Directors has a beneficial interest in the shares of any of the Company’s subsidiaries. Between 31 December 2012 and 31 January 2013, there was no change in the interests in Ordinary Shares shown in the table opposite.

 

134   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents
     Beneficial interest in Ordinary
Shares at 1 January 2012 or
(if later) appointment date 		     Change to beneficial
interest 		    Beneficial interest in Ordinary
Shares at 31 December 2012
or (if earlier) resignation date 		 

Leif Johansson 1

     25,509         3,000        28,509   

Pascal Soriot 2

             3,500        3,500   

Simon Lowth

     54,226         2,734        56,960   

Geneviève Berger 1

             900        900   

Bruce Burlington

     553         1,000        1,553   

Graham Chipchase 1

     650         850        1,500   

Jean-Philippe Courtois

     2,635                2,635   

Rudy Markham

     2,452                2,452   

Nancy Rothwell

     1,832         573        2,405   

Shriti Vadera

     3,000                3,000   

John Varley

     1,744         3,700        5,444   

Marcus Wallenberg

     63,646                63,646   

Former Directors

                         

Louis Schweitzer 3

     16,615                16,615   

David Brennan 3

     246,174         60,430        306,604   

Michele Hooper 4

     2,400                2,400   

 

1   Appointed as a Director on 26 April 2012.
2   Appointed as a Director on 1 October.
3   Ceased to be a Director on 1 June.
4   Ceased to be a Director on 26 April 2012.

Unitised stock plans

David Brennan, in common with other participating executives in the US, has interests in the following plans which were awarded to him prior to him becoming CEO: the AstraZeneca Executive Deferral Plan, the AstraZeneca Executive Deferred Compensation Plan and the AstraZeneca Savings and Security Plan. These are unitised stock plans into which the value of certain previous share incentive awards has been deferred and are not incentive awards in their own right. Participants hold units in each plan, which represent a long-term equity interest in the Company. A unit comprises part cash and part ADSs. The overall unit value can be determined daily by taking the market value of the underlying ADSs and adding the cash position. The ADSs held within these units carry both voting and dividend rights. David Brennan is deemed to have a notional beneficial interest in these ADSs, calculated by reference to the fund value and the closing price of ADSs. Therefore, the number of ADSs in which a notional beneficial interest arises can vary daily as a consequence of stock price movements.

 

Unitised stock plan

   ADSs held at
1 January 2012 		     Net ADSs acquired
during 2012 		    

ADSs held

at 1 June 2012 1

 

AstraZeneca Executive Deferral Plan

     40,002         1,885         41,887   

AstraZeneca Savings and Security Plan

     9,022         391         9,413   

 

1   David Brennan ceased to be a Director on 1 June and ceased to be an employee of the Company on 30 June.

Performance Share Plan

The interests of Directors at 31 December 2012 in Ordinary Shares that are the subject of awards under the PSP are shown below:

 

     Number
of shares 		    Award price
(pence) 		     Price on
vesting
date (pence) 		     Grant date 1      Vesting date 1      Performance period 1  

David Brennan

                                                    

2009 Share Award

     133,347        2280                  27.03.09         27.03.12         01.01.09 – 31.12.11   

2010 Share Award

     127,520        2861                  07.05.10         07.05.13         01.01.10 – 31.12.12   

2011 Share Award

     131,075        2853                  28.03.11         28.03.14         01.01.11 – 31.12.13   

Total at 1 January 2012

     391,942                                               

Partial vesting of 2009 Share Award 2

     (104,010 ) 3,5                2854                              

Partial lapse of 2009 Share Award 2

     (29,337                                            

2012 Share Award

     133,318        2805                  30.03.12         30.03.15         01.01.12 – 31.12.14   

Total at 1 June 2012 6

     391,913 7                                              

Simon Lowth

                                                    

2009 Share Award

     54,276        2280                  27.03.09         27.03.12         01.01.09 – 31.12.11   

2010 Share Award

     52,009        2861                  07.05.10         07.05.13         01.01.10 – 31.12.12   

2011 Share Award

     53,459        2853                  28.03.11         28.03.14         01.01.11 – 31.12.13   

Total at 1 January 2012

     159,744                                               

Partial vesting of 2009 Share Award 2

     (42,335 ) 4,5                2854                              

Partial lapse of 2009 Share Award 2

     (11,941                                            

2012 Share Award

     70,588        2805                  30.03.12         30.03.15         01.01.12 – 31.12.14   

Total at 31 December 2012

     176,056                                               

 

1   UK date convention applies.
2   Share Awards granted in 2009 vested in 2012 at 78% based on the performance conditions and targets (which are set out in the Performance measures under the PSP section from page 129).
3   Following certain mandatory tax deductions, David Brennan became beneficially interested in a net number of 49,571 Ordinary Shares.
4   Following certain mandatory tax deductions, Simon Lowth became beneficially interested in a net number of 20,320 Ordinary Shares.
5   Cash payments equivalent to dividends accruing over the vesting period are made at the date of vesting and are included in ‘Other payments and allowances’ in the Directors’ remuneration tables on page 133.
6   David Brennan ceased to be a Director on 1 June and ceased to be an employee of the Company on 30 June.
7   The Remuneration Committee determined that the Share Awards made to David Brennan in 2011 and 2012 under the PSP should be forfeited on his ceasing to be employed by the Company. The Share Award made in 2010 will vest on a pro rata basis to reflect the period worked since the award of the shares, but only if and to the extent that the relevant performance conditions are met.

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   135

Table of Contents

Corporate Governance | Directors’ Remuneration Report

AstraZeneca Investment Plan

The interests of Directors at 31 December 2012 in Ordinary Shares that are the subject of awards under the AZIP are shown below:

 

     Number of
shares 		    Award price
(pence) 		     Grant date 1      Vesting date 1      Performance period 1  

David Brennan

                                           

2010 Share Award

     21,253        2861         07.05.10         01.01.18         01.01.10 – 31.12.13   

2011 Share Award

     21,845        2853         28.03.11         01.01.19         01.01.11 – 31.12.14   

Total at 1 January 2012

     43,098                                      

2012 Share Award

     22,219        2805         30.03.12         01.01.20         01.01.12 – 31.12.15   

Total at 1 June 2012 2

     65,317 3                                     

Simon Lowth

                                           

2010 Share Award

     8,668        2861         07.05.10         01.01.18         01.01.10 – 31.12.13   

2011 Share Award

     8,909        2853         28.03.11         01.01.19         01.01.11 – 31.12.14   

Total at 1 January 2012

     17,577                                      

2012 Share Award

     11,764        2805         30.03.12         01.01.20         01.01.12 – 31.12.15   

Total at 31 December 2012

     29,341                                      

Pascal Soriot

                                           

Total at 1 October 2012 4

                                          

2012 Share Award

     69,108        2894         26.10.12         01.01.20         01.01.12 – 31.12.15   

Total at 31 December 2012

     69,108                                      

 

1   UK date convention applies.
2   David Brennan ceased to be a Director on 1 June and ceased to be an employee of the Company on 30 June.
3   The Remuneration Committee determined that the Share Awards made to David Brennan in 2011 and 2012 under the AZIP should be forfeited on his ceasing to be employed by the Company. The Share Award made in 2010 will vest on a pro rata basis to reflect the period worked since the award of the shares, but only if and to the extent that the relevant performance conditions are met.
4   Pascal Soriot was appointed as a Director on 1 October.

Deferred Bonus Plan

As described on page 129, there is a requirement for Executive Directors and SET members to defer a certain proportion of any short-term bonus payments into Ordinary Shares or ADSs. The interests of Directors at 31 December 2012 in Ordinary Shares or ADSs that are the subject of awards under these arrangements are shown below:

 

     Number of
shares 		    Award price
(pence) 		     Price on
vesting
date
(pence) 		     Grant date 1      Vesting date 1  

David Brennan

                                           

2009 Award

     17,992        2400                  25.02.09         25.02.12   

2010 Award

     20,718        2817.5                  25.02.10         25.02.13   

2011 Award

     17,725        2977                  25.02.11         25.02.14   

Total at 1 January 2012

     56,435                                      

Vesting of 2009 Award

     (17,992 ) 2,4                2856                     

2012 Award

     15,498        2851                  24.02.12         24.02.15   

Total at 1 June 2012 5

     53,941 6                                     

Simon Lowth

                                           

2009 Award

     9,775        2400                  25.02.09         25.02.12   

2010 Award

     9,760        2817.5                  25.02.10         25.02.13   

2011 Award

     10,281        2977                  25.02.11         25.02.14   

Total at 1 January 2012

     29,816                                      

Vesting of 2009 Award

     (9,775 ) 3,4                2856                     

2012 Award

     9,001        2851                  24.02.12         24.02.15   

Total at 31 December 2012

     29,042                                      

 

1   UK date convention applies.
2   Following certain mandatory tax deductions, David Brennan became beneficially interested in a net number of 8,583 Ordinary Shares.
3   Following certain mandatory tax deductions, Simon Lowth became beneficially interested in a net number of 4,692 Ordinary Shares.
4   Cash payments equivalent to dividends accruing over the vesting period are made at the date of vesting and are included in ‘Other payments and allowances’ in the Directors’ remuneration tables on page 133.
5   David Brennan ceased to be a Director on 1 June and ceased to be an employee of the Company on 30 June.
6   The Remuneration Committee determined that the Share Awards made to David Brennan under the AstraZeneca Deferred Bonus Plan will vest in accordance with the normal vesting timetable at the end of the relevant three year retention periods.

Restricted share award

On 26 October, Pascal Soriot was granted an award of 69,108 restricted shares at an award price of 2894 pence per share. His employment with the Company commenced on 1 October and the restricted shares will vest, subject to his continued employment with the Company, as follows:

 

>  40% will vest on 1 October 2013
>  30% will vest on 1 October 2014
>  30% will vest on 1 October 2015.

 

136   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

Share option plans

The interests of Directors who served during 2012, in options to subscribe for Ordinary Shares, granted under the SOP are included in the following table. None of the Directors in the table below holds options under the AstraZeneca Savings-Related Share Option Plan. There were no grants of options made to Directors under any of the plans in 2012.

 

          Number of
Ordinary
Shares under
option 1 		    Exercise
price per
Ordinary
Share 2 		     First day
exercisable 3,4 		     Last day
exercisable 3,4 		 

David Brennan

   At 1 January 2012 – options over Ordinary Shares      592,975        2375p         24.03.09         26.03.19   
     – market price above option price (Ordinary Shares)      505,244        2271p         19.05.09         26.03.19   
     – market price at or below option price (Ordinary Shares)      87,731        2975p         24.03.09         23.03.16   
     At 1 June 2012 5 – options over Ordinary Shares      592,975 6       2375p         24.03.09         26.03.19   
     – market price above option price (Ordinary Shares)      353,872        2062p         28.03.11         26.03.19   
     – market price at or below option price (Ordinary Shares)      239,103        2839p         24.03.09         29.03.17   
     At 1 January 2012 – options over ADSs      253,223      $ 44.76         28.03.05         23.03.15   
     – market price above option price (ADSs)      110,987      $ 40.35         24.03.08         23.03.15   
     – market price at or below option price (ADSs)      142,236      $ 48.21         28.03.05         25.03.14   
     Lapsed 27 March 2012      (75,695   $ 49.59         28.03.05         27.03.12   
     At 1 June 2012 5 – options over ADSs      177,528 6     $ 42.70         26.03.07         23.03.15   
     – market price above option price (ADSs)             n/a         n/a         n/a   
     – market price at or below option price (ADSs)      177,528      $ 42.70         26.03.07         23.03.15   

Simon Lowth

   At 1 January 2012      65,131        2280p         27.03.12         26.03.19   
     – market price above option price      65,131        2280p         27.03.12         26.03.19   
     – market price at or below option price             n/a         n/a         n/a   
     At 31 December 2012      65,131        2280p         27.03.12         26.03.19   
     – market price above option price      65,131        2280p         27.03.12         26.03.19   
     – market price at or below option price             n/a         n/a         n/a   

 

1   Vesting is subject to satisfying the relevant performance conditions set out in each of the relevant share option plans. Further information on the performance conditions applicable to the SOP is set out in the AstraZeneca Share Option Plan section on page 132.
2   Exercise prices are weighted averages.
3   First and last exercise dates of groups of options, within which period there may be shorter exercise periods.
4   UK date convention applies.
5   David Brennan ceased to be a Director on 1 June and ceased to be an employee of the Company on 30 June.
6   The Remuneration Committee determined that all unexercised options held by David Brennan should be exercised within two years of his ceasing to be employed by the Company with the exception of the option granted in 2009 which should be exercised before his cessation of employment.

Gains by Directors on exercise of share options

The aggregate gains made by Directors on the exercise of share options during the year and the two previous years are set out below:

 

Year

   Gains made by Directors on
the exercise of share options
$ 		    

Gains made by the
highest paid Director

$

 

2012

               

2011

     882,089         112,254   

2010

     260,182         11,454   

 

During 2012, the market price of Ordinary Shares or ADSs was as follows:

 

  

Stock Exchange

   Ordinary Share/ADS market
price at 31 December 2012 		     Range of the Ordinary Share/
ADS market price during 2012 		 

London

     2909.5p         2591p to 3111.5p   

Stockholm

     306.4 SEK         286.2 SEK to 329.5 SEK   

New York

     $47.27         $40.03 to $48.90   

On behalf of the Board

A C N Kemp

Company Secretary

31 January 2013

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   137

Table of Contents

Financial Statements | The value of innovation

 

 

Innovation means

 

LOGO

 

138   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

AstraZeneca’s total contribution to the Russian economy will see over $1.2 billion invested in the five years from 2011, supporting our goal to provide Russian patients access to our portfolio of life-saving prescription medicines.

 

 

LOGO

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   139

Table of Contents

Financial Statements

Preparation of the Financial Statements and Directors’ Responsibilities

 

The Directors are responsible for preparing the Annual Report and Form 20-F Information and the Group and Parent Company Financial Statements in accordance with applicable law and regulations.

Company law requires the Directors to prepare Group and Parent Company Financial Statements for each financial year. Under that law they are required to prepare the Group Financial Statements in accordance with IFRSs as adopted by the EU and applicable law and have elected to prepare the Parent Company Financial Statements in accordance with UK Accounting Standards and applicable law (UK Generally Accepted Accounting Practice).

Under company law, the Directors must not approve the financial statements unless they are satisfied that they give a true and fair view of the state of affairs of the Group and Parent Company and of their profit or loss for that period. In preparing each of the Group and Parent Company Financial Statements, the Directors are required to:

 

> select suitable accounting policies and then apply them consistently
> make judgements and estimates that are reasonable and prudent
> for the Group Financial Statements, state whether they have been prepared in accordance with IFRSs as adopted by the EU
> for the Parent Company Financial Statements, state whether applicable UK Accounting Standards have been followed, subject to any material departures disclosed and explained in the Parent Company Financial Statements
> prepare the financial statements on the going concern basis unless it is inappropriate to presume that the Group and the Parent Company will continue in business.

The Directors are responsible for keeping adequate accounting records that are sufficient to show and explain the Parent Company’s transactions and disclose with reasonable accuracy at any time the financial position of the Parent Company and enable them to ensure that its financial statements comply with the Companies Act 2006. They have general responsibility for taking such steps as are reasonably open to them to safeguard the assets of the Group and to prevent and detect fraud and other irregularities.

Under applicable law and regulations, the Directors are also responsible for preparing a Directors’ Report, Directors’ Remuneration Report and Corporate Governance Statement that complies with that law and those regulations.

The Directors are responsible for the maintenance and integrity of the corporate and financial information included on the Company’s website. Legislation in the UK governing the preparation and dissemination of financial statements may differ from legislation in other jurisdictions.

Directors’ responsibility statement pursuant to DTR 4

The Directors confirm that to the best of our knowledge:

 

> The Financial Statements, prepared in accordance with the applicable set of accounting standards, give a true and fair view of the assets, liabilities, financial position and profit or loss of the Company and the undertakings included in the consolidation taken as a whole.
> The Directors’ Report includes a fair review of the development and performance of the business and the position of the issuer and the undertakings included in the consolidation taken as a whole, together with a description of the principal risks and uncertainties that they face.

On behalf of the Board of Directors on 31 January 2013

Pascal Soriot

Director

 

 

Directors’ Responsibilities for, and Report on,

Internal Control over Financial Reporting

 

The Directors are responsible for establishing and maintaining adequate internal control over financial reporting. AstraZeneca’s internal control over financial reporting is designed to provide reasonable assurance over the reliability of financial reporting and the preparation of consolidated financial statements in accordance with generally accepted accounting principles.

Due to its inherent limitations, internal control over financial reporting may not prevent or detect misstatements. Projections of any evaluation of effectiveness to future periods are subject to the risks that controls may become inadequate because of changes in conditions or that the degree of compliance with the policies or procedures may deteriorate.

 

The Directors assessed the effectiveness of AstraZeneca’s internal control over financial reporting as at 31 December 2012 based on the criteria set forth by the Committee of Sponsoring Organizations of the Treadway Commission in Internal Control-Integrated Framework. Based on this assessment, the Directors believe that, as at 31 December 2012, the internal control over financial reporting is effective based on those criteria.

KPMG Audit Plc, an independent registered public accounting firm, has audited the effectiveness of internal control over financial reporting as at 31 December 2012 and, as explained on page 141, has issued an unqualified report thereon.

 

 

140   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

Auditor’s Reports on the Financial Statements and on Internal Control over Financial Reporting (Sarbanes-Oxley Act Section 404)

 

The report set out below is provided in compliance with International Standards on Auditing (UK and Ireland). KPMG Audit Plc has also issued reports in accordance with standards of the Public Company Accounting Oversight Board in the US, which will be included in the Annual Report on Form 20-F to be filed with the US Securities and Exchange Commission. Those reports are unqualified and include opinions on the Group Financial Statements and on the effectiveness of internal control over financial reporting as at 31 December 2012

 

(Sarbanes-Oxley Act Section 404). The Directors’ statement on internal control over financial reporting is set out on page 140.

KPMG Audit Plc has also reported separately on the Company Financial Statements of AstraZeneca PLC and on the information in the Directors’ Remuneration Report that is described as having been audited. This audit report is set out on page 192.

 

 

Independent Auditor’s Report to the Members of AstraZeneca PLC

 

We have audited the Group Financial Statements of AstraZeneca PLC for the year ended 31 December 2012 set out on pages 142 to 191. The financial reporting framework that has been applied in their preparation is applicable law and International Financial Reporting Standards (IFRSs) as adopted by the EU.

This report is made solely to the Company’s members, as a body, in accordance with Chapter 3 of Part 16 of the Companies Act 2006 and, in respect of the separate opinion in relation to IFRSs as issued by the International Accounting Standards Board (IASB), on terms that have been agreed with the Company. Our audit work has been undertaken so that we might state to the Company’s members those matters we are required to state to them in an auditor’s report and, in respect of the separate opinion in relation to IFRSs as issued by the IASB, those matters that we have agreed to state to them in our report, and for no other purpose. To the fullest extent permitted by law, we do not accept or assume responsibility to anyone other than the Company and the Company’s members, as a body, for our audit work, for this report, or for the opinions we have formed.

Respective responsibilities of Directors and auditor

As explained more fully in the Preparation of the Financial Statements and Directors’ Responsibilities Statement set out on page 140, the Directors are responsible for the preparation of the Group Financial Statements and for being satisfied that they give a true and fair view. Our responsibility is to audit, and express an opinion on, the Group Financial Statements in accordance with applicable law and International Standards on Auditing (UK and Ireland). Those standards require us to comply with the Auditing Practices Board’s Ethical Standards for Auditors.

Scope of the audit of the financial statements

A description of the scope of an audit of financial statements is provided on the Financial Reporting Council’s website at frc.org.uk/auditscopeukprivate.

Opinion on Financial Statements

In our opinion the Group Financial Statements:

 

> give a true and fair view of the state of the Group’s affairs as at 31 December 2012 and of its profit for the year then ended;
> have been properly prepared in accordance with IFRSs as adopted by the EU; and
> have been prepared in accordance with the requirements of the Companies Act 2006 and Article 4 of the IAS Regulation.

 

Separate opinion in relation to IFRSs as issued by the IASB

As explained in the Group Accounting Policies section to the Group Financial Statements set out on pages 146 to 149, the Group, in addition to complying with its legal obligation to apply IFRSs as adopted by the EU, has also applied IFRSs as issued by the IASB.

In our opinion, the Group Financial Statements comply with IFRSs as issued by the IASB.

Opinion on other matter prescribed by the Companies Act 2006

In our opinion the information given in the Directors’ Report for the financial year for which the Group Financial Statements are prepared is consistent with the Group Financial Statements.

Matters on which we are required to report by exception

We have nothing to report in respect of the following:

Under the Companies Act 2006 we are required to report to you if, in our opinion:

 

> certain disclosures of Directors’ Remuneration specified by law are not made; or
> we have not received all the information and explanations we require for our audit.

Under the Listing Rules we are required to review:

 

> the Directors’ Statement, set out on page 146, in relation to going concern;
> the part of the Corporate Governance Statement on pages 110 to 121 relating to the Company’s compliance with the nine provisions of the UK Corporate Governance Code specified for our review; and
> certain elements of the report to shareholders by the Board on Directors’ Remuneration.

Other matters

We have reported separately on the Parent Company Financial Statements of AstraZeneca PLC for the year ended 31 December 2012 and on the information in the Directors’ Remuneration Report that is described as having been audited.

Jimmy Daboo

Senior Statutory Auditor

For and on behalf of KPMG Audit Plc, Statutory Auditor

Chartered Accountants

15 Canada Square, London, E14 5GL

31 January 2013

 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   141

Table of Contents

Financial Statements | Consolidated Statement of Comprehensive Income

Consolidated Statement of Comprehensive Income

for the year ended 31 December

 

                                                                                   
     Notes     

            2012

$m

   

            2011

$m

   

            2010

$m

 

Revenue

     1         27,973        33,591        33,269   

Cost of sales

              (5,393     (6,026     (6,389

Gross profit

              22,580        27,565        26,880   

Distribution costs

              (320     (346     (335

Research and development expense

     2         (5,243     (5,523     (5,318

Selling, general and administrative costs

     2         (9,839     (11,161     (10,445

Profit on disposal of subsidiary

     2,22                1,483          

Other operating income and expense

     2         970        777        712   

Operating profit

     2         8,148        12,795        11,494   

Finance income

     3         528        552        516   

Finance expense

     3         (958     (980     (1,033

Profit before tax

              7,718        12,367        10,977   

Taxation

     4         (1,391     (2,351     (2,896

Profit for the period

              6,327        10,016        8,081   

 

Other comprehensive income:

         

Foreign exchange arising on consolidation

              106        (60     26   

Foreign exchange differences on borrowings designated in net investment hedges

              (46     24        101   

Fair value movements on derivatives designated in net investment hedges

              76                 

Amortisation of loss on cash flow hedge

              1        2        1   

Net available for sale gains taken to equity

              72        31        4   

Actuarial loss for the period

     18         (85     (741     (46

Income tax relating to components of other comprehensive income

     4         (46     198        (61

Other comprehensive income for the period, net of tax

              78        (546     25   

Total comprehensive income for the period

              6,405        9,470        8,106   

 

Profit attributable to:

         

Owners of the Parent

              6,297        9,983        8,053   

Non-controlling interests

              30        33        28   

 

Total comprehensive income attributable to:

         

Owners of the Parent

              6,395        9,428        8,058   

Non-controlling interests

              10        42        48   
                                   

Basic earnings per $0.25 Ordinary Share

     5         $4.99        $7.33        $5.60   

Diluted earnings per $0.25 Ordinary Share

     5         $4.98        $7.30        $5.57   

Weighted average number of Ordinary Shares in issue (millions)

     5         1,261        1,361        1,438   

Diluted weighted average number of Ordinary Shares in issue (millions)

     5         1,264        1,367        1,446   
                                   

Dividends declared and paid in the period

     21         3,619        3,752        3,494   

All activities were in respect of continuing operations.

$m means millions of US dollars.

 

142   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

Financial Statements | Consolidated Statement of Financial Position

Consolidated Statement of Financial Position

at 31 December

 

     Notes     

2012

$m

   

2011

$m

   

2010

$m

 

 

Assets

         

 

Non-current assets

         

Property, plant and equipment

     7         6,089        6,425        6,957   

Goodwill

     8         9,898        9,862        9,871   

Intangible assets

     9         16,448        10,980        12,158   

Derivative financial instruments

     15         389        342        324   

Other investments

     10         199        201        211   

Other receivables

     12         352                 

Deferred tax assets

     4         1,111        1,514        1,475   
                34,486        29,324        30,996   

 

Current assets

         

Inventories

     11         2,061        1,852        1,682   

Trade and other receivables

     12         7,629        8,754        7,847   

Other investments

     10         823        4,248        1,482   

Derivative financial instruments

     15         31        25        9   

Income tax receivable

              803        1,056        3,043   

Cash and cash equivalents

     13         7,701        7,571        11,068   
                19,048        23,506        25,131   

Total assets

              53,534        52,830        56,127   

 

Liabilities

         

Current liabilities

         

Interest-bearing loans and borrowings

     14         (901     (1,990     (125

Trade and other payables

     16         (9,221     (8,975     (8,661

Derivative financial instruments

     15         (3     (9     (8

Provisions

     17         (916     (1,388     (1,095

Income tax payable

              (2,862     (3,390     (6,898
                (13,903     (15,752     (16,787

Non-current liabilities

         

Interest-bearing loans and borrowings

     14         (9,409     (7,338     (9,097

Deferred tax liabilities

     4         (2,576     (2,735     (3,145

Retirement benefit obligations

     18         (2,265     (2,674     (2,472

Provisions

     17         (428     (474     (843

Other payables

     16         (1,001     (385     (373
                        (15,679             (13,606             (15,930

Total liabilities

              (29,582     (29,358     (32,717

Net assets

              23,952        23,472        23,410   

 

Equity

         

 

Capital and reserves attributable to equity holders of the Company

         

Share capital

     20         312        323        352   

Share premium account

              3,504        3,078        2,672   

Capital redemption reserve

              153        139        107   

Merger reserve

              433        433        433   

Other reserves

     19         1,374        1,379        1,377   

Retained earnings

     19         17,961        17,894        18,272   
                23,737        23,246        23,213   

Non-controlling interests

              215        226        197   

Total equity

              23,952        23,472        23,410   

The Financial Statements from page 142 to 191 were approved by the Board on 31 January 2013 and were signed on its behalf by

 

Pascal Soriot        Simon Lowth   
Director    Director   

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   143

Table of Contents

Financial Statements   | Consolidated Statement of Changes in Equity

Consolidated Statement of Changes in Equity

for the year ended 31 December

 

     Share
capital
$m 		    Share
premium
account
$m 		    

Capital
redemption
reserve

$m

     Merger
reserve
$m 		     Other
reserves
$m 		    Retained
earnings
$m 		    Total
attributable
to owners
$m 		    Non-
controlling
interests
$m 		    Total
equity
$m 		 

At 1 January 2010

     363        2,180         94         433         1,392        16,198        20,660        161        20,821   

Profit for the period

                                           8,053        8,053        28        8,081   

Other comprehensive income

                                           5        5        20        25   

Transfer to other reserves 1

                                    (15     15                        

 

Transactions with owners

                     

Dividends

                                           (3,494     (3,494            (3,494

Issue of Ordinary Shares

     2        492                                       494               494   

Repurchase of Ordinary Shares

     (13             13                        (2,604     (2,604            (2,604

Share-based payments

                                           99        99               99   

Transfer from non-controlling interests to payables

                                                         (11     (11

Dividend paid by subsidiary to non-controlling interests

                                                         (1     (1

Net movement

     (11     492         13                 (15     2,074        2,553        36        2,589   

At 31 December 2010

     352        2,672         107         433         1,377        18,272        23,213        197        23,410   

Profit for the period

                                           9,983        9,983        33        10,016   

Other comprehensive income

                                           (555     (555     9        (546

Transfer to other reserves 1

                                    2        (2                     

 

Transactions with owners

                     

Dividends

                                           (3,752     (3,752            (3,752

Issue of Ordinary Shares

     3        406                                       409               409   

Repurchase of Ordinary Shares

     (32             32                        (6,015     (6,015            (6,015

Share-based payments

                                           (37     (37            (37

Transfer from non-controlling interests to payables

                                                         (9     (9

Dividend paid by subsidiary to non-controlling interests

                                                         (4     (4

Net movement

     (29     406         32                 2        (378     33        29        62   

At 31 December 2011

     323        3,078         139         433         1,379        17,894        23,246        226        23,472   

Profit for the period

                                           6,297        6,297        30        6,327   

Other comprehensive income

                                           98        98        (20     78   

Transfer to other reserves 1

                                    (5     5                        

 

Transactions with owners

                     

Dividends

                                           (3,619     (3,619            (3,619

Issue of Ordinary Shares

     3        426                                       429               429   

Repurchase of Ordinary Shares

     (14             14                        (2,635     (2,635            (2,635

Share-based payments

                                           (79     (79            (79

Transfer from non-controlling interests to payables

                                                         (10     (10

Dividend paid by subsidiary to non-controlling interests

                                                         (11     (11

Net movement

     (11     426         14                 (5     67        491        (11     480   

At 31 December 2012

     312        3,504         153         433         1,374        17,961        23,737        215        23,952   

 

1   Amounts charged or credited to other reserves relate to exchange adjustments arising on goodwill.

 

144   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

Financial Statements   | Consolidated Statement of Cash Flows

Consolidated Statement of Cash Flows

for the year ended 31 December

 

     Notes     

            2012

$m

   

            2011

$m

   

            2010

$m

 

 

Cash flows from operating activities

         

Profit before tax

              7,718        12,367        10,977   

Finance income and expense

     3         430        428        517   

Depreciation, amortisation and impairment

              2,518        2,550        2,741   

Decrease/(increase) in trade and other receivables

              755        (1,108     10   

(Increase)/decrease in inventories

              (150     (256     88   

(Decrease)/increase in trade and other payables and provisions

              (1,311     467        (16

Profit on disposal of subsidiary

     22                (1,483       

Non-cash and other movements

              (424     (597     (463

Cash generated from operations

              9,536        12,368        13,854   

Interest paid

              (545     (548     (641

Tax paid

              (2,043     (3,999     (2,533

Net cash inflow from operating activities

              6,948        7,821        10,680   

 

Cash flows from investing activities

         

Acquisitions of business operations

     22         (1,187            (348

Movement in short-term investments and fixed deposits

              3,619        (2,743     (125

Purchase of property, plant and equipment

              (672     (839     (791

Disposal of property, plant and equipment

              199        102        83   

Purchase of intangible assets

              (3,947     (458     (1,390

Disposal of intangible assets

                            210   

Purchase of non-current asset investments

              (46     (11     (34

Disposal of non-current asset investments

              43               5   

Net cash received on disposal of subsidiary

     22                1,772          

Dividends received

              7                 

Interest received

              145        171        174   

Payments made by subsidiaries to non-controlling interests

              (20     (16     (10

Net cash outflow from investing activities

              (1,859     (2,022     (2,226

Net cash inflow before financing activities

              5,089        5,799        8,454   

 

Cash flows from financing activities

         

Proceeds from issue of share capital

              429        409        494   

Repurchase of shares

              (2,635     (6,015     (2,604

Repayment of obligations under finance leases

              (17              

Issue of loans

              1,980                 

Repayment of loans

              (1,750            (1,741

Dividends paid

              (3,665     (3,764     (3,361

Hedge contracts relating to dividend payments

              48        3        (114

Movement in short-term borrowings

              687        46        (8

Net cash outflow from financing activities

              (4,923     (9,321     (7,334

Net increase/(decrease) in cash and cash equivalents in the period

              166        (3,522     1,120   

Cash and cash equivalents at the beginning of the period

              7,434        10,981        9,828   

Exchange rate effects

              (4     (25     33   

Cash and cash equivalents at the end of the period

     13         7,596        7,434        10,981   

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   145

Table of Contents

Financial Statements   | Group Accounting Policies

Group Accounting Policies

 

Basis of accounting and preparation of financial information

The Consolidated Financial Statements have been prepared under the historical cost convention, modified to include revaluation to fair value of certain financial instruments as described below, in accordance with the Companies Act 2006 and International Financial Reporting Standards (IFRSs) as adopted by the EU (adopted IFRSs) in response to the IAS regulation (EC 1606/2002). The Consolidated Financial Statements also comply fully with IFRSs as issued by the International Accounting Standards Board.

During the year the Group adopted the amendments to IFRS 7 ‘Disclosures – Transfers of Financial Assets’ and IAS 12 ‘Deferred Tax: Recovery of Underlying Assets’. The adoption of the amendments did not have a significant effect on the Group’s profit for the period, net assets or cash flows.

The Company has elected to prepare the Company Financial Statements in accordance with UK Accounting Standards. These are presented on pages 193 to 197 and the accounting policies in respect of Company information are set out on page 194.

The Consolidated Financial Statements are presented in US dollars, which is the Company’s functional currency.

In preparing their individual financial statements, the accounting policies of some overseas subsidiaries do not conform with adopted IFRSs. Therefore, where appropriate, adjustments are made in order to present the Consolidated Financial Statements on a consistent basis.

Basis for preparation of financial statements on a going concern basis

Information on the business environment AstraZeneca operates in, including the factors underpinning the industry’s future growth prospects, is included in the Directors’ Report. Details of the product portfolio of the Group (including patent expiry dates for key marketed products), our approach to product development and our development pipeline are covered in detail with additional information by Therapy Area in the Directors’ Report.

The financial position of the Group, its cash flows, liquidity position and borrowing facilities are described in the Financial Review from page 86. In addition, Note 23 to the Financial Statements includes the Group’s objectives, policies and processes for managing its capital, its financial risk management objectives, details of its financial instruments and hedging activities and its exposures to credit, market and liquidity risk. Further details of the Group’s cash balances and borrowings are included in Notes 13 and 14 of the Financial Statements.

The Group has considerable financial resources available. As at 31 December 2012, the Group has $9.8bn in financial resources (cash balances of $7.7bn and undrawn committed bank facilities of $3.0bn which are available until April 2017, with only $0.9bn of debt due within one year). The Group’s revenues are largely derived from sales of products which are covered by patents which provide a relatively high level of resilience and predictability to cash inflows, although our revenue is expected to continue to be significantly impacted by the expiry of patents over the medium term. In addition, recent government price interventions in response to budgetary constraints are expected to continue to adversely affect revenues in many of our mature markets. However, we anticipate new revenue streams from both recently launched medicines and products in development, and the Group has a wide diversity of customers and suppliers across different geographic areas. Consequently, the Directors believe that, overall, the Group is well placed to manage its business risks successfully despite the current uncertain economic outlook.

 

After making enquiries, the Directors have a reasonable expectation that the Company and the Group have adequate resources to continue in operational existence for the foreseeable future. Accordingly, they continue to adopt the going concern basis in preparing the Annual Report and Financial Statements.

Estimates and judgements

The preparation of the financial statements in conformity with generally accepted accounting principles requires management to make estimates and judgements that affect the reported amounts of assets and liabilities at the date of the financial statements and the reported amounts of revenues and expenses during the reporting period. Actual results could differ from those estimates.

Judgements include classification of transactions between profit and the consolidated statement of financial position and the determination of operating segments while estimates focus on areas such as carrying values and estimated lives.

AstraZeneca’s management considers the following to be the most important accounting policies in the context of the Group’s operations.

The accounting policy descriptions set out the areas where judgements and estimates need exercising, the most significant of which are revenue recognition, research and development (including impairment reviews of associated intangible assets), business combinations and goodwill, litigation and environmental liabilities, employee benefits and taxation.

Further information on estimates and critical judgements made in applying accounting policies, including details of significant methods and assumptions used, is included in Notes 4, 6, 8, 9, 18, 22 and 25 in the Financial Statements. Financial risk management policies are detailed in Note 23.

Revenue

Revenues comprise sales and income under co-promotion and co-development agreements.

Income under co-promotion and co-development agreements is recognised when it is earned as defined in the contract and can be reliably estimated. In general, this is upon the sale of the co-promoted/ developed product or upon the delivery of a promotional or developmental service.

Revenues exclude inter-company revenues and value-added taxes and represent net invoice value less estimated rebates, returns and settlement discounts. Revenues are recognised when the significant risks and rewards of ownership have been transferred to a third party. In general, this is upon delivery of the products to wholesalers. In markets where returns are significant (currently only in the US), estimates of returns are accounted for at the point revenue is recognised. In markets where returns are not significant, they are recorded when returned.

For the US market, we estimate the quantity and value of goods which may ultimately be returned at the point of sale. Our returns accruals are based on actual experience over the preceding 12 months for established products together with market-related information such as estimated stock levels at wholesalers and competitor activity which we receive via third party information services. For newly launched products, we use rates based on our experience with similar products or a pre-determined percentage.

When a product faces generic competition particular attention is given to the possible levels of returns and, in cases where the circumstances are such that the level of returns (and, hence, revenue) cannot be measured reliably, revenues are only recognised when the right of return expires, which is generally on ultimate prescription of the product to patients.

 

 

146   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

Research and development

Research expenditure is recognised in profit in the year in which it is incurred.

Internal development expenditure is capitalised only if it meets the recognition criteria of IAS 38 ‘Intangible Assets’. Where regulatory and other uncertainties are such that the criteria are not met, the expenditure is recognised in profit and this is almost invariably the case prior to approval of the drug by the relevant regulatory authority. Where, however, recognition criteria are met, intangible assets are capitalised and amortised on a straight-line basis over their useful economic lives from product launch. At 31 December 2012, no amounts have met recognition criteria.

Payments to in-licence products and compounds from third parties for new research and development projects (in-process research and development), generally taking the form of up front payments and milestones, are capitalised. Where payments made to third parties represent future research and development activities, an evaluation is made as to the nature of the payments. Such payments are expensed if they represent compensation for subcontracted research and development services not resulting in a transfer of intellectual property. By contrast, payments are capitalised if they represent compensation for the transfer of intellectual property developed at the risk of the third party. Since acquired products and compounds will only generate sales and cash inflows following launch, our policy is to minimise the period between final approval and launch if it is within AstraZeneca’s control to do so. Assets capitalised are amortised, on a straight-line basis, over their useful economic lives from product launch. Under this policy, it is not possible to determine precise economic lives for individual classes of intangible assets. However, lives range from three years to 20 years.

Intangible assets relating to products in development (both internally generated and externally acquired) are subject to impairment testing annually. All intangible assets are tested for impairment when there are indications that the carrying value may not be recoverable. Any impairment losses are recognised immediately in profit. Intangible assets relating to products which fail during development (or for which development ceases for other reasons) are tested for impairment at the point of termination and are written down to their recoverable amount (which is usually zero).

Business combinations and goodwill

On the acquisition of a business, fair values are attributed to the identifiable assets and liabilities and contingent liabilities unless the fair value cannot be measured reliably, in which case the value is subsumed into goodwill. Where fair values of acquired contingent liabilities cannot be measured reliably, the assumed contingent liability is not recognised but is disclosed in the same manner as other contingent liabilities. Goodwill is the difference between the fair value of the consideration and the fair value of net assets acquired.

Goodwill arising on acquisitions is capitalised and subject to an impairment review, both annually and when there is an indication that the carrying value may not be recoverable. Between 1 January 1998 and 31 December 2002, goodwill was amortised over its estimated useful life; such amortisation ceased on 31 December 2002.

The Group’s policy up to and including 1997 was to eliminate goodwill arising upon acquisitions against reserves. Under IFRS 1 ‘First-time Adoption of International Financial Reporting Standards’ and IFRS 3 ‘Business Combinations’, such goodwill will remain eliminated against reserves.

Jointly controlled operations

The Group has one arrangement over which it has joint control. The form of this arrangement is a jointly controlled operation under IAS 31 ‘Interests in Joint Ventures’. The Group recognises its share of income that it earns from the jointly controlled operation and

 

its share of expenses incurred. The Group also recognises the assets associated with the jointly controlled operation that it controls and the liabilities it incurs under the jointly controlled operation collaboration agreement.

Employee benefits

The Group accounts for pensions and other employee benefits (principally healthcare) under IAS 19 ‘Employee Benefits’. In respect of defined benefit plans, obligations are measured at discounted present value while plan assets are measured at fair value. The operating and financing costs of such plans are recognised separately in profit; current service costs are spread systematically over the lives of employees and financing costs are recognised in full in the periods in which they arise. Actuarial gains and losses are recognised immediately in other comprehensive income.

Where the calculation results in a surplus to the Group, the recognised asset is limited to the present value of any available future refunds from the plan or reductions in future contributions to the plan. Payments to defined contribution plans are recognised in profit as they fall due.

Taxation

The current tax payable is based on taxable profit for the year. Taxable profit differs from reported profit because taxable profit excludes items that are never taxable or tax deductible. The Group’s current tax assets and liabilities are calculated using tax rates that have been enacted or substantively enacted by the reporting date.

Deferred tax is provided using the balance sheet liability method, providing for temporary differences between the carrying amounts of assets and liabilities for financial reporting purposes and the amounts used for taxation purposes. Deferred tax assets are recognised to the extent that it is probable that taxable profit will be available against which the asset can be utilised. This requires judgements to be made in respect of the availability of future taxable income.

No deferred tax asset or liability is recognised in respect of temporary differences associated with investments in subsidiaries, branches and joint ventures where the Group is able to control the timing of reversal of the temporary differences and it is probable that the temporary differences will not reverse in the foreseeable future.

The Group’s deferred tax assets and liabilities are calculated using tax rates that are expected to apply in the period when the liability is settled or the asset realised based on tax rates that have been enacted or substantively enacted by the reporting date.

Accruals for tax contingencies require management to make judgements and estimates of exposures in relation to tax audit issues. Tax benefits are not recognised unless the tax positions will probably be sustained. Once considered to be probable, management reviews each material tax benefit to assess whether a provision should be taken against full recognition of that benefit on the basis of potential settlement through negotiation and/or litigation. All provisions are included in current liabilities. Any liability to interest on tax liabilities is provided for in the tax charge. See Note 25 for further details.

Share-based payments

All plans are assessed and have been classified as equity settled. The grant date fair value of employee share plan awards is calculated using a modified version of the binomial model. In accordance with IFRS 2 ‘Share-based Payment’, the resulting cost is recognised in profit over the vesting period of the awards, being the period in which the services are received. The value of the charge is adjusted to reflect expected and actual levels of awards vesting, except where the failure to vest is as a result of not meeting a market condition. Cancellations of equity instruments are treated as an acceleration of the vesting period and any outstanding charge is recognised in profit immediately.

 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   147

Table of Contents

Financial Statements   | Group Accounting Policies

 

Property, plant and equipment

The Group’s policy is to write off the difference between the cost of each item of property, plant and equipment and its residual value over its estimated useful life on a straight-line basis. Assets under construction are not depreciated.

Reviews are made annually of the estimated remaining lives and residual values of individual productive assets, taking account of commercial and technological obsolescence as well as normal wear and tear. Under this policy it becomes impractical to calculate average asset lives exactly. However, the total lives range from approximately 10 to 50 years for buildings, and three to 13 years for plant and equipment. All items of property, plant and equipment are tested for impairment when there are indications that the carrying value may not be recoverable. Any impairment losses are recognised immediately in profit.

Borrowing costs

The Group has no borrowing costs with respect to the acquisition or construction of qualifying assets. All other borrowing costs are recognised in profit as incurred and in accordance with the effective interest rate method.

Leases

Leases are classified as finance leases if they transfer substantially all the risks and rewards incidental to ownership, otherwise they are classified as operating leases. Assets and liabilities arising on finance leases are initially recognised at fair value or, if lower, the present value of the minimum lease payments. The discount rate used in calculating the present value of the minimum lease payments is the interest rate implicit in the lease. Finance charges under finance leases are allocated to each reporting period so as to produce a constant periodic rate of interest on the remaining balance of the finance liability. Rentals under operating leases are charged to profit on a straight-line basis.

Subsidiaries

A subsidiary is an entity controlled, directly or indirectly, by AstraZeneca PLC. Control is regarded as the power to govern the financial and operating policies of the entity so as to obtain benefits from its activities.

The financial results of subsidiaries are consolidated from the date control is obtained until the date that control ceases.

Inventories

Inventories are stated at the lower of cost and net realisable value. The first in, first out or an average method of valuation is used. For finished goods and work in progress, cost includes directly attributable costs and certain overhead expenses (including depreciation). Selling expenses and certain other overhead expenses (principally central administration costs) are excluded. Net realisable value is determined as estimated selling price less all estimated costs of completion and costs to be incurred in selling and distribution.

Write-downs of inventory occur in the general course of business and are recognised in cost of sales.

Trade and other receivables

Financial assets included in trade and other receivables are recognised initially at fair value. Subsequent to initial recognition they are measured at amortised cost using the effective interest rate method, less any impairment losses.

Trade and other payables

Financial liabilities included in trade and other payables are recognised initially at fair value. Subsequent to initial recognition they are measured at amortised cost using the effective interest rate method.

Financial instruments

The Group’s financial instruments include interests in leases, trade and other receivables and payables and rights and obligations under employee benefit plans which are dealt with in specific accounting policies.

 

The Group’s other financial instruments include:

> cash and cash equivalents

> fixed deposits
> other investments
> bank and other borrowings
> derivatives.

Cash and cash equivalents

Cash and cash equivalents comprise cash in hand, current balances with banks and similar institutions and highly liquid investments with maturities of three months or less when acquired. They are readily convertible into known amounts of cash and are held at amortised cost.

Fixed deposits

Fixed deposits, comprising principally funds held with banks and other financial institutions, are initially measured at fair value, plus direct transaction costs, and are subsequently remeasured to amortised cost using the effective interest rate method at each reporting date. Changes in carrying value are recognised in profit.

Other investments

Where investments have been classified as held for trading, they are measured initially at fair value and subsequently remeasured to fair value at each reporting date. Changes in fair value are recognised in profit.

In all other circumstances, the investments are classified as ‘available for sale’, are initially measured at fair value (including direct transaction costs) and are subsequently remeasured to fair value at each reporting date. Changes in carrying value due to changes in exchange rates on monetary available for sale investments or impairments are recognised in profit. All other changes in fair value are recognised in other comprehensive income.

Impairments are recorded in profit when there is a decline in the value of an investment that is deemed to be other than temporary. On disposal of the investment, the cumulative amount recognised in other comprehensive income is recognised in profit as part of the gain or loss on disposal.

Bank and other borrowings

The Group uses derivatives, principally interest rate swaps, to hedge the interest rate exposure inherent in a portion of its fixed interest rate debt. In such cases the Group will either designate the debt as fair value through profit or loss when certain criteria are met or as the hedged item under a fair value hedge.

If the debt instrument is designated as fair value through profit or loss, the debt is initially measured at fair value (with direct transaction costs being included in profit as an expense) and is remeasured to fair value at each reporting date with changes in carrying value being recognised in profit (along with changes in the fair value of the related derivative). Such a designation has been made where this significantly reduces an accounting mismatch which would result from recognising gains and losses on different bases.

If the debt is designated as the hedged item under a fair value hedge, the debt is initially measured at fair value (with direct transaction costs being amortised over the life of the bonds), and is remeasured for fair value changes in respect of the hedged risk at each reporting date with changes in carrying value being recognised in profit (along with changes in the fair value of the related derivative).

Other interest-bearing loans are initially measured at fair value (with direct transaction costs being amortised over the life of the bond) and are subsequently remeasured to amortised cost using the effective interest rate method at each reporting date. Changes in carrying value are recognised in profit.

Derivatives

Derivatives are initially measured at fair value (with direct transaction costs being included in profit as an expense) and are subsequently

 

 

148   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

remeasured to fair value at each reporting date. Changes in carrying value are recognised in profit.

Foreign currencies

Foreign currency transactions, being transactions denominated in a currency other than an individual Group entity’s functional currency, are translated into the relevant functional currencies of individual Group entities at average rates for the relevant monthly accounting periods, which approximate to actual rates.

Monetary assets, arising from foreign currency transactions, are retranslated at exchange rates prevailing at the reporting date. Exchange gains and losses on loans and on short-term foreign currency borrowings and deposits are included within finance expense. Exchange differences on all other foreign currency transactions are recognised in operating profit in the individual Group entity’s accounting records.

Non-monetary items arising from foreign currency transactions are not retranslated in the individual Group entity’s accounting records.

In the Consolidated Financial Statements, income and expense items for Group entities with a functional currency other than US dollars are translated into US dollars at average exchange rates, which approximate to actual rates, for the relevant accounting periods. Assets and liabilities are translated at the US exchange rates prevailing at the reporting date. Exchange differences arising on consolidation are recognised in other comprehensive income.

If certain criteria are met, non-US dollar denominated loans or derivatives are designated as net investment hedges of foreign operations. Exchange differences arising on retranslation of net investments, and of foreign currency loans which are designated in an effective net investment hedge relationship, are recognised in other comprehensive income in the Consolidated Financial Statements. Foreign exchange derivatives hedging net investments in foreign operations are carried at fair value. Effective fair value movements are recognised in other comprehensive income, with any ineffectiveness taken to the income statement. Gains and losses accumulated in the translation reserve will be recycled to profit when the foreign operation is sold.

Litigation and environmental liabilities

Through the normal course of business, AstraZeneca is involved in legal disputes, the settlement of which may involve cost to the Group. Provision is made where an adverse outcome is probable and associated costs, including related legal costs, can be estimated reliably. In other cases, appropriate disclosures are included.

Where it is considered that the Group is more likely than not to prevail, or in the rare circumstances where the amount of the legall iability cannot be estimated reliably, legal costs involved in defending the claim are charged to profit as they are incurred.

Where it is considered that the Group has a valid contract which provides the right to reimbursement (from insurance or otherwise) of legal costs and/or all or part of any loss incurred or for which a provision has been established, the best estimate of the amount expected to be received is recognised as an asset only when it is virtually certain.

AstraZeneca is exposed to environmental liabilities relating to its past operations, principally in respect of soil and groundwater remediation costs. Provisions for these costs are made when there is a present obligation and where it is probable that expenditure on remedial work will be required and a reliable estimate can be made of the cost. Provisions are discounted where the effect is material.

Impairment

The carrying values of non-financial assets, other than inventories and deferred tax assets, are reviewed at least annually to determine whether there is any indication of impairment. For goodwill, intangible assets under development and for any other assets where such indication exists, the asset’s recoverable amount is estimated based

on the greater of its value in use and its fair value less cost to sell. In assessing value in use, the estimated future cash flows, adjusted for the risks specific to each asset, are discounted to their present value using a discount rate that reflects current market assessments of the time value of money and the general risks affecting the pharmaceutical industry. For the purpose of impairment testing, assets are grouped together into the smallest group of assets that generates cash inflows from continuing use that are largely independent of the cash flows of other assets. Impairment losses are recognised in profit.

International accounting transition

On transition to using adopted IFRSs in the year ended 31 December 2005, the Company took advantage of several optional exemptions available in IFRS 1 ‘First-time Adoption of International Financial Reporting Standards’. The major impacts which are of continuing importance are detailed below:

 

> Business combinations – IFRS 3 ‘Business Combinations’ has been applied from 1 January 2003, the date of transition, rather than being applied fully retrospectively. As a result, the combination of Astra and Zeneca is still accounted for as a merger, rather than through purchase accounting. If purchase accounting had been adopted, Zeneca would have been deemed to have acquired Astra.
> Cumulative exchange differences – the Group chose to set the cumulative exchange difference reserve at 1 January 2003 to zero.

Applicable accounting standards and interpretations issued but not yet adopted

IFRS 9 ‘Financial Instruments’ was reissued in October 2010. It is applicable to financial assets and financial liabilities. For financial assets it requires classification and measurement in either the amortised cost or the fair value category. For a company’s own debt held at fair value, the standard requires the movement in the fair value as a result of changes in the company’s own credit risk to be included in other comprehensive income. It is effective for accounting periods beginning on or after 1 January 2015. The standard has not yet been endorsed by the EU. The adoption of IFRS 9 is not expected to have a significant impact upon the Group’s net results or net assets.

IFRS 10 ‘Consolidated Financial Statements’, IFRS 11 ‘Joint Arrangements’, IFRS 12 ‘Disclosure of Interests in Other Entities’ and IFRS 13 ‘Fair Value Measurement’ were issued in May 2011, along with consequential amendments to IAS 27 ‘Separate Financial Statements’ and IAS 28 ‘Investments in Associates and Joint Ventures’. The new and revised standards were endorsed by the EU in December 2012, with an effective date of 1 January 2014 (except for IFRS 13 which has an effective date of 1 January 2013) but with early adoption permitted. The Group intends to adopt the new and revised standards from 1 January 2013. The adoption is not expected to have a significant impact upon the Group’s net results, net assets or disclosures.

The amendments to IAS 19 ‘Employee Benefits’ are effective for accounting periods beginning on or after 1 January 2013 and were endorsed by the EU in June 2012. The amendments result in a change to the methodology used in calculating the expected return on pension assets, reported as finance income. Finance income will be lower as a result. On adoption, prior period finance income will be restated with decreases of approximately $70m for 2012 and $85m for 2011. The adoption of the IAS 19 amendments is not expected to have a significant impact on the Group’s net assets.

The amendments to IAS 1 ‘Presentation of Items in Other Comprehensive Income’ and amendments to IAS 32 and IFRS 7 on offsetting financial assets and liabilities are effective for accounting periods beginning on or after 1 July 2012, and 1 January 2014 (IAS 32) and 1 January 2013 (IFRS 7) respectively. They are not expected to have a significant impact upon the Group’s net results, net assets or disclosures. These amendments were endorsed by the EU in 2012.

 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   149

Table of Contents

Financial Statements   | Notes to the Group Financial Statements

Notes to the Group Financial Statements

1 Product revenue information

 

    

            2012

$m

    

            2011

$m

    

            2010

$m

 

 

Cardiovascular:

        

Crestor

     6,253         6,622         5,691   

Atacand

     1,009         1,450         1,483   

Seloken/Toprol-XL

     918         986         1,210   

Onglyza

     323         211         69   

Plendil

     252         256         255   

Zestril

     115         144         157   

Brilinta/Brilique

     89         21           

Byetta

     74                   

Bydureon

     37                   

Others

     461         522         538   

Total Cardiovascular

     9,531         10,212         9,403   

 

Gastrointestinal:

        

Nexium

     3,944         4,429         4,969   

Losec/Prilosec

     710         946         986   

Others

     198         161         133   

Total Gastrointestinal

     4,852         5,536         6,088   

 

Respiratory & Inflammation:

        

Symbicort

     3,194         3,148         2,746   

Pulmicort

     866         892         872   

Rhinocort

     177         212         227   

Others

     178         216         254   

Total Respiratory & Inflammation

     4,415         4,468         4,099   

 

Neuroscience:

        

Seroquel

     2,803         5,828         5,302   

Local anaesthetics

     540         602         605   

Diprivan

     291         294         322   

Zomig

     182         413         428   

Vimovo

     65         34         5   

Others

     42         33         42   

Total Neuroscience

     3,923         7,204         6,704   

 

Oncology:

        

Zoladex

     1,093         1,179         1,115   

Faslodex

     654         546         345   

Iressa

     611         554         393   

Arimidex

     543         756         1,512   

Casodex

     454         550         579   

Others

     134         120         101   

Total Oncology

     3,489         3,705         4,045   

 

Infection and Other:

        

Synagis

     1,038         975         1,038   

Merrem

     396         583         817   

FluMist

     181         161         174   

Other Products

     100         137         147   

Total Infection and Other

     1,715         1,856         2,176   

Astra Tech

             386         535   

Aptium Oncology

     48         224         219   

Total

     27,973         33,591         33,269   

 

150   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

2 Operating profit

Operating profit includes the following items:

Research and development expense

In 2012, research and development includes a $50m impairment following the decision by AstraZeneca not to pursue a regulatory filing for TC-5214. In 2011, research and development includes a $285m impairment charge related to the termination of development of the investigational compound olaparib for the maintenance treatment of serous ovarian cancer and $150m impairment charge related to the intangible assets held in relation to TC-5214. In 2010, research and development included a $445m impairment of intangible assets related specifically to motavizumab. Further details of impairment charges for 2012, 2011 and 2010 are included in Notes 7 and 9.

Selling, general and administrative costs

In 2012, selling, general and administrative costs includes net legal provisions of $72m, in respect of net legal provision charges relating to ongoing Seroquel franchise legal matters, Average Wholesale Price litigation in the US, the Toprol-XL antitrust litigation and Nexium commercial litigation. In 2011, selling, general and administrative costs included $135m of net legal provision charges, all of which were in respect of the ongoing Seroquel franchise legal matters, Average Wholesale Price litigation in the US and the Toprol-XL antitrust litigation. In 2010, selling, general and administrative costs included legal provision charges of $617m, of which $592m was in respect of Seroquel franchise legal matters. The current status of these matters is described in Note 25. These provisions constituted our best estimate at that time of losses expected for these matters. Also included within selling, general and administrative costs in 2010 were gains of $791m arising from changes made to benefits under certain of the Group’s post-retirement benefit plans, chiefly the Group’s UK pension plan. Further details of this gain are included in Note 18.

Profit on disposal of subsidiary

The profit on disposal of subsidiary in 2011 of $1,483m relates to the sale of the Astra Tech business to DENTSPLY International Inc. Further details are included in Note 22.

Other operating income and expense

 

                 2012
$ m 		                2011
$m 		                2010
$m 		 

Royalties

      

  Income

     659        610        522   

  Amortisation

     (92     (51     (59

  Impairment

                   (123

Net gain on disposal of property, plant and equipment

     8        33        66   

Gains on disposal of product rights

     255                 

Net loss on disposal of other intangible assets

                   (1

Other income

     140        226        307   

Other expense

            (41       

Other operating income and expense

     970        777        712   

Royalty amortisation and impairment relates to income streams acquired with MedImmune, and, from 2012, amounts relating to our arrangements with Merck.

Restructuring costs

During 2012, the Group announced the third phase of its restructuring programme, as approved by the SET. The tables below show the costs that have been charged in respect of restructuring programmes by cost category and type. Severance provisions are detailed in Note 17.

 

                 2012
$m 		                   2011
$m 		                    2010
$m 		 

Cost of sales

     136         54         144   

Research and development expense

     791         468         654   

Selling, general and administrative costs

     631          639         404   

Total charge

     1,558         1,161         1,202   
        
    

2012

$m

    

2011

$m

    

2010

$m

 

Severance costs

     819         403         505   

Accelerated depreciation and impairment

     328         290         299   

Other

     411          468         398   

Total charge

     1,558         1,161         1,202   

Other costs are those incurred in designing and implementing the Group’s various restructuring initiatives including internal project costs, external consultancy fees and staff relocation costs.

Financial instruments

Included within operating profit are the following net gains and losses on financial instruments.

 

                 2012
$m 		                2011
$m 		                2010
$m 		 

Gains/(losses) on forward foreign exchange contracts

     139        (75     29   

(Losses)/gains on receivables and payables

     (153     68        (80

Gains/(losses) on available for sale current investments

     12        (22     (2
       (2     (29     (53

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   151

Table of Contents

Financial Statements   | Notes to the Group Financial Statements

3 Finance income and expense

 

                                                        
                  2012
$m 		   

            2011

$m

   

            2010

$m

 

 

Finance income

      

Returns on fixed deposits and equity securities

     18        9        9   

Returns on short-term deposits

     24        37        33   

Expected return on post-employment defined benefit plan assets

     486        502        451   

Fair value gains on debt, interest rate swaps and investments

            4        23   

Total

     528        552        516   

 

Finance expense

      

Interest on debt and commercial paper

     (404     (404     (450

Interest on overdrafts, finance leases and other financing costs

     (22     (29     (29

Interest on post-employment defined benefit plan liabilities

     (507     (539     (543

Fair value charges on debt, interest rate swaps and investments

     (10              

Net exchange losses

     (15     (8     (11

Total

     (958     (980     (1,033

Net finance expense

     (430     (428     (517

Financial instruments

Included within finance income and expense are the following net gains and losses on financial instruments.

 

  

  

    

2012

$m

   

2011

$m

   

2010

$m

 

Interest and fair value adjustments in respect of debt designated at fair value through profit or loss, net of derivatives

     (18     (6     (5

Interest and changes in carrying values of debt designated as hedged items, net of derivatives

     (16     (17     (18

Interest and fair value changes on fixed and short-term deposits and equity securities

     37        45        61   

Interest on debt, overdrafts, finance leases and commercial paper held at amortised cost

     (397     (405     (452

Exchange losses on financial assets and liabilities

     (15     (8     (11
       (409     (391     (425

$22m fair value losses (2011: $10m fair value gains; 2010: $29m fair value gains) on interest rate fair value hedging instruments and $21m fair value gains (2011: $9m fair value losses; 2010: $29m fair value losses) on the related hedged items have been included within interest and changes in carrying values of debt designated as hedged items, net of derivatives. All fair value hedge relationships were effective during the year.

$27m fair value losses (2011: $29m fair value gains; 2010: $33m fair value gains) on derivatives related to debt instruments designated at fair value through profit or loss and $18m fair value gains (2011: $26m fair value losses; 2010: $28m fair value losses) on debt instruments designated at fair value through profit or loss have been included within interest and fair value adjustments in respect of debt designated at fair value through profit or loss, net of derivatives. Ineffectiveness on the net investment hedge taken to profit was $nil (2011: $nil; 2010: $nil).

4 Taxation

Taxation recognised in the profit for the period in the consolidated statement of comprehensive income is as follows:

 

                                                        
    

            2012

$m

   

            2011

$m

   

            2010

$m

 

 

Current tax expense

      

Current year

     1,761        2,680        3,065   

Adjustment for prior years

     (79     (102     370   
       1,682        2,578        3,435   

 

Deferred tax expense

      

Origination and reversal of temporary differences

     (155     (141     (369

Adjustment to prior years

     (136     (86     (170
       (291     (227     (539

Taxation recognised in the profit for the period

     1,391        2,351        2,896   

Taxation relating to components of other comprehensive income is as follows:

 

  

    

2012

$m

   

2011

$m

   

2010

$m

 

 

Current and deferred tax

      

Foreign exchange arising on consolidation

     14        12        (29

Actuarial loss for the period

     28        214        (18

Share-based payments

     7        21        9   

Net available for sale gains recognised in other comprehensive income

     (18              

Deferred tax impact of reduction in Sweden and UK tax rates

     (84     (53     (23

Other

     7        4          

Taxation relating to components of other comprehensive income

     (46     198        (61

 

152   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

4 Taxation continued

Taxation has been provided at current rates on the profits earned for the periods covered by the Group Financial Statements. The 2012 prior period current tax adjustment relates to a benefit of $259m arising from a number of tax settlements (including settlement of a transfer pricing matter), partially offset by an increase in provisions for other tax contingencies and tax accrual to tax return adjustments. The 2011 prior period current tax adjustment relates to a benefit of $520m arising from a number of tax settlements, partially offset by an increase in provisions for other tax contingencies and tax accrual to tax return adjustments. The 2010 prior period current tax adjustment relates mainly to an increase in provisions for tax contingencies and double tax relief partially offset by a benefit of $342m arising from a number of tax settlements and tax accrual to tax return adjustments. The 2012 prior period deferred tax adjustment relates to a benefit of $102m arising from a number of tax settlements (including settlement of a transfer pricing matter) and tax accrual to tax return adjustments. The 2011 and 2010 prior period deferred tax adjustments relate mainly to tax accrual to tax return adjustments and a reclassification from deferred tax to current tax of amounts provided in relation to tax contingencies for prior periods.

To the extent that dividends remitted from overseas subsidiaries, joint ventures and associates are expected to result in additional taxes, appropriate amounts have been provided for. No deferred tax has been provided for unremitted earnings of Group companies overseas as these are considered permanently employed in the business of these companies. Unremitted earnings may be liable to overseas taxes and/or UK taxation (after allowing for double tax relief) if distributed as dividends. The aggregate amount of temporary differences associated with investments in subsidiaries and branches for which deferred tax liabilities have not been recognised totalled approximately $8,655m at 31 December 2012 (2011: $9,155m; 2010: $16,768m).

Factors affecting future tax charges

As a group involved in worldwide operations, AstraZeneca is subject to several factors that may affect future tax charges, principally the levels and mix of profitability in different jurisdictions, transfer pricing regulations, tax rates imposed and tax regime reforms. It is the UK government’s intention to enact legislation which will reduce the main rate of UK Statutory Corporation Tax to 21% by 2014. In 2012, the UK government also enacted legislation as part of its programme of corporate tax reforms including the introduction of a patent box regime, under which UK profits arising from certain UK owned patents will be subject to a reduced rate of UK Statutory Corporation Tax effective 1 April 2013. The Swedish government has enacted legislation to reduce the Sweden Statutory Corporation Tax rate from 26.3% to 22% effective 1 January 2013. Details of material tax exposures and items currently under audit and negotiation are set out in Note 25.

Tax reconciliation to UK statutory rate

The table below reconciles the UK statutory tax charge to the Group’s total tax charge.

 

    

            2012

$m

   

            2011

$m

   

            2010

$m

 

Profit before tax

     7,718        12,367        10,977   

Notional taxation charge at UK corporation tax rate of 24.5% (2011: 26.5%; 2010: 28%)

     1,891        3,277        3,074   

Differences in effective overseas tax rates

     (83     (340     (333

Deferred tax credit relating to reduction in Sweden, UK and other tax rates 1

     (271     (53     (21

Unrecognised deferred tax asset

     (18     5          

Items not deductible for tax purposes

     116        71        12   

Items not chargeable for tax purposes

     (29     (32     (36

Non-taxable gain arising from the Astra Tech disposal

            (389       

Adjustments in respect of prior periods

     (215     (188     200   

Total tax charge for the year

     1,391        2,351        2,896   

 

1   The 2012 item relates to the reduction in the Sweden Statutory Corporation Tax rate from 26.3% to 22% effective 1 January 2013 and the UK Statutory Corporation Tax rate from 25% (the tax rate which was substantively enacted as effective from 1 April 2012 as at 31 December 2011) to the tax rate of 23% effective from 1 April 2013. The 2011 item relates to the reduction in the UK Statutory Corporation Tax rate from 27% (the tax rate which was substantively enacted as effective from 1 April 2011 as at 31 December 2010) to the tax rate of 25% effective from 1 April 2012. The 2010 item relates to the reduction in the UK Statutory Corporation Tax rate from 28% to 27% effective from 1 April 2011.

The tax rate of 18% for the year ended 31 December 2012 is lower than the UK Statutory Corporation Tax rate of 24.5% mainly as a result of the $230m adjustment to deferred tax balances following substantive enactment of a reduction in the Sweden Statutory Corporation Tax rate from 26.3% to 22% effective 1 January 2013, the $240m release of a tax provision following the settlement of a transfer pricing matter and the difference in effective overseas tax rates as discussed below. Excluding the effects of the one-off benefits totalling $470m mentioned above, the tax rate is 24.1%.

AstraZeneca is domiciled in the UK but operates in other countries where the tax rates and tax laws are different to those in the UK. The impact of differences in effective overseas tax rates on the Group’s overall tax charge is shown above. Profits arising from our manufacturing operation in Puerto Rico are granted special status and are taxed at a reduced rate compared with the normal rate of tax in that territory under a tax incentive grant that expires in 2016.

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   153

Table of Contents

Financial Statements   | Notes to the Group Financial Statements

4 Taxation continued

Deferred tax

The movements in the net deferred tax balance during the year are as follows:

 

   

Property,

plant and

equipment

$m

   

Intangible

assets

$m

   

Pension

and post-

retirement

benefits

$m

   

Inter-

company

inventory

transfers

$m

   

Untaxed

reserves 1
$m

   

Accrued

expenses

$m

   

Share

schemes

$m

   

Deferred

capital

gains

$m

   

Losses and

tax credits

carried

forward 5

$m

   

Other

$m

   

Total

$m

 

Net deferred tax balance at 1 January 2010

    (208     (2,893     912        952        (1,474     470        129        (71     231        (3     (1,955

Taxation expense

    131        465        (178     3        24        66        (5     2        50        (19     539   

Other comprehensive income

                  (46                          4                      1        (41

Additions through business combinations 2

           (143                                                      2        (141

Exchange

    (6     5        (9     15        (81     12        (1     3        (10            (72

Net deferred tax balance at 31 December 2010

    (83     (2,566     679        970        (1,531     548        127        (66     271        (19     (1,670

Taxation expense

    297        142        (137     40        (36     57        (16     5        (129     4        227   

Other comprehensive income

                  159                             (9                   4        154   

Disposal of subsidiary undertaking 3

    9        41        (4     (3            (1                   (5            37   

Exchange

    (3     (1     (6     (8     34        21                      (4     (2     31   

Net deferred tax balance at 31 December 2011

    220        (2,384     691        999        (1,533     625        102        (61     133        (13     (1,221

Taxation expense

    30        11        (115     (83     333        (30     (69     5        180        29        291   

Other comprehensive income

                  (46                          (10                   5        (51

Additions through business combinations 4

           (527                          2        30               98               (397

Exchange

    (21     (17     23        5        (84     3        4        (3            3        (87

Net deferred tax balance at 31 December 2012

    229        (2,917     553        921        (1,284     600        57        (59     411        24        (1,465

 

1   Untaxed reserves relate to taxable profits where the tax liability is deferred to later periods.
2   The deferred tax liability of $143m relates to the acquisition of Novexel.
3   The deferred tax adjustment of $37m relates to the Astra Tech disposal.
4   The deferred tax liability of $397m relates to the acquisition of Ardea.
5   Includes losses and tax credits carried forward which will expire within 15 to 20 years.

The net deferred tax balance, before the offset of balances within countries, consists of:

 

   

Property,

plant and

equipment

$m

   

Intangible

assets

$m

   

Pension

and post-

retirement

benefits

$m

   

Inter-

company

inventory

transfers

$m

   

Untaxed

reserves

$m

   

Accrued

expenses

$m

   

Share

schemes
$m

   

Deferred

capital

gains

$m

   

Losses and

tax credits

carried
forward

$m

    Other
$m 		    Total
$m 		 

Deferred tax assets at 31 December 2010

    357        54        686        988               558        127               271        25        3,066   

Deferred tax liabilities at 31 December 2010

    (440     (2,620     (7     (18     (1,531     (10            (66            (44     (4,736

Net deferred tax balance at 31 December 2010

    (83     (2,566     679        970        (1,531     548        127        (66     271        (19     (1,670

Deferred tax assets at 31 December 2011

    429        53        699        1,027               647        102               133        32        3,122   

Deferred tax liabilities at 31 December 2011

    (209     (2,437     (8     (28     (1,533     (22            (61            (45     (4,343

Net deferred tax balance at 31 December 2011

    220        (2,384     691        999        (1,533     625        102        (61     133        (13     (1,221

Deferred tax assets at 31 December 2012

    353        44        561        961               656        57               411        36        3,079   

Deferred tax liabilities at 31 December 2012

    (124     (2,961     (8     (40     (1,284     (56            (59            (12     (4,544

Net deferred tax balance at 31 December 2012

    229        (2,917     553        921        (1,284     600        57        (59     411        24        (1,465

Analysed in the statement of financial position, after offset of balances within countries, as:

 

                                                              
    

2012

$m

   

2011

$m

   

2010

$m

 

Deferred tax assets

     1,111        1,514        1,475   

Deferred tax liabilities

     (2,576     (2,735     (3,145

Net deferred tax balance

     (1,465     (1,221     (1,670

Unrecognised deferred tax assets

Deferred tax assets of $120m have not been recognised in respect of deductible temporary differences (2011: $169m; 2010: $128m) because it is not probable that future taxable profit will be available against which the Group can utilise the benefits therefrom.

5 Earnings per $0.25 Ordinary Share

 

                                                        
     2012      2011      2010  

Profit for the year attributable to equity holders ($m)

     6,297         9,983         8,053   

Basic earnings per Ordinary Share

     $4.99         $7.33         $5.60   

Diluted earnings per Ordinary Share

     $4.98         $7.30         $5.57   

Weighted average number of Ordinary Shares in issue for basic earnings (millions)

     1,261         1,361         1,438   

Dilutive impact of share options outstanding (millions)

     3         6         8   

Diluted weighted average number of Ordinary Shares in issue (millions)

     1,264         1,367         1,446   

There are no options, warrants or rights outstanding in respect of unissued shares except for employee share option schemes. The number of options outstanding and the weighted average exercise price of these options is shown in Note 24. The earnings figures used in the calculations above are post-tax.

 

154   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

6 Segment information

AstraZeneca is engaged in a single business activity of pharmaceuticals and the Group does not have multiple operating segments. Our pharmaceuticals business consists of the discovery and development of new products, which are then manufactured, marketed and sold. All of these functional activities take place (and are managed) globally on a highly integrated basis. We do not manage these individual functional areas separately.

We consider that the SET is AstraZeneca’s chief operating decision making body (as defined by IFRS 8). The operation of the SET is principally driven by the management of the commercial operations, R&D, and manufacturing and supply. The SET also includes Finance, HR and Corporate Affairs, Compliance and General Counsel representation. All significant operating decisions are taken by the SET. While members of the SET have responsibility for implementation of decisions in their respective areas, operating decision making is at SET level as a whole. Where necessary these are implemented through cross-functional sub-committees that consider the Group-wide impact of a new decision. For example, product launch decisions would be initially considered by the SET and, on approval, passed to an appropriate sub-team for implementation. The impacts of being able to develop, produce, deliver and commercialise a wide range of pharmaceutical products drive the SET decision making process.

In assessing performance, the SET reviews financial information on an integrated basis for the Group as a whole, substantially in the form of, and on the same basis as, the Group’s IFRS Financial Statements. The high upfront cost of discovering and developing new products coupled with the relatively insignificant and stable unit cost of production means that there is not the clear link that exists in many manufacturing businesses between the revenue generated on an individual product sale and the associated cost and hence margin generated on a product. Consequently, the profitability of individual drugs or classes of drugs is not considered a key measure of performance for the business and is not monitored by the SET.

Resources are allocated on a Group-wide basis according to need. In particular, capital expenditure, in-licensing, and R&D resources are allocated between activities on merit, based on overall therapeutic considerations and strategy under the aegis of the Group’s Portfolio Investment Board to facilitate a Group-wide single combined discovery and development strategy. The Group’s acquisitions in the biologics area, MedImmune and Cambridge Antibody Technology Group plc (CAT), have been integrated into the existing management structure of AstraZeneca both for allocation of resources and for assessment and monitoring of performance purposes. As such, although biologics is a relatively new technological area for the Group, it does not operate as a separate operating segment.

Geographic areas

The tables below show information by geographic area and, for revenue and property, plant and equipment, material countries. The figures show the revenue, operating profit and profit before tax made by companies located in that area/country, together with segment assets, segment assets acquired, net operating assets and property, plant and equipment owned by the same companies; export sales and the related profit are included in the area/country where the legal entity resides and from which those sales were made.

 

                                                              
     Revenue  
    

2012

$m

   

2011

$m

   

2010

$m

 

 

UK

      

External

     1,843        1,980        1,952   

Intra-Group

     6,939        9,901        9,957   
       8,782        11,881        11,909   

 

Continental Europe

      

Belgium

     293        343        331   

France

     1,393        1,799        1,929   

Germany

     763        1,121        1,151   

Italy

     773        951        1,000   

Spain

     506        688        762   

Sweden

     466        964        1,157   

Others

     2,003        2,363        2,440   

Intra-Group

     5,067        5,101        5,144   
       11,264        13,330        13,914   

 

The Americas

      

Canada

     1,069        1,589        1,492   

US

     11,074        13,745        14,010   

Others

     1,326        1,452        1,387   

Intra-Group

     2,353        2,819        2,341   
       15,822        19,605        19,230   

 

Asia, Africa & Australasia

      

Australia

     1,050        1,166        981   

Japan

     2,748        2,905        2,458   

China

     1,511        1,261        1,047   

Others

     1,155        1,264        1,172   

Intra-Group

     70        70        67   
       6,534        6,666        5,725   

Continuing operations

     42,402        51,482        50,778   

Intra-Group eliminations

     (14,429     (17,891     (17,509
       27,973        33,591        33,269   

Export sales from the UK totalled $8,072m for the year ended 31 December 2012 (2011: $11,056m; 2010: $10,944m). Intra-Group pricing is determined on an arm’s length basis.

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   155

Table of Contents

Financial Statements | Notes to the Group Financial Statements

6 Segment information continued

 

     Operating profit           Profit before tax  

Profit from

                2012
$ m 		                 2011
$m 		                 2010
$m 		                       2012
$m 		                 2011
$m 		                 2010
$m 		 

UK

     397         2,221         3,258              4         1,803         3,098   

Continental Europe 1

     3,539         5,210         4,591              3,522         5,202         4,581   

The Americas

     3,705         4,813         3,278              3,687         4,828         2,932   

Asia, Africa & Australasia

     507         551         367              505         534         366   

Continuing operations

     8,148         12,795         11,494              7,718         12,367         10,977   
                    
     Non-current assets 2           Total assets  
    

2012

$m

    

2011

$m

    

2010

$m

         

2012

$m

    

2011

$m

    

2010

$m

 

UK

     2,743         2,941         3,397              12,316         15,752         17,171   

Continental Europe

     3,673         3,785         4,470              6,796         6,811         7,596   

The Americas

     25,767         20,090         20,808              30,708         26,673         28,175   

Asia, Africa & Australasia

     803         652         522              3,714         3,594         3,185   

Continuing operations

     32,986         27,468         29,197              53,534         52,830         56,127   
                    
     Assets acquired 3           Net operating assets 4  
    

2012

$m

    

2011

$m

    

2010

$m

         

2012

$m

    

2011

$m

    

2010

$m

 

UK

     350         414         314              2,519         3,361         3,273   

Continental Europe

     379         344         1,053              4,006         4,113         4,827   

The Americas 5

     6,760         314         1,125              22,940         18,395         18,795   

Asia, Africa & Australasia

     229         177         107              2,328         2,380         2,021   

Continuing operations

     7,718         1,249         2,599              31,793         28,249         28,916   

 

1   2011 includes profit on disposal of Astra Tech (see Note 22).
2   ‘Non-current assets’ exclude deferred tax assets and derivative financial instruments.
3   Included in ‘Assets acquired’ are those assets that are expected to be used during more than one period (property, plant and equipment, goodwill and intangible assets).
4   ‘Net operating assets’ exclude short-term investments, cash, short-term borrowings, loans, derivative financial instruments, retirement benefit obligations and non-operating receivables and payables.
5   Assets acquired in 2012 include those related to Amylin and Ardea (see Notes 9 and 22).

 

                                            
     Property, plant and equipment  
    

            2012

$m

    

2011

$m

    

2010

$m

 

UK

     1,353         1,387         1,628   

Sweden

     1,183         1,408         1,647   

US

     2,197         2,309         2,381   

Rest of the world

     1,356         1,321         1,301   

Continuing operations

     6,089         6,425         6,957   

 

Geographic markets

The table below shows revenue in each geographic market in which customers are located.

 

  

  

    

2012

$m

    

2011

$m

    

2010

$m

 

UK

     668         866         1,033   

Continental Europe

     7,042         8,896         9,315   

The Americas

     13,075         16,484         16,629   

Asia, Africa & Australasia

     7,188         7,345         6,292   

Continuing operations

     27,973         33,591         33,269   

Revenue is recognised at the point of delivery, which is usually when title passes to the wholesaler. Transactions with two wholesalers (2011: two; 2010: two) individually represented greater than 10% of total revenue. The values of these transactions recorded as revenue were $3,517m and $3,155m (2011: $4,298m and $4,170m; 2010: $4,164m and $4,129m).

 

156   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

7 Property, plant and equipment

 

    

Land and

buildings

$m

   

Plant and

equipment

$m

   

Assets in course

of construction

$m

   

Total property,

plant and

equipment

$m

 

 

Cost

        

At 1 January 2010

     5,336        8,803        1,029        15,168   

Capital expenditure

     13        225        570        808   

Transfer of assets into use

     342        668        (1,010       

Disposals and other movements

     (40     (449     (4     (493

Exchange adjustments

     48        46        6        100   

At 31 December 2010

     5,699        9,293        591        15,583   

Capital expenditure

     18        168        621        807   

Transfer of assets into use

     261        294        (555       

Disposals and other movements

     62        (738     (10     (686

Reduction on disposal of subsidiaries

     (87     (170     (15     (272

Exchange adjustments

     (42     (68     (12     (122

At 31 December 2011

     5,911        8,779        620        15,310   

Capital expenditure

     37        229        502        768   

Additions through business combinations

            4               4   

Transfer of assets into use

     123        391        (514       

Disposals and other movements

     (370     (1,050     (49     (1,469

Exchange adjustments

     149        292        17        458   

At 31 December 2012

     5,850        8,645        576        15,071   

 

Depreciation

        

At 1 January 2010

     1,967        5,899        (5     7,861   

Charge for year

     302        774               1,076   

Impairment

     2        20               22   

Disposals and other movements

     (29     (396     5        (420

Exchange adjustments

     32        55               87   

At 31 December 2010

     2,274        6,352               8,626   

Charge for year

     271        815               1,086   

Disposals and other movements

     (62     (542            (604

Reduction on disposal of subsidiaries

     (22     (99            (121

Exchange adjustments

     (26     (76            (102

At 31 December 2011

     2,435        6,450               8,885   

Charge for year

     280        743               1,023   

Disposals and other movements

     (129     (1,116            (1,245

Exchange adjustments

     82        237               319   

At 31 December 2012

     2,668        6,314               8,982   

 

Net book value

        

At 31 December 2010

     3,425        2,941        591        6,957   

At 31 December 2011

     3,476        2,329        620        6,425   

At 31 December 2012

     3,182        2,331        576        6,089   

There were no impairment charges in 2012 or 2011.

Impairment charges in 2010 were due to the termination of the Certriad co-promotion with Abbott and various productivity initiatives. These costs were recognised in cost of sales and research and development respectively.

 

                                                  
    

             2012

$m

    

            2011

$m

    

2010

$m

 

The net book value of land and buildings comprised:

        

Freeholds

     3,122         3,449         3,395   

Leaseholds

     60         27         30   

Included within plant and equipment are Information Technology assets held under finance leases with a net book value of $79m (2011 and 2010: $nil).

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   157

Table of Contents

Financial Statements | Notes to the Group Financial Statements

8 Goodwill

 

                                            
    

2012

$m

    

2011

$m

   

2010

$m

 

 

Cost

       

At 1 January

     10,186         10,206        10,228   

Exchange and other adjustments

     7         (20     (22

Additions through business combinations

     30                  

At 31 December

     10,223         10,186        10,206   

 

Amortisation and impairment losses

       

At 1 January

     324         335        339   

Exchange and other adjustments

     1         (11     (4

At 31 December

     325         324        335   

Net book value at 31 December

     9,898         9,862        9,871   

For the purpose of impairment testing of goodwill, the Group is regarded as a single cash-generating unit.

The recoverable amount is based on value in use using discounted risk-adjusted projections of the Group’s pre-tax cash flows over 10 years which is considered by the Board as a reasonable period given the long development and life-cycle of a medicine. The projections include assumptions about product launches, competition from rival products and pricing policy as well as the possibility of generics entering the market. In setting these assumptions we consider our past experience, external sources of information (including information on expected increases and ageing of the populations in our established markets and the expanding patient population in newer markets), our knowledge of competitor activity and our assessment of future changes in the pharmaceutical industry. The 10 year period is covered by internal budgets and forecasts. Given that internal budgets and forecasts are prepared for all projections, no general growth rates are used to extrapolate internal budgets and forecasts for the purposes of determining value in use. No terminal value is included as these cash flows are more than sufficient to establish that an impairment does not exist. The methods used to determine recoverable amounts have remained consistent with the prior year.

In arriving at value in use, we disaggregate our projected pre-tax cash flows into groups reflecting similar risks and tax effects. For each group of cash flows we use an appropriate discount rate reflecting those risks and tax effects. In arriving at the appropriate discount rate for each group of cash flows, we adjust AstraZeneca’s post-tax weighted average cost of capital (7.0% for 2012, 2011 and 2010) to reflect the impact of relevant industry risks, the time value of money and tax effects. The weighted average pre-tax discount rate we used was approximately 10% (2011: 10%; 2010: 10%).

As a further check, we compare our market capitalisation to the book value of our net assets and this indicates significant surplus at 31 December 2012 (and 31 December 2011 and 31 December 2010).

No goodwill impairment was identified.

The Group has also performed sensitivity analysis calculations on the projections used and discount rate applied. The Directors have concluded that, given the significant headroom that exists, and the results of the sensitivity analysis performed, there is no significant risk that reasonable changes in any key assumptions would cause the carrying value of goodwill to exceed its value in use.

 

158   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

9 Intangible assets

 

    

Product,

marketing and

distribution rights

$m

   

Other

intangibles

$m

   

Software

development

costs

$m

   

Total

$m

 

 

Cost

        

At 1 January 2010

     14,353        2,304        1,212        17,869   

Additions through business combinations

     548                      548   

Additions – separately acquired

     1,017        20        206        1,243   

Disposals

     (239     (2            (241

Exchange and other adjustments

     125        13        (19     119   

At 31 December 2010

     15,804        2,335        1,399        19,538   

Additions – separately acquired

     189        14        239        442   

Reduction on disposal of subsidiaries

            (152            (152

Exchange and other adjustments

     (94     (9     (4     (107

At 31 December 2011

     15,899        2,188        1,634        19,721   

Additions through business combinations

     1,464                      1,464   

Additions – separately acquired

     5,228        12        212        5,452   

Exchange and other adjustments

     271        (65     59        265   

At 31 December 2012

     22,862        2,135        1,905        26,902   

Amortisation and impairment losses

        

At 1 January 2010

     3,727        1,148        768        5,643   

Amortisation for year

     573        121        116        810   

Impairment

     699        131        3        833   

Disposals

            (1            (1

Exchange and other adjustments

     89        26        (20     95   

At 31 December 2010

     5,088        1,425        867        7,380   

Amortisation for year

     652        119        140        911   

Impairment

     552        1               553   

Reduction on disposal of subsidiaries

            (39            (39

Exchange and other adjustments

     (46     (32     14        (64

At 31 December 2011

     6,246        1,474        1,021        8,741   

Amortisation for year

     1,039        95        162        1,296   

Impairment

     192        1        6        199   

Exchange and other adjustments

     182        8        28        218   

At 31 December 2012

     7,659        1,578        1,217        10,454   

 

Net book value

        

At 31 December 2010

     10,716        910        532        12,158   

At 31 December 2011

     9,653        714        613        10,980   

At 31 December 2012

     15,203        557        688        16,448   

 

Other intangibles consist mainly of licensing and rights to contractual income streams.

 

Amortisation charges are recognised in profit as follows:

 

  

  

    

Product,

marketing and

distribution rights

$m

   

Other

intangibles

$m

   

Software

development

costs

$m

   

Total

$m

 

 

Year ended 31 December 2010

        

Cost of sales

     87                      87   

Research and development expense

            24               24   

Selling, general and administrative costs

     486        22        116        624   

Other operating income and expense

            75               75   
       573        121        116        810   

 

Year ended 31 December 2011

        

Cost of sales

     129                      129   

Research and development expense

            27               27   

Selling, general and administrative costs

     523        24        140        687   

Other operating income and expense

            68               68   
       652        119        140        911   

 

Year ended 31 December 2012

        

Cost of sales

     325                      325   

Research and development expense

            25               25   

Selling, general and administrative costs

     673        13        162        848   

Other operating income and expense

     41        57               98   
         1,039          95        162          1,296   

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   159

Table of Contents

Financial Statements | Notes to the Group Financial Statements

9 Intangible assets continued

Impairment charges are recognised in profit as follows:

 

    

Product,

marketing and

distribution rights

$m

    

Other

intangibles

$m

    

Software

development

costs

$m

    

Total

$m

 

 

Year ended 31 December 2010

           

Cost of sales

     128                         128   

Research and development expense

     571                         571   

Selling, general and administrative costs

             3         3         6   

Other operating income and expense

             128                 128   
       699         131         3         833   

 

Year ended 31 December 2011

           

Research and development expense

     548         1                 549   

Selling, general and administrative costs

     4                         4   
       552         1                 553   

 

Year ended 31 December 2012

           

Research and development expense

     185         1                 186   

Selling, general and administrative costs

     7                 6         13   
       192         1         6         199   

Amortisation and impairment charges

The 2012 impairment of product, marketing and distribution rights includes a charge of $50m following the decision by AstraZeneca not to pursue a regulatory filing for TC-5214, based on the final results of Phase III efficacy and tolerability studies of the compound as an adjunct therapy to an anti-depressant in patients with major depressive disorder who do not respond adequately to initial anti-depressant treatment. The remaining $149m charge relates to the termination of other development projects during the year.

The 2011 impairment of product, marketing and distribution rights includes a charge of $285m following the termination of development of the investigational compound olaparib for the maintenance treatment of serous ovarian cancer. The 2011 impairment of product, marketing and distribution rights also includes an impairment of $150m reflecting a lower probability of success assessment for TC-5214, based on the results of the first two of four Phase III efficacy and tolerability studies. The remaining $117m charge relates to the termination of other development projects during the year.

The 2010 impairment of product, marketing and distribution rights results from the withdrawal of the biological licence application pending at the FDA for motavizumab ($445m) and the termination of the lesogaberan development ($128m) and other development projects in the year. The 2010 impairment of other intangibles chiefly results from a reassessment of the future royalties expected to be received relating to the HPV cervical cancer vaccine.

The write downs in value of intangible assets, other than those arising from termination of research and development activities, were determined based on value in use calculations using discounted risk-adjusted projections of the products’ expected cash flows over a period reflecting the patent-protected lives of the individual products. The full period of projections is covered by internal budgets and forecasts. In arriving at the appropriate discount rate to use for each product, we adjust AstraZeneca’s post-tax weighted average cost of capital (7.0% for 2012, 2011 and 2010) to reflect the impact of risks and tax effects specific to the individual products. The weighted average pre-tax discount rate we used was approximately 14% (2011: 14%; 2010: 14%).

Significant assets

 

    Description  

Carrying value

$m

   

Remaining amortisation

period

 

Advance payment 1

 

Product, marketing and distribution rights

    386        6 years   

Partial retirement 1

 

Product, marketing and distribution rights

    610        2-15 years   

First Option 1

 

Product, marketing and distribution rights

    1,428        14-18 years   

Second Option 1

 

Product, marketing and distribution rights

    1,652        3-4 years   

Intangible assets arising from the acquisition of CAT

 

Product, marketing and distribution rights

    251        3 and 8 years   

RSV franchise assets arising from the acquisition of MedImmune

 

Product, marketing and distribution rights

    3,618        13 years   

Intangible assets arising from the acquisition of MedImmune

 

Licensing and contractual income

    398        6-7 years   

Intangible assets arising from the acquisition of MedImmune

 

Product, marketing and distribution rights

    548        19 years   

Intangible assets arising from the collaboration with BMS 2

 

Product, marketing and distribution rights

    540        10-11 years   

Bydureon (weekly) asset arising from the Amylin collaboration with BMS 3

 

Product, marketing and distribution rights

    2,502        18 years   

Other intangible assets arising from the Amylin collaboration with BMS 3

 

Product, marketing and distribution rights

    779        10-18 years   

Intangible assets arising from the acquisition of Novexel 4

 

Product, marketing and distribution rights

    300        Not amortised   

Intangible assets arising from the acquisition of Ardea 4

 

Product, marketing and distribution rights

    1,464        Not amortised   

 

1   These assets are associated with the restructuring of the joint venture with Merck & Co., Inc.
2   These assets arise from the collaboration agreement with BMS for Onglyza and Forxiga .
3   These assets arise from the collaboration agreement with BMS for the related Amylin products.
4   Assets in development are not amortised but are tested annually for impairment.

 

160   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

9 Intangible assets continued

Collaboration with BMS on Amylin products

On 8 August 2012, BMS completed its acquisition of Amylin. On that date, AstraZeneca and BMS entered into collaboration arrangements, based substantially on the framework of the existing diabetes alliance, regarding the development and commercialisation of Amylin’s portfolio of products. Under the terms of the collaboration, the companies will jointly undertake the global selling and marketing activities in relation to the collaboration products. BMS will undertake all manufacturing activities with AstraZeneca receiving collaboration product at cost. Profits and losses arising from the collaboration will be shared equally.

The total consideration for AstraZeneca’s participation in the collaboration is $3.7bn, including an amount of $135m relating to an option of AstraZeneca contained in the collaboration agreement to acquire certain additional governance rights in respect of the collaboration. The Group notified BMS of its decision to exercise the option in August 2012 and the balance of $135m will be payable once applicable anti-trust and competition approvals are received by AstraZeneca. The Group expects to make this payment in the first half of 2013. Upon such payment, the additional governance rights of AstraZeneca granted by the option will become legally effective.

AstraZeneca considers that the key strategic and financial decisions over which the collaboration agreement and the governance rights that are subject to the option grant joint control, represent the activities most relevant in affecting the success of the collaboration. AstraZeneca accounts for the collaboration as a jointly controlled operation. The Group has recognised a 50% share of collaboration revenues amounting to $128m, cost of sales of $36m and other costs, excluding amortisation, of $133m, in its income statement from 9 August 2012. An amount of $165m was owed to BMS under this arrangement, recorded within trade and other payables, at 31 December 2012.

AstraZeneca’s payment to BMS for its participation in the collaboration primarily results in the purchase of intangible assets, valued at $3,358m, related to the collaboration products: Byetta (exenatide) injection and Bydureon (exenatide extended-release for injectable suspension/exenatide 2mg powder and solvent for prolonged release suspension for injection) that are approved for use in both the US and Europe, Symlin (pramlinitide acetate) injection that is approved for use in the US, and metreleptin, a leptin analogue currently under review at the US Food and Drug Administration (FDA) for the treatment of diabetes and/or hypertriglyceridaemia in patients with rare forms of inherited or acquired lipodystrophy. In addition, a prepayment of $0.4bn has been recognised representing payments in advance for collaboration products.

Arrangements with Merck

In 1982, Astra set up a joint venture with Merck & Co., Inc. (now Merck Sharp & Dohme Corp., a subsidiary of the new Merck & Co., Inc. that resulted from the merger with Schering-Plough) (‘Merck’) for the purposes of selling, marketing and distributing certain Astra products in the US. In 1998, this joint venture was restructured (the ‘Restructuring’). Under the agreements relating to the Restructuring (the ‘Agreements’), a US limited partnership (the ‘Partnership’) was formed, in which Merck is the limited partner and AstraZeneca is the general partner, and AstraZeneca obtained control of the joint venture’s business subject to certain limited partner and other rights held by Merck and its affiliates. These rights provide Merck with safeguards over the activities of the Partnership and place limitations on AstraZeneca’s commercial freedom to operate. The Agreements provide, in part, for:

 

> Annual contingent payments; and
> Termination arrangements which cause Merck to relinquish its interests in AstraZeneca’s products and activities in stages, some of which are mandatory and others optional.

The termination arrangements and payments include:

 

> the Advance Payment
> the Partial Retirement
> the True-Up
> the Loan Note Receivable
> the First Option
> the Second Option.

AstraZeneca considers that the termination arrangements described above represent the acquisition, in stages, of Merck’s interests in the Partnership and Agreement products (including Merck’s rights to contingent payments). Once all payments are made, AstraZeneca will have unencumbered discretion in its operations in the US market. AstraZeneca anticipates that the benefits that accrue under all of the termination arrangements arise from:

 

> The substantial freedom over products acquired or discovered after the merger of Astra and Zeneca in 1999; and
> Enhanced contributions from, and substantial freedom over, those products that have already been launched (for example, Prilosec, Nexium, Brilinta, Pulmicort, Symbicort, Rhinocort and Atacand ) and those that are in development.

Economic benefits include relief from contingent payments and other cost efficiencies, together with the strategic advantages of increased freedom to operate.

The intangible assets relating to purchased product rights are subject to impairment testing and would be partially or wholly impaired if a product is withdrawn or if activity in any of the affected therapy areas is significantly curtailed.

Annual Contingent Payments

AstraZeneca makes ongoing payments to Merck based on sales of certain of its products in the US (the ‘contingent payments’ on the Agreement products). Contingent payments in respect of Prilosec and Nexium will continue until the Second Option is exercised and consummated (as discussed under Second Option below). Contingent payments on all other agreement products have ceased as discussed under First Option below.

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   161

Table of Contents

Financial Statements | Notes to the Group Financial Statements

9 Intangible assets continued

Advance Payment

The merger between Astra and Zeneca in 1999 triggered the first step in the termination arrangements. Merck relinquished all rights, including contingent payments on future sales, to potential Astra products with no existing or pending US patents at the time of the merger. As a result, AstraZeneca now has rights to such products and is relieved of potential obligations to Merck and restrictions in respect of those products (including annual contingent payments), affording AstraZeneca substantial freedom to exploit the products as it sees fit. At the time of the merger, the Advance Payment of $967m was made. The Advance Payment has been accounted for as an intangible asset and is being amortised over 20 years. Although the rights obtained apply in perpetuity, the period of amortisation of 20 years is used to reflect the typical timescale of development and marketing of a product.

Partial Retirement, True-Up and Loan Note Receivable

On 17 March 2008, AstraZeneca made a net cash payment to Merck of approximately $2.6bn in connection with the Partial Retirement, the True-Up and the Loan Note Receivable. This payment resulted in AstraZeneca acquiring Merck’s interests in certain AstraZeneca products (including Pulmicort, Rhinocort, Symbicort and Toprol- XL ), AstraZeneca ceasing contingent payments on these products and AstraZeneca obtaining the ability to exploit these products and other opportunities in the Respiratory therapy area. Intangible assets of $994m were recognised at the time with the balance of the net payment ($1,656m) representing payments on account for future product rights associated with the First Option and the Second Option as detailed below. These ‘non-refundable deposits’ were classified as intangible assets.

First Option

On 26 February 2010, AstraZeneca exercised the First Option. Payment of $647m to Merck was made on 30 April 2010. This payment resulted in AstraZeneca acquiring Merck’s interests in products covered by the First Option including Entocort, Atacand, Plendil and certain products in development at the time (principally Brilinta and lesogaberan; development of lesogaberan subsequently was discontinued). Also on 30 April 2010, contingent payments on these products ceased with respect to periods after this date and AstraZeneca obtained the ability to exploit these products and other opportunities in the Cardiovascular and Neuroscience Therapy Areas. These rights were valued at $1,829m and were recognised as intangible assets from 26 February 2010 ($1,182m having been transferred from non-refundable deposits to supplement the payment of $647m to Merck). Of these rights, $689m was allocated to contingent payment relief and $1,140m to intangible assets reflecting the ability to fully exploit the products in the Cardiovascular and Neuroscience Therapy Areas. The remaining non-refundable deposits of $474m relate to benefits that would be secured upon AstraZeneca exercising the Second Option.

Second Option

The Agreements provided that AstraZeneca may exercise a Second Option to purchase Merck’s interests in the Merck affiliates that hold the limited partner and other rights referred to above. Exercise of the Second Option would result in the repurchase by AstraZeneca of Merck’s interests in Prilosec and Nexium in the US. This option was exercisable by AstraZeneca in May to October of 2012, or in 2017, or if combined annual sales of the two products fell below a minimum amount.

On 26 June 2012, AstraZeneca and Merck agreed to amend certain provisions of the Agreements with respect to the Second Option.

The principal areas covered by the amendments are a change in the timing for AstraZeneca to exercise the Second Option, and agreement on the valuation methodology for setting certain aspects of the option exercise price. Under the amended Agreements, Merck has granted to AstraZeneca a new Second Option exercisable by AstraZeneca between 1 March 2014 and 30 April 2014, with closing on 30 June 2014. Options exercisable in 2017 or if combined annual sales fall below a minimum amount also remain available to AstraZeneca. In addition to this revised timing for the Second Option, AstraZeneca and Merck have also reached agreement on the valuation methodology for setting certain components of the option exercise price for a 2014 exercise. In lieu of third-party appraisals, the valuation for a 2014 exercise is now a fixed sum of $327m, based on a shared view by AstraZeneca and Merck of the forecasts for sales of Nexium and Prilosec in the US market. The agreed amount that would be payable on 30 June 2014 is subject to a true-up in 2018 that replaces a shared forecast with actual sales for the period from closing in 2014 to June 2018. In addition, the exercise price for the Second Option also includes a multiple of ten times Merck’s average 1% annual profit allocation in the Partnership for the three years prior to exercise. AstraZeneca currently expects this amount to be around $80m. The component of the exercise price of the Second Option that includes the net present value of up to 5% of future US sales of Vimovo , with the precise amount dependent on an annual sales threshold that has not yet been achieved and the timing of the option exercise, will continue.

AstraZeneca believes that the amendments provide a greater degree of certainty to the valuation of the Second Option that is preferable to the previous arrangements and, barring unforeseen circumstances, AstraZeneca now intends to exercise the Second Option in 2014.

Under the amendments, if AstraZeneca exercises in 2014, Merck’s existing rights to manufacture Nexium and Prilosec would cease upon closing. In connection with the amendments, Merck also granted AstraZeneca flexibility to exploit certain commercial opportunities with respect to Nexium .

AstraZeneca now considers that exercise of the Second Option is virtually certain. This judgement is supported by management’s view that: AstraZeneca is fully committed to exercising the Second Option in 2014, barring unforeseen circumstances; external announcements of that intention constructively oblige AstraZeneca to exercise in 2014, barring unforeseen circumstances; and the Second Option price is highly favourable, giving economic compulsion for AstraZeneca to exercise in 2014. As such, AstraZeneca has applied an accounting treatment to reflect the Second Option as if the date of exercise were 26 June 2012 (the date of amendment of the Agreements), resulting in liabilities to Merck of approximately $1.5bn ($1.1bn of which will be paid by way of monthly contingent payments between 1 July 2012 and 30 June 2014 and the balance as a lump sum on 30 June 2014), and a corresponding increase to intangible assets, from that date. These intangible assets, and the $474m from the First Option (detailed above), in aggregate, reflect the value of the ability to exploit opportunities in the Gastrointestinal Therapy Area and relief from contingent payments.

 

162   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

10 Other investments

 

    

2012

                $m

    

2011

                $m

    

2010

                $m

 

 

Non-current investments

        

Equity securities available for sale

     199         201         211   
       199         201         211   

 

Current investments

        

Equity securities and bonds available for sale

     748         296         355   

Equity securities held for trading

     29         25         20   

Fixed deposits

     46         3,927         1,107   
       823         4,248         1,482   

The equity securities and bonds available for sale in current investments of $748m (2011: $296m; 2010: $355m) are held in an escrow account. Further details of this escrow account are included in Note 18.

Impairment charges of $2m in respect of available for sale securities are included in other operating income and expense in profit (2011: $3m; 2010: $2m).

Equity securities and bonds available for sale, and equity securities held for trading, are held on the consolidated statement of financial position at fair value. The fair value of listed investments is based on year end quoted market prices. For unlisted investments, cost is considered to approximate to fair value, as detailed below. Fixed deposits are held at amortised cost with carrying value being a reasonable approximation of fair value given their short-term nature.

None of the financial assets or liabilities have been reclassified in the year.

Fair value hierarchy

The table below analyses financial instruments, contained within other investments and carried at fair value, by valuation method. The different levels have been defined as follows:

 

> Level  1: quoted prices (unadjusted) in active markets for identical assets or liabilities.
> Level  2: inputs other than quoted prices included within Level 1 that are observable for the asset or liability,     either directly (ie as prices) or indirectly (ie derived from prices).
> Level  3: inputs for the asset or liability that are not based on observable market data (unobservable inputs).

 

    

Level 1

                $m

    

Level 2

                $m

    

Level 3

                $m

    

Total

                $m

 

 

2010

           

Equity securities and bonds available for sale

     399                 167         566   

Equity securities held for trading

     20                         20   

Total

     419                 167         586   

 

2011

           

Equity securities and bonds available for sale

     338                 159         497   

Equity securities held for trading

     25                         25   

Total

     363                 159         522   

 

2012

           

Equity securities and bonds available for sale

     809                 138         947   

Equity securities held for trading

     29                         29   

Total

     838                 138         976   

Equity securities available for sale which are analysed at Level 3 represent investments in private biotech companies. In the absence of specific market data, these unlisted investments are held at cost, adjusted as necessary for impairments, which approximates to fair value. Hence, carrying value is adjusted only for additions, sales and permanent impairment and for no other movement. Consequently, in the current year, no change has been made to the fair value of individual investments.

11 Inventories

 

    

2012

                $m

    

2011

                $m

    

2010

                $m

 

Raw materials and consumables

     620         588         539   

Inventories in process

     876         645         665   

Finished goods and goods for resale

     565         619         478   
       2,061         1,852         1,682   

The Group recognised $3,019m (2011: $3,447m; 2010: $3,547m) of inventories as an expense within cost of sales during the year.

Inventory write-offs in the year amounted to $120m (2011: $51m; 2010: $69m).

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   163

Table of Contents

Financial Statements | Notes to the Group Financial Statements

12 Trade and other receivables

Non-current other receivables

Non-current other receivables of $352m (2011: $nil; 2010: $nil) consist of prepayments in relation to our jointly controlled operation with BMS. Further details of this prepayment are included in Note 9.

Current trade and other receivables

 

    

2012

                $m

   

2011

                $m

   

2010

                $m

 

 

Amounts due within one year

      

Trade receivables

     5,760        6,696        6,328   

Less: Amounts provided for doubtful debts (Note 23)

     (64     (66     (81
       5,696        6,630        6,247   

Other receivables

     750        1,172        607   

Prepayments and accrued income

     923        725        733   
       7,369        8,527        7,587   

 

Amounts due after more than one year

      

Other receivables

     85        65        64   

Prepayments and accrued income

     175        162        196   
       260        227        260   

Trade and other receivables

     7,629        8,754        7,847   

With the exception of a receivable of $nil (2011: $nil; 2010: $25m) held within other receivables, that arose on the acquisition of Novexel and the subsequent transaction with Forest, and which is held at fair value (see Note 22), all other financial assets are held on the consolidated statement of financial position at amortised costs with carrying value being a reasonable approximation of fair value. The Novexel-related receivable falls within level 3 of the fair value hierarchy as defined in Note 10.

13 Cash and cash equivalents

 

    

2012

                $m

   

2011

                $m

   

2010

                $m

 

Cash at bank and in hand

     1,304        1,488        1,750   

Short-term deposits

     6,397        6,083        9,318   

Cash and cash equivalents

     7,701        7,571        11,068   

Unsecured bank overdrafts

     (105     (137     (87

Cash and cash equivalents in the cash flow statement

     7,596        7,434        10,981   

The Group holds $301m (2011: $543m; 2010: $370m) of cash and cash equivalents which is required to meet insurance solvency, capital and security requirements and which, as a result, is not readily available for the general purposes of the Group.

Cash and cash equivalents are held on the consolidated statement of financial position at amortised cost. Fair value approximates to carrying value.

14 Interest-bearing loans and borrowings

 

         

Repayment

dates

  

2012

                  $m

    

2011

                  $m

    

2010

                  $m

 

 

Current liabilities

              

Bank overdrafts

        On demand      105         137         87   

Finance leases

               22                   

5.4% Callable bond

   US dollars    2012              1,769           

Other loans

        Within one year      774         84         38   
                 901         1,990         125   

 

Non-current liabilities

              

Finance leases

               62                   

5.4% Callable bond

   US dollars    2012                      1,800   

5.4% Callable bond

   US dollars    2014      805         834         837   

5.125% Non-callable bond

   euros    2015      990         969         993   

5.9% Callable bond

   US dollars    2017      1,895         1,896         1,855   

1.95% Callable bond

   US dollars    2019      995                   

7% Guaranteed debentures

   US dollars    2023      399         387         359   

5.75% Non-callable bond

   pounds sterling    2031      561         536         535   

6.45% Callable bond

   US dollars    2037      2,717         2,716         2,718   

4% Callable bond

   US dollars    2042      985                   
                 9,409         7,338         9,097   

All loans and borrowings above are unsecured, except for finance leases which are secured against the Information Technology assets to which they relate (see Note 7).

 

164   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

14 Interest-bearing loans and borrowings continued

Set out below is a comparison by category of carrying values and fair values of all the Group’s interest-bearing loans and borrowings at 31 December 2012, 31 December 2011 and 31 December 2010.

 

    

Instruments in a

fair value hedge

relationship 1

$m

    

Instruments

designated

at fair value 2

$m

    

Amortised

cost 3

$m

    

Total

carrying

value

$m

    

Fair

value

$m

 

 

2010

              

Overdrafts

                     87         87         87   

Loans due within one year

                     38         38         38   

Loans due after more than one year

     1,659         1,196         6,242         9,097         10,022   

Total

     1,659         1,196         6,367         9,222         10,147   

 

2011

                                            

Overdrafts

                     137         137         137   

Loans due within one year

     770                 1,083         1,853         1,891   

Loans due after more than one year

     899         1,221         5,218         7,338         8,765   

Total

     1,669         1,221         6,438         9,328         10,793   

 

2012

                                            

Overdrafts

                     105         105         105   

Finance leases due within one year

                     22         22         22   

Finance leases due after more than one year

                     62         62         62   

Loans due within one year

                     774         774         774   

Loans due after more than one year

     900         1,204         7,243         9,347         10,897   

Total

     900         1,204         8,206         10,310         11,860   

 

1   Instruments designated as hedged items in fair value hedge relationships with respect to interest rate risk include a designated portion of the US dollars 5.9% callable bond repayable in 2017.
2   Instruments designated at fair value through profit or loss include the US dollar 5.4% callable bond repayable in 2014 and the US dollar 7% guaranteed debentures repayable in 2023.
3   Included within borrowings held at amortised cost are amounts designated as hedges of net investments in foreign operations of $1,551m (2011: $1,505m; 2010: $1,528m) held at amortised cost. The fair value of these borrowings was $1,808m at 31 December 2012 (2011: $1,752m; 2010: $1,687m).

The fair value of fixed-rate publicly traded debt is based on year end quoted market prices; the fair value of floating rate debt is nominal value, as mark to market differences would be minimal given the frequency of resets. The carrying value of loans designated at fair value through profit or loss is the fair value, this falls within the Level 1 valuation method as defined in Note 10. For loans designated in a fair value hedge relationship, carrying value is initially measured at fair value and remeasured for fair value changes in respect of the hedged risk at each reporting date. All other loans are held at amortised cost.

A loss of $10m was made during the year on the fair value of bonds designated at fair value through profit or loss, due to decreased credit risk. A gain of $34m has been made on these bonds since designation due to increased credit risk. Changes in credit risk had no material effect on any other financial assets and liabilities recognised at fair value in the Group’s Financial Statements. The change in fair value attributable to changes in credit risk is calculated as the change in fair value not attributable to market risk. The amount payable at maturity on bonds designated at fair value through profit or loss is $1,037m.

The interest rates used to discount future cash flows for fair value adjustments, where applicable, are based on market swap curves at the reporting date, and were as follows:

 

     2012      2011      2010  

Loans and borrowings

     0.6% to 2.0%         0.9% to 2.3%         0.7% to 4.0%   

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   165

Table of Contents

Financial Statements | Notes to the Group Financial Statements

15 Derivative financial instruments

Derivative financial instruments consist of interest rate swaps (included in instruments designated at fair value if related to debt designated at fair value or instruments in a fair value hedge relationship if formally designated as in a fair value hedge relationship), cross-currency swaps (included in instruments designated in net investment hedges) and forward foreign exchange contracts (included below in other derivatives).

 

    

Non-current

assets

$m

    

Current

assets

$m

    

Current

liabilities

$m

   

Total

$m

 

Designated in a fair value hedge

     164                        164   

Related to instruments designated at fair value through profit or loss

     160                        160   

Other derivatives

             9         (8     1   

31 December 2010

     324         9         (8     325   
          
    

Non-current

assets

$m

    

Current

assets

$m

    

Current

liabilities

$m

   

Total

$m

 

Designated in a fair value hedge

     153         20                173   

Related to instruments designated at fair value through profit or loss

     189                        189   

Other derivatives

             5         (9     (4

31 December 2011

     342         25         (9     358   
          
    

Non-current

assets

$m

    

Current

assets

$m

    

Current

liabilities

$m

   

Total

$m

 

Designated in a fair value hedge

     151                        151   

Related to instruments designated at fair value through profit or loss

     162                        162   

Designated as a net investment hedge

     76                        76   

Other derivatives

             31         (3     28   

31 December 2012

     389         31         (3     417   

All derivatives are held at fair value and fall within Level 2 of the fair value hierarchy as defined in Note 10. None of the derivatives have been reclassified in the year.

The fair value of interest rate swaps and cross-currency swaps is estimated using appropriate zero coupon curve valuation techniques to discount future contractual cash flows based on rates at current year end.

The fair value of forward foreign exchange contracts is estimated by discounting the future contractual cash flows using appropriate yield curves based on market forward foreign exchange rates at the year end. The majority of forward foreign exchange contracts for existing transactions had maturities of less than one month from year end.

The interest rates used to discount future cash flows for fair value adjustments, where applicable, are based on market swap curves at the reporting date, and were as follows:

 

     2012      2011      2010  

Derivatives

     0.6% to 2.0%         0.9% to 2.3%         0.7% to 4.0%   

 

16 Trade and other payables

 

  

    

2012

$m

    

2011

              $m

    

2010

              $m

 

 

Current liabilities

        

Trade payables

     2,449         2,155         2,257   

Value added and payroll taxes and social security

     231         343         323   

Rebates and chargebacks

     2,486         3,285         2,839   

Accruals

     3,200         2,474         2,297   

Other payables

     855         718         945   
       9,221         8,975         8,661   

Non-current liabilities

        

Accruals

     710         113         104   

Other payables

     291         272         269   
       1,001         385         373   

With the exception of a payable of $nil (2011: $nil; 2010: $50m) held within other payables, that arose on the acquisition of Novexel and the subsequent transaction with Forest, and which is held at fair value (see Note 22), all other financial liabilities are held on the consolidated statement of financial position at amortised cost with carrying value being a reasonable approximation of fair value. The Novexel-related payable falls within Level 3 of the fair value hierarchy as defined in Note 10.

 

166   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

17 Provisions for liabilities and charges

 

    

Severance

$m

   

Environmental

$m

   

Employee

benefits

$m

   

Legal

$m

   

Other

provisions

$m

   

Total

$m

 

At 1 January 2010

     511        112        95        648        320        1,686   

Charge for year

     497        48        11        617        188        1,361   

Cash paid

     (335     (43            (709     (22     (1,109

Reversals

     (26                   (1     (22     (49

Exchange and other movements

     12        2        21        7        7        49   

At 31 December 2010

     659        119        127        562        471        1,938   

Charge for year

     450        5        16        135        110        716   

Cash paid

     (377     (32     (17     (153     (78     (657

Reversals

     (55                          (85     (140

Exchange and other movements

     (13            16        (4     6        5   

At 31 December 2011

     664        92        142        540        424        1,862   

Charge for year

     873        22        19        90        92        1,096   

Cash paid

     (853     (27     (20     (513     (63     (1,476

Reversals

     (65                   (18     (91     (174

Exchange and other movements

     18        1        7        1        9        36   

At 31 December 2012

     637        88        148        100        371        1,344   
            
                      

2012

$m

   

2011

$m

   

2010

$m

 

Due within one year

                             916        1,388        1,095   

Due after more than one year

                             428        474        843   
                               1,344        1,862        1,938   

AstraZeneca is undergoing a global restructuring initiative which involves rationalisation of the Global Supply Chain, the Sales and Marketing Organisation, IS and business support infrastructure and R&D. Employee costs in connection with the initiatives are recognised in severance provisions.

Details of the environmental and legal provisions are provided in Note 25.

Employee benefit provisions include the executive deferred bonus plan. Further details are included in Note 24.

Other provisions comprise amounts relating to specific contractual or constructive obligations and disputes.

No provision has been released or applied for any purpose other than that for which it was established.

18 Post-retirement benefits

Pensions

Background

The Company and most of its subsidiaries offer retirement plans which cover the majority of employees in the Group. Many of these plans are ‘defined contribution’, where AstraZeneca’s contribution and resulting charge is fixed at a set level or is a set percentage of employees’ pay. However, several plans, mainly in the UK, the US and Sweden, are ‘defined benefit’, where benefits are based on employees’ length of service and average final salary (typically averaged over one, three or five years). The major defined benefit plans, apart from the collectively bargained Swedish plan (which is still open to employees born before 1979), have been closed to new entrants since 2000.

The major defined benefit plans are funded through legally separate, fiduciary-administered funds. The cash funding of the plans, which may from time to time involve special payments, is designed, in consultation with independent qualified actuaries, to ensure that the assets together with future contributions should be sufficient to meet future obligations. The funding is monitored rigorously by AstraZeneca and appropriate fiduciaries specifically with reference to AstraZeneca’s credit rating, market capitalisation, cash flows and the solvency of the relevant pension scheme.

Financing Principles

97% of the Group’s defined benefit obligations at 31 December 2012 are in schemes within the UK, the US, Sweden or Germany. In these countries, the pension obligations are funded with reference to the following financing principles:

 

> The Group has a fundamental belief in funding the benefits it promises to employees.
> The Group considers its pension arrangements in the context of its broader capital structure. In general, it does not believe in committing excessive capital for funding while it has better uses of capital within the business nor does it wish to generate surpluses.
> The pension funds are not part of the Group’s core business. The Group believes in taking some rewarded risks with the investments underlying the funding, subject to a medium to long-term plan to reduce those risks if opportunities arise.
> The Group recognises that deciding to hold certain investments may cause volatility in the funding position. The Group would not wish to amend its contribution level for relatively small deviations from its preferred funding level, because it is expected that there will be short-term volatility, but it is prepared to react appropriately to more significant deviations.
> In the event that local regulations require an additional level of financing, the Group would consider the use of alternative methods of providing this that do not require immediate cash funding but help mitigate exposure of the pension arrangement to the credit risk of the Group.

These principles are appropriate to AstraZeneca’s business at the present date; should circumstances change they may require review.

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   167

Table of Contents

Financial Statements | Notes to the Group Financial Statements

18 Post-retirement benefits continued

AstraZeneca has developed a funding framework to implement these principles. This determines the cash contributions payable to the pension funds, but does not affect the IAS 19 liabilities. To reduce the risk of committing excess capital to pension funds, liability valuations are based on the expected return on the actual pension assets, rather than a corporate bond yield. At present, this puts a different, lower value on the liabilities than IAS 19.

UK

With regard to the Group’s UK defined benefit fund, the above principles are modified in light of the UK regulatory requirements and resulting discussions with the Pension Fund Trustee. The most recent full actuarial valuation was carried out at 31 March 2010. The next valuation is due at 31 March 2013.

Under the agreed funding principles for the UK, cash contributions will be paid to the UK Pension Fund to target a level of assets in excess of the current expected cost of providing benefits. In addition, AstraZeneca will make contributions to an escrow account which will be held outside of the UK Pension Fund. The escrow account assets will be payable to the fund in agreed circumstances, for example, in the event of AstraZeneca and the Pension Fund Trustee agreeing on a change to the current long-term investment strategy.

The market value of the fund’s assets at the valuation date was £3,129m ($4,832m equivalent), representing 79% of the fund’s actuarially assessed liabilities (Technical Provisions). The Company agreed to fund the shortfall by making payments of £72.5m ($112m) a year until 31 December 2011 and then lump sum payments totalling £715m ($1,103m). The first of these lump sum payments of £180m ($278m) was paid into the UK Pension Fund in December 2011 from existing investments held in escrow for the Pension Fund. A further £300m ($463m) was paid into the UK Pension Fund during January 2012 from existing investments held in escrow and the balance will be paid in due course. This is in addition to the contributions required to meet the ongoing benefits accruing in the region of £24m ($37m) per annum . In 2011, £132m ($213m) was paid into the escrow account and a further £230m ($355m) was paid in during January 2012. At 31 December 2012, £462m ($748m) of escrow fund assets are included within other investments (see Note 10).

Under the agreed funding principles used to set the Technical Provisions, the key assumptions as at 31 March 2010 are as follows: long-term UK price inflation set at 3.8%  per annum , salary increases at 0% per annum (as a result of pensionable pay levels being frozen in 2010), pension increases at 3.55%  per annum and investment returns at 5.9%  per annum .

During the first half of 2010, following consultation with its UK employees’ representatives, AstraZeneca introduced a freeze on pensionable pay at 30 June 2010 levels for defined benefit members of the UK Pension Fund. The defined benefit fund remains open to existing members and employees who choose to leave the defined benefit fund will retain a deferred pension in addition to being offered membership in a new Group Self Invested Personal Pension Plan.

The amendment to the UK defined benefit fund to freeze pensionable pay at 30 June 2010 levels represents an accounting curtailment of certain pension obligations. The majority of members opted to remain in the defined benefit fund and continue benefit accrual with frozen pensionable pay. In accordance with IAS 19, the scheme obligations were revalued by the scheme actuaries immediately prior to the change and assumptions reviewed at that date. The resulting credit of $693m was recognised in profit in 2010.

Rest of Group

The IAS 19 positions as at 31 December 2012 are shown below for each of the other countries with significant defined benefit plans. These plans account for 92% of the Group’s defined benefit obligations outside of the UK. These plans are funded in line with the financing principles and contributions paid as prescribed by the funding framework.

 

> The US defined benefits programme was actuarially revalued at 31 December 2012, when plan obligations were $1,917m and plan assets were $1,679m. This includes obligations in respect of the non-qualified plan which is largely unfunded.
> The Swedish defined benefits programme was actuarially revalued at 31 December 2012, when plan obligations were estimated to amount to $1,889m and plan assets were $1,125m.
> The German defined benefits programme was actuarially revalued at 31 December 2012, when plan obligations amounted to $355m and plan assets were $23m.

On current bases, it is expected that contributions (excluding those in respect of past service cost) during the year ending 31 December 2013 to the four main countries will be $537m.

Post-retirement benefits other than pensions

In the US, and to a lesser extent in certain other countries, AstraZeneca’s employment practices include the provision of healthcare and life assurance benefits for retired employees. As at 31 December 2012, some 3,528 retired employees and covered dependants currently benefit from these provisions and some 8,893 current employees will be eligible on their retirement. AstraZeneca accrues for the present value of such retiree obligations over the working life of the employee. In practice, these benefits will be funded with reference to the financing principles.

The cost of post-retirement benefits other than pensions for the Group in 2012 was $16m (2011: $12m; 2010: $18m). Plan assets were $301m and plan obligations were $363m at 31 December 2012. These benefit plans have been included in the disclosure of post-retirement benefits under IAS 19.

 

168   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

18 Post-retirement benefits continued

Financial assumptions

Qualified independent actuaries have updated the actuarial valuations under IAS 19 of the major defined benefit schemes operated by the Group to 31 December 2012. The assumptions used by the actuaries are chosen from a range of possible actuarial assumptions which, due to the long-term nature of the schemes, may not necessarily be borne out in practice. These assumptions were as follows:

 

     2012      2011  
     UK     Rest of Group      UK     Rest of Group  

Inflation assumption

     3.1%        2.2%         3.2%        2.3%   

Rate of increase in salaries

     1       3.4%         1       3.4%   

Rate of increase in pensions in payment

     2.9%        1.1%         3.1%        0.9%   

Discount rate

     4.5%        3.6%         4.8%        4.1%   

Long-term rate of return expected at 31 December

         

Equities

     7.5%        7.4%         7.5%        7.4%   

Bonds

     4.2%        3.3%         4.5%        3.8%   

Others

     2.8%        4.0%         2.8%        3.8%   

Rate of increase in medical costs (initial rate)

     10.0%        8.2%         10.0%        9.0%   

 

1   Pensionable pay frozen at 30 June 2010 levels following UK fund changes.

The expected return on assets is determined with reference to the expected long-term level of dividends, interest and other returns derived from the plan assets, together with realised and unrealised gains or losses on the plan assets, less any costs of administering the plan, less any tax payable by the plan. The expected returns are based on long-term market expectations and analysed on a regular basis to ensure that any sustained movements in underlying markets are reflected.

Demographic assumptions

The mortality assumptions are based on country-specific mortality tables. These are compared to actual AstraZeneca experience and adjusted where sufficient data is available. Additional allowance for future improvements in life expectancy is included for all major schemes where there is credible data to support this continuing trend.

The table below illustrates life expectancy assumptions at age 65 for male members retiring in 2012 and members expected to retire in 2032 (2011: 2011 and 2031 respectively).

 

     Life expectancy assumption for a male member retiring at age 65  

Country

   2012      2032      2011      2031  

UK

     23.1         24.8         22.9         24.7   

US

     20.1         21.5         20.0         21.4   

Sweden

     20.4         22.4         20.4         22.4   

Germany

     18.6         21.3         18.3         21.0   

Post-retirement scheme deficit

The assets and obligations of the defined benefit schemes operated by the Group at 31 December 2012, as calculated in accordance with IAS 19 ‘Employee Benefits’, are shown below. The fair values of the schemes’ assets are not intended to be realised in the short term and may be subject to significant change before they are realised. The present value of the schemes’ obligations is derived from cash flow projections over long periods and is therefore inherently uncertain.

 

     2012     2011  
    

UK

$m

   

    Rest of Group

$m

   

Total

                     $m

   

UK

                     $m

   

    Rest of Group

$m

   

Total

                     $m

 

 

Scheme assets

            

Equities

     2,828        1,147        3,975        2,221        1,084        3,305   

Bonds

     3,280        1,660        4,940        2,961        1,382        4,343   

Others

     742        336        1,078        506        365        871   

Total fair value of scheme assets

     6,850        3,143        9,993        5,688        2,831        8,519   

Present value of scheme obligations

     (7,740     (4,524     (12,264     (7,042     (4,157     (11,199

Past service cost not yet recognised

            6        6               6        6   

Deficit in the scheme as recognised

in the statement of financial position

     (890     (1,375     (2,265     (1,354     (1,320     (2,674

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   169

Table of Contents

Financial Statements | Notes to the Group Financial Statements

18 Post-retirement benefits continued

Fair value of scheme assets

     2012     2011  
    

UK

$m

   

Rest of Group

$m

   

Total

$m

   

UK

$m

   

Rest of Group

$m

   

Total

$m

 

At beginning of year

     5,688        2,831        8,519        5,149        2,618        7,767   

Expected return on scheme assets

     342        144        486        340        162        502   

Expenses

     (5            (5     (7            (7

Actuarial gains/(losses)

     275        207        482        (4     35        31   

Settlements

            (61     (61                     

Exchange

     289        26        315               (38     (38

Employer contributions

     584        262        846        487        246        733   

Participant contributions

     8               8        9        3        12   

Benefits paid

     (331     (266     (597     (286     (195     (481

Scheme assets’ fair value at end of year

     6,850        3,143        9,993        5,688        2,831        8,519   

 

The actual return on the plan assets was a gain of $968m (2011: gain of $533m).

 

Movement in post-retirement scheme obligations

  

  

     2012     2011  
    

UK

$m

   

Rest of Group

$m

   

Total

$m

   

UK

$m

   

Rest of Group

$m

   

Total

$m

 

Present value of obligation in scheme at beginning of year

     (7,042     (4,157     (11,199     (6,554     (3,691     (10,245

Current service cost

     (41     (108     (149     (49     (110     (159

Past service cost

     (77     (50     (127     (32     (37     (69

Participant contributions

     (8            (8     (9     (3     (12

Benefits paid

     331        266        597        286        195        481   

Other finance expense

     (343     (164     (507     (364     (175     (539

Expenses

     5               5        7               7   

Actuarial loss

     (224     (343     (567     (328     (444     (772

Settlements and curtailments

            111        111               53        53   

Exchange

     (341     (79     (420     1        55        56   

Present value of obligations in scheme at end of year

     (7,740     (4,524     (12,264     (7,042     (4,157     (11,199

The obligation arises from the following plans:

 

  

     2012     2011  
    

UK

$m

   

Rest of Group

$m

   

Total

$m

   

UK

$m

   

Rest of Group

$m

   

Total

$m

 

Funded

     (7,709     (3,961     (11,670     (7,016     (3,689     (10,705

Unfunded

     (31     (563     (594     (26     (468     (494

Total

     (7,740     (4,524     (12,264     (7,042     (4,157     (11,199

Consolidated Statement of Comprehensive Income disclosures

The amounts that have been charged to the consolidated statement of comprehensive income, in respect of defined benefit schemes for the year ended 31 December 2012, are set out below:

 

  

   

     2012     2011  
    

UK

$m

   

Rest of Group

$m

   

Total

$m

   

UK

$m

   

Rest of Group

$m

   

Total

$m

 

 

Operating profit

            

Current service cost

     (41     (108     (149     (49     (110     (159

Past service cost

     (77     (50     (127     (32     (37     (69

Settlements and curtailments

            50        50               53        53   

Total charge to operating profit

     (118     (108     (226     (81     (94     (175

 

Finance expense

            

Expected return on post-retirement scheme assets

     342        144        486        340        162        502   

Interest on post-retirement scheme obligations

     (343     (164     (507     (364     (175     (539

Net return

     (1     (20     (21     (24     (13     (37

Charge before taxation

     (119     (128     (247     (105     (107     (212

 

Other comprehensive income

            
Difference between the actual return and the expected return on the post-retirement scheme assets      275        207        482        (4     35        31   

Experience losses arising on the post-retirement scheme obligations

     (12     (147     (159     (11     (10     (21
Changes in assumptions underlying the present value of the post-retirement scheme obligations      (212     (196     (408     (317     (434     (751

Actuarial gains/(losses) recognised

     51        (136     (85     (332     (409     (741

 

170   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

18 Post-retirement benefits continued

Included in total assets and obligations for the UK is $427m (2011: $388m) in respect of members’ defined contribution sections of the scheme. Group costs in respect of defined contribution schemes during the year were $249m (2011: $262m). $127m past service cost in 2012 relates predominantly to enhanced pensions on early retirement in the UK and Sweden. $50m settlements and curtailments credit in 2012 predominantly relate to a settlement credit of $30m recognised in the US, where a proportion of deferred inactive participants who are not yet eligible for retirement elected to exchange their plan benefit for immediate cash lump sums, and a $25m curtailment credit recognised in Sweden as a consequence of the Södertälje site closure. During 2011, the Group disposed of Astra Tech (see Note 22) resulting in a curtailment gain of $44m.

Actuarial gains and losses

                 2012                 2011                 2010                 2009                 2008  

 

UK

          

Present value of obligations ($m)

     (7,740     (7,042     (6,554     (7,055     (5,029

Fair value of scheme assets ($m)

     6,850        5,688        5,149        4,853        3,835   

Deficit in the scheme ($m)

     (890     (1,354     (1,405     (2,202     (1,194

Experience adjustments on:

          

Scheme assets

          

Amount ($m)

     275        (4     244        293        (1,185

Percentage of scheme assets

     4.0%        0.1%        4.7%        6.0%        30.9%   

Scheme obligations

          

Amount ($m)

     (224     (328     (221     (1,218     972   

Percentage of scheme obligations

     2.9%        4.7%        3.4%        17.3%        19.3%   

 

Rest of Group

          

Present value of obligations ($m)

     (4,524     (4,157     (3,691     (3,591     (3,591

Fair value of scheme assets ($m)

     3,143        2,831        2,618        2,402        2,013   

Deficit in the scheme ($m)

     (1,381     (1,326     (1,073     (1,189     (1,578

 

Experience adjustments on:

          

Scheme assets

          

Amount ($m)

     207        35        (4     180        (700

Percentage of scheme assets

     6.6%        1.2%        0.2%        7.5%        34.8%   

 

Scheme obligations

          

Amount ($m)

     (343     (444     (65     176        (319

Percentage of scheme obligations

     7.6%        10.7%        1.8%        4.9%        8.9%   

 

Total

          

Present value of obligations ($m)

     (12,264     (11,199     (10,245     (10,646     (8,620

Fair value of scheme assets ($m)

     9,993        8,519        7,767        7,255        5,848   

Deficit in the scheme ($m)

     (2,271     (2,680     (2,478     (3,391     (2,772

 

Experience adjustments on:

          

Scheme assets

          

Amount ($m)

     482        31        240        473        (1,885

Percentage of scheme assets

     4.8%        0.4%        3.1%        6.5%        32.2%   

 

Scheme obligations

          

Amount ($m)

     (567     (772     (286     (1,042     653   

Percentage of scheme obligations

     4.6%        6.9%        2.8%        9.8%        7.6%   

Transactions with pension schemes

In 2011, the Group made loans to the UK and Swedish pension schemes to enable these schemes to manage their short-term liquidity requirements. The maximum balance outstanding in 2012 was $1m and the amount outstanding at 31 December 2012 was $1m.

Reserves

Included within the retained earnings reserve are accumulated actuarial gains and losses, and related deferred tax balances. Movements on this balance are as follows:

 

    

2012

                $m

   

2011

                $m

   

2010

                $m

 

At 1 January

     (2,447     (1,865     (1,800

Actuarial losses

     (85     (741     (46

Deferred tax

     (46     159        (19

At 31 December

     (2,578     (2,447     (1,865

The cumulative amount of actuarial losses before deferred tax recognised in other comprehensive income is $3,308m (2011: $3,223m; 2010: $2,482m).

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   171

Table of Contents

Financial Statements | Notes to the Group Financial Statements

18 Post-retirement benefits continued

Discount rate sensitivity

The following table shows the US dollar effect of a 1% change in the discount rate on the retirement benefits obligations in our four main defined benefit pension obligation countries.

 

                                                                                           
     2012     2011  
     +1%      –1%     +1%      –1%  

UK ($m)

     1,028         (1,201     934         (1,088

US ($m)

     224         (257     229         (262

Sweden ($m)

     370         (466     299         (374

Germany ($m)

     63         (77     41         (49

Total ($m)

     1,685         (2,001     1,503         (1,773

Sensitivity of medical cost assumptions

 

  

     Effect of change in medical cost assumption increase/(decrease)  
     2012     2011  
     +1%      –1%     +1%      –1%  

Current service and interest cost of net periodic post-employment medical costs ($m)

     1         (1     1         (1

Accumulated post-employment benefit obligation for medical costs ($m)

     11         (12     10         (10

19 Reserves

Retained earnings

The cumulative amount of goodwill written off directly to reserves resulting from acquisitions, net of disposals, amounted to $685m (2011: $680m; 2010: $682m) using year end rates of exchange. At 31 December 2012, 55,555 shares, at a cost of $4m, have been deducted from retained earnings (2011: 36,177 shares, at a cost of $2m; 2010: 57,717 shares, at a cost of $3m).

There are no significant statutory or contractual restrictions on the distribution of current profits of subsidiaries, joint ventures or associates; undistributed profits of prior years are, in the main, permanently employed in the businesses of these companies. The undistributed income of AstraZeneca companies overseas might be liable to overseas taxes and/or UK taxation (after allowing for double taxation relief) if they were to be distributed as dividends (see Note 4).

 

                                                                    
    

2012

$m

   

2011

$m

   

2010

$m

 

 

Cumulative translation differences included within retained earnings

      

Balance at beginning of year

     1,760        1,798        1,656   

Foreign exchange arising on consolidation

     106        (60     26   

Exchange adjustments on goodwill (recorded against other reserves)

     5        (2     15   

Foreign exchange differences on borrowings designated in net investment hedges

     (46     24        101   

Fair value movement on derivatives designated in net investment hedges

     76                 

Net exchange movement in retained earnings

     141        (38     142   

Balance at end of year

     1,901        1,760        1,798   

Other reserves

The other reserves arose from the cancellation of £1,255m of share premium account by the Company in 1993 and the redenomination of share capital ($157m) in 1999. The reserves are available for writing off goodwill arising on consolidation and, subject to guarantees given to preserve creditors at the date of the court order, are available for distribution.

 

20 Share capital of the Company

                                                              
     Allotted, called-up and fully paid  
    

2012

$m

    

2011

$m

    

2010

$m

 

Issued Ordinary Shares ($0.25 each)

     312         323         352   

Redeemable Preference Shares (£1 each – £50,000)

                       
       312         323         352   

The Redeemable Preference Shares carry limited class voting rights and no dividend rights. This class of shares is capable of redemption at par at the option of the Company on the giving of seven days’ written notice to the registered holder of the shares.

The movements in the number of Ordinary Shares during the year can be summarised as follows:

 

                                                                    
     No. of shares  
     2012     2011     2010  

At 1 January

     1,292,355,052        1,409,023,452        1,450,958,562   

Issues of shares

     12,241,784        10,739,989        11,756,397   

Repurchase of shares

     (57,817,288     (127,408,389     (53,691,507

At 31 December

     1,246,779,548        1,292,355,052        1,409,023,452   

 

172   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

20 Share capital of the Company continued

Share repurchases

During the year, the Company repurchased 57.8m Ordinary Shares at an average price of 2879 pence per share (2011: 127.4m Ordinary Shares at an average price of 2932 pence per share; 2010: 53.7m Ordinary Shares at an average price of 3111 pence per share). These shares were subsequently cancelled.

Share schemes

A total of 12.2m Ordinary Shares were issued during the year in respect of share schemes (2011: 10.7m Ordinary Shares; 2010: 11.8m Ordinary Shares). Details of movements in the number of Ordinary Shares under option are shown in Note 24; details of options granted to Directors are shown in the Directors’ Remuneration Report from page 122.

Shares held by subsidiaries

No shares in the Company were held by subsidiaries in any year.

21 Dividends to shareholders

                                                                                                     
    

2012

Per share

    

2011

Per share

    

2010

Per share

    

2012

$m

    

2011

$m

    

2010

$m

 

Final

     $1.95         $1.85         $1.71         2,495         2,594         2,484   

Interim

     $0.90         $0.85         $0.70         1,124         1,158         1,010   
       $2.85         $2.70         $2.41         3,619         3,752         3,494   

The second interim dividend, to be confirmed as final, is $1.90 per Ordinary Share and $2,369m in total. This will be payable on 18 March 2013.

On payment of the dividends, exchange gains of $3m (2011: gains of $3m; 2010: gains of $19m) arose. These exchange gains are included in Note 3.

22 Acquisitions and disposals

2012 acquisitions

Ardea

On 19 June 2012, AstraZeneca completed the acquisition of Ardea. Ardea is a US (San Diego, California) based biotechnology company focused on the development of small molecule therapeutics for the treatment of serious diseases. AstraZeneca acquired 100% of Ardea’s shares for cash consideration of $1,268m. The acquisition strengthens our research and development capabilities in the respiratory and inflammation therapy area.

In most business acquisitions, there is a part of the cost that is not capable of being attributed in accounting terms to identifiable assets and liabilities acquired and is therefore recognised as goodwill. In the case of the acquisition of Ardea, this goodwill is underpinned by a number of elements, which individually cannot be quantified. Most significant among these is the premium attributable to a highly-skilled workforce and established experience in the field of gout.

Ardea’s results have been consolidated into the Group’s results from 20 June 2012. For the period from acquisition to 31 December 2012, Ardea’s revenues were immaterial, in the context of the Group’s revenue, and its loss after tax was $43m. If the acquisition had taken effect at the beginning of the reporting period (1 January 2012), on a pro forma basis, the revenue of the combined Group for 2012 would have been unchanged and the profit after tax would have been $6,245m. This pro forma information has been prepared taking into account any amortisation, interest costs and related tax effects but does not purport to represent the results of the combined Group that actually would have occurred had the acquisition taken place on 1 January 2012 and should not be taken to be representative of future results.

 

                                                  
    

Book value

$m

   

Fair value

adjustment

$m

   

Fair value

$m

 

 

Non-current assets:

      

Intangible assets

            1,464        1,464   

Other

     4               4   
       4        1,464        1,468   

Current assets

     199               199   

Current liabilities

     (31     (1     (32

 

Non-current liabilities:

      

Deferred tax liabilities

            (397     (397

Total assets acquired

     172        1,066        1,238   

Goodwill

                     30   

Consideration

                     1,268   

Less: Cash and cash equivalents acquired

                     (81

Net cash outflow

                     1,187   

Acquisition costs arising on the acquisition of $12m were expensed within selling, general and administrative costs in 2012.

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   173

Table of Contents

Financial Statements | Notes to the Group Financial Statements

22 Acquisitions and disposals continued

2011 disposals

Astra Tech

On 31 August 2011, the Group completed the sale of the Astra Tech business to DENTSPLY International Inc. On the loss of control, the Group derecognised the assets and liabilities of the subsidiary. The surplus arising on the loss of control is recognised in profit. Astra Tech’s results were consolidated for the period until disposal and contributed $386m in 2011 (2010: $535m) in revenue and $16m in 2011 (2010: $55m) in profit after tax.

 

     $m  

Non-current assets

     281   

Current assets

     193   

Current liabilities

     (104

Non-current liabilities

     (91

Net book value of assets disposed

     279   

Fees and other disposal costs

     59   

Exchange recycled on disposal

     (26

Profit on disposal

     1,483   

Consideration

     1,795   

Less: Cash held in disposed undertaking

     (23

Net cash consideration

     1,772   

The gain on disposal of Astra Tech is non-taxable.

2010 acquisitions

Novexel

On 3 March 2010, AstraZeneca completed the acquisition of Novexel. Novexel is a research company focused on the infection therapy area and is based in France. This acquisition strengthens our research capabilities in the infection therapy area. AstraZeneca acquired 100% of Novexel’s shares for an upfront consideration of $427m; with additional consideration of up to $75m becoming payable to Novexel shareholders on the completion of certain development milestones. At both the date of acquisition and at 31 December 2010, the fair value of this contingent consideration was $50m. For the ten month period post-acquisition to the end of 2010 and the full 2010 year, Novexel had no revenues and its loss was immaterial.

 

     Book value
$m 		   

Fair value

adjustment

$m

   

Fair value

$m

 

Non-current assets

     1        548        549   

Current assets

     89               89   

Current liabilities

     (18            (18

Non-current liabilities

     (85     (58     (143

Total assets acquired

     (13     490        477   

Goodwill

                       

Fair value of total consideration

                     477   

Less: Fair value of contingent consideration

                     (50

Total upfront consideration

                     427   

Less: Cash and cash equivalents acquired

                     (79

Net cash outflow

                     348   

Subsequent to the completion of the acquisition of Novexel, AstraZeneca entered into a collaboration with Forest on the future co-development and commercialisation of two late-stage antibiotic development programmes acquired with Novexel: ceftazidime/NXL-104 (CAZ-104) and ceftaroline/NXL-104 (CEF-104). These antibiotic combinations utilise Novexel’s novel investigational beta-lactamase inhibitor NXL-104 to overcome antibiotic resistance and treat the increasing number of infections resistant to existing therapies. In addition, Forest acquired rights to CAZ-104 in North America and bought down payment obligations to Novexel in relation to CEF-104 from previous existing licence arrangements. In consideration for these rights, Forest paid Novexel, then an AstraZeneca Group company, a sum of $210m on 3 March 2010 and will also pay additional sums equivalent to half of any future specified development milestone payments that become payable by AstraZeneca. This consideration is equivalent to the fair value attributed on acquisition to those assets and hence there was no profit impact from this divestment.

In 2011, the contingent consideration of $50m became fully payable. The fair value of the remaining contingent consideration arising on the Novexel acquisition is $nil.

 

174   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

23 Financial risk management objectives and policies

The Group’s principal financial instruments, other than derivatives, comprise bank overdrafts, finance leases, loans, current and non-current investments, cash and short-term deposits. The main purpose of these financial instruments is to manage the Group’s funding and liquidity requirements. The Group has other financial assets and liabilities such as trade receivables and trade payables, which arise directly from its operations.

The principal financial risks to which the Group is exposed are those of liquidity, interest rate, foreign currency and credit. Each of these is managed in accordance with Board-approved policies. These policies are set out below.

The Group uses foreign currency borrowings, foreign currency forwards, cross-currency swaps and interest rate swaps for the purpose of hedging its foreign currency and interest rate risks. The Group may designate certain financial instruments as either fair value hedges or net investment hedges in accordance with IAS 39. Key controls applied to transactions in derivative financial instruments are: to use only instruments where good market liquidity exists, to revalue all financial instruments regularly using current market rates and to sell options only to offset previously purchased options. The Group does not use derivative financial instruments for speculative purposes.

Capital management

The capital structure of the Group consists of shareholders’ equity (Note 20), debt (Note 14) and cash (Note 13). For the foreseeable future, the Board will maintain a capital structure that supports the Group’s strategic objectives through:

 

> managing funding and liquidity risk
> optimising shareholder return
> maintaining a strong, investment-grade credit rating.

Funding and liquidity risk are reviewed regularly by the Board and managed in accordance with policies described below.

The Board’s distribution policy comprises a regular cash dividend, and subject to business needs, a share repurchase component. The Board regularly reviews its shareholders’ return strategy and in 2012 decided to suspend share repurchases in order to retain strategic flexibility. In addition, we are restating our dividend cover target in terms of reported earnings adjusted for restructuring costs, intangible asset amortisation and impairments and other items as determined by the Group, and are targeting two times cover on this measure.

The Group’s net funds position (loans and borrowings net of cash and cash equivalents, current investments and derivative financial instruments) has decreased from $2,849m at the beginning of the year to a net debt position of $1,369m at 31 December 2012 as a result of reduced operating cash inflows, substantial investment activities and share repurchases in 2012, offset by reduced tax cash outflows and fixed deposits maturing in the year.

Liquidity risk

The Board reviews the Group’s ongoing liquidity risks annually as part of the planning process and on an ad hoc basis. The Board considers short-term requirements against available sources of funding, taking into account forecast cash flows. The Group manages liquidity risk by maintaining access to a number of sources of funding which are sufficient to meet anticipated funding requirements. Specifically, the Group uses US commercial paper, committed bank facilities and cash resources to manage short-term liquidity and manages long-term liquidity by raising funds through the capital markets. The Group is assigned short-term credit ratings of P-1 by Moody’s and A-1+ by Standard and Poor’s. The Group’s long-term credit rating is A1 negative outlook by Moody’s and AA- stable outlook by Standard and Poor’s.

In addition to cash and cash equivalents of $7,701m, fixed deposits of $46m, less overdrafts of $105m at 31 December 2012, the Group has committed bank facilities of $3.0bn available to manage liquidity. At 31 December 2012, the Group has issued $1,551m under a Euro Medium Term Note programme and $7,796m under a SEC-registered programme. The Group regularly monitors the credit standing of the banking group and currently does not anticipate any issue with drawing on the committed facilities should this be necessary. The committed facilities of $3.0bn mature in April 2017 and were undrawn at 31 December 2012.

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   175

Table of Contents

Financial Statements | Notes to the Group Financial Statements

23 Financial risk management objectives and policies continued

The maturity profile of the anticipated future contractual cash flows including interest in relation to the Group’s financial liabilities, on an undiscounted basis and which, therefore, differs from both the carrying value and fair value, is as follows:

 

    

Bank

overdrafts

and other

loans

$m

   

Bonds

$m

   

Finance

leases

$m

   

Trade

and other

payables

$m

    

Total

non-derivative

financial

instruments

$m

   

Interest

rate swaps

$m

   

Cross-

currency

swaps

$m

   

Total

derivative

financial

instruments

$m

   

Total

$m

 

Within one year

     128        518               8,640         9,286        (120            (120     9,166   

In one to two years

            2,268               373         2,641        (121            (121     2,520   

In two to three years

            423                       423        (87            (87     336   

In three to four years

            1,153                       1,153        (69            (69     1,084   

In four to five years

            1,379                       1,379        (50            (50     1,329   

In more than five years

            10,095                       10,095        (192            (192     9,903   
       128        15,836               9,013         24,977        (639            (639     24,338   

Effect of interest

     (3     (7,012                    (7,015     639               639        (6,376
Effect of discounting, fair values and issue costs             273                       273        (324            (324     (51

31 December 2010

     125        9,097               9,013         18,235        (324            (324     17,911   
                   
    

Bank

overdrafts

and other

loans

$m

   

Bonds

$m

   

Finance

leases

$m

   

Trade

and other

payables

$m

    

Total

non-derivative

financial

instruments

$m

   

Interest

rate swaps

$m

   

Cross-

currency

swaps

$m

   

Total

derivative

financial

instruments

$m

   

Total

$m

 

Within one year

     226        2,267               8,975         11,468        (117            (117     11,351   

In one to two years

            422               385         807        (84            (84     723   

In two to three years

            1,152                       1,152        (67            (67     1,085   

In three to four years

            1,352                       1,352        (49            (49     1,303   

In four to five years

            332                       332        (49            (49     283   

In more than five years

            9,764                       9,764        (137            (137     9,627   
       226        15,289               9,360         24,875        (503            (503     24,372   

Effect of interest

     (5     (6,490                    (6,495     503               503        (5,992
Effect of discounting, fair values and issue costs             308                       308        (362            (362     (54

31 December 2011

     221        9,107               9,360         18,688        (362            (362     18,326   
                   
    

Bank

overdrafts

and other

loans

$m

   

Bonds

$m

   

Finance

leases

$m

   

Trade

and other

payables

$m

    

Total

non-derivative

financial

instruments

$m

   

Interest

rate swaps

$m

   

Cross-

currency

swaps

$m

   

Total

derivative

financial

instruments

$m

   

Total

$m

 

Within one year

     881        484        23        9,221         10,609        (85     (12     (97     10,512   

In one to two years

            1,214        23        1,001         2,238        (67     (12     (79     2,159   

In two to three years

            1,435        23                1,458        (49     (12     (61     1,397   

In three to four years

            393        21                414        (49     (12     (61     353   

In four to five years

            2,143        11                2,154        (48     (12     (60     2,094   

In more than five years

            10,766                       10,766        (90     (96     (186     10,580   
       881        16,435        101        10,222         27,639        (388     (156     (544     27,095   

Effect of interest

     (2     (7,340     (17             (7,359     388        86        474        (6,885
Effect of discounting, fair values and issue costs             252                       252        (313     (6     (319     (67

31 December 2012

     879        9,347        84        10,222         20,532        (313     (76     (389     20,143   

Where interest payments are on a floating rate basis, it is assumed that rates will remain unchanged from the last business day of each year ended 31 December.

It is not expected that the cash flows in the maturity profile could occur significantly earlier or at significantly different amounts.

Market risk

Interest rate risk

The Group maintains a mix of fixed and floating rate debt. The portion of fixed rate debt was approved by the Board and any variation requires Board approval. A significant portion of the long-term debt entered into in 2007 in order to finance the acquisition of MedImmune has been held at fixed rates of interest. The Group uses interest rate swaps and forward rate agreements to manage this mix.

At 31 December 2012, the Group held interest rate swaps with a notional value of $1.8bn, converting the 5.4% callable bond maturing in 2014, and the 7% guaranteed debentures payable in 2023 to floating rates and partially converting the 5.9% callable bond maturing in 2017 to floating rates. No new interest rate swaps were entered into during 2012 or 2011. At 31 December 2012, swaps with a notional value of $0.75bn were designated in fair value hedge relationships and swaps with a notional value of $1.0bn related to debt designated as fair value through profit or loss. Designated hedges are expected to be effective and therefore the impact of ineffectiveness on profit is not expected to be material. The accounting treatment for fair value hedges and debt designated as fair value through profit or loss is disclosed in the Group Accounting Policies section from page 146.

The majority of surplus cash is currently invested in US dollar liquidity funds earning floating rates of interest.

 

176   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

23 Financial risk management objectives and policies continued

The interest rate profile of the Group’s interest-bearing financial instruments, as at 31 December 2012, 31 December 2011 and 31 December 2010 is set out below. In the case of current and non-current financial liabilities, the classification includes the impact of interest rate swaps which convert the debt to floating rate.

 

     2012      2011      2010  
    

Total

$m

    

Fixed rate

$m

    

Floating rate

$m

    

Total

$m

    

Fixed rate

$m

    

Floating rate

$m

    

Total

$m

    

Fixed rate

$m

    

Floating rate

$m

 

 

Financial liabilities

                          
Interest-bearing loans and borrowings                                                                                 

Current

     901         22         879         1,990         999         991         125                 125   

Non-current

     9,409         7,306         2,103         7,338         5,215         2,123         9,097         6,242         2,855   
       10,310         7,328         2,982         9,328         6,214         3,114         9,222         6,242         2,980   

 

Financial assets

                          

Fixed deposits

     46                 46         3,927                 3,927         1,107                 1,107   

Cash and cash equivalents

     7,701                 7,701         7,571                 7,571         11,068                 11,068   
       7,747                 7,747         11,498                 11,498         12,175                 12,175   

In addition to the financial assets above, there are $7,924m (2011: $8,747m; 2010: $7,829m) of other current and non-current asset investments and other financial assets on which no interest is received.

Foreign currency risk

The US dollar is the Group’s most significant currency. As a consequence, the Group results are presented in US dollars and exposures are managed against US dollars accordingly.

Translational

Approximately 62% of Group external sales in 2012 were denominated in currencies other than the US dollar, while a significant proportion of manufacturing and research and development costs were denominated in pounds sterling and Swedish krona. Surplus cash generated by business units is substantially converted to, and held centrally in, US dollars. As a result, operating profit and total cash flow in US dollars will be affected by movements in exchange rates.

This currency exposure is managed centrally, based on forecast cash flows including the principal currencies of Swedish krona (SEK), pounds sterling (GBP), euro (EUR), Australian dollar (AUD), Canadian dollar (CAD), Japanese yen (JPY), Romanian leu (RON) and Russian ruble (RUB). The impact of movements in exchange rates is mitigated significantly by the correlations which exist between the major currencies to which the Group is exposed and the US dollar. Monitoring of currency exposures and correlations is undertaken on a regular basis and hedging is subject to pre-execution approval.

Where there is non-US dollar debt and an underlying net investment of that amount in the same currency, the Group applies net investment hedging. As at 31 December 2012, 5.4% of interest-bearing loans and borrowings were denominated in pounds sterling and 9.6% of interest-bearing loans and borrowings were denominated in euros. Exchange differences on the retranslation of debt designated as net investment hedges are recognised in other comprehensive income to the extent that the hedge is effective. Any ineffectiveness is taken to profit. Exchange differences on foreign currency borrowings not designated in a hedge relationship are taken to profit.

During 2012, the Group entered into a cross-currency swap to convert $750m of the 1.95% 2019 maturing bond into fixed Japanese yen debt. This instrument was designated in a net investment hedge against the foreign currency risk of the Group’s Japanese yen net assets. Fair value movements on the revaluation of the cross-currency swap are recognised in other comprehensive income to the extent that the hedge is effective. Any ineffectiveness would be taken to profit.

Transactional

One hundred percent of the Group’s major transactional currency exposures on working capital balances, which typically extend for up to three months, are hedged, where practicable, using forward foreign exchange contracts against individual Group companies’ reporting currency. In addition, the Group’s external dividend, which is paid principally in pounds sterling and Swedish krona, is fully hedged from announcement to payment date. Foreign exchange gains and losses on forward contracts transacted for transactional hedging are taken to profit.

The table below sets out the principal foreign exchange contracts outstanding at 31 December 2012, 31 December 2011 and 31 December 2010 along with the underlying gross exposure as defined above.

 

    

GBP

$m

   

SEK

$m

   

EUR

$m

   

AUD

$m

   

JPY

$m

   

CAD

$m

   

RON

$m

   

RUB

$m

 

 

2010

                

Gross exposure

     732        (806     478        117        133        33        82        129   

Forward exchange contracts

     (38     806        (478     (117     (133     (33     (83     (129

Net exposure

     694 1                                          (1       

 

2011

                

Gross exposure

     (1,097     (785     588                109                212                102                112                230   

Forward exchange contracts

     1,097        785        (588     (109     (212     (102     (112     (230

Net exposure

                                                        

 

2012

                

Gross exposure

     (889     (1,055             472        65        257        54        112        259   

Forward exchange contracts

     889                1,055        (472     (65     (257     (54     (112     (259

Net exposure

                                                        

 

1   The sterling hedge position as at 31 December 2010 was updated in early January 2011.

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   177

Table of Contents

Financial Statements | Notes to the Group Financial Statements

23 Financial risk management objectives and policies continued

Sensitivity analysis

The sensitivity analysis set out below summarises the sensitivity of the market value of our financial instruments to hypothetical changes in market rates and prices. The range of variables chosen for the sensitivity analysis reflects our view of changes which are reasonably possible over a one-year period. Market values are the present value of future cash flows based on market rates and prices at the valuation date. For long-term debt, an increase in interest rates results in a decline in the fair value of debt.

The sensitivity analysis assumes an instantaneous 100 basis point change in interest rates in all currencies from their levels at 31 December 2012, with all other variables held constant. Based on the composition of our long-term debt portfolio as at 31 December 2012, a 1% increase in interest rates would result in an additional $30m in interest expense being incurred per year. The exchange rate sensitivity analysis assumes an instantaneous 10% change in foreign currency exchange rates from their levels at 31 December 2012, with all other variables held constant. The +10% case assumes a 10% strengthening of the US dollar against all other currencies and the -10% case assumes a 10% weakening of the US dollar.

Each incremental 10% movement in foreign currency exchange rates would have approximately the same effect as the initial 10% detailed in the table below and each 1% change in interest rates would have approximately the same effect as the 1% detailed in the table below.

31 December 2010

                                                                   
     Interest rates     Exchange rates  
     +1%      -1%     +10%     -10%  

Increase/(decrease) in fair value of financial instruments ($m)

     595         (684     36        (36

Impact on profit: (loss)/gain ($m)

                    (133     133   

Impact on equity: gain/(loss) ($m)

                    169        (169

31 December 2011

                                                                   
     Interest rates     Exchange rates  
     +1%      -1%     +10%     -10%  

Increase/(decrease) in fair value of financial instruments ($m)

     654         (777     (15     15   

Impact on profit: (loss)/gain ($m)

                    (190     190   

Impact on equity: gain/(loss) ($m)

                    175        (175

31 December 2012

                                                                   
     Interest rates     Exchange rates  
     +1%      -1%     +10%     -10%  

Increase/(decrease) in fair value of financial instruments ($m)

     853         (1,005     12        (12

Impact on profit: (loss)/gain ($m)

                    (231     231   

Impact on equity: gain/(loss) ($m)

                    243        (243

There has been no change in the methods and assumptions used in preparing the above sensitivity analysis over the three-year period.

Credit risk

The Group is exposed to credit risk on financial assets, such as cash balances (including fixed deposits and cash and cash equivalents), derivative instruments, trade and other receivables. The Group is also exposed in its net asset position to its own credit risk in respect of the 2023 debentures and 2014 bonds which are accounted for at fair value through profit and loss.

Trade and other receivables

Trade receivable exposures are managed locally in the operating units where they arise and credit limits are set as deemed appropriate for the customer. The Group is exposed to customers ranging from government-backed agencies and large private wholesalers to privately owned pharmacies, and the underlying local economic and sovereign risks vary throughout the world. Where appropriate, the Group endeavours to minimise risks by the use of trade finance instruments such as letters of credit and insurance. The Group establishes an allowance for impairment that represents its estimate of incurred losses in respect of specific trade and other receivables where it is deemed that a receivable may not be recoverable. When the debt is deemed irrecoverable, the allowance account is written off against the underlying receivable.

In the US, sales to three wholesalers accounted for approximately 73% of US sales (2011: three wholesalers accounted for approximately 75%; 2010: three wholesalers accounted for approximately 73%).

 

178   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

23 Financial risk management objectives and policies continued

The ageing of trade receivables at the reporting date was:

 

    

2012

$m

   

2011

$m

   

2010

$m

 

Not past due

     5,322        6,249        5,953   

Past due 0-90 days

     288        177        104   

Past due 90-180 days

     41        82        67   

Past due > 180 days

     45        122        123   
         5,696                  6,630                  6,247   
      
    

2012

$m

   

2011

$m

   

2010

$m

 

 

Movements in provisions for trade receivables

      

Balance at beginning of year

     66        81        81   

Income statement credit

            (10     (1

Amounts utilised, exchange and other movements

     (2     (5     1   

Balance at end of year

     64        66        81   

The allowance for impairment has been calculated based on past experience and is in relation to specific customers. Given the profile of our customers, including large wholesalers and government-backed agencies, no further credit risk has been identified with the trade receivables not past due other than those balances for which an allowance has been made.

Other financial assets

The Group may hold significant cash balances as part of its normal operations, with the amount of cash held at any point reflecting the level of cash flow generated by the business and the timing of the use of that cash. The majority of excess cash is centralised within the Group treasury entity and is subject to counterparty risk on the principal invested. This risk is mitigated through a policy of prioritising security and liquidity over return, and as such cash is only invested in high credit quality investments. Counterparty limits are set according to the assessed risk of each counterparty and exposures are monitored against these limits on a regular basis. The majority of the Group’s cash is invested in US dollar AAA-rated liquidity funds and short-term bank deposits.

The most significant concentration of financial credit risk at 31 December 2012 was $6,589m invested in five US dollar AAA-rated liquidity funds. The liquidity fund portfolios are managed by the related external third party fund managers to maintain the AAA rating. No more than 15% of fund value is invested within each individual fund. There were no other significant concentrations of financial credit risk at the reporting date.

All financial derivatives are transacted with commercial banks, in line with standard market practice. The Group has agreements with some bank counterparties whereby the parties agree to post cash collateral, for the benefit of the other, equivalent to the market valuation of the derivative positions above a predetermined threshold. The carrying value of such cash collateral held by the Group at 31 December 2012 was $230m (2011: $21m; 2010: $13m).

24 Employee costs and share plans for employees

Employee costs

The average number of people, to the nearest hundred, employed by the Group is set out in the table below. In accordance with the Companies Act 2006, this includes part-time employees.

 

     2012      2011      2010  

 

Employees

        

UK

     7,900         8,700         10,100   

Continental Europe

     16,100         19,200         20,100   

The Americas

     15,300         18,000         18,300   

Asia, Africa & Australasia

     14,200         13,900         13,200   

Continuing operations

     53,500                 59,800                 61,700   

Geographical distribution described in the table above is by location of legal entity employing staff. Certain staff will spend some or all of their activity in a different location.

The number of people employed by the Group at the end of 2012 was 51,700 (2011: 57,200; 2010: 61,100).

The costs incurred during the year in respect of these employees were:

 

    

2012

$m

    

2011

$m

    

2010

$m

 

Salaries

     4,192         4,631         4,837   

Social security costs

     664         783         693   

Pension costs

     525         490         501 1  

Other employment costs

     362         496         408   
         5,743                   6,400                   6,439   

 

1   Pension costs excludes gains of $791m arising from changes made to benefits under certain of the Group’s post-retirement benefit plans.

Severance costs of $846m are not included above (2011: $431m; 2010: $531m).

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   179

Table of Contents

Financial Statements | Notes to the Group Financial Statements

24 Employee costs and share plans for employees continued

The Directors believe that, together with the basic salary system, the Group’s employee incentive schemes provide competitive and market-related packages to motivate employees. They should also align the interests of employees with those of shareholders, as a whole, through long-term share ownership in the Company. The Group’s current UK, Swedish and US schemes are described below; other arrangements apply elsewhere.

Bonus plans

The AstraZeneca UK Performance Bonus Plan

Employees of participating AstraZeneca UK companies are invited to participate in this bonus plan, which rewards strong individual performance. Bonuses in respect of performance during 2012 will be paid in cash, as they were in 2011 and 2010. The Company also offers UK employees the opportunity to buy Partnership Shares (Ordinary Shares). Employees may invest up to £1,500 over a 12 month accumulation period and purchase Partnership Shares in the Company with the total proceeds at the end of the period. The purchase price for the shares is the lower of the price at the beginning or the end of the 12 month period. In 2010, the Company introduced a Matching Share element in respect of Partnership Shares, the first award of which was made in 2011. Partnership Shares and Matching Shares are held in the HM Revenue & Customs (HMRC)-approved All-Employee Share Plan. At the Company’s AGM in 2002, shareholders approved the issue of new shares for the purposes of the All-Employee Share Plan.

The AstraZeneca Executive Annual Bonus Scheme

This scheme is a performance bonus scheme for Directors and senior employees who do not participate in the AstraZeneca UK Performance Bonus Plan. Annual bonuses are paid in cash and reflect both corporate and individual performance measures. The Remuneration Committee has discretion to reduce or withhold bonuses if business performance falls sufficiently short of expectations in any year such as to make the payment of bonuses inappropriate.

The AstraZeneca Deferred Bonus Plan

This plan was introduced in 2006 and is used to defer a portion of the bonus earned under the AstraZeneca Executive Annual Bonus Scheme into Ordinary Shares in the Company for a period of three years. The plan currently operates only in respect of Executive Directors and members of the SET. Awards of shares under this plan are typically made in February each year, the first award having been made in February 2006.

Sweden

In Sweden, an all-employee performance bonus plan is in operation, which rewards strong individual performance. Bonuses are paid 50% into a fund investing in AstraZeneca equities and 50% in cash. The AstraZeneca Executive Annual Bonus Scheme, the AstraZeneca Performance Share Plan and the AstraZeneca Global Restricted Stock Plan all operate in respect of relevant AstraZeneca employees in Sweden.

US

In the US, there are two all-employee short-term or annual performance bonus plans in operation to differentiate and reward strong individual performance. Annual bonuses are paid in cash. There is also one senior staff long-term incentive scheme, under which 76 participants may be eligible for awards granted as AstraZeneca ADSs. AstraZeneca ADSs necessary to satisfy the awards are purchased in the market or funded via a share trust. The AstraZeneca Performance Share Plan and the AstraZeneca Global Restricted Stock Plan operate in respect of relevant employees in the US.

Share plans

The charge for share-based payments in respect of share plans is $139m (2011: $153m; 2010: $120m). The plans are equity settled.

The AstraZeneca Performance Share Plan

This plan was approved by shareholders in 2005 for a period of 10 years. Generally, awards can be granted at any time, but not during a close period of the Company. The first grant of awards was made in June 2005. The main grant of awards in 2012 under the plan was in March, with a further smaller grant in August. Awards granted under the plan vest after three years and can be subject to the achievement of performance conditions. For awards to all participants in 2012, except employees of MedImmune, 50% of the award will vest subject to the performance of the Company’s total shareholder return (TSR) compared with that of a selected peer group of other pharmaceutical companies, and 50% will vest subject to the achievement of a net cash flow target. A separate performance condition applies to employees of MedImmune. The Remuneration Committee has responsibility for agreeing any awards under the plan and for setting the policy for the way in which the plan should be operated, including agreeing performance targets and which employees should be invited to participate. Further details of this plan can be found in the Directors’ Remuneration Report from page 122.

 

    

Shares

’000

     WAFV 1
pence 		    

WAFV 1

$

 

Shares awarded in March 2010

     2,002         1495         22.38   

Shares awarded in May 2010

     436         1431         21.48   

Shares awarded in August 2010

     139         1614         24.95   

Shares awarded in November 2010

     4         n/a         25.11   

Shares awarded in March 2011

               2,964                   1427                   23.09   

Shares awarded in August 2011

     127         1421         23.33   

Shares awarded in March 2012

     3,283         1403         22.41   

Shares awarded in August 2012

     38         1480         23.50   

 

1   Weighted average fair value.

 

180   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

24 Employee costs and share plans for employees continued

The AstraZeneca Investment Plan

This plan was introduced in 2010 and approved by shareholders at the 2010 AGM. The main grant of awards in 2012 under the plan was in March, with a further smaller grant in October. Awards granted under the plan vest after eight years and are subject to performance conditions measured over a period of between three and eight years. For awards granted in 2012, the performance conditions relate to the annual dividend paid to shareholders and dividend cover over a four year performance period. The awards are then subject to a four year holding period before they can vest. The Remuneration Committee has responsibility for agreeing any awards under the plan and for setting the policy for the way in which the plan should be operated, including agreeing performance targets and which employees should be invited to participate. Further details of this plan can be found in the Directors’ Remuneration Report from page 122.

 

    

Shares

’000

    

        WAFV

pence

    

        WAFV

$

 

Shares awarded in May 2010

     76         2575         38.66   

Shares awarded in August 2010

     15         2904         n/a   

Shares awarded in March 2011

     95         2853         46.18   

Shares awarded in August 2011

     3         2841         n/a   

Shares awarded in March 2012

     113         2805         44.82   

Shares awarded in October 2012

     69         2894         n/a   

The AstraZeneca Global Restricted Stock Plan

This plan was introduced in 2010. The main grant of awards in 2012 under the plan was in March, with a further smaller grant in August. This plan provides for the grant of restricted stock unit (RSU) awards to selected below SET-level employees and is used in conjunction with the AstraZeneca Performance Share Plan to provide a mix of RSUs and performance shares. Awards typically vest on the third anniversary of the date of grant and are contingent on continued employment with the Company. The Remuneration Committee has responsibility for agreeing any awards under the plan and for setting the policy for the way in which the plan should be operated.

 

    

Shares

’000

    

        WAFV

pence

    

        WAFV

$

 

Shares awarded in March 2010

     2,672         2989         44.75   

Shares awarded in August 2010

     8         3227         49.89   

Shares awarded in March 2011

     2,706         2853         46.18   

Shares awarded in August 2011

     54         2841         46.65   

Shares awarded in March 2012

     2,916         2805         44.82   

Shares awarded in August 2012

     26         2959         47.00   

The AstraZeneca Restricted Share Plan

This plan was introduced in 2008 and provides for the grant of restricted share awards to key employees, excluding Executive Directors. Awards are made on an ad hoc basis with variable vesting dates. The plan has been used five times in 2012 to make awards to 161 employees. The Remuneration Committee has responsibility for agreeing any awards under the plan and for setting the policy for the way in which the plan should be operated.

 

     Shares
’000 		             WAFV
pence 		             WAFV
$ 		 

Shares awarded in February 2010

     159         2954         47.70   

Shares awarded in May 2010

     25         2861         42.96   

Shares awarded in August 2010

     108         3227         49.89   

Shares awarded in November 2010

     27         n/a         50.21   

Shares awarded in December 2010

     20         n/a         48.30   

Shares awarded in January 2011

     2         2955         n/a   

Shares awarded in February 2011

     136         3030         48.55   

Shares awarded in March 2011

     29         n/a         46.37   

Shares awarded in May 2011

     14         3052         50.45   

Shares awarded in July 2011

     21         3026         n/a   

Shares awarded in August 2011

     27         2841         46.65   

Shares awarded in November 2011

     10         n/a         49.02   

Shares awarded in February 2012

     10         3067         48.20   

Shares awarded in March 2012

     371         2805         44.82   

Shares awarded in July 2012

     5         n/a         46.94   

Shares awarded in August 2012

     188         2959         47.00   

Shares awarded in October 2012 1

     69         2894         n/a   

 

1   This is an award of restricted shares, granted to Pascal Soriot under an arrangement, the details of which are identical to the rules of the AstraZeneca Restricted Share Plan.

The fair values were determined using a modified version of the binomial model. This method incorporated expected dividends but no other features into the measurements of fair value. The grant date fair values of share awards disclosed in this section do not take account of service and non-market related performance conditions.

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   181

Table of Contents

Financial Statements | Notes to the Group Financial Statements

24 Employee costs and share plans for employees continued

Share option plans

The charge for share-based payments in respect of share options is $7m (2011: $37m; 2010: $53m) which is comprised entirely of equity-settled transactions. At 31 December 2012, the only significant options outstanding were under the AstraZeneca Share Option Plan.

AstraZeneca Share Option Plan

This is a share option plan for employees of participating AstraZeneca Group companies which was approved by shareholders at the Company’s AGM in 2000 for a period of 10 years. The first grant of options occurred in August 2000. The final grant of options under the plan was in August 2009, since when no further grants have been or will be made. Options are not transferable. Options were granted over AstraZeneca Ordinary Shares or ADSs.

The price per Ordinary Share payable upon the exercise of an option is not less than an amount equal to the average of the middle-market closing price for an Ordinary Share or ADS of the Company on the London or New York Stock Exchange on the three consecutive dealing days immediately before the date of grant (or as otherwise agreed with HM Revenue & Customs). Where the option is an option to subscribe, the price payable upon exercise cannot be less than the nominal value of an Ordinary Share of the Company.

An option will normally be exercisable between three and 10 years following its grant provided any relevant performance condition has been satisfied. Options may be satisfied by the issue of new Ordinary Shares or by existing Ordinary Shares purchased in the market. The Remuneration Committee sets the policy for the Company’s operation of the plan including as regards whether any performance target(s) will apply to the grant and/or exercise of each eligible employee’s option. Options normally lapse on cessation of employment. Exercise is, however, permitted for a limited period following cessation of employment either for reasons of injury or disability, redundancy or retirement, or at the discretion of the Remuneration Committee, and on an amalgamation, take-over or winding-up of the Company.

 

             AstraZeneca Share Option Plan  
        

Options

’000

   

WAEP 1

pence

 

Options outstanding at 1 January 2010

         62,398        2601   

Options exercised

         (10,144     2538   

Options forfeited

         (3,189     2470   

Options outstanding at 31 December 2010

         49,065        2439   

Options exercised

         (10,408     2125   

Options forfeited

         (3,435     2933   

Options outstanding at 31 December 2011

         35,222        2484   

Options exercised

         (11,648     2219   

Options forfeited

         (3,861     3128   

Options outstanding at 31 December 2012

         19,713        2513   
                      

Range of exercise prices

                 1882 to 3335   

Weighted average remaining contractual life

                 1468 days   

Options exercisable

         19,713        2513   

 

1   Weighted average exercise price.

The fair value of options was estimated at the date of grant, being prior to 1 January 2010, using the Black-Scholes option pricing model based on weighted average exercise price, expected volatility, dividend yield, risk-free interest rates and expected lives. Expectations of early exercise were incorporated into the model.

The expected volatility was based on the historic volatility (calculated based on the weighted average remaining life of the share options) adjusted for any expected changes to future volatility due to publicly available information. No other features of options granted were incorporated into the measurement of fair value.

 

182   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

25 Commitments and contingent liabilities

 

    

2012

$m

    

        2011

$m

    

        2010

$m

 

Commitments

        
Contracts placed for future capital expenditure on property, plant and equipment and software development costs not provided for in these accounts      245         190         259   

Guarantees and contingencies arising in the ordinary course of business, for which no security has been given, are not expected to result in any material financial loss.

Research and development collaboration payments

The Group has various ongoing collaborations including in-licensing and similar arrangements with development partners. Such collaborations may require the Group to make payments on achievement of stages of development, launch or revenue milestones, although the Group generally has the right to terminate these agreements at no cost. The Group recognises research and development milestones as intangible assets once it is committed to payment, which is generally when the Group reaches set trigger points in the development cycle. Revenue-related milestones are recognised as intangible assets on product launch at a value based on the Group’s long-term revenue forecasts for the related product. The table below indicates potential development and revenue-related payments that the Group may be required to make under such collaborations.

 

    

Total

$m

   

Under 1 year

$m

   

Years 1 and 2

$m

   

Years 3 and 4

$m

   

Years 5

and greater

$m

 

Future potential research and development milestone payments

     3,129        296        584        699        1,550   

Future potential revenue milestone payments

     4,337               5        40        4,292   

The table includes all potential payments for achievement of milestones under ongoing research and development arrangements. Revenue-related milestone payments represent the maximum possible amount payable on achievement of specified levels of revenue as set out in individual contract agreements, but exclude variable payments that are based on unit sales (eg royalty-type payments) which are expensed as the associated sale is recognised. The table excludes any payments already capitalised in the financial statements for the year ended 31 December 2012.

The future payments we disclose represent contracted payments and, as such, are not discounted and are not risk adjusted. As detailed in the Principal risks and uncertainties section from page 75, the development of any pharmaceutical product candidate is a complex and risky process that may fail at any stage in the development process due to a number of factors (including items such as failure to obtain regulatory approval, unfavourable data from key studies, adverse reactions to the product candidate or indications of other safety concerns). The timing of the payments is based on the Group’s current best estimate of achievement of the relevant milestone.

Environmental costs and liabilities

The Group’s expenditure on environmental protection, including both capital and revenue items, relates to costs which are necessary for implementing internal systems and programmes, and meeting legal and regulatory requirements for processes and products.

They are an integral part of normal ongoing expenditure for carrying out the Group’s research, manufacturing and commercial operations and are not separated from overall operating and development costs. There are no known changes in legal, regulatory or other requirements resulting in material changes to the levels of expenditure for 2010, 2011 or 2012.

In addition to expenditure for meeting current and foreseen environmental protection requirements, the Group incurs costs in investigating and cleaning up land and groundwater contamination. In particular, AstraZeneca has environmental liabilities at some currently or formerly owned, leased and third party sites.

In the US, Zeneca Inc., and/or its indemnitees, have been named as potentially responsible parties (PRPs) or defendants at approximately 19 sites where Zeneca Inc. is likely to incur future environmental investigation, remediation, operation and maintenance costs under federal, state, statutory or common law environmental liability allocation schemes (together, US Environmental Consequences). Similarly, Stauffer Management Company LLC (SMC), which was established in 1987 to own and manage certain assets of Stauffer Chemical Company acquired that year, and/or its indemnitees, have been named as PRPs or defendants at 28 sites where SMC is likely to incur US Environmental Consequences. AstraZeneca has also given indemnities to third parties for a number of sites outside the US. These environmental liabilities arise from legacy operations that are not currently part of the Group’s business and, at most of these sites, remediation, where required, is either completed or nearing completion.

 

AstraZeneca has made provisions for the estimated costs of future environmental investigation, remediation, operation and maintenance activity beyond normal ongoing expenditure for maintaining the Group’s R&D and manufacturing capacity and product ranges, where a present obligation exists, it is probable that such costs will be incurred and they can be estimated reliably. With respect to such estimated future costs, there were provisions at 31 December 2012 in the aggregate of $88m (2011: $92m; 2010: $119m), mainly relating to the US. Where we are jointly liable or otherwise have cost-sharing agreements with third parties, we reflect only our share of the obligation. Where the liability is insured in part or in whole by insurance or other arrangements for reimbursement, an asset is recognised to the extent that this recovery is virtually certain.

It is possible that AstraZeneca could incur future environmental costs beyond the extent of our current provisions. The extent of such possible additional costs is inherently difficult to estimate due to a number of factors, including: (1) the nature and extent of claims that may be asserted in the future; (2) whether AstraZeneca has or will have any legal obligation with respect to asserted or unasserted claims; (3) the type of remedial action, if any, that may be selected at sites where the remedy is presently not known; (4) the potential for recoveries from or allocation of liability to third parties; and (5) the length of time that the environmental investigation, remediation and liability allocation process can take. Notwithstanding and subject to the foregoing, we estimate the potential additional loss for future environmental investigation, remediation, remedial operation and maintenance activity above and beyond our provisions to be, in aggregate, between $50m to $90m (2011: $50m to $90m; 2010: $20m to $40m) which relates solely to the US.

 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   183

Table of Contents

Financial Statements | Notes to the Group Financial Statements

 

25 Commitments and contingent liabilities continued

Legal proceedings

AstraZeneca is involved in various legal proceedings considered typical to its business, including actual or threatened litigation and/or actual or potential government investigations relating to employment matters, product liability, commercial disputes, pricing, sales and marketing practices, infringement of IP rights, the validity of certain patents and competition laws. The more significant matters are discussed below.

Most of the claims involve highly complex issues. Often these issues are subject to substantial uncertainties and, therefore, the probability of a loss, if any, being sustained and an estimate of the amount of any loss is difficult to ascertain. Consequently, for a majority of these claims, it is not possible to make a reasonable estimate of the expected financial effect, if any, that will result from ultimate resolution of the proceedings. In these cases, AstraZeneca discloses information with respect to the nature and facts of the cases.

With respect to each of the legal proceedings described below, other than those for which provision has been made, we are unable to make estimates of the possible loss or range of possible losses at this stage, other than as set forth in this section. We also do not believe that disclosure of the amount sought by plaintiffs, if known, would be meaningful with respect to those legal proceedings. This is due to a number of factors, including: (1) the stage of the proceedings (in many cases trial dates have not been set) and the overall length and extent of pre-trial discovery; (2) the entitlement of the parties to an action to appeal a decision; (3) clarity as to theories of liability, damages and governing law; (4) uncertainties in timing of litigation; and (5) the possible need for further legal proceedings to establish the appropriate amount of damages, if any.

While there can be no assurance regarding the outcome of any of the legal proceedings referred to in this Note 25, based on management’s current and considered view of each situation, we do not currently expect them to have a material adverse effect on our financial position. This position could of course change over time, not least because of the factors referred to above.

In cases that have been settled or adjudicated, or where quantifiable fines and penalties have been assessed and which are not subject to appeal (or other similar forms of relief), or where a loss is probable and we are able to make a reasonable estimate of the loss, we indicate the loss absorbed or the amount of the provision accrued. Further details of the legal provisions taken during the year are provided in Note 17.

Where it is considered that the Group is more likely than not to prevail, legal costs involved in defending the claim are charged to profit as they are incurred.

Where it is considered that the Group has a valid contract which provides the right to reimbursement (from insurance or otherwise) of legal costs and/or all or part of any loss incurred or for which a provision has been established, and we consider recovery to be virtually certain, the best estimate of the amount expected to be received is recognised as an asset.

Assessments as to whether or not to recognise provisions or assets, and of the amounts concerned, usually involve a series of complex judgements about future events and can rely heavily on estimates and assumptions. AstraZeneca believes that the provisions recorded are adequate based on currently available information and that the insurance recoveries recorded will be received. However, given the inherent uncertainties involved in assessing the outcomes of these cases, and in estimating the amount of the potential losses and the associated insurance recoveries, we could in the future incur judgments or insurance settlements that could have a material adverse effect on our results in any particular period.

 

IP claims include challenges to the Group’s patents on various products or processes and assertions of non-infringement of patents. A loss in any of these cases could result in loss of patent protection or loss of exclusivity on the related product. The consequences of any such loss could be a significant decrease in product sales, which could have a material adverse effect on our results. The lawsuits filed by AstraZeneca for patent infringement against companies that have filed ANDAs in the US, seeking to market generic forms of products sold by the Group prior to the expiry of the applicable patents covering these products, typically also involve allegations of non-infringement, invalidity and unenforceability of these patents by the ANDA filers. In the event that the Group is unsuccessful inth ese actions or the statutory 30 month stay expires before a ruling is obtained, the ANDA filers involved will also have the ability, subject to FDA approval, to introduce generic versions of the product concerned.

AstraZeneca has full confidence in, and will vigorously defend and enforce, its IP.

Over the course of the past several years, including in 2012, a significant number of commercial litigation claims in which AstraZeneca is involved have been resolved, particularly in the US, thereby reducing potential contingent liability exposure arising from such litigation. Similarly, in part due to patent litigation and settlement developments, greater certainty has been achieved regarding possible generic entry dates with respect to some of our patented products. At the same time, like other companies in the pharmaceutical sector and other industries, AstraZeneca continues to be subject to government investigations around the world.

Patent Litigation

Arimidex (anastrozole)

Patent/regulatory proceedings outside the US

In March 2012, the Canadian Federal Court of Appeal dismissed Mylan Pharmaceuticals ULC’s appeal against a decision prohibiting the Canadian Minister of Health from issuing it with a marketing authorisation. There is no remaining Arimidex litigation in Canada.

Atacand Plus (candesartan cilexetil/hydrochlorothiazide)

Patent/regulatory proceedings outside the US

In Canada, in February and May 2012, AstraZeneca settled notice of compliance proceedings with Cobalt Pharmaceuticals Inc., and Apotex Inc. respectively allowing each company to enter the Canadian market on 23 September 2012, or earlier, in certain circumstances. Generic candesartan cilexetil/hydrochlorothiazide entered the Canadian market in September 2012. There is no remaining Atacand Plus litigation in Canada.

Crestor (rosuvastatin calcium)

US patent litigation/regulatory proceedings

In December 2012, the US Court of Appeals for the Federal Circuit affirmed the decision of the US District Court for the District of Delaware that the substance patent protecting Crestor is valid and enforceable. The Federal Circuit also held that Apotex Corp. (Apotex) was liable as a submitter and is therefore bound by the District Court’s decision. In January 2013, defendants Aurobindo Pharma Limited, Teva Pharmaceuticals USA, Inc., Mylan Pharmaceuticals Inc., Sun Pharmaceutical Industries, LTD., and, separately, Apotex, filed petitions for rehearing and rehearing en banc of aspects of the Federal Circuit’s decision.

AstraZeneca is also engaged in patent litigation in the US District Court for the District of Delaware in which it contends that a §505(b)(2) NDA for rosuvastatin zinc tablets infringes the substance patent for Crestor tablets. In March 2012, the Court ruled that, based on the NDA application alone, it did not have subject matter jurisdiction over AstraZeneca’s claims for infringement of its patents relating to methods of using rosuvastatin compounds to treat certain cardiovascular conditions. In November 2012, the Court ruled that

 

 

184   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

25 Commitments and contingent liabilities continued

defendant Watson Laboratories, Inc. (Watson) was precluded from relitigating its defence of invalidity. In December 2012, defendant EGIS Pharmaceuticals PLC was dismissed from the case by stipulation where it conceded the validity and enforceability of the Crestor substance patent and also agreed to be bound by any judgment against Watson. Trial took place in December 2012 on the sole remaining issue of infringement of the substance patent. The Court will render a decision after submission of post-trial briefs from both parties.

As previously reported, in November 2011, AstraZeneca filed a Citizen Petition with the FDA in respect of Crestor requesting the FDA to withhold approval of any generic rosuvastatin drug product that omits from its labelling the diabetes-related warning and adverse reaction information which AstraZeneca was required to include in Crestor ’s labelling when the FDA approved Crestor ’s primary prevention of cardiovascular disease indication. In May 2012, the FDA denied the Petition.

AstraZeneca is also defending a patent infringement lawsuit filed in April 2011 in the US District Court for the District of South Carolina by Palmetto Pharmaceuticals, LLC (Palmetto), which, among other claims, asserts that AstraZeneca’s Crestor sales induce infringement of a Palmetto patent.

Patent proceedings outside the US

AstraZeneca is engaged in proceedings in Australia, Brazil, Canada, Malaysia, Mexico, Portugal and Singapore regarding patent and/ or regulatory exclusivity for Crestor . Generic drug manufacturers have commenced sales of generic rosuvastatin drug products in Brazil, Canada, Malaysia and Mexico.

In Australia, as previously reported in 2011, AstraZeneca instituted proceedings against Apotex Pty Ltd asserting infringement of various formulation and method patents for Crestor . In January 2012, AstraZeneca instituted similar proceedings against Watson Pharma Pty Ltd. and Actavis Australia Pty Ltd. AstraZeneca was granted preliminary injunctions against all three parties. A trial was held in October 2012 and a decision is pending.

In Canada, in February 2012, AstraZeneca reached settlement with Pharmascience Inc. (PMS) resolving the litigation regarding AstraZeneca’s Crestor substance patent and, as part of the agreement, PMS was permitted to enter the Canadian market on 2 April 2012, or earlier, in certain circumstances. Generic rosuvastatin calcium entered the Canadian market in April 2012.

Entocort EC (budesonide)

US patent litigation

In April 2012, the US Court of Appeals for the Federal Circuit affirmed the US District Court for the District of Delaware’s decision that Mylan Pharmaceuticals Inc.’s generic budesonide product does not infringe AstraZeneca’s patent protecting Entocort EC .

Losec/Prilosec (omeprazole)

US patent litigation

AstraZeneca continues litigation to recover patent infringement damages against Andrx Pharmaceuticals, Inc., and Apotex Corp. and Apotex Inc.

Patent proceedings outside the US

In Canada, the AstraZeneca patent infringement proceeding against Apotex Inc. regarding omeprazole capsules and tablets remains pending.

In May 2012, in Canada, the Federal Court found AstraZeneca liable to Apotex Inc. for section 8 damages arising from notice of compliance proceedings that had been finally dismissed in December 2003. The actual amount of damages owing, if any, will be determined at a future date by a court reference procedure. AstraZeneca has appealed the Federal Court’s decision.

 

Nexium (esomeprazole magnesium)

US patent litigation

In 2012, AstraZeneca entered into separate agreements with three generic companies settling AstraZeneca’s patent infringement action against each generic company’s ANDA product. As part of each settlement, each generic company was granted a licence to enter the US market with its proposed ANDA version of generic esomeprazole magnesium on 27 May 2014, subject to regulatory approval, or earlier, in certain circumstances.

In January 2012, AstraZeneca received a Paragraph IV notice letter from Mylan Laboratories Ltd. (Mylan Laboratories). In March 2012, AstraZeneca commenced a patent infringement action in the US District Court for the District of New Jersey against Mylan Laboratories regarding its generic ANDA product. Trial against Mylan Laboratories may be scheduled in 2013.

In 2011, AstraZeneca commenced a patent infringement action in the US District Court for the District of New Jersey against Hanmi USA Inc., et al. (Hanmi) in response to the filing of an NDA under §505(b)(2) for FDA approval to market 20mg and 40mg esomeprazole strontium capsules. Trial against Hanmi may be scheduled in 2013.

Patent proceedings outside the US

AstraZeneca is involved in proceedings in several countries outside the US regarding patent and/or regulatory exclusivity for Nexium , including Australia, Austria, Belgium, Brazil, Canada, China, the Czech Republic, Denmark, Estonia, Finland, France, Germany, Italy, Latvia, Lithuania, Malaysia, Mexico, the Netherlands, Norway, Philippines, Poland, Portugal, Singapore, Slovenia, Sweden, Switzerland and Turkey. There is generic entry in many European markets.

In the European Patent Office (EPO), in June and July 2011, the Opposition Division revoked EP 1020461 (the ’461 patent) (which relates to Nexium ) and EP 1020460 (the ’460 patent) (which relates to Nexium i.v.). AstraZeneca appealed the Opposition Division’s decision. In November 2012, separate EPO Technical Boards of Appeal granted AstraZeneca’s appeals and maintained both the ’461 patent and the ’460 patent.

In Canada, in March 2012, AstraZeneca discontinued its notice of compliance proceeding pending with Mylan Pharmaceuticals ULC (Mylan) with respect to the Canadian Nexium substance patent number 2.290.963 after Mylan withdrew its notice of allegation.

Also, in Canada, in October 2012, the Federal Court prohibited Pharmascience Inc. from receiving a marketing authorisation for its esomeprazole magnesium product until May 2018.

Pulmicort Respules (budesonide inhalation suspension)

US patent litigation

AstraZeneca’s consolidated patent infringement lawsuits against various generic companies for infringement of US patents directed to methods of use and the formulation and form of active ingredient for Pulmicort Respules began trial on 7 November 2012 in the US District Court for the District of New Jersey. Closing arguments are scheduled for 8 February 2013 and AstraZeneca expects a decision shortly thereafter.

Seroquel IR (quetiapine fumarate)

US regulatory proceedings

In March 2012, in response to the FDA’s notice that generic Seroquel IR had been granted final approval, AstraZeneca filed al awsuit in the US District Court for the District of Columbia seeking a temporary restraining order to vacate these approvals, and an injunction to enjoin any further approvals of generic quetiapine. In June 2012, the Court denied AstraZeneca’s motion for summary judgment and granted the FDA’s cross motion for summary judgment on the issue of exclusivity for Seroquel IR . In July 2012, AstraZeneca appealed that ruling to the US Court of Appeals for the District of Columbia Circuit. Generic quetiapine fumarate ( Seroquel IR ) entered the US market in March 2012.

 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   185

Table of Contents

Financial Statements | Notes to the Group Financial Statements

 

25 Commitments and contingent liabilities continued

Seroquel XR (an extended release formulation of quetiapine fumarate)

US patent litigation/regulatory proceedings

In October 2011, the US District Court for the District of New Jersey conducted a trial in the patent infringement actions involving the Seroquel XR formulation patent against certain generic drug manufacturers. In March 2012, the Court found the Seroquel XR formulation patent to be valid. The Court also found that Anchen Pharmaceuticals, Inc., Osmotica Pharmaceutical Corporation, Torrent Pharmaceuticals Limited, Torrent Pharma Inc., Mylan Pharmaceuticals Inc. and Mylan Inc. have infringed the Seroquel XR formulation patent. The decision has been appealed.

In July 2012, AstraZeneca settled its patent infringement action against Intellipharmaceutics Corp. and Intellipharmaceutics International Inc. (together, Intellipharmaceutics) pending in the US District Court for the Southern District of New York by granting a licence to the Seroquel XR product patent, effective 1 November 2016, or earlier, in certain circumstances.

In July 2012, AstraZeneca received a Paragraph IV notice letter from Amneal Pharmaceuticals, LLC (Amneal) relating to Seroquel XR . In August 2012, AstraZeneca commenced a patent infringement action against Amneal and related Amneal entities in the US District Court for the District of New Jersey. In January 2013, AstraZeneca settled its patent infringement action against Amneal by granting a licence to the Seroquel XR product patent, effective 1 November 2016, or earlier, in certain circumstances.

In September 2012, AstraZeneca received a Paragraph IV notice letter from Lupin Ltd. (Lupin) relating to Seroquel XR . In November 2012, AstraZeneca commenced a patent infringement action against Lupin in the US District Court for the District of New Jersey.

Patent proceedings outside the US

In the Netherlands, in March 2012, the District Court in the Hague upheld the validity of the formulation patent protecting Seroquel XR .

In the UK, in March 2012, the UK High Court found the Seroquel XR formulation patent invalid.

In Spain, in July 2012, the Commercial Court in Barcelona found the Seroquel XR formulation patent valid.

In Germany, in September 2012, the Regional Court in Düsseldorf affirmed preliminary injunctions against Heumann Pharma GmbH & Co, Heumann Verwaltungs GmbH, Ratiopharm GmbH, CT Arzneimittel GmbH and AbZ Pharma GmbH. However, in November 2012, the Federal Patent Court found the Seroquel XR patent invalid and outstanding injunctions have been lifted.

Generic versions of Seroquel XR have been launched in Austria, Denmark, Germany, Italy, Portugal, UK, Romania and elsewhere. While AstraZeneca continues to have confidence in the patent protecting Seroquel XR and will continue to take appropriate legal action, additional generic launches and adverse court rulings are possible.

Symbicort (budesonide/formoterol)

US patent litigation

AstraZeneca is defending a complaint alleging patent infringement filed in the US District Court for the Eastern District of Texas by Accuhale LLC (Accuhale). Accuhale is purportedly the owner of US patent no. 5,718,355, which Accuhale alleges is infringed by sales of Symbicort .

 

Vimovo (naproxen/esomeprazole magnesium)

US patent litigation

In January 2013, AstraZeneca and Pozen commenced a patent-infringement action in the US District Court for the District of New Jersey in response to an ANDA challenge to seven patents listed in the Orange Book including the patent in-licensed from Pozen. Three additional patent-infringement actions regarding generic versions of Vimovo are also pending in the Court.

Zestril (lisinopril dihydrate)

Patent/regulatory proceedings outside the US

As previously disclosed, in 1996, two of AstraZeneca’s predecessor companies, Zeneca Limited and Zeneca Pharma Inc. (as licensees), Merck & Co., Inc. and Merck Frosst Canada Inc. (together Merck Group) commenced a patent infringement action in Canada against Apotex, Inc. (Apotex), alleging infringement of Merck Group’s lisinopril patent. In 2010, after having established Apotex’s liability, AstraZeneca and the Merck Group initiated proceedings to recover damages and that damages claim remains pending.

Product Liability Litigation

Crestor (rosuvastatin calcium)

AstraZeneca is defending 15 lawsuits in California state courts involving a total of 263 plaintiffs claiming physical injury from treatment with Crestor . The lawsuits allege multiple types of injuries including diabetes mellitus, various cardiac injuries, rhabdomyolysis, and liver and kidney injuries. Fourteen cases have been consolidated into one co-ordinated proceeding in Los Angeles, California.

Iressa (gefitinib)

Between 2004 and 2008, seven claims were filed against AstraZeneca in Japan, in the Osaka and Tokyo District Courts alleging that Iressa caused a fatal incidence of interstitial lung disease in Japanese patients. As previously reported, in November 2011, the Tokyo High Court reversed the Tokyo District Court’s decision and ruled that neither AstraZeneca, nor the Japanese Ministry of Health, Labour and Welfare (MHLW), had any liability for any of the claims. Following that decision, on 25 May 2012, the Osaka High Court reversed the Osaka District Court decision and ruled that neither AstraZeneca, nor the MHLW, had any liability for any of the claims. The plaintiffs have appealed both decisions to the Japanese Supreme Court.

Nexium (esomeprazole magnesium)

As previously disclosed, AstraZeneca has been named as a defendant in product liability lawsuits brought by plaintiffs alleging bone deterioration, loss of bone density and/or bone fractures caused by Nexium and/or Prilosec in various federal and state courts in the US. Currently, there are approximately 1,900 plaintiffs. In December 2012, the US Judicial Panel on Multi-District Litigation ordered that the federal cases be co-ordinated for proceedings in the US District Court for the Central District of California.

Seroquel IR (quetiapine fumarate)

With regard to Seroquel IR product liability litigation in the US, AstraZeneca is aware of approximately 10 cases in active litigation in various jurisdictions. Provisions associated with diabetes-related claims were reduced by approximately $18m in 2012.

Four putative class actions were initiated in Canada in the provinces of Alberta, British Columbia, Ontario and Quebec, alleging that AstraZeneca failed to provide adequate warnings in connection with an alleged association between Seroquel IR and the onset of diabetes. Class certification was denied in the Ontario proceedings in 2012 and in Quebec in 2011. Both decisions were appealed. On 12 December 2012, the Quebec Court of Appeal approved plaintiff’s motion to abandon the appeal of the lower court’s decision to deny class certification.

 

 

186   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

25 Commitments and contingent liabilities continued

With regard to insurance coverage for the substantial legal defence costs and settlements that have been incurred in connection with the Seroquel IR product liability claims in the US related to alleged diabetes and/or other related injuries (which now exceed the total amount of insurance coverage available), disputes continue with insurers and legal proceedings have commenced in the UK about the availability of coverage under certain insurance policies. These policies have aggregate coverage limits of $300m. No insurance receivable can be recognised under applicable accounting standards at this time.

Commercial Litigation

Crestor (rosuvastatin calcium)

On 29 November 2012, a Motion to Certify a Claim as a Class Action and Related Statement of Claim were filed in Israel in the District Court in Tel Aviv – Jaffa, against AstraZeneca and four other pharmaceutical companies. With respect to AstraZeneca, in addition to other causes of action, the Statement of Claim alleges that AstraZeneca engaged in deception and failed to disclose material facts to consumers of Crestor regarding certain adverse events associated with the drug.

Nexium (esomeprazole magnesium)

Of the various putative class actions in the US alleging that AstraZeneca’s promotion, advertising and pricing of Nexium to physicians, consumers and third party payers was unfair, unlawful and deceptive, only one case remains pending. In the Massachusetts State Court case, AstraZeneca reached an agreement in principle to settle the matter in September 2012, and a provision has been taken. Plaintiffs’ motion for preliminary approval of the settlement will be heard by the Court on 5 February 2013. The Delaware State Court case has been stayed since May 2005.

Seroquel (quetiapine fumarate)

Of the various state law claims brought by state Attorneys General generally alleging that AstraZeneca made false and/or misleading statements in marketing and promoting Seroquel , AstraZeneca remains in litigation with the Attorney General of Mississippi. In 2012, AstraZeneca settled the cases brought by the Attorneys General of the states of Montana, New Mexico, South Carolina and Utah, and also finalised previously reported agreements in principle with Alaska and Arkansas. In December 2012, AstraZeneca also agreed in principle to a settlement of similar claims with the Attorney General of Kentucky, which was finalised in January 2013. Provisions for the foregoing settlements were taken in 2012.

Synagis (palivizumab)

In September 2011, MedImmune, filed an action against Abbott International, LLC (Abbott) in the Circuit Court for Montgomery County, Maryland, seeking a declaratory judgment in a contract dispute. Abbott’s motion to dismiss was granted. In September 2011, Abbott filed a parallel action against MedImmune in the Illinois State Court. Abbott’s motion to hold the disputed funds in escrow was rejected. In February 2012, the Court denied MedImmune’s motion to dismiss and is expected to set a trial date for 2013.

Toprol-XL (metoprolol succinate)

AstraZeneca is defending anti-trust claims in the US regarding the listing and enforcement of patents protecting Toprol-XL . In March 2013, the US District Court for the District of Delaware will hold a hearing to review the agreement in principle to settle the remaining claims alleged by the end-payers, for which a provision was taken in 2012.

 

Other Commercial Litigation

Co-Payment Subsidy Litigation

In March 2012, the New England Carpenters Health and Welfare Fund, on behalf of a proposed class of payers that reimbursed consumers for Nexium and Crestor prescriptions as to which AstraZeneca subsidised the consumer’s co-payment obligation, brought an action against AstraZeneca in the US District Court for the Eastern District of Pennsylvania. On 5 September 2012, the plaintiffs voluntarily dismissed their complaint against AstraZeneca while reserving the right to file a new complaint against AstraZeneca in the future.

Shionogi Arbitration Crestor Royalty Calculation

In July 2012, Shionogi & Co. Ltd initiated arbitration proceedings to resolve issues relating to the treatment of certain excise taxes and other specific items in the calculation of royalties on Crestor sales.

Nexium Settlement Anti-trust Litigation

AstraZeneca is a defendant in numerous nearly identical putative class actions alleging that AstraZeneca’s settlements of patent litigation relating to Nexium violated US anti-trust law and various state laws. In December 2012, the US Judicial Panel on Multi-District Litigation ordered that the cases be co-ordinated for proceedings in the US District Court for the District of Massachusetts.

Average Wholesale Price (AWP) litigation

Of the various lawsuits against AstraZeneca and other pharmaceutical manufacturers involving allegations that, by causing the publication of allegedly inflated wholesale list prices, defendants caused entities to overpay for prescription drugs, AstraZeneca remains in litigation with the Attorneys General of the states of Utah, Wisconsin, and, as discussed below, with the Commonwealth of Kentucky.

During 2012, settlements were reached with the Attorneys General of the states of Louisiana and Oklahoma and provisions were taken.

AstraZeneca prevailed in its appeal before the Commonwealth ofK entucky Court of Appeals. In that case, AstraZeneca sought reversal of the judgment against it in the case brought by the Attorney General of Kentucky and the corresponding award of damages and penalties. Following the underlying 2009 trial, a Kentucky jury found AstraZeneca liable under the Commonwealth of Kentucky’s Consumer Protection and Medicaid Fraud statutes and awarded $14.72m in compensatory damages and $100 in punitive damages. The trial court subsequently awarded an additional $5.4m in statutory penalties. On 12 October 2012, the Kentucky Court of Appeals reversed the trial court’s decision and held that AstraZeneca was not liable for damages. The Court of Appeals remanded the case to the trial court for entry of judgment in favour of AstraZeneca. On 13 November 2012, the Commonwealth filed its Motion for Discretionary Review (appeal) in the Kentucky Supreme Court.

There are no remaining AWP cases pending against MedImmune.

Medco qui tam litigation (Schumann)

AstraZeneca has been named as a defendant in a lawsuit filed in Federal Court in Philadelphia under the qui tam (whistleblower) provisions of the federal and certain state False Claims Acts alleging overpayments by federal and state governments resulting from alleged false pricing information reported to the government and improper payments intended to influence the formulary status of Prilosec and Nexium to Medco and its customers. The action was initially filed in September 2003 but remained under seal until July 2009, at which time AstraZeneca was served with a copy of the amended complaint following the US government’s decision not to intervene in the case. On 25 January 2013, the Court granted AstraZeneca’s motion and dismissed the case with prejudice.

 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   187

Table of Contents

Financial Statements | Notes to the Group Financial Statements

 

25 Commitments and contingent liabilities continued

Average Manufacturer’s Price qui tam litigation (Streck)

AstraZeneca is one of several manufacturers named as a defendant in a lawsuit filed in the US Federal Court in Philadelphia under the qui tam (whistleblower) provisions of the federal and certain state False Claims Acts alleging inaccurate reporting of Average Manufacturer’s Prices to the Centers for Medicare and Medicaid Services. The action was initially filed in October 2008 but remained under seal until May 2011, following the US government’s decision not to intervene in the case with regard to certain manufacturers, including AstraZeneca. As to AstraZeneca, the Court dismissed plaintiffs’ claims, both state and federal, for all Average Manufacturer Price submissions made before 1 January 2007 but denied AstraZeneca’s motion to dismiss all claims regarding submissions made after 1 January 2007.

Drug importation and anti-trust litigation

As previously disclosed, in August 2004, Californian retail pharmacy plaintiffs filed an action in the Superior Court of California alleging a conspiracy by AstraZeneca and other pharmaceutical manufacturer defendants to set the price of drugs sold in California at or above the Canadian sales price for those drugs and otherwise restrict the importation of pharmaceuticals into the US. After the court granted the defendants’ motion for summary judgment, and that decision was affirmed on appeal, in October 2012, the plaintiffs filed a petition for review by the California Supreme Court, which was denied.

Employment – wage/hour litigation

On 18 June 2012, the US Supreme Court in Christopher vs. SmithKline Beecham Corporation (GSK) handed down a decision concerning whether pharmaceutical sales representatives are exempt from overtime pay regulations under the US Department of Labor’s outside sales exemption. The decision favoured GSK and by implication AstraZeneca and the pharmaceutical industry as a whole. As a result of the Christopher decision, the final wage and hour class action lawsuits against AstraZeneca were dismissed in October 2012.

Government investigations/proceedings

Except as otherwise noted, the precise parameters of the following inquiries are unknown, and AstraZeneca is not in a position at this time to predict the scope, duration or outcome of these matters, including whether they will result in any liability to AstraZeneca.

Losec/Prilosec (omeprazole)

European Commission case

In December 2012, the Court of Justice of the EU ruled on the cross-appeals from the General Court of the EU’s judgment regarding the European Commission’s 2005 decision fining AstraZeneca 60m (reduced to €52.5m by the General Court) for abuse of a dominant position regarding omeprazole. The Court of Justice dismissed all of the cross-appeals and confirmed the judgment of the General Court in all material respects. No further appeals are possible.

Nexium (esomeprazole magnesium)

Department of Justice/Attorney General of Texas investigation

AstraZeneca has received a subpoena from the Department of Justice and a Civil Investigative Demand issued by the Attorney General of Texas in connection with an investigation of the possible submission of false or otherwise improper pricing information for certain formulations of Nexium to the Centers for Medicare and Medicaid Services. The Department of Justice has filed a notice of non-intervention in the federal case. The Attorney General of Texas has stated that it plans to file a similar notice in the Texas False Claims Act case pending in state court in Texas. AstraZeneca and counsel for relator are currently negotiating the language of stipulations of dismissal. AstraZeneca expects these cases to be formally dismissed shortly.

 

Dutch National Competition Authority investigation

In the Dutch National Competition Authority (NMa) investigation into alleged abuse of a dominant position, the investigation team issued a report alleging foreclosure of generic versions of certain proton pump inhibitors other than esomeprazole. The file has now been passed to the Legal Department of the NMa. AstraZeneca completed its defence in April 2012 and awaits a decision by the Board of the NMa later in 2013.

Federal Trade Commission inquiry

In 2012, AstraZeneca completed its response to the 2008 Civil Investigative Demand from the US Federal Trade Commission seeking information regarding the Nexium patent litigation settlement with Ranbaxy Laboratories Ltd.

Seroquel (quetiapine fumarate)

Attorney General of Texas investigation

In July 2012, AstraZeneca received a civil investigative demand from the Office of the Attorney General for the State of Texas in connection with an investigation related to sales and marketing activities potentially involving Seroquel .

Synagis (palivizumab)

As previously disclosed, on 30 June 2011, MedImmune received a demand from the US Attorney’s Office for the Southern District of New York requesting certain documents related to the sales and marketing activities of Synagis . On 1 July 2011, MedImmune received a similar court order to produce documents from the Office of the Attorney General for the State of New York Medicaid and Fraud Control Unit pursuant to what the government attorneys advised was a joint investigation. MedImmune has accepted receipt of these requests and is co-ordinating with the government offices to provide the appropriate responses and co-operate with any related investigation.

In May 2012, MedImmune, received a subpoena duces tecum from the Office of Attorney General for the State of Florida Medicaid and Fraud Control Unit requesting certain documents related to the sales and marketing activities of Synagis . MedImmune has accepted receipt of the request and is co-ordinating with the Florida government to provide the appropriate responses and co-operate with any related investigation. AstraZeneca is unaware of the nature or focus of the investigation, however, based on the nature of the requests it appears to be similar to the inquiries from the State of New York and Department of Justice (which is mentioned above).

Other government investigations/proceedings

Foreign Corrupt Practices Act

In connection with an investigation into Foreign Corrupt Practices Act issues in the pharmaceutical industry, AstraZeneca has received inquiries from the US Department of Justice and the SEC regarding, among other things, sales practices, internal controls, certain distributors and interactions with healthcare providers and other government officials in several countries. AstraZeneca is co-operating with these inquiries. AstraZeneca is investigating indications of inappropriate conduct in certain countries, including China. Resolution of this matter could involve the payment of fines and/or other remedies.

 

 

188   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

25 Commitments and contingent liabilities continued

Serbia

In August 2011, AstraZeneca’s Representative Office in Belgrade, Serbia was served with a criminal indictment alleging that local employees of AstraZeneca and several other pharmaceutical companies who are also named defendants in the indictment, made allegedly improper payments to physicians at the Institute of Oncology and Radiology of Serbia. The indictment was subsequently amended. In March 2012, the Court denied AstraZeneca’s request to dismiss the amended indictment and joined the proceedings against AstraZeneca and the other named pharmaceutical companies with the pending proceedings against the allegedly involved individual defendants. AstraZeneca has filed an appeal with the Serbian Constitutional Court.

India

On 23 February 2012, the Indian Central Bureau of Investigation filed a First Information Report in the court in Delhi against AstraZeneca and public officials of the Central Procurement Agency of the Delhi Directorate of Health Services (DHS) in connection with circumstances surrounding the submission by AstraZeneca of an alleged false affidavit in relation to pricing as part of a tender for Meronem entered into by AstraZeneca with the DHS in 2009. AstraZeneca is co-operating with the investigation.

Other US Attorney’s Offices investigations

The US Attorney’s Offices in Alabama, Delaware and Texas are conducting investigations related to sales and marketing activities potentially involving more than one product, including Crestor and Seroquel XR , in response to the filing of qui tam (whistleblower) lawsuits.

The US Attorney’s Office for the District of Delaware, Criminal Division, is conducting an investigation relating to AstraZeneca’s relationship with Medco and sales of Nexium, Plendil, Prilosec and Toprol-XL .

Additional government inquiries

As is true for most, if not all, major prescription pharmaceutical companies operating in the US, AstraZeneca is currently involved in multiple US federal and state inquiries into drug marketing and pricing practices. In addition to the investigations described above, various federal and state law enforcement offices have, from time to time, requested information from the Company. There have been no material developments in those matters.

Tax

Where tax exposures can be quantified, an accrual is made based on best estimates and management’s judgement. Details of the movements in relation to material tax exposures are discussed below. As accruals can be built up over a long period of time but the ultimate resolution of tax exposures usually occurs at a point in time and given the inherent uncertainties in assessing the outcomes of these exposures (which sometimes can be binary in nature), we could, in future periods, experience adjustments to these accruals that have a material positive or negative effect on our results in any particular period.

 

Transfer pricing and other international tax contingencies

The total net accrual included in the Group Financial Statements to cover the worldwide exposure to transfer pricing audits is $423m, a reduction of $226m compared to 2011 primarily due to the settlement of a transfer pricing matter as detailed in Note 4.

AstraZeneca faces a number of transfer pricing audits in jurisdictions around the world and, in some cases, is in dispute with the tax authorities. The issues under discussion are often complex and can require many years to resolve. Accruals for tax contingencies require management to make estimates and judgements with respect to the ultimate outcome of a tax audit, and actual results could vary from these estimates. The international tax environment presents increasingly challenging dynamics for the resolution of transfer pricing disputes. These disputes usually result in taxable profits being increased in one territory and correspondingly decreased in another. Our balance sheet positions for these matters reflect appropriate corresponding relief in the territories affected. Management considers that at present such corresponding relief will be available, but given the challenges in the international tax environment will keep this aspect under careful review.

Management continues to believe that AstraZeneca’s positions on all its transfer pricing audits and disputes are robust and that AstraZeneca is appropriately provided.

For transfer pricing audits where AstraZeneca and the tax authorities are in dispute, AstraZeneca estimates the potential for reasonably possible additional losses above and beyond the amount provided to be up to $522m (2011: $375m); however, management believes that it is unlikely that these additional losses will arise. It is possible that some of these contingencies may reduce in the future to the extent that any tax authority challenge is unsuccessful, or matters lapse following expiry of the relevant statutes of limitation resulting in a reduction in the tax charge in future periods.

Other tax contingencies

Included in the tax accrual is $1,846m relating to a number of other tax contingencies, an increase of $174m mainly due to the impact of an additional year of transactions relating to contingencies for which accruals had already been established and exchange rate effects. For these tax exposures, AstraZeneca does not expect material additional losses. It is, however, possible that some of these contingencies may reduce in the future if any tax authority challenge is unsuccessful or matters lapse following expiry of the relevant statutes of limitation resulting in a reduction in the tax charge in future periods.

Timing of cash flows and interest

It is not possible to estimate the timing of tax cash flows in relation to each outcome, however, it is anticipated that a number of significant disputes may be resolved over the next one to two years. Included in the provision is an amount of interest of $248m (2011: $291m). Interest is accrued as a tax expense.

 

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   189

Table of Contents

Financial Statements | Notes to the Group Financial Statements

26 Operating leases

Total rentals under operating leases charged to profit were as follows:

 

                                            
    

2012

$m

    

2011

$m

    

2010

$m

 

Operating leases

     197         215         212   

The future minimum lease payments under operating leases that have initial or remaining terms in excess of one year at 31 December 2012 were as follows:

 

                                            
    

2012

$m

    

2011

$m

    

2010

$m

 

 

Obligations under leases comprise:

        

Not later than one year

     102         92         161   

Later than one year and not later than five years

     223         178         242   

Later than five years

     109         122         103   

Total future minimum lease payments

     434         392         506   

27 Statutory and other information

 

                                            
    

2012

$m

    

2011

$m

    

2010

$m

 

Fees payable to KPMG Audit Plc and its associates:
Group audit fee

     2.2         2.4         2.3   

Fees payable to KPMG Audit Plc and its associates for other services:
The audit of subsidiaries pursuant to legislation

     5.0         5.5         6.5   

Audit-related assurance services

     2.2         2.4         3.3   

Tax compliance services

     0.8         0.8         0.6   

Tax advisory services

     0.1         0.1         0.5   

Other assurance services

     1.1         2.5         0.1   

Fees payable to KPMG Audit Plc in respect of the Group’s pension schemes:

        

The audit of subsidiaries’ pension schemes

     0.5         0.6         0.6   
       11.9         14.3         13.9   

Audit-related assurance services include fees of $1.7m (2011: $1.9m; 2010: $2.4m) in respect of section 404 of the Sarbanes-Oxley Act.

Other assurance services include assurance services provided in relation to the Group’s long-term debt issuance in 2012.

Related party transactions

The Group had no material related party transactions which might reasonably be expected to influence decisions made by the users of these Financial Statements.

Key management personnel compensation

Key management personnel are defined for the purpose of disclosure under IAS 24 ‘Related Party Disclosures’ as the members of the Board and the members of the SET.

 

                                            
    

2012

$000

    

2011

$000

    

2010

$000

 

Short-term employee benefits

     19,451         19,973         21,925   

Post-employment benefits

     2,137         2,155         1,793   

Termination benefits

     1,672                   

Share-based payments

     15,304         16,064         11,563   
       38,564         38,192         35,281   

Total remuneration is included within employee costs (see Note 24). Further details of Directors’ emoluments are included in the Directors’ Remuneration Report from pages 122 to 137.

Subsequent events

There were no material subsequent events.

 

190   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

Financial Statements | Principal Subsidiaries

Principal Subsidiaries

 

At 31 December 2012

  Country    

Percentage

of voting share

capital held

    Principal activity

 

UK

     

AstraZeneca UK Limited

    England        100      Research and development, manufacturing, marketing

AstraZeneca Treasury Limited

    England        100      Treasury
                     

 

Continental Europe

     

AstraZeneca Dunkerque Production SCS

    France        100      Manufacturing

AstraZeneca SAS

    France        100      Research, manufacturing, marketing

Novexel SA

    France        100      Research

AstraZeneca GmbH

    Germany        100      Development, manufacturing, marketing

AstraZeneca Holding GmbH

    Germany        100      Manufacturing, marketing

AstraZeneca SpA

    Italy        100      Marketing

AstraZeneca Farmaceutica Spain SA

    Spain        100      Marketing

AstraZeneca AB

    Sweden        100      Research and development, manufacturing, marketing

AstraZeneca BV

    Netherlands        100      Marketing

LLC AstraZeneca Pharmaceuticals

    Russia        100      Marketing
                     

 

The Americas

     

AstraZeneca do Brasil Limitada

    Brazil        100      Manufacturing, marketing

AstraZeneca Canada Inc.

    Canada        100      Research, marketing

AZ Reinsurance Limited

    Cayman Islands        100      Insurance and reinsurance underwriting

IPR Pharmaceuticals Inc.

    Puerto Rico        100      Development, manufacturing, marketing

Ardea Biosciences, Inc.

    US        100      Research and development

AstraZeneca LP

    US        99      Research and development, manufacturing, marketing

AstraZeneca Pharmaceuticals LP

    US        100      Research and development, manufacturing, marketing

Zeneca Holdings Inc.

    US        100      Manufacturing, marketing

MedImmune, LLC

    US        100      Research and development, manufacturing, marketing
                     

 

Asia, Africa & Australasia

     

AstraZeneca Pty Limited

    Australia        100      Development, manufacturing, marketing

AstraZeneca Pharmaceuticals Co., Limited

    China        100      Research and development, manufacturing, marketing

AZ (Wuxi) Trading Co. Limited

    China        100      Marketing

AstraZeneca KK

    Japan        80      Manufacturing, marketing

All shares are held indirectly.

The companies and other entities listed above are those whose results or financial position principally affected the figures shown in the Group Financial Statements. A full list of subsidiaries, joint ventures and associates will be annexed to the Company’s next annual return filed with the Registrar of Companies. The country of registration or incorporation is stated alongside each company. The accounting year ends of subsidiaries and associates are 31 December. AstraZeneca operates through 217 subsidiaries worldwide. Products are manufactured in 16 countries worldwide and are sold in over 100 countries. The Group Financial Statements consolidate the Financial Statements of the Company and its subsidiaries at 31 December 2012.

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   191

Table of Contents

Financial Statements | Independent Auditor’s Report to the Members of AstraZeneca PLC

Independent Auditor’s Report to the Members of AstraZeneca PLC

 

We have audited the Parent Company Financial Statements of AstraZeneca PLC for the year ended 31 December 2012 set out on pages 193 to 197. The financial reporting framework that has been applied in their preparation is applicable law and UK Accounting Standards (UK Generally Accepted Accounting Practice).

This report is made solely to the Company’s members, as a body, in accordance with Chapter 3 of Part 16 of the Companies Act 2006. Our audit work has been undertaken so that we might state to the Company’s members those matters we are required to state to them in an auditor’s report and for no other purpose. To the fullest extent permitted by law, we do not accept or assume responsibility to anyone other than the Company and the Company’s members, as a body, for our audit work, for this report, or for the opinions we have formed.

Respective responsibilities of directors and auditor

As explained more fully in the Preparation of the Financial Statements and Directors’ Responsibilities Statement set out on page 140, the Directors are responsible for the preparation of the Parent Company Financial Statements and for being satisfied that they give a true and fair view. Our responsibility is to audit, and express an opinion on, the Parent Company Financial Statements in accordance with applicable law and International Standards on Auditing (UK and Ireland). Those standards require us to comply with the Auditing Practices Board’s Ethical Standards for Auditors.

Scope of the audit of the financial statements

A description of the scope of an audit of financial statements is provided on the Financial Reporting Council’s website at frc.org.uk/auditscopeukprivate.

Opinion on financial statements

In our opinion the Parent Company Financial Statements:

 

> give a true and fair view of the state of the Company’s affairs as at 31 December 2012;
> have been properly prepared in accordance with UK
     Generally Accepted Accounting Practice; and
> have been prepared in accordance with the requirements of the Companies Act 2006.

 

Opinion on other matters prescribed by the Companies Act 2006

In our opinion:

 

> the part of the Directors’ Remuneration Report to be audited has been properly prepared in accordance with the Companies Act 2006; and
> the information given in the Directors’ Report for the financial year for which the financial statements are prepared is consistent with the Parent Company Financial Statements.

Matters on which we are required to report by exception

We have nothing to report in respect of the following matters where the Companies Act 2006 requires us to report to you if, in our opinion:

 

> adequate accounting records have not been kept by the Parent Company, or returns adequate for our audit have not been received from branches not visited by us; or
> the Parent Company Financial Statements and the part of the Directors’ Remuneration Report to be audited are not in agreement with the accounting records and returns; or
> certain disclosures of Directors’ Remuneration specified by law are not made; or
> we have not received all the information and explanations we require for our audit.

Other matter

We have reported separately on the Group Financial Statements of AstraZeneca PLC for the year ended 31 December 2012.

Jimmy Daboo

Senior Statutory Auditor

For and on behalf of KPMG Audit Plc, Statutory Auditor

Chartered Accountants

15 Canada Square, London, E14 5GL

31 January 2013

 

 

192   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

Financial Statements | Company Balance Sheet

Company Balance Sheet

at 31 December

AstraZeneca PLC

 

                                                  
     Notes     

2012

$m

    

2011

$m

 

 

Fixed assets

        

Fixed asset investments

     1         25,349         23,421   

 

Current assets

        

Debtors – other

              3         1   

Debtors – amounts owed by Group undertakings

              6,589         1,937   
                6,592         1,938   

 

Creditors: Amounts falling due within one year

        

Non-trade creditors

     2         (956      (3,217

Interest-bearing loans and borrowings

     3                 (1,749
                (956      (4,966

Net current assets/(liabilities)

              5,636         (3,028

Total assets less current liabilities

              30,985         20,393   

 

Creditors: Amounts falling due after more than one year

        

Amounts owed to Group undertakings

     3         (283      (283

Interest-bearing loans and borrowings

     3         (8,742      (6,714
                (9,025      (6,997

Net assets

              21,960         13,396   

 

Capital and reserves

        

Called-up share capital

     6         312         323   

Share premium account

     4         3,504         3,078   

Capital redemption reserve

     4         153         139   

Other reserves

     4         2,904         2,983   

Profit and loss account

     4         15,087         6,873   

Shareholders’ funds

     5         21,960         13,396   

$m means millions of US dollars.

The Company Financial Statements from page 193 to 197 were approved by the Board on 31 January 2013 and were signed on its behalf by

 

Pascal Soriot

   Simon Lowth   

Director

   Director   

Company’s registered number 2723534

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   193

Table of Contents

Financial Statements | Company Accounting Policies

Company Accounting Policies

 

Basis of accounting

The Company Financial Statements are prepared under the historical cost convention, modified to include revaluation to fair value of certain financial instruments as described below, in accordance with the Companies Act 2006 and UK Generally Accepted Accounting Practice (UK GAAP). The Group Financial Statements are presented on pages 142 to 191 and have been prepared in accordance with IFRS as adopted by the EU and as issued by the IASB and in accordance with the Group Accounting Policies set out on pages 146 to 149.

The following paragraphs describe the main accounting policies under UK GAAP, which have been applied consistently.

New accounting standards

The Company has adopted the Amendments to FRS 29 (IFRS 7) ‘Disclosures – Transfers of Financial Assets’ during the year. The adoption had no impact on the net results or net assets of the Company.

Foreign currencies

Profit and loss account items in foreign currencies are translated into US dollars at average rates for the relevant accounting periods. Assets and liabilities are translated at exchange rates prevailing at the date of the Company Balance Sheet. Exchange gains and losses on loans and on short-term foreign currency borrowings and deposits are included within net interest payable. Exchange differences on all other transactions, except relevant foreign currency loans, are taken to operating profit.

Taxation

The charge for taxation is based on the result for the year and takes into account taxation deferred because of timing differences between the treatment of certain items for taxation and for accounting purposes. Full provision is made for the effects of these differences. Deferred tax assets are recognised where it is more likely than not that the amount will be realised in the future. These estimates require judgements to be made including the forecast of future taxable income. Deferred tax balances are not discounted.

 

Accruals for tax contingencies require management to make judgements and estimates in relation to tax audit issues. Tax benefits are not recognised unless the tax positions will probably be sustained. Once considered to be probable, management reviews each material tax benefit to assess whether a provision should be taken against full recognition of that benefit on the basis of potential settlement through negotiation and/or litigation.

Any recorded exposure to interest on tax liabilities is provided for in the tax charge. All provisions are included in creditors due within one year.

Investments

Fixed asset investments, including investments in subsidiaries, are stated at cost and reviewed for impairment if there are indications that the carrying value may not be recoverable.

Share-based payments

The issuance by the Company to employees of its subsidiaries of a grant over the Company’s options represents additional capital contributions by the Company to its subsidiaries. An additional investment in subsidiaries results in a corresponding increase in shareholders’ equity. The additional capital contribution is based on the fair value of the grant issued, allocated over the underlying grant’s vesting period.

Financial instruments

Loans and other receivables are held at amortised cost. Long-term loans payable are held at amortised cost.

Litigation

Through the normal course of business, the AstraZeneca Group is involved in legal disputes, the settlement of which may involve cost to the Company. Provision is made where an adverse outcome is probable and associated costs can be estimated reliably. In other cases, appropriate descriptions are included.

 

 

194   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

Financial Statements | Notes to the Company Financial Statements

Notes to the Company Financial Statements

1 Fixed asset investments

 

                                                  
     Investments in subsidiaries  
    

Shares

$m

    

Loans

$m

    

Total

$m

 

Cost and net book value at 1 January 2012

     16,427         6,994         23,421   

Additions

             1,980         1,980   

Impairment

     (21              (21

Capital contribution

     (79              (79

Exchange

             45         45   

Amortisation

             3         3   

Cost and net book value at 31 December 2012

     16,327         9,022         25,349   

During the year management conducted an impairment review of the Company’s investment in AstraZeneca Holding GmbH because of a deterioration in the trading outlook in Germany. The review indicated that AstraZeneca Holding GmbH’s carrying amount exceeded its value by $21m and consequently the carrying amount has been written down by this amount. The impairment loss has been recognised in operating costs within the profit and loss account.

A list of principal subsidiaries is included on page 191.

2 Non-trade creditors

 

                                 
    

2012

$m

    

2011

$m

 

 

Amounts due within one year

     

Short-term borrowings (unsecured)

     792         14   

Other creditors

     158         170   

Amounts owed to Group undertakings

     6         3,033   
       956         3,217   

3 Loans

 

                                                           
           

Repayment

dates

    

2012

$m

    

2011

$m

 

 

Amounts due within one year

           

Interest-bearing loans and borrowings (unsecured)

           

5.4% Callable bond

     US dollars         2012                 1,749   

 

Amounts due after more than one year

           

Amounts owed to subsidiaries (unsecured)

           

7.2% Loan

     US dollars         2023         283         283   

Interest-bearing loans and borrowings (unsecured)

           

5.4% Callable bond

     US dollars         2014         749         749   

5.125% Non-callable bond

     euros         2015         990         969   

5.9% Callable bond

     US dollars         2017         1,745         1,744   

1.95% Callable bond

     US dollars         2019         995           

5.75% Non-callable bond

     pounds sterling         2031         561         536   

6.45% Callable bond

     US dollars         2037         2,717         2,716   

4% Callable bond

     US dollars         2042         985           
                         8,742         6,714   

 

                                 
    

2012

$m

    

2011

$m

 

Loans or instalments thereof are repayable:

     

After five years from balance sheet date

     5,541         5,279   

From two to five years

     2,735         1,718   

From one to two years

     749           

Within one year

             1,749   

Total unsecured

     9,025         8,746   

All loans are at fixed interest rates. Accordingly, the fair values of the loans will change as market rates change. However, since the loans are held at amortised cost, changes in interest rates and the credit rating of the Company do not have any effect on the Company’s net assets.

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   195

Table of Contents

Financial Statements   | Notes to the Company Financial Statements

4 Reserves

 

                                                                                                                                         
     Share
premium
account
$m 		    

Capital

redemption

reserve

$m

    

Other

reserves

$m

    

Profit

and loss

account

$m

    

2012

Total

$m

    

2011

Total

$m

 

At beginning of year

     3,078         139         2,983         6,873         13,073         19,476   

Profit for the year

                             14,467         14,467         2,961   

Dividends

                             (3,619      (3,619      (3,752

Amortisation of loss on cash flow hedge

                             1         1         2   

Share-based payments

                     (79              (79      (37

Share repurchases

             14                 (2,635      (2,621      (5,983

Issue of AstraZeneca PLC Ordinary Shares

     426                                 426         406   

At end of year

     3,504         153         2,904         15,087         21,648         13,073   

Distributable reserves at end of year

                     1,841         15,087         16,928         8,714   

As permitted by section 408(4) of the Companies Act 2006, the Company has not presented its own profit and loss account.

At 31 December 2012, $15,087m (2011: $6,873m) of the profit and loss account reserve was available for distribution. Included in other reserves is a special reserve of $157m, arising on the redenomination of share capital in 1999.

Included within other reserves at 31 December 2012 is $1,063m (2011: $1,142m) in respect of cumulative share-based payment awards. These amounts are not available for distribution.

5 Reconciliation of movement in shareholders’ funds

 

                                             
    

2012

$m

    

2011

$m

 

At beginning of year

     13,396         19,828   

Net profit for the financial year

     14,467         2,961   

Dividends

     (3,619      (3,752

Amortisation of loss on cash flow hedge

     1         2   

Share-based payments

     (79      (37

Issue of AstraZeneca PLC Ordinary Shares

     429         409   

Repurchase of AstraZeneca PLC Ordinary Shares

     (2,635      (6,015

Net increase/(decrease) in shareholders’ funds

     8,564         (6,432

Shareholders’ funds at end of year

     21,960         13,396   

Details of dividends paid and payable to shareholders are given in Note 21 to the Group Financial Statements.

6 Share capital

 

                                 
     Allotted, called-up and fully paid  
    

2012

$m

    

2011

$m

 

Issued Ordinary Shares ($0.25 each)

     312         323   

Redeemable Preference Shares (£1 each – £50,000)

               
       312         323   

The Redeemable Preference Shares carry limited class voting rights and no dividend rights. This class of shares is capable of redemption at par at the option of the Company on the giving of seven days’ written notice to the registered holder of the shares.

The movements in share capital during the year can be summarised as follows:

 

                                                 
     No. of shares      $m  

At 1 January 2012

     1,292,355,052         323   

Issues of shares

     12,241,784         3   

Repurchase of shares

     (57,817,288      (14

At 31 December 2012

     1,246,779,548         312   

Share repurchases

During the year, the Company repurchased 57.8m Ordinary Shares at an average price of 2879 pence per share (2011: 127.4m Ordinary Shares at an average price of 2932 pence per share).

Share schemes

A total of 12.2m Ordinary Shares were issued during the year in respect of share schemes (2011: 10.7m Ordinary Shares). Details of movements in the number of Ordinary Shares under option are shown in Note 24 to the Group Financial Statements; details of options granted to Directors are shown in the Directors’ Remuneration Report.

Shares held by subsidiaries

No shares in the Company are held by subsidiaries.

 

196   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

7 Litigation and environmental liabilities

In addition to those matters disclosed below, there are other cases where the Company is named as a party to legal proceedings. These include the Seroquel IR product liability litigation and the Nexium product liability litigation each of which are described more fully in Note 25 to the Group Financial Statements.

Foreign Corrupt Practices Act

In connection with an investigation into Foreign Corrupt Practices Act issues in the pharmaceutical industry, AstraZeneca has received inquiries from the US Department of Justice and the SEC regarding, among other things, sales practices, internal controls, certain distributors and interactions with healthcare providers and other government officials in several countries. AstraZeneca is co-operating with these inquiries. AstraZeneca is investigating indications of inappropriate conduct in certain countries, including China. Resolution of this matter could involve the payment of fines and/or other remedies.

Dutch National Competition Authority investigation

In the Dutch National Competition Authority (NMa) investigation into alleged abuse of a dominant position, the investigation team issued a report alleging foreclosure of generic versions of certain proton pump inhibitors other than esomeprazole. The file has now been passed to the Legal Department of the NMa. AstraZeneca completed its defence in April 2012 and awaits a decision by the Board of the NMa later in 2013.

Other

The Company has guaranteed the external borrowing of a subsidiary in the amount of $288m.

8 Statutory and other information

The Directors were paid by another Group company in 2012 and 2011.

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   197

Table of Contents

Financial Statements | Group Financial Record

Group Financial Record

 

For the year ended 31 December

  

2008

$m

   

2009

$m

   

2010

$m

   

2011

$m

   

2012

$m

 

 

Revenue and profits

          

Revenue

     31,601        32,804        33,269        33,591        27,973   

Cost of sales

     (6,598     (5,775     (6,389     (6,026     (5,393

Distribution costs

     (291     (298     (335     (346     (320

Research and development expense

     (5,179     (4,409     (5,318     (5,523     (5,243

Selling, general and administrative costs

     (10,913     (11,332     (10,445     (11,161     (9,839

Profit on disposal of subsidiary

                          1,483          

Other operating income and expense

     524        553        712        777        970   

Operating profit

     9,144        11,543        11,494        12,795        8,148   

Finance income

     854        462        516        552        528   

Finance expense

     (1,317     (1,198     (1,033     (980     (958

Profit before tax

     8,681        10,807        10,977        12,367        7,718   

Taxation

     (2,551     (3,263     (2,896     (2,351     (1,391

Profit for the period

     6,130        7,544        8,081        10,016        6,327   

Other comprehensive income for the period, net of tax

     (1,906     (54     25        (546     78   

Total comprehensive income for the period

     4,224        7,490        8,106        9,470        6,405   

Profit attributable to:

          

Equity holders of the Company

     6,101        7,521        8,053        9,983        6,297   

Non-controlling interests

     29        23        28        33        30   

 

Earnings per share

          

Earnings per $0.25 Ordinary Share (basic)

     $4.20        $5.19        $5.60        $7.33        $4.99   

Earnings per $0.25 Ordinary Share (diluted)

     $4.20        $5.19        $5.57        $7.30        $4.98   

Dividends

     $1.90        $2.09        $2.41        $2.70        $2.85   

 

Return on revenues

          

Operating profit as a percentage of revenues

     28.9%        35.2%        34.5%        38.1%        29.1%   

Ratio of earnings to fixed charges

     13.5        19.9        24.0        28.5        19.9   
          

At 31 December

  

2008

$m

   

2009

$m

   

2010

$m

   

2011

$m

   

2012

$m

 

 

Statement of Financial Position

          

Property, plant and equipment, goodwill and intangible assets

     29,240        29,422        28,986        27,267        32,435   

Other investments and non-current receivables

     605        446        535        543        940   

Deferred tax assets

     1,236        1,292        1,475        1,514        1,111   

Current assets

     15,869        23,760        25,131        23,506        19,048   

Total assets

     46,950        54,920        56,127        52,830        53,534   

Current liabilities

     (13,415     (17,640     (16,787     (15,752     (13,903

Non-current liabilities

     (17,475     (16,459     (15,930     (13,606     (15,679

Net assets

     16,060        20,821        23,410        23,472        23,952   

Share capital

     362        363        352        323        312   

Reserves attributable to equity holders

     15,550        20,297        22,861        22,923        23,425   

Non-controlling interests

     148        161        197        226        215   

Total equity and reserves

     16,060        20,821        23,410        23,472        23,952   
          

For the year ended 31 December

  

2008

$m

   

2009

$m

   

2010

$m

   

2011

$m

   

2012

$m

 

 

Cash flows

          

Net cash inflow/(outflow) from:

          

Operating activities

     8,742        11,739        10,680        7,821        6,948   

Investing activities 1

     (3,881     (2,444     (2,226     (2,022     (1,859

Financing activities 1

     (6,377     (3,661     (7,334     (9,321     (4,923
       (1,516     5,634        1,120        (3,522     166   

 

1   Investing activities and Financing activities were restated in 2011 to reclassify cash paid in hedge contracts relating to dividend payments from Investing activities to Financing activities.

For the purpose of computing the ratio of earnings to fixed charges, earnings consist of the income from continuing ordinary activities before taxation of Group companies and income received from companies owned 50% or less, plus fixed charges. Fixed charges consist of interest on all indebtedness, amortisation of debt discount and expense and that portion of rental expense representative of the interest factor.

 

198   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

Additional Information | Development Pipeline

Development Pipeline

as at 31 December 2012

Throughout the development process, we strive to obtain patent protection consistent with our patent process (as described in the Intellectual Property section from page 35). However, until marketing approval in individual countries is obtained, it is not possible to accurately predict the maximum period of product protection available from any such patents. While the most significant uncertainties for development pipeline products progressing to launch are meeting development targets and obtaining regulatory marketing approvals (as detailed in the Risk section from page 74), the date and language of any actual marketing approval will crucially determine the length of Patent Term Extension and the full range, if any, of pending patents that will protect the marketed product. Further details of possible periods of patent, RDP and related IP protections which may protect pipeline products once marketed are included from page 35.

Line Extensions

 

                Date     Estimated Filing  

Compound

  Mechanism   Area Under Investigation   Phase  

Commenced

Phase

    US     EU     Japan     China  

Cardiovascular

                                                   

Axanum

 

proton pump inhibitor +

low dose aspirin FDC

 

low dose aspirin associated

peptic ulcer in high-risk CV

patients

  III             Withdrawn        Launched        2016           

Brilinta/Brilique EUCLID

  ADP receptor antagonist   outcomes study in patients with peripheral artery disease   III     4Q 2012        2016        2016        2016        2017   

Brilinta/Brilique

PEGASUS-TIMI 54

  ADP receptor antagonist   outcomes study in patients with prior myocardial infarction   III     4Q 2010        2015        2015        2015        2017   

Bydureon EXSCEL #

  GLP-1 receptor agonist   outcomes study   III     2Q 2010        2018                           

Bydureon Dual

Chamber Pen #

  GLP-1 receptor agonist   diabetes   III             3Q 2013                           

Forxiga (dapagliflozin)/

metformin FDC #

 

SGLT2 inhibitor + metformin

FDC

  diabetes   III     3Q 2007                Filed                   

Forxiga ( dapagliflozin) #

  SGLT2 inhibitor   diabetes – add on to DPP-4   III     1Q 2010                Filed                   

Forxiga (dapagliflozin) #

  SGLT2 inhibitor   diabetes –add on to insulin and add on to metformin long-term data   III     2Q 2008                Filed                   

Forxiga (dapagliflozin) #

  SGLT2 inhibitor   diabetes – in patients with high CV risk – Study 18 and 19 long-term data   III     1Q 2010                1H 2014                   

Forxiga (dapagliflozin) #

  SGLT2 inhibitor   diabetes – triple therapy (dapa+met+SU)   III     1Q 2011                1Q 2013                   

Kombiglyze XR/

Komboglyze FDC # *

 

DPP-4 inhibitor + metformin

FDC

  diabetes   III             Launched        Launched                1H 2014   

SaxaDapa FDC #

  DPP-4 inhibitor/SGLT2 inhibitor   diabetes   III     2Q 2012        2015        2015                   

Onglyza SAVOR-TIMI 53 #

  DPP-4 inhibitor   outcomes study   III     2Q 2010        4Q 2013        4Q 2013                2H 2014   

Gastrointestinal

                                                   

Entocort

  glucocorticoid steroid   Crohn’s disease/ulcerative colitis   III             Launched        Launched        2015           

Nexium

  proton pump inhibitor   peptic ulcer bleeding   III             Filed**        Launched        n/a        Launched   

Neuroscience

                                                   

Diprivan #

  sedative and anaesthetic   conscious sedation   III                     Launched        1H 2014        Launched   

Oncology

                                                   

Faslodex

  oestrogen receptor antagonist   1 st line advanced breast cancer   III     4Q 2012        2016        2016        2016        2016   

Iressa

  EGFR tyrosine kinase inhibitor   treatment beyond progression   III     1Q 2012                2015        2015        2015   

Respiratory & Inflammation

                                           

Symbicort ***

 

inhaled steroid/long-acting

beta 2 -agonist

 

Breath Actuated Inhaler

asthma/COPD

  III     4Q 2011        1H 2014                           

 

#   Partnered product.
* Kombiglyze XR in the US; Komboglyze FDC in the EU.
** 2 nd CRL received from FDA in 2011. AstraZeneca response submitted to FDA in December 2012.
*** Excludes Symbicort pMDI post marketing LABA in December.

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   199

Table of Contents

Additional Information | Development Pipeline

as at 31 December 2012

NCEs

Phase III/Registration

 

                Date     Estimated Filing  

Compound

  Mechanism   Area Under Investigation   Phase  

Commenced

Phase

    US     EU     Japan     China  

Cardiovascular

                                                   

Brilinta/Brilique

  ADP receptor antagonist   arterial thrombosis   III             Launched        Launched        2Q 2013        Approved   

Forxiga (dapagliflozin) #

  SGLT2 inhibitor   diabetes   III             Filed     Launched        1Q 2013        1Q 2013   

metreleptin #

  leptin analogue   lipodystrophy   III             2Q 2013                n/a           

Infection

                                                   

CAZ AVI # (CAZ104)

 

beta lactamase inhibitor/

cephalosporin

  serious infections   III     1Q 2012        n/a        2H 2014        2H 2014        2016   

Q-LAIV Flu Vaccination**

 

live, attenuated, intranasal

influenza virus vaccine

(quadrivalent)

  seasonal influenza   III             Approved        Filed                   

Zinforo # (ceftaroline)

 

extended spectrum

cephalosporin with affinity

to penicillin-binding proteins

  pneumonia/skin infections   III             n/a        Launched                1H 2014   

Neuroscience

                                                   

naloxegol (NKTR-118) #

 

oral peripherally-acting

mu-opioid receptor antagonist

 

opioid-induced constipation

  III     2Q 2011        3Q 2013        3Q 2013                   

Oncology

                                                   

Caprelsa

 

VEGFR/EGFR tyrosine kinase

inhibitor with RET kinase activity

 

medullary thyroid cancer

  III             Launched        Launched        2015        Filed   

Respiratory & Inflammation

                                           

brodalumab #

  anti-IL-17R MAb   psoriasis   III     3Q 2012        2015        2015                   

fostamatinib #

 

spleen tyrosine kinase (SYK)

inhibitor

  rheumatoid arthritis   III     3Q 2010        4Q 2013        4Q 2013                   

lesinurad

  selective inhibitor of URAT1  

chronic management of

hyperuricaemia in patients

with gout

  III     4Q 2011        1H 2014        1H 2014        2017        2017   

 

#      Partnered product.

*     CRL received in January 2012.

**    sBLA in US; MAA in EU.

             

NCEs

Phases I and II

 

             
                Date     Estimated Filing  

Compound

  Mechanism   Area Under Investigation   Phase  

Commenced

Phase

    US     EU     Japan     China  

Cardiovascular

                                                   

AZD1722#

  NHE3 inhibitor  

end stage renal disease/chronic

kidney disorder

  I     4Q 2010                                   

Gastrointestinal

                                                   

tralokinumab

  anti-IL-13 MAb   ulcerative colitis   II     2Q 2012                                   

Infection

                                                   

AZD5847

 

oxazolidinone anti-bacterial

inhibitor

  tuberculosis   II     4Q 2012                                   

CXL #

 

beta lactamase inhibitor/

cephalosporin

  MRSA   II     4Q 2010                                   

ATM AVI

  BL/BLI  

targeted serious bacterial

infections

  I     4Q 2012                                   

MEDI-550

 

pandemic influenza

virus vaccine

  pandemic influenza prophylaxis   I     2Q 2006                                   

MEDI-557

 

anti-RSV MAb – extended

half-life

 

RSV prevention in high-risk

adults (COPD/CHF/other)

  I     3Q 2007                                   

MEDI-559

  paediatric RSV vaccine   RSV prophylaxis   I     4Q 2008                                   

Neuroscience

                                                   

AZD3241

 

myeloper-oxidase (MPO)

inhibitor

  Parkinson’s disease   II     2Q 2012                                   

AZD3480 #

 

alpha 4 /beta 2 neuronal

nicotinic receptor agonist

  Alzheimer’s disease   II     3Q 2007                                   

AZD5213

 

histamine-3 receptor

antagonist

  Alzheimer’s disease   II     2Q 2012                                   

AZD6765

  NMDA receptor antagonist   major depressive disorder   II     3Q 2007                                   

AZD1446 #

 

alpha 4 /beta 2 neuronal

nicotinic receptor agonist

  Alzheimer’s disease   I     4Q 2008                                   

AZD3293 #

  beta-secretase   Alzheimer’s disease   I     4Q 2012                                   

MEDI5117

  anti-IL6 MAb   rheumatoid arthritis   I     2Q 2012                                   

 

200   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

NCEs

Phases I and II continued

 

               

Date

Commenced

Phase

    Estimated Filing  

Compound

  Mechanism   Area Under Investigation   Phase     US     EU   Japan     China  

Oncology

                                                  

AZD4547

  FGFR tyrosine kinase inhibitor   solid tumours   II     4Q 2011                               

fostamatinib #

 

spleen tyrosine kinase

(SYK) inhibitor

  haematological malignancies   II     1Q 2012                               

MEDI-551 #

  anti-CD19 MAb   haematological malignancies   II     1Q 2012                               

MEDI-573 #

  anti-IGF MAb   metastatic breast cancer   II     4Q 2011                               

MEDI-575 #

  anti-PDGFR-alpha MAb   non-small cell lung cancer   II     2Q 2011                               

olaparib

  PARP inhibitor  

gBRCAm ovarian cancer,

gBRCAm breast cancer,

gastric cancer

  II     1Q 2012                               

selumetinib # (AZD6244)

(ARRY-142886)

  MEK inhibitor   solid tumours   II     4Q 2006                               

tremelimumab

  anti-CTLA4 MAb   solid tumours   II     3Q 2004                               

AZD1208

  PIM kinase inhibitor   haematological malignancies   I     1Q 2012                               

AZD2014

  TOR kinase inhibitor   solid tumours   I     1Q 2010                               

AZD5363 #

  AKT inhibitor   solid tumours   I     4Q 2010                               

AZD8330 # (ARRY 424704)

  MEK inhibitor   solid tumours   I     1Q 2007                               

AZD9150

  STAT3 inhibitor   haematological malignancies   I     1Q 2012                               

MEDI0639 #

  anti-DLL-4 MAb   solid tumours   I     2Q 2012                               

MEDI3617 #

  anti-ANG-2 MAb   solid tumours   I     4Q 2010                               

MEDI4736 #

  anti-PD-L1 MAb   solid tumours   I     3Q 2012                               

MEDI-565 #

  anti-CEA BiTE   solid tumours   I     1Q 2011                               

MEDI6469 #

  murine anti-OX40 MAb   solid tumours   I     1Q 2006                               

moxetumomab pasudotox #

 

anti-CD22 recombinant

immunotoxin

  haematological malignancies   I     2Q 2007                               

volitinib #

  MET inhibitor   solid tumours   I     1Q 2012                               

Respiratory & Inflammation

                                               

AZD2115 #

  MABA   COPD   II     2Q 2012                               

AZD5069

  CXCR2   asthma   II     4Q 2010                               

AZD5423 #

  inhaled SGRM   COPD   II     4Q 2010                               

benralizumab #

  anti-IL-5R MAb   asthma/COPD   II     4Q 2008                               

mavrilimumab #

  anti-GM-CSFR MAb   rheumatoid arthritis   II     1Q 2010                               

MEDI-546 #

  anti-IFN-alphaR MAb   SLE   II     1Q 2012                               

MEDI7183 #

  anti-a4b7 MAb   Crohn’s disease/ulcerative colitis   II     4Q 2012                               

MEDI8968 #

  anti-IL-1R MAb   COPD   II     4Q 2011                               

sifalimumab #

  anti-IFN-alpha MAb   SLE   II     3Q 2008                               

tralokinumab

  anti-IL-13 MAb   asthma/IPF   II     1Q 2008                               

AZD8848 #

  inhaled TLR7   asthma   I     2Q 2012                               

AZD7594 #

  inhaled SGRM   COPD   I     4Q 2012                               

MEDI2070 #

  anti-IL-23 MAb   Crohn’s disease   I     2Q 2010                               

MEDI4212

  anti-IgE MAb   asthma   I     1Q 2012                               

MEDI-551 #

  anti-CD19 MAb   multiple sclerosis   I     3Q 2012                               

MEDI5872 #

  anti-B7RP1 MAb   SLE   I     4Q 2008                               

MEDI7814

  anti-C5/C5a MAb   COPD   I     1Q 2012                               

MEDI9929 #

  anti-TSLP MAb   asthma   I     4Q 2008                               

RDEA3170

  selective inhibitor of URAT1  

chronic management of

hyperuricaemia in patients

with gout

  I     3Q 2011                               

 

#   Partnered product.

Comments

Submission dates shown for assets in Phase III and beyond.

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   201

Table of Contents

Additional Information | Development Pipeline

as at 31 December 2012

Discontinued Projects between 31 December 2011 and 31 December 2012

 

NCE/Line Extension

  Compound   Reason for Discontinuation   Area Under Investigation

Cardiovascular

           

NCE

  AZD2820   Safety/Efficacy   obesity

NCE

  AZD4017   Safety/Efficacy   glaucoma

NCE

  AZD2927   Safety/Efficacy   atrial fibrillation

Infection

           

NCE

  AZD9773   Safety/Efficacy   severe sepsis

NCE

  AZD5099   Safety/Efficacy   serious infections

NCE

  MEDI-534   Safety/Efficacy   RSC/PIV prophylaxis

Neuroscience

           

NCE

  AZD2423   Safety/Efficacy   chronic neuropathic pain

NCE

  AZD3839   Safety/Efficacy   Alzheimer’s disease

NCE

  MEDI-578   Regulatory   OA pain

NCE

  TC-5214   Safety/Efficacy   major depressive disorder (monotherapy)

NCE

  TC-5214   Safety/Efficacy   major depressive disorder (adjunct)

Oncology

           

NCE

  AZD1480   Safety/Efficacy   solid tumours

NCE

  AZD3514   Safety/Efficacy   prostate cancer

NCE

  AZD8931   Safety/Efficacy   breast cancer chemo. combi./solid tumours

NCE

 

selumetinib (AZD6244)

(ARRY-142886)/MK2206 #

  Study completed   solid tumours

Respiratory & Inflammation

           

NCE

  AZD8683   Safety/Efficacy   COPD

NCE

  MEDI-570   Safety/Efficacy   SLE

NCE

  AZD1981   Safety/Efficacy   asthma/COPD

NCE

  AZD2423   Safety/Efficacy   COPD

 

#   Partnered product.

Completed Projects

 

            Launch Status  

Compound

  Mechanism   Area Under Investigation               US     EU     Japan     China  

Cardiovascular

                                   

Crestor #

  statin   outcomes in subjects with elevated CRP     Launched        Launched                Launched   

Gastrointestinal

                                   

Nexium

  proton pump inhibitor   GERD     Launched        Launched        Launched        Launched   

Infection

                                   

FluMist/Fluenz

 

live, attenuated, intranasal influenza

virus vaccine

  influenza     Launched        Launched                   

Neuroscience

                                   

EMLA

  local anaesthetic   topical anaesthesia             Launched        Launched           

Oncology

                                   

Iressa

  EGFR tyrosine kinase inhibitor   1st line EGFR mut+ NSCLC             Launched        Launched        Launched   

Faslodex

  oestrogen receptor antagonist  

high dose (500mg) 2 nd line advanced

breast cancer

    Launched        Launched        Launched           

Ranmark # (denosumab)

  anti-RANKL MAb  

bone disorders stemming from bone

metastasis

                    Launched           

Respiratory & Inflammation

                                   

Oxis

  long-acting beta 2 -agonist   COPD             Launched        Launched        Launched   

Symbicort

  inhaled steroid/long-acting beta 2 -agonist   COPD     Launched        Launched        Launched        Launched   

Symbicort

  inhaled steroid/long-acting beta 2 -agonist   SMART             Launched        Launched        Launched   

 

#   Partnered product.

Comments

As disclosure of compound information is balanced by the business need to maintain confidentiality, information in relation to some compounds listed here has not been disclosed at this time.

 

202   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

Additional Information | Shareholder Information

Shareholder Information

AstraZeneca PLC share listings and prices

 

                                                                          
     2008      2009      2010      2011      2012  

Ordinary Shares in issue – millions

                                            

At year end

     1,447         1,451         1,409         1,292         1,247   

Weighted average for year

     1,453         1,448         1,438         1,361         1,261   

Stock market price – per Ordinary Share

                                            

Highest (pence)

     2888         2947         3385         3194         3111.5   

Lowest (pence)

     1748         2147         2732         2543.5         2591   

At year end (pence)

     2807         2910.5         2922         2975         2909.5   

Percentage analysis of issued share capital at 31 December

 

  

By size of account

Number of Ordinary Shares

  

2008

%

    

2009

%

    

2010

%

    

2011

%

    

2012

%

 

1 – 250

     0.5         0.5         0.5         0.6         0.6   

251 – 500

     0.7         0.7         0.6         0.7         0.7   

501 – 1,000

     0.9         0.8         0.8         0.8         0.8   

1,001 – 5,000

     1.2         1.1         1.1         1.2         1.1   

5,001 – 10,000

     0.2         0.2         0.2         0.2         0.2   

10,001 – 50,000

     1.0         1.1         1.0         1.0         1.0   

50,001 – 1,000,000

     13.6         13.0         12.8         13.8         12.6   

Over 1,000,000 1

     81.9         82.6         83.0         81.7         83.0   

 

1   Includes Euroclear and ADR holdings.

At 31 December 2012, the Company had 111,111 registered holders of 1,246,779,548 Ordinary Shares. There were 122,617 holders of Ordinary Shares held under the Euroclear Services Agreement, representing 12.9% of the issued share capital of the Company and approximately 235,000 holders of ADRs, representing 11.0% of the issued share capital of the Company. The ADRs, each of which is equivalent to one Ordinary Share, are issued by JPMorgan Chase Bank (JPMorgan).

During 2012, under AstraZeneca’s share repurchase programme, which was introduced in 1999, 57.8 million Ordinary Shares were repurchased and subsequently cancelled at a total cost of $2,635 million, representing 4.6% of the total issued share capital of the Company at 31 December 2012. The average price paid per Ordinary Share in 2012 was 2879 pence. This brings the total number of Ordinary Shares repurchased to date since the beginning of the repurchase programme in 1999, to 615.2 million Ordinary Shares (at an average price of 2777 pence per Ordinary Share) for a consideration, including expenses, of $29,352 million. The excess of the consideration over the nominal value was charged against the profit and loss account reserve. Ordinary Shares issued in respect of share schemes in 2012 totalled 12.2 million. The Company suspended its share repurchase programme effective 1 October.

In 1999, in connection with the merger between Astra and Zeneca through which the Company was formed, the Company’s share capital was redenominated in US dollars. On 6 April 1999, Zeneca shares were cancelled and US dollar shares issued, credited as fully paid on the basis of one dollar share for each Zeneca share then held. This was achieved by a reduction of capital under section 135 of the Companies Act 1985. Upon the reduction of capital becoming effective, all issued and unissued Zeneca shares were cancelled and the sum arising as a result of the share cancellation credited to a special reserve, which was converted into US dollars at the rate of exchange prevailing on the record date. This US dollar reserve was then applied in paying up, at par, newly created US dollar shares.

At the same time as the US dollar shares were issued, the Company issued 50,000 Redeemable Preference Shares for cash, at par. The Redeemable Preference Shares carry limited class voting rights, no dividend rights and are capable of redemption, at par, at the option of the Company on the giving of seven days’ written notice to the registered holder of the Redeemable Preference Shares.

A total of 826 million Ordinary Shares were issued to Astra shareholders who accepted the merger offer before the final closing date, 21 May 1999. The Company received acceptances from Astra shareholders representing 99.6% of Astra’s shares and the remaining 0.4% was acquired in 2000, for cash.

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   203

Table of Contents

Additional Information | Shareholder Information

Since April 1999, following the merger of Astra and Zeneca, the principal markets for trading in the shares of the Company are the London Stock Exchange (LSE), the Stockholm Stock Exchange (SSE) and the New York Stock Exchange (NYSE). The table below sets out, for 2011 and 2012, the reported high and low share prices of the Company, on the following bases:

 

> For shares listed on the LSE, the reported high and low middle market closing quotations are derived from the Daily Official List.
> For shares listed on the SSE, the high and low closing sales prices are as stated in the Official List.
> For ADSs listed on the NYSE, the reported high and low sales prices are as reported by Dow Jones (ADR quotations).

 

          Ordinary LSE      Ordinary SSE      ADS  
                  High (pence)      Low (pence)              High (SEK)      Low (SEK)              High (US$)      Low (US$)  

2011

   – Quarter 1      3073.5         2801.5         320.6         289.0         49.38         45.40   
     – Quarter 2      3194.0         2895.0         328.5         294.2         52.40         46.60   
     – Quarter 3      3166.5         2543.5         324.5         269.3         51.08         40.95   
     – Quarter 4      3080.5         2731.5         319.0         293.7         49.89         42.53   

2012

   – Quarter 1      3111.5         2778.5         329.5         294.5         48.58         44.18   
     – Quarter 2      2867.0         2591.0         309.3         286.2         46.22         40.03   
     – Quarter 3      3096.0         2882.0         326.4         307.3         48.36         45.01   
     – Quarter 4      3042.5         2792.5         326.3         300.8         48.90         44.34   
     – July      3002.5         2882.0         326.4         311.8         47.34         45.01   
     – August      3096.0         2936.5         324.8         309.0         48.21         46.79   
     – September      2976.0         2888.5         316.9         307.3         48.36         46.34   
     – October      2951.0         2860.0         313.2         307.0         47.63         45.82   
     – November      2966.5         2792.5         316.7         300.8         47.55         44.34   
     – December      3042.5         2909.5         326.3         306.4         48.90         46.88   

Major shareholdings

At 31 January 2013, the following had disclosed an interest in the issued Ordinary Share capital of the Company in accordance with the requirements of rule 5.1.2 of the UK Listing Authority’s Disclosure and Transparency Rules:

 

Shareholder

   Number of
shares 		     Date of
disclosure to
Company 1 		     Percentage of
issued share
capital 		 

BlackRock, Inc.

     100,885,181         8 December 2009         8.08   

Invesco Limited

     72,776,277         6 October 2009         5.83   

Axa SA

     56,991,117         3 February 2009         4.57   

Investor AB

     51,587,810         2 February 2012         4.13   

Legal & General Investment Management Limited

     57,675,232         5 August 2010         4.62   

 

1   Since the date of disclosure to the Company, the interest of any person listed above in Ordinary Shares may have increased or decreased. No requirement to notify the Company of any increase or decrease would have arisen unless the holding moved up or down through a whole number percentage level. The percentage level may increase (on the cancellation of shares following a repurchase of shares under the Company’s share repurchase programme) or decrease (on the issue of new shares under any of the Company’s share plans).

So far as the Company is aware, no other person held a notifiable interest in shares, comprising 3% or more of the issued Ordinary Share capital of the Company.

Changes in the percentage ownership held by major shareholders during the past three years are set out below. Major shareholders do not have different voting rights.

 

     Percentage of issued share capital  

Shareholder

       31 Jan 2013      2 Feb 2012      27 Jan 2011      28 Jan 2010  

BlackRock, Inc.

     8.08         7.87         7.18         6.94   

Invesco Limited

     5.83         5.67         5.18         5.01   

Axa SA

     4.57         4.44         4.06         3.92   

Investor AB

     4.13         4.02         3.67         3.55   

Legal & General Investment Management Limited

     4.62         4.50         4.10         4.64   

ADSs evidenced by ADRs issued by JPMorgan, as depositary, are listed on the NYSE. At 31 January 2013, the proportion of Ordinary Shares represented by ADSs was 11.17% of the Ordinary Shares outstanding.

Number of registered holders of Ordinary Shares at 31 January 2013:

 

> In the US        743
> Total 110,421

Number of record holders of ADRs at 31 January 2013:

 

> In the US     2,103
> Total     2,122

So far as the Company is aware, it is neither directly nor indirectly owned or controlled by one or more corporations or by any government.

 

204   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

At 31 January 2013, the total amount of the Company’s voting securities owned by Directors and officers of the Company was:

 

Title of class

   Amount
owned 		     Percentage of
class 		 

Ordinary Shares

     274,159         0.02   

The Company does not know of any arrangements, the operation of which might result in a change in the control of the Company.

Related party transactions

During the period 1 January 2013 to 31 January 2013, there were no transactions, loans, or proposed transactions between the Company and any related parties which were material to either the Company or the related party, or which were unusual in their nature or conditions (see also Note 27 to the Financial Statements on page 190).

Options to purchase securities from registrant or subsidiaries

(a) At 31 January 2013, options outstanding to subscribe for Ordinary Shares were:

 

Number of shares

   Subscription
price (pence) 		     Normal expiry date  

19,572,351

     1882 – 3335         2013 – 2019   

The weighted average subscription price of options outstanding at 31 January 2013 was 2542 pence. All options were granted under Company employee share schemes.

(b) Included in paragraph (a) are options granted to Directors and officers of the Company as follows:

 

Number of shares

   Subscription
price (pence) 		     Normal expiry date  

299,060

     1882 – 3335         2014 – 2019   

 

(c) Included in paragraph (b) are options granted to individually named Directors. Details of these option holdings at 31 December 2012 are shown in the Share option plans table on page 137.

During the period 1 January 2013 to 31 January 2013, no Director exercised any options.

Dividend payments

For Ordinary Shares listed on the LSE and the SSE and ADRs listed on the NYSE, the record date for the second interim dividend for 2012, payable on 18 March 2013, is 15 February 2013 and the ex-dividend date is 13 February 2013.

The record date for the first interim dividend for 2013, payable on 16 September 2013, is 16 August 2013.

Future dividends will normally be paid as follows:

 

First interim: Announced in July and paid in September.
Second interim: Announced in January and paid in March.

Shareview

The Company’s shareholders with internet access may visit the website, shareview.co.uk, and register their details to create a portfolio. Shareview is a free and secure online service from the Company’s registrars, Equiniti Limited, which gives access to shareholdings, including balance movements, indicative share prices and information about recent dividends.

ShareGift

The Company welcomes and values all of its shareholders, no matter how many or how few shares they own. However, shareholders who have only a small number of shares whose value makes it uneconomic to sell them, either now or at some stage in the future, may wish to consider donating them to charity through ShareGift, an independent charity share donation scheme. One feature of the scheme is that there is no gain or loss for UK capital gains tax purposes on gifts of shares through ShareGift, and it may now also be possible to obtain UK income tax relief on the donation. Further information about ShareGift can be found on its website, sharegift.org, or by contacting ShareGift on 020 7930 3737 or at 17 Carlton House Terrace, London SW1Y 5AH. ShareGift is administered by The Orr Mackintosh Foundation, registered charity number 1052686. More information about the UK tax position on gifts of shares to ShareGift can be obtained from HM Revenue & Customs on their website, hmrc.gov.uk.

The Unclaimed Assets Register

The Company supplies unclaimed dividend data to the Unclaimed Assets Register (UAR), which provides investors who have lost track of shareholdings with an opportunity to search the UAR’s database of unclaimed financial assets on payment of a small fixed fee. The UAR donates part of the search fee to charity. The UAR can be contacted on 0870 241 1713 or at PO Box 9501, Nottingham NG80 1WD.

Results

Unaudited trading results of AstraZeneca in respect of the first three months of 2013 will be published on 25 April 2013 and results in respect of the first six months of 2013 will be published on 1 August 2013.

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   205

Table of Contents

Additional Information | Shareholder Information

Documents on display

The Articles and other documents concerning the Company which are referred to in this Annual Report may be inspected at the Company’s registered office at 2 Kingdom Street, London W2 6BD.

Taxation for US residents

The following summary of material UK and US federal income tax consequences of ownership of Ordinary Shares or ADRs held as capital assets by the US resident holders described below is based on current UK and US federal income tax law, including the US/UK double taxation convention relating to income and capital gains, which entered into force on 31 March 2003 (the Convention). This summary does not describe all of the tax consequences that may be relevant in light of the US resident holders’ particular circumstances and tax consequences applicable to US resident holders subject to special rules (such as certain financial institutions, entities treated as partnerships for US federal income tax purposes, persons whose functional currency for US federal income tax purposes is not the US dollar, tax-exempt entities, or persons holding Ordinary Shares or ADRs in connection with a trade or business conducted outside of the US). US resident holders are urged to consult their tax advisers regarding the UK and US federal income tax consequences of the ownership and disposition of Ordinary Shares or ADRs in their particular circumstances.

This summary is based in part on representations of JPMorgan as depositary for ADRs and assumes that each obligation in the deposit agreement among the Company, JPMorgan and the holders from time to time of ADRs and any related agreements will be performed in accordance with its terms. The US Treasury has expressed concerns that parties to whom American depository shares are released before shares are delivered to the depositary (pre-release), or intermediaries in the chain of ownership between holders and the issuer of the security underlying the American depository shares, may be taking actions that are inconsistent with the claiming, by US holders of American depository shares, of foreign tax credits for US federal income tax purposes. Such actions would also be inconsistent with the claiming of the reduced tax rates, described below, applicable to dividends received by certain non-corporate US resident holders. Accordingly, the availability of the reduced tax rates for dividends received by certain non-corporate US resident holders could be affected by actions that may be taken by parties to whom ADRs are pre-released.

For the purposes of this summary, the term ‘US resident holder’ means a beneficial owner of Ordinary Shares or ADRs that is, for US federal income tax purposes, a citizen or resident of the US, a corporation (or other entity taxable as a corporation) created or organised in or under the laws of the US, any state in the US or the District of Columbia, or an estate or trust the income of which is subject to US federal income taxation regardless of its source.

This summary assumes that we are not, and will not become, a passive foreign investment company, as discussed below.

UK and US income taxation of dividends

The UK does not currently impose a withholding tax on dividends paid by a UK company, such as the Company.

For US federal income tax purposes, distributions paid by the Company to a US resident holder are included in gross income as foreign source ordinary dividend income to the extent paid out of the Company’s current or accumulated earnings and profits, calculated in accordance with US federal income tax principles. Because the Company does not maintain calculations of its earning and profits under US federal income tax principles, it is expected that distributions generally will be reported to US resident holders as dividends. The amount of the dividend will be the US dollar amount received by the depositary for US resident holders of ADRs (or, in the case of Ordinary Shares, the US dollar value of the pounds sterling payments made, determined at the spot pound sterling/US dollar rate on the date the dividend is received by the US resident holders, regardless of whether the dividend is converted into US dollars), and it will not be eligible for the dividends received deduction generally available to US corporations. If the dividend is converted into US dollars on the date of receipt, US resident holders of Ordinary Shares generally should not be required to recognise foreign currency gains or losses in respect of the dividend income. They may have foreign currency gain or loss if the amount of such dividend is converted into US dollars after the date of its receipt.

Subject to applicable limitations and the discussion above regarding concerns expressed by the US Treasury, dividends received by certain non-corporate US resident holders of Ordinary Shares or ADRs may be taxable at favourable US federal income tax rates. US resident holders should consult their own tax advisers to determine whether they are subject to any special rules which may limit their ability to be taxed at this favourable rate.

Taxation on capital gains

Under present UK law, individuals who are neither resident nor ordinarily resident in the UK, and companies which are not resident in the UK, will not be liable for UK tax on capital gains made on the disposal of their Ordinary Shares or ADRs, unless such Ordinary Shares or ADRs are held in connection with a trade, profession or vocation carried on in the UK through a branch or agency or other permanent establishment.

A US resident holder will generally recognise US source capital gains or losses for US federal income tax purposes on the sale or exchange of Ordinary Shares or ADRs in an amount equal to the difference between the US dollar amount realised and such holder’s US dollar tax basis in the Ordinary Shares or ADRs. US resident holders should consult their own tax advisers about the treatment of capital gains, which may be taxed at lower rates than ordinary income for non-corporate US resident holders and capital losses, the deductibility of which may be limited.

Passive Foreign Investment Company (PFIC) rules

We believe that we were not a PFIC for US federal income tax purposes for the year ended 31 December 2012. However, since PFIC status depends on the composition of our income and assets and the market value of our assets (including, among others, less than 25% owned equity investments) from time to time, there can be no assurance that we will not be considered a PFIC for any taxable year. If we were treated as a PFIC for any taxable year during which Ordinary Shares or ADRs were held, certain adverse tax consequences could apply to US resident holders.

 

206   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

Information reporting and backup withholding

Payments of dividends and sales proceeds that are made within the US or through certain US-related financial intermediaries may be subject to information reporting and backup withholding, unless (i) the US resident holder is a corporation or other exempt recipient or (ii) in the case of backup withholding, the US resident holder provides a correct taxpayer identification number and certifies that it is not subject to backup withholding. The amount of any backup withholding from a payment to a US resident holder will be allowed as a credit against the holder’s US federal income tax liability and may entitle the holder to a refund, provided that the required information is supplied to the Internal Revenue Service (IRS) on time.

Certain US resident holders who are individuals (and under proposed US Treasury regulations, certain entities), may be required to report information relating to securities issued by non-US persons (or foreign accounts through which the securities are held), generally on IRS Form 8938, subject to certain exceptions (including an exception for securities held in accounts maintained by US financial institutions). US resident holders should consult their tax advisers regarding their reporting obligations with respect to the Ordinary Shares or ADRs.

UK inheritance tax

Under the current Double Taxation (Estates) Convention (the Estate Tax Convention) between the US and the UK, Ordinary Shares or ADRs held by an individual shareholder who is domiciled for the purposes of the Estate Tax Convention in the US, and is not for the purposes of the Estate Tax Convention a national of the UK, will generally not be subject to UK inheritance tax on the individual’s death or on a chargeable gift of the Ordinary Shares or ADRs during the individual’s lifetime, provided that any applicable US federal gift or estate tax liability is paid, unless the Ordinary Shares or ADRs are part of the business property of a permanent establishment of the individual in the UK or, in the case of a shareholder who performs independent personal services, pertain to a fixed base situated in the UK. Where the Ordinary Shares or ADRs have been placed in trust by a settlor who, at the time of settlement, was a US domiciled shareholder, the Ordinary Shares or ADRs will generally not be subject to UK inheritance tax unless the settlor, at the time of settlement, was a UK national, or the Ordinary Shares or ADRs are part of the business property of a permanent establishment of the individual in the UK or, in the case of a shareholder who performs independent personal services, pertain to a fixed base situated in the UK. In the exceptional case where the Ordinary Shares or ADRs are subject to both UK inheritance tax and US federal gift or estate tax, the Estate Tax Convention generally provides for double taxation to be relieved by means of credit relief.

UK stamp duty reserve tax and stamp duty

A charge to UK stamp duty or UK stamp duty reserve tax (SDRT) may arise on the deposit of Ordinary Shares in connection with the creation of ADRs. The rate of stamp duty or SDRT will generally be 1.5% of the value of the consideration or, in some circumstances, the value of the Ordinary Shares. However, following a recent ruling in the UK, there is no 1.5% SDRT charge on the issue of Ordinary Shares (or, where it is integral to the raising of new capital, the transfer of Ordinary Shares) into the ADR arrangement.

No UK stamp duty will be payable on the acquisition or transfer of existing ADRs provided that any instrument of transfer or written agreement to transfer is executed outside the UK and remains at all times outside the UK. An agreement for the transfer of ADRs will not give rise to a liability for SDRT.

A transfer of or an agreement to transfer Ordinary Shares will generally be subject to UK stamp duty or SDRT at 0.5% of the amount or value of any consideration, provided, in the case of stamp duty, it is rounded to the nearest £5.

Transfers of Ordinary Shares into CREST will generally not be subject to stamp duty or SDRT unless such a transfer is made for a consideration in money or money’s worth, in which case a liability to SDRT will arise, usually at the rate of 0.5% of the value of the consideration. Paperless transfers of Ordinary Shares within CREST are generally liable to SDRT at the rate of 0.5% of the value of the consideration. CREST is obliged to collect SDRT from the purchaser on relevant transactions settled within the system.

Exchange controls and other limitations affecting security holders

There are no governmental laws, decrees or regulations in the UK restricting the import or export of capital or affecting the remittance of dividends, interest or other payments to non-resident holders of Ordinary Shares or ADRs.

There are no limitations under English law or the Articles on the right of non-resident or foreign owners to be the registered holders of, or to exercise voting rights in relation to, Ordinary Shares or ADRs or to be registered holders of notes or debentures of Zeneca Wilmington Inc. or the Company.

Exchange rates

The following information relating to average and spot exchange rates used by AstraZeneca is provided for convenience:

 

     SEK/US$      US$/GBP  

Average rates (statement of comprehensive income, statement of cash flows)

     

2010

     7.2504         1.5453   

2011

     6.5059         1.5996   

2012

     6.7782         1.5834   

End of year spot rates (statement of financial position)

     

2010

     6.7511         1.5422   

2011

     6.9050         1.5443   

2012

     6.5176         1.6171   

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   207

Table of Contents

Additional Information | Corporate Information

Corporate Information

 

History and development of the Company

AstraZeneca PLC was incorporated in England and Wales on 17 June 1992 under the Companies Act 1985. It is a public limited company domiciled in the UK. The Company’s registered number is 2723534 and its registered office is at 2 Kingdom Street, London W2 6BD (telephone +44 (0)20 7604 8000). From February 1993 until April 1999, the Company was called Zeneca Group PLC. On 6 April 1999, the Company changed its name to AstraZeneca PLC.

The Company was formed when the pharmaceutical, agrochemical and specialty chemical businesses of Imperial Chemical Industries PLC were demerged in 1993. In 1999, the Company sold the specialty chemical business. Also in 1999, the Company merged with Astra of Sweden. In 2000, it demerged the agrochemical business and merged it with the similar agribusiness of Novartis to form a new company called Syngenta AG.

In 2007, the Group acquired MedImmune, a biologics and vaccines business based in the US.

The Group owns and operates numerous R&D, production and marketing facilities worldwide. Its corporate office is at 2 Kingdom Street, London W2 6BD.

Articles

Objects

The Company’s objects are unrestricted.

Any amendment to the Articles requires the approval of shareholders by a special resolution at a general meeting of the Company.

Directors

The Board has the authority to manage the business of the Company, for example, through powers to allot and repurchase its shares, subject where required to shareholder resolutions. Subject to certain exceptions, Directors do not have power to vote at Board meetings on matters in which they have a material interest.

The quorum for meetings of the Board is a majority of the full Board, of whom at least four must be Non-Executive Directors. In the absence of a quorum, the Directors do not have power to determine compensation arrangements for themselves or any member of the Board.

The Board may exercise all the powers of the Company to borrow money. Variation of these borrowing powers would require the passing of a special resolution of the Company’s shareholders.

All Directors must retire from office at the Company’s AGM each year and may present themselves for election or re-election. Directors are not prohibited, upon reaching a particular age, from submitting themselves for election or
re-election.

Within two months of the date of their appointment, Directors are required to beneficially own Ordinary Shares of an aggregate nominal amount of at least $125, which currently represents 500 shares.

Rights, preferences and restrictions attaching to shares

As at 31 December 2012, the Company had 1,246,779,548 Ordinary Shares and 50,000 Redeemable Preference Shares in issue. The Ordinary Shares represent 99.98% and the Redeemable Preference Shares represent 0.02% of the Company’s total share capital (these percentages have been calculated by reference to the closing mid-point US$/GBP exchange rate on 31 December 2012 as published in the London edition of the Financial Times newspaper). As agreed by the shareholders at the Company’s AGM held on 29 April 2010, the Articles were amended with immediate effect to remove the requirement for the Company to have an authorised share capital, the concept of which was abolished under the Companies Act 2006. Each Ordinary Share carries the right to vote at general meetings of the Company. The rights and restrictions attaching to the Redeemable Preference Shares differ from those attaching to Ordinary Shares as follows:

 

> The Redeemable Preference Shares carry no rights to receive dividends.
> The holders of Redeemable Preference Shares have no rights to receive notices of, attend or vote at general meetings except in certain limited circumstances. They have one vote for every 50,000 Redeemable Preference Shares held.
> On a distribution of assets of the Company, on a winding-up or other return of capital (subject to certain exceptions), the holders of Redeemable Preference Shares have priority over the holders of Ordinary Shares to receive the capital paid up on those shares.
> Subject to the provisions of the Companies Act 2006, the Company has the right to redeem the Redeemable Preference Shares at any time on giving not less than seven days’ written notice.

There are no specific restrictions on the transfer of shares in the Company, which is governed by the Articles and prevailing legislation.

The Company is not aware of any agreements between holders of shares that may result in restrictions on the transfer of shares or that may result in restrictions on voting rights.

Action necessary to change the rights of shareholders

In order to vary the rights attached to any class of shares, the consent in writing of the holders of three-quarters in nominal value of the issued shares of that class or the sanction of an extraordinary resolution passed at a general meeting of such holders is required.

General meetings

AGMs and other general meetings, as from time to time may be required, where a special resolution is to be passed or a Director is to be appointed, require 21 clear days’ notice to shareholders. Subject to the Companies Act 2006, other general meetings require 14 clear days’ notice.

For all general meetings, a quorum of two shareholders present in person or by proxy, and entitled to vote on the business transacted, is required unless each of the two persons present are corporate representatives of the same corporation; or each of the two persons present are proxy of the same shareholder.

Shareholders and their duly appointed proxies and corporate representatives are entitled to be admitted to general meetings.

Limitations on the rights to own shares

There are no limitations on the rights to own shares.

Property

Substantially all of our properties are held freehold, free of material encumbrances and are fit for their purpose.

 

 

208   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

Additional Information | Glossary

Glossary

Market definitions

 

United States of America

  Other Established Markets       Emerging Markets        

US

  Western Europe   Japan   Emerging Europe   China   Other Emerging ROW
    Austria       Albania*       Egypt
    Belgium   Canada   Belarus*   Emerging Asia Pacific   Gulf States
    Denmark       Bosnia and Herzegovina   Bangladesh*   Israel*
    Finland   Other Established ROW   Bulgaria   Cambodia*   Latin America
    France   Australia   Croatia   Hong Kong   Lebanon*
    Germany   New Zealand   Czech Republic   India   Maghreb
    Greece       Estonia*   Indonesia*   Saudi Arabia
    Iceland*       Georgia*   Laos*   South Africa
    Ireland       Hungary   Malaysia    
    Italy       Kazakhstan*   Philippines    
    Luxembourg*       Latvia*   Singapore    
    Netherlands       Lithuania*   South Korea    
    Norway       Macedonia*   Sri Lanka*    
    Portugal       Poland   Taiwan    
    Spain       Romania*   Thailand    
    Sweden       Russia   Vietnam*    
    Switzerland       Serbia and Montenegro*        
    UK       Slovakia        
           

Slovenia*

       
           

Turkey

       
           

Ukraine*

       

Rest of World means Other Established Markets and Emerging Markets.

Established Markets means the US and Other Established Markets.

Established ROW means Canada, Japan and Other Established ROW.

Latin America includes Argentina, Brazil, Chile, Colombia, Costa Rica*, El Salvador*, Guatemala*, Honduras*, Mexico, Nicaragua*, Panama*, Peru* and Venezuela.

Gulf States includes Bahrain*, Dubai*, Kuwait*, Oman*, Qatar* and UAE.

Maghreb means Algeria, Morocco and Tunisia*.

*IMS Health, IMS Midas Quantum Q3 2012 data is not available or AstraZeneca does not subscribe for IMS Health quarterly data for these countries.

The above table is not an exhaustive list of all the countries in which AstraZeneca operates.

US equivalents

 

Terms used in this Annual Report

   US equivalent or brief description

Accruals

   Accrued expenses

Allotted

   Issued

Called-up share capital

   Issued share capital

Creditors

   Liabilities/payables

Debtors

   Receivables and prepaid expenses

Earnings

   Net income

Employee share schemes

   Employee stock benefit plans

Fixed asset investments

   Non-current investments

Freehold

   Ownership with absolute rights in perpetuity

Interest payable

   Interest expense

Loans

   Long-term debt

Prepayments

   Prepaid expenses

Profit

   Income

Profit and loss account

   Income statement/consolidated statement of comprehensive income

Share premium account

   Premiums paid in excess of par value of Ordinary Shares

Short-term investments

   Redeemable securities and short-term deposits

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   209

Table of Contents

Additional Information | Glossary

 

Glossary

The following abbreviations and expressions have the following meanings when used in this Annual Report:

Abbott – Abbott Laboratories, Inc. with respect to Crestor and Synagis .

Affordable Care Act – the Patient Protection and Affordable Care Act which was signed into law on 23 March 2010 as amended by the Health Care and Education Reconciliation Act which was signed into law on 30 March 2010.

ADR – an American Depositary Receipt evidencing title to an ADS.

ADS – an American Depositary Share representing one underlying Ordinary Share.

AGM – an Annual General Meeting of the Company.

Amgen – Amgen, Inc.

Amylin – Amylin Pharmaceuticals, LLC (formerly Amylin Pharmaceuticals, Inc.).

ANDA – an abbreviated new drug application, which is a marketing approval application for a generic drug submitted to the FDA.

Annual Report – this Annual Report and Form 20-F Information 2012.

API – active pharmaceutical ingredient.

Ardea – Ardea Biosciences, Inc.

Ardelyx – Ardelyx, Inc.

Articles – the Articles of Association of the Company.

Astra – Astra AB, being the company with whom the Company merged in 1999.

Astra Tech – Astra Tech AB.

AstraZeneca – the Company and its subsidiaries.

AZIP – AstraZeneca Investment Plan.

biologic(s) – a class of drugs based on large protein molecules that have a therapeutic effect.

biosimilar(s) – a copy of a biologic that is sufficiently similar to meet regulatory requirements, which can compete with patented biologics once they have come off patent.

BMS – Bristol-Myers Squibb Company.

Board – the Board of Directors of the Company.

Bureau Veritas – Bureau Veritas UK Limited.

CEO – the Chief Executive Officer of the Company.

CER – constant exchange rates.

CFO – the Chief Financial Officer of the Company.

CHMP – the Committee for Medicinal Products for Human Use, being a committee of the EMA.

CIS – Commonwealth of Independent States.

Code of Conduct – the Group’s Code of Conduct.

Company or Parent Company – AstraZeneca PLC (formerly Zeneca Group PLC (Zeneca)).

Complete Response Letter (CRL) – a letter issued by the FDA communicating its decision to a drug company that its NDA or biological licensing application is not approvable as submitted. The submitting drug company is required to respond to the Complete Response Letter if it wishes to pursue an approval for its submission.

Corporate Integrity Agreement (CIA) – the agreement described in the US Corporate Integrity Agreement reporting section on page 39.

Dainippon Sumitomo – Dainippon Sumitomo Pharmaceuticals Co., Limited.

Director – a director of the Company.

earnings per share (EPS) – profit for the year after tax and minority interests, divided by the weighted average number of Ordinary Shares in issue during the year.

EFPIA – European Federation of Pharmaceutical Industries and Associations.

EMA – the European Medicines Agency.

EMEA – Europe, Middle East and Africa.

EU – the European Union.

FDA – the US Food and Drug Administration, which is part of the US Department of Health and Human Services Agency, which is the regulatory authority for all pharmaceuticals (including biologics and vaccines) and medical devices in the US.

Forest – Forest Laboratories Holdings Limited.

GAAP – Generally Accepted Accounting Principles.

GERD – gastro oesophageal reflux disease.

GI – gastrointestinal.

GIA – AstraZeneca’s group internal audit function.

gross margin – the margin, as a percentage, by which sales exceed the cost of sales, calculated by dividing the difference between the two by the sales figure.

Group – AstraZeneca PLC and its subsidiaries.

GSK – GlaxoSmithKline plc.

HR – human resources.

IAS – International Accounting Standards.

IAS 19 – IAS 19 Employee Benefits.

IAS 32 – IAS 32 Financial Instruments: Presentation.

IAS 39 – IAS 39 Financial Instruments: Recognition and Measurement.

IASB – International Accounting Standards Board.

IFRS – International Financial Reporting Standards or International Financial Reporting Standard, as the context requires.

IFRS 8 – IFRS 8 Operating Segments.

IP – intellectual property.

Ironwood – Ironwood Pharmaceuticals, Inc.

IS – information services.

IT – information technology.

KPI – key performance indicator.

krona or SEK – references to the currency of Sweden.

Lean – means enhancing value for customers with fewer resources.

MAA – a marketing authorisation application, which is an application for authorisation to place medical products on the market. This is a specific term used in the EU and European Economic Area markets.

MAb – monoclonal antibody, a biologic that is specific, that is, it binds to and attacks one particular antigen.

MedImmune – MedImmune, LLC (formerly MedImmune, Inc.).

Merck – Merck Sharp & Dohme Corp. (formerly Merck & Co., Inc.).

NDA – a new drug application to the FDA for approval to market a new medicine in the US.

NCE – new chemical entity.

Novartis – Novartis Pharma A.G.

Novexel – Novexel S.A.

NSAID – a non-steroidal anti-inflammatory drug.

NYSE – the New York Stock Exchange.

n/m – not meaningful.

operating profit – sales, less cost of sales, less operating costs, plus operating income.

Ordinary Share – an ordinary share of $0.25 each in the share capital of the Company.

Orphan Drug – a drug which has been approved for use in a relatively low-incidence indication (an orphan indication) and has been rewarded with a period of market exclusivity; the period of exclusivity and the available orphan indications vary between markets.

OTC – over-the-counter.

Paediatric Exclusivity – in the US, a six month period of exclusivity to market a drug which is awarded by the FDA in return for certain paediatric clinical studies using that drug. This six month period runs from the date of relevant patent expiry. Analogous provisions are available in certain other territories (eg European SPC paediatric extensions).

Patent Term Extension (PTE) – an extension of up to five years in the term of a US patent relating to a drug which compensates for delays in marketing resulting from the need to obtain FDA approval. The analogous right in the EU is a supplementary protection certificate (SPC).

Pfizer – Pfizer, Inc.

Phase I – the phase of clinical research where a new drug or treatment is tested in small groups of people (20 to 80) to check that the drug can achieve appropriate concentrations in the body, determine a safe dosage range and identify side effects. This phase includes healthy volunteer studies.

Phase II – the phase of clinical research which includes the controlled clinical activities conducted to evaluate the effectiveness of the drug in patients with the disease under study and to begin to determine the safety profile of the drug. Phase II studies are typically conducted in a relatively small number of patients and can be divided into Phase IIa studies, which tend to be designed to assess dosing requirements, and Phase IIb studies, which tend to assess safety and efficacy.

Phase III – the phase of clinical research which is performed to gather additional information about effectiveness and safety of the drug, often in a comparative setting, to evaluate the overall benefit/risk profile of the drug. Phase III studies usually include between several hundred and several thousand patients.

pounds sterling, £, GBP, pence or p – references to the currency of the UK.

Pozen – POZEN INC.

primary care – general healthcare provided by physicians who generally have first contact with patients and who may have continuing care for them.

Proof of Concept – data demonstrating that a candidate drug results in a clinical change on an acceptable endpoint or surrogate in patients with the disease.

PSP – AstraZeneca Performance Share Plan.

R&D – research and development.

Redeemable Preference Share – a redeemable preference share of £1 each in the share capital of the Company.

Regulatory Data Protection – see the Intellectual Property section from page 35.

Regulatory Exclusivity – any of the IP rights arising from generation of clinical data and includes Regulatory Data Protection, Paediatric Exclusivity and Orphan Drug status.

Responsible Business Plan – the plan described in the Responsible Business section from page 48, further details of which can be found at our website, astrazeneca.com/responsible/management-and-measurement/responsible-business-plan.

RSV – respiratory syncytial virus.

Sarbanes-Oxley Act – the US Sarbanes-Oxley Act of 2002.

SEC – the US Securities and Exchange Commission, the governmental agency that regulates the US securities industry/stock market.

Seroquel franchise Seroquel IR and Seroquel XR.

SET – Senior Executive Team.

SHE – Safety, Health and Environment.

SFDA – State Food and Drug Administration of China.

SG&A costs – selling, general and administrative costs.

Six Sigma – a rigorous and disciplined methodology that uses data and statistical analysis to measure and improve a company’s operational performance by identifying and eliminating defects.

SOP – AstraZeneca Share Option Plan.

specialty care – specific healthcare provided by medical specialists who do not generally have first contact with patients.

Targacept – Targacept, Inc.

Teva – Teva Pharmaceuticals USA, Inc.

TKI – tyrosine kinase inhibitor.

TSR – total shareholder return, being the total return on a share over a period of time, including dividends reinvested.

UK – United Kingdom of Great Britain and Northern Ireland.

UK Corporate Governance Code – the UK Corporate Governance Code published by the Financial Reporting Council in May 2010 that sets out standards of good practice in corporate governance for the UK.

US – United States of America.

US dollar, US$, USD or $ – references to the currency of the US.

WHO – the World Health Organization, the United Nations’ specialised agency for health.

 

 

210   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

Additional Information | Trade marks

Trade marks

AstraZeneca, the AstraZeneca logotype and the AstraZeneca symbol are all trade marks of the AstraZeneca group of companies.

The following brand names which appear in italics in this Annual Report are trade marks of the Group:

 

Trade mark

   Comments

Accolate

    

Arimidex

    

Atacand

   Atacand Plus in rest of world (not in the US or the EU)

Axanum

   Not in the US

Brilinta

   In the US and rest of world (not in the EU)

Brilique

   In the EU

Caprelsa

    

Casodex

    

Crestor

    

Diprivan

    

EMLA

   Not in the US or the EU

Entocort

    

Faslodex

    

FluMist

   In the US and the rest of world. Fluenz in the EU.

Iressa

    

Merrem

   Meronem in the EU and rest of world (not in the US)

Naropin

   Not in the US or the EU

Nexium

    

Nolvadex

    

Oxis Turbuhaler

   Not in the US or the EU

Plendil

    

Losec/Prilosec

   In the EU and rest of world (not in the US). Prilosec in the US

Pulmicort

    

Pulmicort Respules

    

Pulmicort Turbuhaler

    

Rhinocort

    

Seloken Zoc

   Not in the US. Seloken , Seloken XL, Seloken Zoc or Seloken Zok in rest of world (not in the US or the EU)

Seroquel

    

Seroquel IR

    

Seroquel XR

    

Symbicort

    

Symbicort SMART

   Not in the US

Symbicort Turbuhaler

   Not in the US or the EU

Synagis

   In the US. Abbott owns the trade mark for Synagis in rest of world (not in the US or the EU)

Tenormin

    

Toprol-XL

   In the US. Seloken/Betaloc Zok in rest of world (not in the US or the EU)

Vimovo

    

Xylocaine

   Not in the US or the EU

Zestril

    

Zoladex

    

Zomig

   Not in the US

The following brand names which appear in italics in this Annual Report are trade marks licensed to the Group by the entities set out below:

 

Trade mark

   Owner    Comments

Bydureon

   Amylin – North & South Americas; AstraZeneca – rest of world (not in the US or the EU)    Ownership dependent upon geography

Byetta

   Amylin – North & South Americas; AstraZeneca – rest of world (not in the US or the EU)    Ownership dependent upon geography

Cubicin

   Cubist Pharmaceuticals, Inc.     

Forxiga

   BMS     

Kombiglyze XR

   BMS     

Kombiglyze

   BMS     

Komboglyze

   BMS     

Linzess

   Ironwood    Brand name for linaclotide in the US

Onglyza

   BMS     

Ranmark

   Daiichi Sankyo Company, Limited     

Symlin

   Amylin – North & South Americas; AstraZeneca Pharmaceuticals LP – rest of world (not in the    Ownership dependent upon geography
     US or the EU)     

Teflaro

   Forest    Brand name for ceftaroline in the US

Zinforo

   Forest    Ownership of Zinforo trade mark was assigned from AstraZeneca to Forest in April 2012

The following brand names which appear in italics throughout this Annual Report are not owned by or licensed to the Group and are owned by the entities set out below:

 

Trade mark

   Owner     

Lipitor

   Pfizer Ireland Pharmaceuticals     

Plavix

   Sanofi     

 

LOGO

 

 

AstraZeneca Annual Report and Form 20-F Information 2012   211

Table of Contents

Additional Information | Index

 

2012 performance summary    24
Accounting policies    146, 194
Acquisitions and disposals    173
Amgen    31, 55, 68, 93
Amylin    31, 55, 71, 93, 161
Annual general meeting    121, 208
Ardea    31, 69, 90, 173
Articles of association    206, 208
Astra Tech    174
Audit Committee    75, 115
Biologics    17, 19, 30
Board    106, 110
Branches    120

Business background

and results overview

   86
Capitalisation    94
Cardiovascular    52
Cash and cash equivalents    148, 164
Chairman’s Statement    6
Chief Executive Officer’s Review    8
Clinical Trials    33, 34
Code of Conduct    47
Commitments and contingent liabilities    183
Community Investment    49
Company history    203, 208
Competition    16, 78

Compliance and

Group Internal Audit

   47, 75, 115

Consolidated statement

of Cash Flows

   145

Consolidated statement

of Changes in Equity

   144

Consolidated statement

of Comprehensive Income

   142

Consolidated statement

of Financial Position

   143
Corporate governance    104
Diabetes    52, 54
Directors’ interest in shares    134
Directors’ remuneration    122
Directors’ responsibility statement    140
Diversity    43, 44
Dividends    7, 94, 173, 205
Earnings per ordinary share    5, 154
Emerging Markets    13, 73, 77, 209

Employee costs and share

plans for employees

   179
Established Markets    38, 72, 209
Ethics    33, 39, 47
Finance income and expense    152
Financial instruments    148, 166
Financial position 2011    97
Financial position 2012    92
Financial risk management    99, 175
Financial summary    2
Gastrointestinal    56
Glossary    209
Goodwill    92, 97, 101, 147, 158
Group Financial Record    198
Group Financial Statements    140
Growth drivers    16
Human Rights    45
Independent auditor’s report    141, 192
Infection    58
Inflammation    see Respiratory & Inflammation

 

Intangible assets   92, 97, 101, 159
Intellectual Property   35

Interest-bearing loans

and borrowings

  164
Inventories   148, 163
Ironwood   31, 57
Key performance indicators   26
Leases   148, 190
Lifecycle of a medicine   14
Litigation   102, 149, 184
Market definitions   209
Medicines   2, 14, 30, 50
Neuroscience   61

Nomination and

Governance Committee

  117
Oncology   65
Operating profit   2, 4, 89, 151
Operational overview   4
Other investments   148, 163
Patents   see Intellectual Property
Patient safety   34
People   5, 24, 28, 43, 179
Pharmaceutical industry   16
Pipeline   4, 24, 26, 30, 51, 199
Political donations   120
Portfolio Investment Board   119
Post-retirement benefits   102, 131, 167
Pricing   18, 38
Principal risks and uncertainties   75
Product revenue information   150
Property, plant and equipment   148, 157
Provisions for liabilities and charges   167
Regulatory requirements   17
Related party transactions   190, 205
Relations with shareholders   114
Remuneration Committee   117
Research and Development   30, 147, 151
Reserves   171
Respiratory & Inflammation   67
Responsible Business   28, 48
Restructuring   21, 151
Results of operations 2011   95
Results of operations 2012   89
Revised Core financial measures   97
Safety, health and wellbeing   46
Sales and Marketing   37
Sales by geographical area   70
Sales by Therapy Area   50
Science Committee   118
Segment information   155
Senior Executive Team   108, 118
Share capital   172, 196, 203
Share repurchase   7, 94, 173, 196
Statutory and other information   190
Strategy   20
Subsidiaries   191
Supply and Manufacturing   40
Taxation   99, 103, 147, 152, 189, 194
Taxation information for shareholders   206
Trade and other payables   148, 166
Trade and other receivables   148, 164
Trade marks   211
Transactions with directors   133
World pharmaceutical markets   16

 

 

 

212   AstraZeneca Annual Report and Form 20-F Information 2012

Table of Contents

 

Important information for readers of this Annual Report

Cautionary statement regarding forward-looking statements

The purpose of this Annual Report is to provide information to the members of the Company. The Company and its Directors, employees, agents and advisers do not accept or assume responsibility to any other person to whom this Annual Report is shown or into whose hands it may come and any such responsibility or liability is expressly disclaimed. In order, among other things, to utilise the ‘safe harbour’ provisions of the US Private Securities Litigation Reform Act of 1995 and the UK Companies Act 2006, we are providing the following cautionary statement: This Annual Report contains certain forward-looking statements with respect to the operations, performance and financial condition of the Group. Forward-looking statements are statements relating to the future which are based on information available at the time such statements are made, including information relating to risks and uncertainties. Although we believe that the forward-looking statements in this Annual Report are based on reasonable assumptions, the matters discussed in the forward-looking statements may be influenced by factors that could cause actual outcomes and results to be materially different from those expressed or implied by these statements. The forward-looking statements reflect knowledge and information available at the date of the preparation of this Annual Report and the Company undertakes no obligation to update these forward-looking statements. We identify the forward-looking statements by using the words ‘anticipates’, ‘believes’, ‘expects’, ‘intends’ and similar expressions in such statements. Important factors that could cause actual results to differ materially from those contained in forward-looking statements, certain of which are beyond our control, include, among other things, those factors identified in the Principal risks and uncertainties section from page 75 of this Annual Report. Nothing in this Annual Report should be construed as a profit forecast.

 

Inclusion of Reported performance, Core financial measures and constant exchange rate growth rates

AstraZeneca’s determination of non-GAAP measures together with our presentation of them within our financial information may differ from similarly titled non-GAAP measures of other companies.

 

Statements of competitive position, growth rates and sales

In this Annual Report, except as otherwise stated, market information regarding the position of our business or products relative to its or their competition is based upon published statistical sales data for the 12 months ended 30 September 2012 obtained from IMS Health, a leading supplier of statistical data to the pharmaceutical industry. For the US, dispensed new or total prescription data and audited sales data are taken, respectively, from IMS Health National Prescription Audit and IMS National Sales Perspectives for the 12 months ended 31 December 2012; such data is not adjusted for Medicaid and similar rebates. Except as otherwise stated, these market share and industry data from IMS Health have been derived by comparing our sales revenue to competitors’ and total market sales revenues for that period. Except as otherwise stated, growth rates are given at CER. For the purposes of this Annual Report, unless otherwise stated, references to the world pharmaceutical market or similar phrases are to the 54 countries contained in the IMS Health MIDAS Quantum database, which amounted to approximately 92% (in value) of the countries audited by IMS Health.

 

AstraZeneca websites

Information on or accessible through our websites, including astrazeneca.com, astrazenecaclinicaltrials.com and medimmune.com, does not form part of and is not incorporated into this Annual Report.

 

External/third party websites

Information on or accessible through any third party or external website does not form part of and is not incorporated into this Annual Report.

 

Figures

Figures in parentheses in tables and in the Financial Statements are used to represent negative numbers.

  LOGO

 

Table of Contents

 

LOGO

 

Exhibit 15.2

REPORT OF INDEPENDENT REGISTERED PUBLIC ACCOUNTING FIRM

The Board of Directors and Stockholders
AstraZeneca PLC:
 
We have audited the accompanying Consolidated Statements of Financial Position of AstraZeneca PLC and subsidiaries (“AstraZeneca”) as of 31 December 2012, 2011 and 2010, and the related Consolidated Statements of Comprehensive Income, Changes in Equity, and Cash Flows for each of the years in the three-year period ended 31 December 2012 presented on pages 142 to 191. These Consolidated Financial Statements are the responsibility of the AstraZeneca’s management. Our responsibility is to express an opinion on these Consolidated Financial Statements based on our audits.
 
We conducted our audits in accordance with the standards of the Public Company Accounting Oversight Board (United States) (“PCAOB”). Those standards require that we plan and perform the audit to obtain reasonable assurance about whether the financial statements are free of material misstatement. An audit includes examining, on a test basis, evidence supporting the amounts and disclosures in the financial statements. An audit also includes assessing the accounting principles used and significant estimates made by management, as well as evaluating the overall financial statement presentation.  We believe that our audits provide a reasonable basis for our opinion.
 
In our opinion, the Consolidated Financial Statements referred to above present fairly, in all material respects, the financial position of AstraZeneca as of 31 December 2012, 2011 and 2010, and the results of its operations and its cash flows for each of the years in the three-year period ended 31 December 2012, in conformity with International Financial Reporting Standards (“IFRSs”) as issued by the International Accounting Standards Board and IFRSs as adopted by the European Union.
 
We also have audited, in accordance with the standards of the Public Company Accounting Oversight Board (United States), AstraZeneca Plc’s internal control over financial reporting as of 31 December 2012, based on criteria established in Internal Control – Integrated Framework issued by the Committee of Sponsoring Organizations of the Treadway Commission (“COSO”), and our report dated 31 January 2013 expressed an unqualified opinion on the effectiveness of the Company’s internal control over financial reporting.
 

 
/s/ KPMG Audit Plc

KPMG Audit Plc
15 Canada Square
London
United Kingdom
E14 5GL


31 January 2013


Exhibit 15.3
 
 
CONSENT OF INDEPENDENT REGISTERED PUBLIC ACCOUNTING FIRM
 
The Board of Directors
AstraZeneca PLC
 
We consent to the incorporation by reference in the registration statements (No. 33-83774, No. 333-145848, No. 333-114165 and No. 333-171306) on Form F-3 and registration statements (No. 333-09060, No. 333-09062, No. 33-65362, No. 33-65366, No. 333-12310, No. 333-12426, No. 333-12428, No. 333-13328, No. 333-13918, No. 333-124689, No. 333-152767 and No. 333-170381) on Form S-8 of AstraZeneca PLC of our reports dated January 31, 2013 with respect to the consolidated statements of financial position of AstraZeneca PLC and subsidiaries as of December 31, 2012, 2011 and 2010, and the related consolidated statements of comprehensive income, changes in equity and cash flows for each of the years in the three-year period ended December 31, 2012, and the effectiveness of internal control over financial reporting as of December 31, 2012, which reports appear in the 2012 Annual Report on Form 20-F of AstraZeneca PLC.
 
 
/s/ KPMG Audit Plc
 
KPMG Audit Plc
 
London
United Kingdom
25 March 2013
 
 
 
 
 
Exhibit 15.4

[IMS HEALTH HQ LIMITED LETTERHEAD]



AstraZeneca PLC
Legal & Secretary’s Department
2 Kingdom Street
London
W2 6BD
For the attention of Adrian Kemp
By fax 020 7604 8151 & by post


25 March, 2013


Dear Ladies and Gentlemen

IMS DATA DISCLOSURE FOR ANNUAL REPORT AND FORM 20-F INFORMATION 2012

In connection with the anticipated filing by AstraZeneca PLC (“AstraZeneca”) of a Form 20-F with the US Securities and Exchange Commission, IMS Health HQ Limited hereby authorizes AstraZeneca to refer to IMS Health and certain pharmaceutical industry data derived by IMS Health, as identified (highlighted in yellow) on the pages annexed hereto as Exhibit A, a selection of pages from AstraZeneca’s Annual Report and Form 20-F Information for the fiscal year ended December 31, 2012 (the “Annual Report”), which is incorporated by reference in the registration statements No. 33-83774 for AstraZeneca and Zeneca Wilmington Inc. and No. 333-145848, No. 333-114165 and No. 333-171306 for AstraZeneca, each on Form F-3, and in the registration statements No. 333-09060, No. 333-09062, No. 33-65362, No, 33-65366, No. 333-12310, No. 333-12426, No. 333-12428, No. 333-13328, No. 333-13918, No. 333-124689, No. 333-152767 and No. 333-170381 on Form S-8 for AstraZeneca.

IMS Health’s authorization is subject to AstraZeneca’s acknowledgement and agreement that:

1)  
IMS Health has not been provided with a full copy of the draft Annual Report but only a very limited number of pages from the documents as indicated above;

2)  
IMS Health has not undertaken an independent review of the information disclosed in the Annual Report other than to discuss our observations as to the accuracy of the information relating to IMS Health and certain pharmaceutical industry data derived by IMS Health;

3)  
AstraZeneca acknowledges and agrees that IMS Health shall not be deemed an “Expert” in respect of AstraZeneca’s securities filings, and AstraZeneca agrees that it shall not characterize IMS Health as such; and

4)  
AstraZeneca accepts full responsibility for the disclosure of all information and data, including that relating to IMS Health, set forth in the Annual Report as filed with the SEC and agrees to indemnify IMS Health from any third party claims that may arise therefrom.
 
 
 
 
 
Please indicate your agreement to the foregoing by signing in the space indicated below. Our authorization will not become effective until accepted and agreed by AstraZeneca.


Very truly yours,


/s/ James E. Salitan
James E. Salitan
Vice President and Associate General Counsel, EMEA Region
For and on behalf of IMS Health HQ Limited



ACCEPTED AND AGREED

this 25th day of March 2013

AstraZeneca PLC


/s/ Adrian Kemp
Name: Adrian Kemp
Title: Company Secretary
 
 
 
 
 
 
 

Exhibit A

 

LOGO

 

Distinctive capabilities

AstraZeneca has clear strengths that allow us to create value for patients and for shareholders:

 

> Good underlying science. External opinion leaders confirm that we have strong disease knowledge, research portfolios, and related technology platforms in a number of areas, particularly in oncology, and respiratory and inflammation.
> Unique scientific capabilities. Few pharmaceutical companies in the world, if any, can match the combination of capabilities that we have in small molecules, biologics, immunotherapies and antibody engineering. These capabilities allow us to produce combination therapies (such as drug antibody conjugates and bispecifics) and customisable molecules, both targeted to specific patient populations.
> Strong therapy area franchises, brands and commercial capability . Over the past decade, we have developed strong commercial franchises that address respiratory, cardiovascular, oncology and neuroscience diseases. We continue to develop these strong therapeutic area positions: for example, Brilinta/Brilique and the diabetes portfolio we are commercialising jointly with BMS provide the next phase of development for our cardiovascular and metabolic disease franchise. We have strong commercial capability in developing, marketing and
  selling primary care, specialty care-led and specialty care products.
> Strong Emerging Markets presence. We combine global reach with local customer relationships. We do this particularly well in Emerging Markets, where we invested early and where our decentralised approach to sales and marketing has allowed us to develop and act on local customer insight. For example, we are the second largest pharmaceutical company in China by sales.

As we look ahead, the future success of an innovation-driven R&D-based business such as AstraZeneca must be based on the twin foundations of a focus on patients and great science. We are one of only a handful of companies to span the entire life-cycle of a medicine from discovery, early and late-stage development to the global commercialisation of primary care, specialty care-led and specialty care medicines. Using these skills and capabilities we can make a real difference to the health of a broad range of patients in disease areas where there is unmet medical need in more than 100 markets around the world. We also harness these skills and capabilities in partnership with others, such as the relationships we have with BMS and Amgen.

 

Health connects us all

We know we cannot deliver on our commitment to improve healthcare on our own. We work closely with others in the healthcare community to understand their needs and challenges, and how we can combine skills and resources to achieve common goals. To be able to do this, people must have confidence in both what we do and how we do it. We know that their trust depends on us acting with integrity and staying true to our core values.

The principles of Courage, Collaboration and Creativity frame our values. They describe what we stand for as a company, and the behaviours we need to demonstrate to achieve our strategic priorities. These values reflect our belief that health connects us all. They guide our actions and shape the culture that underpins our drive for business success.

 

 

LOGO

 

AstraZeneca Annual Report and Form 20-F Information 2012   13

Strategy | Our industry

 

LOGO

 

Our industry

Introduction

The pharmaceutical industry has doubled in value since 2000, driven by a large number of FDA approvals in the second half of the 1990s and by the increased use of medicines around the world in the wake of global economic growth in that period. Now, many of the drivers of demand and supply in the industry are under pressure.

Nonetheless, as the figure above shows, the world pharmaceutical market grew by 2.5% in 2012. Average revenue growth in Established Markets was 1.5% while that in Emerging Markets was over seven times higher at 11.1%. The top five pharmaceutical markets in the world remained the US, Japan, Germany, France and China, with the US representing 39.3% of global pharmaceutical sales (2011: 38.1%).

On the demand side, underlying demographic trends remain favourable to long-term industry growth. These are outlined below. However, securing recognition (through reimbursement approval) and reward (through favourable pricing and sales) for innovation is becoming more difficult, as there are intensifying pricing pressures, particularly in Established Markets which are facing rising healthcare costs. Our challenge is to work with governments and other payers to ensure they understand the value of pharmaceutical innovation in order for us to achieve adequate commercial returns on our investment. We also face increased competition from generic medicines as some of the world’s most successful drugs come off patent. Finally, greater regulatory constraints are being placed on the pharmaceutical industry by governments and those who pay for medicines.

On the supply side, the industry faces an ongoing and significant R&D productivity challenge. R&D costs have risen significantly over the past decade, while industry-wide probability of success from pre-clinical to launch continues to decline. For example, the median large pharmaceutical company success rate for 2007 to 2011 in delivering a compound from pre-clinical studies to launch was 2%. These factors are considered in more detail below.

The industry remains highly competitive. Our competitors are other large research-based pharmaceutical companies that discover, develop and sell innovative, patent-protected prescription medicines and vaccines, as well as smaller biotechnology and vaccine companies, and companies that produce generic medicines. While many of our peers are confronting similar challenges, strategically these challenges are being met in different ways. For example, while some companies have pursued a focused strategy, others have diversified by acquiring or building branded generics businesses or consumer portfolios, arguing that this enables them to better meet changing customer needs and smooth risk for shareholders.

While most companies continued to pursue their existing strategies in 2012, there were exceptions with some companies moving away from diversification. Key trends across the industry included ongoing efforts to improve R&D innovation and productivity, expansion of geographic scope, especially in Emerging Markets and Japan, and the pursuit of operational efficiency. There was an increase in business development and partnering at all stages of product development, with a continued increase in peer collaboration.

Growth drivers

Expanding patient populations

The world population is expected to rise from its current level of some seven billion and reach nine billion by 2050. In addition, the number of people who can access healthcare continues to increase, particularly among the elderly. Globally, it is estimated that between 2000 and 2050, the number of people aged 60 years and over will increase from 605 million to two billion.

Faster-developing economies, such as China, India and Brazil, offer new opportunities for the pharmaceutical industry to help an expanding number of patients who can benefit from innovative medicines. Developing markets now represent approximately 85% of the world population and over 22% of the world’s pharmaceutical revenues. Pharmaceutical revenues in those markets therefore continued to grow faster than those in Established Markets in 2012. As the Estimated pharmaceutical market growth 2011-2016 figure on page 20 shows, we expect this trend will continue.

Unmet medical need

In most developed markets, ageing populations and certain lifestyle choices such as smoking, a poor diet and lack of exercise drive an increased incidence of non-communicable diseases (NCDs) such as cancer, cardiovascular/ metabolic and respiratory diseases which require long-term management. In 2008, almost two-thirds of deaths globally were from NCDs and 80% of those were in lower and middle income countries. For example, in South Asia it is estimated that deaths from NCDs will increase from half to almost three-quarters of all deaths between 2008 and 2030. It is also estimated that nearly one-third of the world’s diabetes patients will come from

 

16   AstraZeneca Annual Report and Form 20-F Information 2012

Strategy | Our industry

 

LOGO

 

So far as the development of biosimilars is concerned, health authorities continue to face the challenge of developing robust standards to ensure their safety, effectiveness and quality. For further information on biosimilars, see the Patent expiries and genericisation section below.

Efforts to harmonise regulations globally continue, yet the number of regulations and their impact continue to multiply. Clinical trials that support the registration of products in a given regulatory jurisdiction must be relevant to a variety of patient demographics. Programmes using foreign clinical trial data also need to meet each individual health authority’s requirements and be relevant to their population. Health authorities continue to redefine patient safety assessment processes. In addition, in emerging pharmaceutical markets, health authorities are developing their own individual requirements and safety initiatives.

One impact of the growing complexity and globalisation of clinical studies, and the pressure on industry and healthcare budgets, has been an increase in industry collaborations with health authorities. These are driving innovation and streamlining regulatory processes, as well as defining and clarifying approval requirements for new technology and approaches such as personalised healthcare. They are also accelerating the development of treatments that address public health priorities.

In another trend, health technology assessors and payers are increasingly assessing not only the safety of products but also their relative effectiveness and value. Consequently, there is a heightened interest by health authorities in both comparative clinical effectiveness and the ongoing benefit/risk assessment of medicines after they have been approved. This is resulting in a greater focus on incorporating validated health outcome measures into clinical trials and the development of clinical comparative evidence.

However, it remains the case that when applications are supported by strong data and compelling benefit/risk propositions, regulators are approving drugs that address unmet medical need.

Pricing pressure

The pricing and reimbursement environment in many markets continues to be highly challenging. Most pharmaceutical sales are generated in highly regulated markets where governments and private payers, such as insurance companies, exert various levels of control on pricing and reimbursement. Cost-containment, including containment of spending on pharmaceuticals, continues to be a focus. A wave of austerity programmes following the current global economic downturn further constrain healthcare providers and tougher economic conditions constrain those patients who pay directly for their medicines. Additional challenges may arise if suppliers and distributors face credit-related difficulties. At the same time, significant extra resources are required by pharmaceutical companies to demonstrate to payers the economic as well as therapeutic value of medicines.

In 2012, pressures on pricing included the implementation of a variety of drug price control mechanisms and other regulatory reforms, as well as the introduction of fixed hospital tariffs which can act as a method of controlling drug costs by incentivising hospitals to choose cheaper generic alternatives over patent-protected medicines.

In the US, the Affordable Care Act has already had a direct impact on healthcare activities despite the fact that many of the healthcare coverage expansion provisions of the Affordable Care Act do not take effect until 2014. For example, in 2010 there was an increase in the mandatory Medicaid rebates. In addition, the pharmaceutical industry, including AstraZeneca, is making prescription drugs more affordable to senior citizens through, for example, helping to close the coverage gap in the Medicare Part D prescription drug programme. The industry continues to work with policymakers and regulators with a view to ensuring that they strike a balance between containing costs, improving outcomes and promoting an environment that fosters medical innovation.

In August 2011, as part of the bipartisan agreement to raise the federal debt ceiling, the US Congress created the Joint Select Committee on Deficit Reduction (Committee). The Committee was empowered to recommend a package of $1.2 trillion in cost savings with the requirement that, if the Committee failed to reach an agreement, the savings would be achieved through across the board spending cuts (sequestration).

 

18   AstraZeneca Annual Report and Form 20-F Information 2012

LOGO

 

The Committee discussions ended without reaching an agreement and, barring future action by Congress, sequestration was to take effect on 2 January 2013. Sequestration would have impacted most federal government healthcare programmes with broad reductions in federal government spending. On 3 January 2013, President Barack Obama signed a bill that avoided sequestration. The bill allowed the US Congress and the President an additional two months to address the sequestration challenge. As Congress and the President continue to discuss how to reduce government expenditure, some policymakers may look to the pharmaceutical industry to help achieve the cost savings they seek.

In Europe, governments have issued new legislation on mandatory discounts, clawbacks and referencing rules, driving prices down, especially in the distressed economies of Greece, Portugal and Spain. It has been estimated that in Greece, Ireland, Italy, Portugal and Spain the pharmaceutical industry accommodated price cuts and discounts of more than 7 billion in 2010 and 2011, which amounted to 8% of the industry’s turnover in these countries. In Germany, Europe’s largest pharmaceutical market, manufacturers are now required to prove the additional benefit of their drugs over existing alternatives. Only by showing additional benefit can the drug avoid being transferred to the German reference pricing system, where, for each drug group, a single reimbursement level or reference price is set.

Elsewhere, in China, the triennial maximum retail drug price review took place in 2012, with more stringent rules being imposed compared with previous rounds of cuts, while in Japan biennial cuts are expected to continue. In Latin America, pricing is increasingly controlled by governments, for example in Colombia and Venezuela.

More information regarding the impact of price controls and reductions, as well as the impact of healthcare reform in the US, can be found in the Principal risks and uncertainties section from page 75. The principal aspects of price regulation in our major markets are described further in the Geographical Review from page 70.

Patent expiries and genericisation

We are in the middle of a period in which some of the biggest selling drugs the industry has ever produced face patent expiry. As a consequence, payers, physicians and patients in Established Markets will have access to low price, generic alternatives in many important classes of primary care drugs. For example, in the US in 2012, generics constituted 84% of the market by volume.

Patents only protect pharmaceutical products for a finite period and the expiry or early loss of patents often leads to the availability of generics. Generic versions of drugs are very competitive with significantly lower pricing than the innovator equivalents. This is partly due to lower investment by generic manufacturers in R&D and market development. While generic competition has traditionally occurred when patents

expire, it can also occur where the validity of patents is disputed or successfully challenged before expiry. Such early challenges by generics have increased with generics companies increasingly willing to launch products ‘at risk’, for example, prior to resolution of the relevant patent litigation. This trend is likely to continue, resulting in significant market presence for the generic version during the period in which litigation remains unresolved, even though the courts may subsequently rule that the innovative product is properly protected by a valid patent. The unpredictable nature of patent litigation has led innovators to seek to settle such challenges on terms acceptable to both innovator and generic manufacturer. However, some competition authorities have sought to challenge the scope and/or availability of this type of settlement agreement.

Biologics have, to date, sustained longer life-cycles than traditional small molecule pharmaceuticals and have faced less generic competition. This is due to a more complex manufacturing process for biologics compared with small molecule medicines. It is also due to the inherent difficulties in producing a biosimilar which, as a biological equivalent, rather than an exact chemical copy, could require additional clinical trials. However, with regulatory authorities in Europe and the US continuing to implement abbreviated approvals pathways for biosimilar versions, innovative biologics are likely to become increasingly subject to competition from biosimilars.

 

LOGO

 

AstraZeneca Annual Report and Form 20-F Information 2012   19

Strategy | Our strategy

 

LOGO

 

Building trust

The pharmaceutical industry faces a challenge in building and maintaining trust, particularly with governments and regulators. The last 10 years have seen a significant increase in the number of settlements between innovator companies and governmental and regulatory authorities for violations of a variety of laws. These include breaches of sales and marketing practices, inducements of physicians to administer a company’s products and breaches of anti-trust legislation. For some audiences, there is a perception that pharmaceutical companies place their commercial goals above the interests of patients, physicians and payers. Companies are taking steps to change this perception by embedding a culture of ethics and integrity, adopting higher standards of governance and improving relationships with employees, shareholders and other stakeholders.

Our strategy

AstraZeneca’s mission is to make the most meaningful difference to health through great medicines.

Our strategic review has confirmed our belief that biopharmaceuticals remain an attractive business, with strong underlying drivers of demand: expanding and ageing populations, a growing chronic disease burden, and increasing wealth through

economic growth, especially in Emerging Markets. While the hurdles to adopting new products have been raised, there remains a willingness to pay for differentiated, innovative medicines.

We further believe that AstraZeneca has the skills and capabilities to take advantage of these opportunities and turn them into long-term value. We will do this by exploiting and further developing our competitive advantage: an innovation and science-led organisation capturing the best of biologics, small molecules, immunotherapies and antibody engineering.

Our revised strategy is to compete as a global biopharmaceutical business delivering great medicines to patients through innovative science and excellence in development and commercialisation:

 

> global – in that we believe we combine global reach with local customer relationships and have the ability to meet healthcare needs in both developed and developing markets efficiently and effectively
> biopharmaceutical – in that we will develop both chemical (small molecule) and biological (large molecule) medicines available by prescription, targeting those product categories where medical innovation or brand equity will continue to enable us to make acceptable levels of return on our investments
> innovative   science – in that we believe that innovative science must be the foundation for procuring differentiated, novel medicines that benefit patients and for which payers will pay
> excellence in development and commercialisation – in that we believe we have strong commercial franchises and capability in developing, marketing and selling primary care, specialty care-led and specialty care products.

We are currently completing the strategic review that we began in 2012. We plan to hold a Capital Markets Day in March 2013 to provide a more detailed exposition of our strategic priorities.

Changes to the Senior Executive Team

In January 2013, we unveiled changes to our Senior Executive Team that came into immediate effect. Membership of the SET has been expanded to include increased representation of AstraZeneca’s scientific expertise, key products and key markets. Changes included the creation of:

 

> three senior R&D roles responsible for discovery and early-stage development in small molecules; discovery and early-stage development in biologics; and late-stage development
> three roles representing the commercial regions: North America; Europe; and International.

 

20   AstraZeneca Annual Report and Form 20-F Information 2012

LOGO

 

A further role will be responsible for global portfolio and product strategy, bridging the R&D and sales organisations. An appointment will be made at a later date.

The new SET structure is designed to provide sharper management focus on our key pipeline assets, product portfolio and key regions, as well as devolving and accelerating decision making. It draws heavily from the leadership talent within AstraZeneca, with the six new members being internal appointments. The full membership of the SET, together with information about individual members and their responsibilities, is shown in the Senior Executive Team section on pages 108 and 109.

Restructuring

Since 2007, we have undertaken significant efforts to restructure and reshape our business to improve long-term competitiveness.

The first phase was completed in 2009.

The second phase, which featured a significant change programme in R&D, began in 2010. The restructuring actions for this phase of the programme were completed in 2011, at a total programme cost of $2.1 billion. Headcount changes associated with this phase, involving an estimated 9,000 positions, were also completed. Total annual benefits of $1.9 billion were to be delivered by the end of 2014 in connection with this phase of the programme, of which $1.5 billion had been achieved by the end of 2012.

A third phase of restructuring was announced in February 2012. This phase, comprising initiatives across the supply chain, SG&A and R&D, carries an estimated programme cost of $2.1 billion (approximately $1.7 billion in cash costs). Restructuring costs of $1,558 million associated with this third phase were taken in 2012, together with $261 million that was charged in the fourth quarter of 2011. Most of the remaining costs of approximately $300 million will be taken in 2013. To date, actions involving around 6,300 of the estimated 7,300 positions to be impacted in connection with this phase of the programme have been completed. When completed, this phase is expected to deliver an estimated $1.6 billion in annual benefits by the end of 2014, of which approximately $350 million was realised by the end of 2012.

These restructuring programmes have been delivering their targeted benefits, and are designed to continue to provide the headroom to make appropriate investments to drive future growth and value, such as Emerging Markets commercial infrastructure and expansion of our research capabilities in biologics.

Medium-term planning assumptions

We believe challenging market conditions will persist in 2013, including continued government interventions in price. The revenue impact from the loss of exclusivity will also continue to affect our performance. In the context of the ongoing update to our strategy, we have withdrawn the planning assumptions for revenue and margin evolution for the period 2010 to 2014 that we had outlined in January 2010.

 

LOGO

 

AstraZeneca Annual Report and Form 20-F Information 2012   21

Performance | Therapy Area Review

 

LOGO

 

LOGO

LOGO

LOGO

Therapy area world market

(MAT/Q3/12) ($bn)

 

LOGO

 

 

LOGO

Our marketed products

Cardiovascular diseases

  > Crestor 1 (rosuvastatin calcium) is a statin used for the treatment of dyslipidaemia and hypercholesterolemia. In some markets it is also indicated to slow the progression of atherosclerosis and to reduce the risk of first cardiovascular (CV) events.
  > Atacand 2 (candesartan cilexetil) is an angiotensin II antagonist used for the 1 st line treatment of hypertension and symptomatic heart failure.
  > Seloken/Toprol-XL (metoprolol succinate) is a beta-blocker once daily tablet used for 24-hour control of hypertension and for use in heart failure and angina.
  > Tenormin (atenolol) is a cardioselective beta-blocker used for hypertension, angina pectoris and other CV disorders.
  > Plendil (felodipine) is a calcium antagonist used for the treatment of hypertension and angina.
  > Zestril 3 (lisinopril dihydrate) is an angiotensin-converting enzyme inhibitor used for the treatment of a wide range of CV diseases, including hypertension.
  > Axanum (acetylsalicylic acid (ASA) and esomeprazole) is a fixed-dose combination indicated for prevention of CV events in high-risk CV patients in need of daily low-dose ASA treatment and who are at risk of gastric ulcers.
  > Brilinta/Brilique (ticagrelor) is an oral antiplatelet for the treatment of acute coronary syndromes (ACS).

 

 

LOGO

Diabetes

  > Forxiga 4 (dapagliflozin) is a selective and reversible inhibitor of human sodium-glucose co-transporter 2 (SGLT2 inhibitor) indicated as an adjunct to diet and exercise as a once daily oral medication to improve glycaemic control in adult patients with Type 2 diabetes mellitus as add on combination therapy or as monotherapy in metformin-intolerant patients.
  > Komboglyze 4 (saxagliptin and metformin HCl) is an immediate release fixed-dose combination indicated as an adjunct to diet and exercise to improve glycaemic control in adult patients with Type 2 diabetes mellitus inadequately controlled on their maximally tolerated dose of metformin alone or those already being treated with the combination of saxagliptin and metformin as separate tablets.
  > Kombiglyze XR 4 (saxagliptin and metformin XR) is an extended release fixed-dose combination indicated as an adjunct to diet and exercise to improve glycaemic control in adults with Type 2 diabetes mellitus when treatment with both saxagliptin and metformin is appropriate.
  > Onglyza 4 (saxagliptin) is a DPP-IV inhibitor used for the treatment of Type 2 diabetes.
  > Byetta 4 (exenatide injection) is an injectable medicine indicated to improve blood sugar (glucose) control along with diet and exercise in adults with Type 2 diabetes mellitus.
  > Bydureon 4 (exenatide extended release injectable suspension) is an injectable medicine indicated to improve blood sugar (glucose) along with diet and exercise in adults with Type 2 diabetes mellitus.
  > Symlin 4 (pramlintide acetate) is an injected amylin analogue for the treatment of Type 1 and Type 2 diabetes in patients with inadequate glycaemic control on meal-time insulin.

 

  1   Licensed from Shionogi & Co. Ltd.
  2   Licensed from Takeda Chemicals Industries Ltd.
  3   Licensed from Merck.
  4   Co-developed and co-commercialised with BMS.

 

52   AstraZeneca Annual Report and Form 20-F Information 2012

LOGO

 

    World     US     Western Europe     Established ROW     Emerging Markets     Prior year  

2012

 

Sales
$m

   

Reported
growth
%

   

CER
growth
%

   

Sales
$m

   

Reported
growth
%

   

Sales
$m

   

Reported
growth
%

   

CER
growth
%

   

Sales
$m

   

Reported
growth
%

   

CER
growth
%

   

Sales
$m

   

Reported
growth
%

   

CER
growth
%

   

World
sales

$m

 

Crestor

    6,253        (6     (4     3,164        3        1,156        (6     2        1,269        (24     (23     664               4        6,622   

Atacand

    1,009        (30     (27     150        (18     422        (42     (39     142        (33     (33     295        (9     (3     1,450   

Seloken/
Toprol–XL

    918        (7     (4     320        (21     70        (18     (12     30        (21     (21     498        8        13        986   

Onglyza

    323        53        53        237        52        47        38        38        13        86        86        26        86        86        211   

Plendil

    252        (2     (2     4        (50     18        (22     (17     12        (14     (14     218        3        2        256   

Tenormin

    229        (15     (13     10        (9     50        (15     (8     106        (15     (15     63        (16     (12     270   

Brilinta/
Brilique

    89        324        348        19        73        55        n/m        n/m        3        n/m        n/m        12        n/m        n/m        21   

Byetta

    74        n/m        n/m        74        n/m                                                                         

Bydureon

    37        n/m        n/m        37        n/m                                                                         

Others*

    347        (12     (8     25        150        157        (17     (12     32        (15     (15     133        (15     (12     396   

Total

    9,531        (7     (4     4,040        5        1,975        (16     (10     1,607        (23     (23     1,909               4        10,212   
                             

2011

                                                                                         

Crestor

    6,622        16        13        3,074        16        1,225        10        5        1,662        25        15        661        9        8        5,691   

Atacand

    1,450        (2     (6     182        (16     731        (1     (6     213        (5     (13     324        6        7        1,483   

Seloken/
Toprol–XL

    986        (19     (20     404        (41     85        (7     (12     38        (3     (13     459        17        15        1,210   

Onglyza

    211        206        206        156        189        34        240        240        7        250        250        14        367        367        69   

Plendil

    256               (4     8        (47     23        (15     (19     14               (7     211        6        2        255   

Tenormin

    270        (2     (8     11        (15     59        (3     (8     125        (2     (10     75               (1     276   

Brilinta/
Brilique

    21        n/m        n/m        11        n/m        9        n/m        n/m                             1        n/m        n/m          

Zestril

    144        (8     (11     10               71        (12     (16     14        (18     (24     49               (2     157   

Others

    252        (4     (7            (100     119        5               25        (4     (15     108                      262   

Total

    10,212        9        5        3,856        6        2,356        6        1        2,098        18        9        1,902        9        8        9,403   

 

* Includes Zestril

For a detailed narrative explanation of the financial performance of our products please see the Geographical Review from page 70.

 

AstraZeneca is one of the world leaders in cardiovascular (CV) medicines, working to improve the treatment of diseases that cause 17 million deaths each year.

We aim to build on our strong position, with a particular focus on thrombosis (blood clotting), atherosclerosis (hardening of the arteries), metabolic diseases, and diabetes and its complications. Despite improvements in the quality of diagnosis and treatment, the unmet medical need remains high and these disease areas, and their complications, continue to grow worldwide (both in Established Markets and Emerging Markets) as a consequence of the spread of a westernised lifestyle.

We are developing potential new therapies using a variety of approaches, including small molecules, antibodies, peptides and proteins, to address unmet medical need in the treatment of obesity, diabetes and heart disease.

Cardiovascular diseases

Hypertension (high blood pressure) and dyslipidaemia (abnormal levels of blood cholesterol) damage the arterial wall which may lead to atherosclerosis. CV events driven by atherosclerotic disease remain the leading cause of death in the western world. Lipid-modifying therapy, primarily statins, is a cornerstone for the treatment of atherosclerosis.

Acute coronary syndromes (ACS) is an umbrella term for sudden chest pain and other symptoms due to insufficient blood supply (ischaemia) to the heart muscle. ACS is the acute culmination of ischaemic heart disease. There remains a significant need to improve outcomes and reduce the costs of treating ACS.

Our 2012 focus

Globally, Crestor has continued to gain market share (by value) since its launch in 2003, with its differentiated profile in managing cholesterol levels and its more recent label indications for slowing the progression of atherosclerosis and reducing the risk of CV events in some markets.

Crestor is the only statin with an atherosclerosis indication in the US which is not limited by disease severity or restricted to patients with coronary heart disease. A competitor to Crestor , atorvastatin ( Lipitor ), was available in generic form in the US from late 2011, and from May several generic atorvastatin products have become available in the market.

Fewer than half the people thought to have high levels of low-density lipoprotein cholesterol (LDL-C) (so-called ‘bad cholesterol’) are diagnosed and treated. Of treated patients, only about half reach their doctors’ recommended cholesterol targets using existing treatments. Study data has shown that the usual 10mg starting dose of Crestor is more effective at lowering LDL-C and produces greater achievement of LDL-C goals than commonly prescribed doses of other statins. Crestor also produces an increase in high-density lipoprotein cholesterol (HDL-C) (so-called ‘good cholesterol’) across the dose range and has again been shown to reduce atherosclerotic plaque in the SATURN study published in 2011.

 

LOGO

 

AstraZeneca Annual Report and Form 20-F Information 2012   53

Performance | Therapy Area Review

 

LOGO

 

LOGO

Therapy area world market

(MAT/Q3/12) ($bn)

 

LOGO

For a detailed narrative explanation of the financial performance of our products please see the Geographical Review from page 70.

LOGO

 

LOGO

 

LOGO

Our marketed products

  > Nexium (esomeprazole magnesium) is the first proton pump inhibitor (PPI) used for the treatment of acid-related diseases to offer clinical improvements over other PPIs and other treatments.
  > Losec/Prilosec (omeprazole) is used for the short-term and long-term treatment of acid-related diseases.
  > Entocort (budesonide) is a locally acting corticosteroid used for the treatment of inflammatory bowel disease.

 

LOGO

 

Our financial performance

 

    World     US     Western Europe     Established ROW     Emerging Markets     Prior year  

2012

  Sales
$m 		    Reported
growth
% 		    CER
growth
% 		    Sales
$m 		    Reported
growth
% 		    Sales
$m 		    Reported
growth
% 		    CER
growth
% 		    Sales
$m 		    Reported
growth
% 		    CER
growth
% 		    Sales
$m 		    Reported
growth
% 		    CER
growth
% 		   

World
sales

$m

 

Nexium

    3,944        (11     (10     2,272        (5     417        (45     (41     476        (12     (11     779        7        11        4,429   

Losec/Prilosec

    710        (25     (24     30        (21     188        (22     (17     316        (29     (29     176        (20     (20     946   

Others

    198        24        25        145        44        38        (17     (11     6                      9        29        29        161   

Total

    4,852        (12     (11     2,447        (4     643        (39     (34     798        (20     (19     964        1        4        5,536   
                             

2011

                                                                                         

Nexium

    4,429        (11     (12     2,397        (11     762        (37     (39     540        19        10        730        18        20        4,969   

Losec/Prilosec

    946        (4     (11     38        (21     242        (4     (10     447        2        (7     219        (12     (15     986   

Others

    161        21        19        101        33        46        2        (2     7        17        17        7        17               133   

Total

    5,536        (9     (11     2,536        (10     1,050        (30     (33     994        11        2        956        9        10        6,088   

 

56   AstraZeneca Annual Report and Form 20-F Information 2012

Performance | Therapy Area Review

 

LOGO

 

LOGO

Therapy area world market

(MAT/Q3/12) ($bn)

 

LOGO

LOGO

 

LOGO

Our marketed products

Respiratory syncytial virus (RSV)

  > Synagis (palivizumab) is a humanised MAb used for the prevention of serious lower respiratory tract disease caused by RSV in paediatric patients at high risk of acquiring RSV disease.

Serious bacterial infections

  > Zinforo 1 (ceftaroline fosamil) is a novel injectable cephalosporin used in community-acquired pneumonia (CAP) and complicated skin and soft tissue infections (CSSTI).
  > Cubicin 2 (daptomycin) is a cyclic lipopeptide anti-bacterial used for the treatment of serious infections in hospitalised patients.
  > Merrem/Meronem 3 (meropenem) is a carbapenem anti-bacterial used for the treatment of serious infections in hospitalised patients.

Influenza virus

  > FluMist/Fluenz (influenza vaccine live, intra-nasal) is an intra-nasal live, attenuated, trivalent influenza vaccine.

 

  1   Licensed from Forest.
  2   Licensed from Cubist Pharmaceuticals, Inc.
  3   Licensed from Dainippon Sumitomo.

 

LOGO

 

Our financial performance

 

    World     US     Western Europe     Established ROW     Emerging Markets     Prior year  

2012

  Sales
$m 		   

Reported

growth
%

   

CER

growth
%

    Sales
$m 		   

Reported

growth
%

    Sales
$m 		   

Reported

growth
%

   

CER

growth
%

   

Sales

$m

   

Reported

growth

%

   

CER

growth

%

    Sales
$m 		   

Reported

growth
%

   

CER

growth
%

   

World
sales

$m

 

Synagis

    1,038        6        6        611        7        427        5        5                                                  975   

Merrem/Meronem

    396        (32     (29     38        (7     64        (64     (62     18        (66     (66     276        (11     (6     583   

FluMist

    181        12        12        174        9        3        n/m        n/m        3        n/m        n/m        1                      161   

Others

    100        (31     (28     58        (25     6        (33     (11     16        (20     (20     20        (35     (32     137   

Total

    1,715        (8     (7     881        4        500        (16     (15     37        (49     (49     297        (13     (8     1,856   
                             

2011

                                                                                         

Synagis

    975        (6     (6     570        (12     404        3        3                             1                      1,038   

Merrem/Meronem

    583        (29     (30     41        (68     179        (45     (48     53        (7     (14     310        2               817   

FluMist

    161        (7     (7     160        (8                                               1                      174   

Non Seasonal Flu

    7        (82     (82     7        (82                                                                    39   

Others

    130        19        17        70        3        10        n/m        n/m        20               (25     30        55        90        108   

Total

    1,856        (15     (15     848        (19     593        (18     (19     73        (5     (17     342        5        6        2,176   

For a detailed narrative explanation of the financial performance of our products please see the Geographical Review from page 70.

 

58   AstraZeneca Annual Report and Form 20-F Information 2012

LOGO

LOGO

Therapy area world market

(MAT/Q3/12) ($bn)

 

LOGO

LOGO

 

Our marketed products

Psychiatry

  > Seroquel IR (quetiapine fumarate) is an atypical anti-psychotic drug generally approved for the treatment of schizophrenia and bipolar disorder (mania, depression and maintenance).
  > Seroquel XR (an extended release formulation of quetiapine fumarate) is generally approved for the treatment of schizophrenia, bipolar disorder, major depressive disorder (MDD) and, in some countries, for generalised anxiety disorder (GAD).

Analgesia and anaesthesia

  > Zomig (zolmitriptan) is used for the acute treatment of migraines with or without aura and Zomig Nasal Spray is indicated for the acute treatment of cluster headache in some territories.
  > Diprivan (propofol) is an intravenous general anaesthetic used in the induction and maintenance of general anaesthesia,

LOGO

 

for use in intensive care sedation and conscious sedation for surgical as well as diagnostic procedures.

  > Vimovo 1 (naproxen/esomeprazole magnesium) 375/20-500/20mg delayed-release tablet is generally approved for symptomatic relief in the treatment of rheumatoid arthritis, osteoarthritis and ankylosing spondylitis in patients at risk of developing NSAID-associated gastric and/or duodenal ulcers.
  > Naropin (ropivacaine) is used as a long-acting local anaesthetic for surgical anaesthesia and acute pain management.
  > Xylocaine (lidocaine) is a widely used, short-acting local anaesthetic for topical and regional anaesthesia.
  > EMLA (lidocaine and prilocaine) is used as a local anaesthetic for topical application to prevent pain associated with injections and superficial surgical procedures.

 

  1   Licensed from Pozen.

 

Our financial performance

 

    World     US     Western Europe     Established ROW     Emerging Markets     Prior year  

2012

  Sales
$m 		    Reported
growth
% 		    CER
growth
% 		    Sales
$m 		    Reported
growth
% 		    Sales
$m 		    Reported
growth
% 		    CER
growth
% 		    Sales
$m 		    Reported
growth
% 		    CER
growth
% 		    Sales
$m 		    Reported
growth
% 		    CER
growth
% 		   

World
Sales

$m

 

Seroquel XR

    1,509        1        4        811        4        446        (9     (2     97        9        10        155        17        27        1,490   

Seroquel IR

    1,294        (70     (70     697        (79     226        (59     (56     202        (11     (12     169        (23     (20     4,338   

Local Anaesthetics

    540        (10     (7            (100     201        (17     (11     206                      133        (8     (4     602   

Diprivan

    291        (1     2               (100     32        (24     (19     78        (6     (6     181        15        19        294   

Zomig

    182        (56     (54     12        (92     103        (41     (37     55        (19     (19     12        (8     8        413   

Vimovo

    65        91        97        25        19        19        217        233        14        133        133        7        n/m        n/m        34   

Others

    42        30        36        16        n/m        11        (35     (29     1        (33     (33     14        17        25        33   

Total

    3,923        (46     (44     1,561        (64     1,038        (32     (27     653        (4     (4     671        (1     4        7,204   
                             

2011

                                                                                         

Seroquel XR

    1,490        29        27        779        22        490        36        30        89        46        34        132        40        41        1,154   

Seroquel IR

    4,338        5        3        3,344        8        546        (3     (8     228        2        (8     220        (15     (17     4,148   

Local Anaesthetics

    602               (6     10        (66     242        (9     (13     205        10               145        16        13        605   

Diprivan

    294        (9     (13     12        (73     42        (16     (20     83        9        1        157        4        (1     322   

Zomig

    413        (4     (7     158        (10     174        1        (4     68        (1     (9     13        18        9        428   

Vimovo

    34        n/m        n/m        21        n/m        6        n/m        n/m        6        n/m        n/m        1        n/m        n/m        5   

Others

    33        (21     (24     1               17        (37     (41     3                      12        9        9        42   

Total

    7,204        7        5        4,325        8        1,517        6        1        682        10        1        680        5        2        6,704   

For a detailed narrative explanation of the financial performance of our products please see the Geographical Review from page 70.

 

LOGO

 

AstraZeneca Annual Report and Form 20-F Information 2012   61

LOGO

 

 

LOGO

Therapy area world market

(MAT/Q3/12) ($bn)

 

LOGO

LOGO

 

LOGO

Our marketed products

  > Arimidex (anastrozole) is an aromatase inhibitor used for the treatment of breast cancer.
  > Zoladex (goserelin acetate implant), in one and three month depots 1 , is a luteinising hormone-releasing hormone (LHRH) agonist used for the treatment of prostate cancer, breast cancer and certain benign gynaecological disorders.
  > Casodex (bicalutamide) is an anti-androgen therapy used for the treatment of prostate cancer.
  > Iressa (gefitinib) is used as an epidermal growth factor receptor-tyrosine kinase (EGFR-TK) inhibitor that acts to block signals for cancer cell growth and survival in advanced non-small cell lung cancer.
  > Faslodex (fulvestrant) is an injectable oestrogen receptor antagonist used for the treatment of hormone receptor-positive metastatic breast cancer for post-menopausal women whose disease has progressed following treatment with prior endocrine therapy.
  > Nolvadex (tamoxifen citrate) remains a widely used breast cancer treatment outside the US.
  > Caprelsa (vandetanib) is a kinase inhibitor indicated for the treatment of symptomatic or progressive medullary thyroid cancer (MTC) in patients with unresectable (non-operable) locally advanced or metastatic disease.

 

  1 Depots are subcutaneous or intra-muscular injections.

 

Our financial performance

 

    World     US     Western Europe     Established ROW     Emerging Markets     Prior year  

2012

  Sales
$m 		    Reported
growth
% 		    CER
growth
% 		    Sales
$m 		   

Reported

growth

%

    Sales
$m 		    Reported
growth
% 		    CER
growth
% 		    Sales
$m 		   

Reported

growth

%

   

CER

growth

%

    Sales
$m 		   

Reported

growth

%

   

CER

growth

%

   

World
sales

$m

 

Zoladex

    1,093        (7     (5     24        (38     221        (16     (12     448        (9     (9     400        4        9        1,179   

Faslodex

    654        20        24        310        17        186        (4     4        62        n/m        n/m        96        16        27        546   

Iressa

    611        10        12               (100     142        12        20        222        9        9        247        12        12        554   

Arimidex

    543        (28     (26     21        (50     124        (52     (49     279        (9     (9     119        (18     (16     756   

Casodex

    454        (17     (16     (3     n/m        51        (36     (31     301        (17     (17     105        (6     (4     550   

Others

    134        13        15        25        108        17        31        46        63                      29        (6     (3     120   

Total

    3,489        (6     (3     377        7        741        (21     (15     1,375        (4     (4     996        2        6        3,705   
                             

2011

                                                                                         

Zoladex

    1,179        6        3        39        (15     262        (5     (9     494        10               384        12        18        1,115   

Faslodex

    546        58        55        264        71        193        56        48        6        n/m        n/m        83        30        28        345   

Iressa

    554        41        32        2        (50     127        159        147        204        12        2        221        40        34        393   

Arimidex

    756        (50     (53     42        (91     260        (55     (56     308        7        (2     146        (3     (6     1,512   

Casodex

    550        (5     (12     (6     (138     80        (29     (33     364        5        (5     112        9        7        579   

Others

    120        19        12        12        71        13        18        18        64        10               31        24        20        101   

Total

    3,705        (8     (12     353        (51     935        (19     (22     1,440        8        (1     977        16        16        4,045   

For a detailed narrative explanation of the financial performance of our products please see the Geographical Review from page 70.

 

LOGO

 

AstraZeneca Annual Report and Form 20-F Information 2012   65

Performance | Therapy Area Review

 

LOGO

 

We aim to build on our position as one of the world leaders in cancer treatment with established brands such as Zoladex and Arimidex and growing brands such as Faslodex and Iressa.

 

Our future growth will be driven through targeting the right treatments, both small molecules and biologics, to the right patients, using companion diagnostics where appropriate. This approach is driving the growth of Iressa and is a key focus in the development of our early stage portfolio.

 

Our 2012 focus

Arimidex , first launched in 1995, remains a leading global hormonal therapy for patients with early breast cancer. This success is largely based on the extensive long-term efficacy and safety results of the ATAC study, which showed Arimidex to be significantly superior to tamoxifen at preventing breast cancer recurrence during and beyond the five year treatment course.

 

Zoladex , a luteinising hormone-releasing hormone (LHRH) agonist, is approved in 120 countries for the treatment of prostate cancer, breast cancer and certain benign gynaecological disorders. In non-metastatic prostate cancer, Zoladex has been shown to improve overall survival, both when used in addition to radical prostatectomy and when used in addition to radiotherapy. In breast cancer, Zoladex is widely approved for use in advanced breast cancer in pre-menopausal women. In a number of countries, Zoladex is also approved for the adjuvant treatment of early stage pre-menopausal breast cancer as an alternative to and/or in addition to chemotherapy. Zoladex offers proven survival benefits for breast cancer patients with a favourable tolerability profile.

 

Casodex and Zoladex are both leading endocrine therapies for the treatment of prostate cancer. Casodex is used as a 50mg tablet for the treatment of advanced prostate cancer and as a 150mg tablet for the treatment of locally advanced prostate cancer.

 

Iressa is approved in 89 countries and is one of the leading epidermal growth factor receptor-tyrosine kinase (EGFR-TK) inhibitors in Japan and the Asia Pacific region where it is marketed for pre-treated advanced non-small cell lung cancer

 

(NSCLC). Outside the EU, indications are being sought or expanded from the pre-treated setting to include 1 st line patients whose tumours harbour activating mutations of the epidermal growth factor receptor (EGFR). In the EU, Iressa is the first personalised medicine for the treatment of adults with locally advanced or metastatic NSCLC with activating mutations.

 

Faslodex 500mg is now approved in 65 countries including the member states of the EU, the US and Japan. It offers an additional, efficacious, hormonal therapy option for patients with hormone-receptor positive advanced breast cancer. It is given by once monthly injections and is approved for the treatment of hormone-receptor positive advanced breast cancer in post-menopausal women whose disease has progressed following treatment with a prior endocrine therapy. We are now exploring the efficacy and safety of Faslodex 500mg compared to Arimidex in the 1 st line advanced breast cancer setting (hormone-naïve patients) in the Phase III FALCON trial.

 

Caprelsa fights cancer through two proven mechanisms: blocking the development of tumour blood supply by inhibition of the vascular endothelial growth factor pathway and by inhibiting the growth and survival of the tumour through EGFR and rearranged during transfection (RET) pathways. Caprelsa was approved by the FDA and granted Orphan Drug status in April 2011, and was approved in the EU in February 2012 for the treatment of medullary thyroid cancer (MTC) in patients with unresectable locally advanced or metastatic disease. Caprelsa is also approved in Canada and remains under review by other regulatory agencies around the world.

 

In the pipeline

Our early oncology pipeline includes a range of novel compounds that target signalling pathways believed to be pivotal in cancer cell growth and survival as well as DNA repair mechanisms. Despite set-backs in earlier Phase II trials, olaparib, a poly ADP-ribose polymerase (PARP) inhibitor, continues in Phase II trials in relapsed ovarian cancer, gastric cancer and germline BRCA mutation positive cancers. Olaparib has been approved to begin Phase III in 2013 pending the results of ongoing trials.

 

Selumetinib, a potent mitogen-activated protein kinase (MEK) inhibitor licensed from Array BioPharma, Inc., continues in Phase II development.

 

We are also developing potential new cancer drugs using a variety of biologics approaches. Our investigational biologics are directed towards molecular targets with a strong role in cancer progression and incorporate innovative technologies, providing the potential to eliminate cancer cells in more effective ways. Within biologics, we continue to progress a discovery and clinical pipeline that is balanced across different anti-tumour approaches, including disrupting cancer cells’ ability to grow or communicate (growth factor and survival signalling), modulating the blood supply that tumours need to grow (vascular modulation) and activating a patient’s own immune system to eliminate cancer cells (immune-mediated therapy).

 

We currently have five investigational biologics in Phase I clinical trials and four in Phase II clinical trials. Additional drug candidates are expected to progress into clinical trials in 2013. Moxetumomab is a monoclonal antibody approved to begin Phase III testing in hairy cell leukemia in 2013.

 

  LOGO

 

 

66   AstraZeneca Annual Report and Form 20-F Information 2012

LOGO

LOGO

Therapy area world market

(MAT/Q3/12) ($bn)

 

LOGO

LOGO

 

LOGO

Our marketed products

  > Symbicort pMDI (budesonide/formoterol in a pressurised metered-dose inhaler) is a combination of an inhaled corticosteroid and a fast onset, long-acting beta 2 -agonist used for maintenance treatment of asthma and chronic obstructive pulmonary disease (COPD), including chronic bronchitis and emphysema in the US.
  > Symbicort Turbuhaler (budesonide/ formoterol in a dry powder inhaler) is a combination of an inhaled corticosteroid and a fast onset, long-acting beta 2 -agonist used for maintenance treatment of asthma and COPD. In asthma, it is also approved for Maintenance And Reliever Therapy (SMART). Symbicort Turbuhaler is used in most parts of the world outside the US.
  > Pulmicort Turbuhaler (budesonide in a dry powder inhaler) is an inhaled corticosteroid used for maintenance treatment of asthma.
  > Pulmicort Respules (budesonide inhalation suspension) is a corticosteroid administered via a nebuliser for the treatment of asthma in both children and adults.
  > Rhinocort (budesonide) is a nasal steroid used as a treatment for allergic rhinitis (hay fever), perennial rhinitis and nasal polyps.
  > Oxis Turbuhaler (formoterol in a dry powder inhaler) is a fast onset, long-acting beta 2 -agonist used for the treatment of bronchial-obstructive symptoms in asthma and COPD.
  > Accolate (zafirlukast) is an oral leukotriene receptor antagonist used for the treatment of asthma.

 

Our financial performance

 

    World     US     Western Europe     Established ROW     Emerging Markets     Prior year  

2012

  Sales
$m 		    Reported
growth
% 		    CER
growth
% 		    Sales
$m 		    Reported
growth
% 		    Sales
$m 		    Reported
growth
%% 		   

CER

growth

    Sales
$m 		    Reported
growth
% 		    CER
growth
% 		    Sales
$m 		    Reported
growth
% 		    CER
growth
% 		   

World
sales

$m

 

Symbicort

    3,194        1        5        1,003        19        1,313        (8     (3     443        6        7        435        (3     3        3,148   

Pulmicort

    866        (3     (1     233        (16     156        (17     (12     127        1        1        350        17        19        892   

Rhinocort

    177        (17     (14     55        (26     28        (24     (19     17        (15     (15     77        (5     (1     212   

Others

    178        (17     (14     10        25        92        (16     (11     23        4        4        53        (30     (28     216   

Total

    4,415        (1     2        1,301        8        1,589        (10     (5     610        4        5        915        1        5        4,468   
                             

2011

                                                                                         

Symbicort

    3,148        15        11        846        17        1,434        5               418        46        35        450        21        19        2,746   

Pulmicort

    892        2               279        (9     189        (12     (16     126        11        2        298        25        23        872   

Rhinocort

    212        (7     (9     74        (20     37        (5     (10     20        25        13        81        3               227   

Others

    216        (15     (19     8        (80     109        (8     (13     23        5               76        4        1        254   

Total

    4,468        9        6        1,207        4        1,769        2        (3     587        34        24        905        19        17        4,099   

For a detailed narrative explanation of the financial performance of our products please see the Geographical Review from page 70.

 

LOGO

 

AstraZeneca Annual Report and Form 20-F Information 2012   67

Performance | Therapy Area Review

 

LOGO

 

We aim to build on our strong position in the respiratory and inflammation area through the growth of key products, with new indications and market launches, including chronic obstructive pulmonary disease (COPD), as well as through developing a strong pipeline of novel small molecule and biologics approaches to COPD and asthma.

We aspire to enter the rheumatology market through our biologics pipeline and targeted small molecule approaches such as fostamatinib. With our acquisition of Ardea we have expanded our inflammation focus to include gout.

COPD and asthma

According to WHO, COPD, a serious lung disease that includes chronic bronchitis and/or emphysema, is currently the fourth leading cause of death worldwide, with future increases anticipated. Current treatment has recently demonstrated the potential for some survival benefit but the impact of medication on the course of the disease is small and the prognosis of the COPD patient remains poor. In asthma, unmet medical need for patients whose asthma is inadequately controlled by current treatments remains an important issue and disease normalisation is currently not optimally achieved by any approved treatment.

The typical treatment for both COPD and asthma is a fixed-dose combination of an inhaled corticosteroid (ICS) with a long-acting beta 2 -agonist (LABA) (for example Symbicort ) or for COPD specifically, an inhaled long-acting muscarinic antagonist as either monotherapy or adjunctive to ICS/LABA treatment. Other major asthma treatments include monotherapy ICSs, oral leukotriene receptor antagonists and/or oral steroids for severe disease and (in combination with antibiotics) for exacerbations, as well as a MAb targeting allergic asthma for moderate to severe asthma patients. Over recent years, studies employing patient-centric tools, such as the asthma control questionnaire, have revealed surprisingly low asthma control at all severities, highlighting an underestimated medical need.

Our 2012 focus

Symbicort improves symptoms and provides a clinically important improvement in the health of many patients with either asthma or COPD by providing effective and rapid control of the symptoms.

Symbicort pMDI is indicated in the US for the treatment of asthma in patients 12 years of age and older. The COPD indication was approved and launched in the US in early 2009. In June 2010, the US Prescribing Information was updated to include the FDA’s new recommendations for appropriate use of asthma medications containing LABAs. The class label changes for all LABA-containing products are specific to the treatment of asthma and do not apply to the treatment of COPD.

Symbicort Turbuhaler was originally launched in markets outside the US in 2000 and in Japan in 2010 for the treatment of adult asthma and is co-promoted in Japan with Astellas Pharma, Inc. The COPD indication and the SMART treatment regimen were approved in Japan in 2012.

Symbicort SMART (Symbicort Maintenance And Reliever Therapy) provides improved asthma control including less risk for exacerbations relative to comparators and simplifies asthma management through the use of only one inhaler for both maintenance and relief of asthma symptoms. As well as being a cost-effective treatment, the Symbicort SMART approach reduces the usage of both inhaled and oral corticosteroids compared to other treatment options.

Pulmicort is one of the world’s leading inhaled corticosteroids for the treatment of asthma and is available in several forms. Teva has had an exclusive licence to sell a generic version of Pulmicort Respules in the US since 2009. Pulmicort continues to face increasing challenge from generic products. Patents protecting Pulmicort have been subject to a number of challenges in different jurisdictions. Details of these matters are included in Note 25 to the Financial Statements from page 184.

Clinical studies

In April 2012, the FDA provided AstraZeneca with a Post-marketing Requirement for a Symbicort LABA safety study, designed to be pooled with similar studies with other

LABA products. AstraZeneca is required to conduct a trial comparing Symbicort Inhalation Aerosol with Pulmicort to evaluate the risk of serious asthma outcomes (hospitalisations, intubation, death) in 11,700 adult and adolescent patients. Recruitment in the trial is ongoing.

In the pipeline

Building on our capabilities in combinations and inhaler device development demonstrated through our experience with Symbicort , we are aiming to further improve the mainstay of treatment for COPD patients by combining bronchodilators, being developed in collaboration with Pulmagen Therapeutics (Synergy) Limited, with inhaled anti-inflammatory compounds such as inhaled selective glucocorticoid receptor agonists (AZD5423, which continues in Phase II), being developed in collaboration with Bayer Schering Pharma AG. Additionally, we are targeting inflammation in COPD using oral routes of administration with AZD5069, a CXCR2 antagonist that targets neutrophils which is in Phase II. MEDI8968, an anti-interleukin-IL-1 receptor MAb, and benralizumab, an anti-interleukin-5 receptor MAb, are both in Phase II development for severe to very severe COPD.

We are targeting uncontrolled asthma focusing on reducing the rate of annual asthma exacerbations through small molecule approaches such as a CRTh2 receptor antagonist and toll-like receptor 7 agonists (being developed in collaboration with Dainippon Sumitomo). Biological treatments in Phase IIb include benralizumab and tralokinumab, a MAb that targets interleukin-13. Also, in Phase II, brodalumab is an anti-interleukin-17 receptor MAb (being developed in collaboration with Amgen) for asthma.

In April 2012, AstraZeneca and Amgen agreed to jointly develop and commercialise five MAbs from Amgen’s clinical inflammation portfolio including brodalumab. The collaboration will provide Amgen with additional resources to optimally progress its portfolio, and Amgen will benefit from the strong respiratory, inflammation and asthma development expertise of AstraZeneca’s biologics capabilities. The collaboration will also capitalise on AstraZeneca’s global commercial reach in respiratory and gastrointestinal diseases.

 

68   AstraZeneca Annual Report and Form 20-F Information 2012

Performance | Geographical Review

 

LOGO

 

2012 in brief

> In the US, sales were down 21% to $10,655 million (2011: $13,426 million; 2010: $13,727 million). Loss of exclusivity on Seroquel IR in March 2012 as well as the impact of increased generic competition experienced by our other mature brands was partially offset by strong performance from our key brands, Brilinta, Crestor, Onglyza, Symbicort and Faslodex .
> AstraZeneca is the fourth largest pharmaceutical company in the US, with a 5% market share of US pharmaceuticals by sales value.
> AstraZeneca is the eighth largest prescription-based pharmaceutical company in Western Europe, with a 3.4% market share of sales by value.
> Sales in Western Europe were down 19% to $6,486 million (2011: $8,501 million; 2010: $9,168 million). Key drivers of the decline were the volume erosion on Atacand, Seroquel IR, Nexium, Arimidex and Meronem , following entry of generic competition and the negative price and volume impact primarily related to government interventions, particularly in Greece, Italy, Portugal and Spain. This development was partially offset by revenue growth from Brilique, Onglyza, Vimovo and Iressa .
> Established ROW sales were down 14%. The entry of generic competition of Crestor in Canada, and Seroquel IR and Arimidex in Australia was partially offset by the successful first full year of launch of Nexium and Faslodex in Japan.
> Emerging Markets sales increased by 4% to $5,752 million (2011: $5,763 million; 2010: $5,198 million) with sales growth in China of 17% and also in Russia of 17%.

2011 in brief

> In the US, sales were down 2% to $13,426 million (2010: $13,727 million). The pricing impact from US healthcare reform measures lowered revenue by around 3.3%. Good growth for Crestor , the Seroquel franchise, Symbicort and Onglyza , broadly offset the impact of generic competition for Arimidex, Toprol-XL and Merrem , and declines in Nexium .
> Sales in Western Europe were down 11% to $8,501 million (2010: $9,168 million), due largely to volume erosion on Nexium, Arimidex and Meronem . This was partially offset by volume growth attributable to Crestor , Seroquel XR , Symbicort , Iressa and Faslodex .
> Established ROW sales were up 4%, driven by continued growth of Symbicort , Crestor , Nexium and the Seroquel franchise. In 2011, AstraZeneca became the largest research-based pharmaceutical company in Canada by sales value.
> Emerging Markets sales increased by 10% to $5,763 million (2010: $5,198 million), with sales growth in China of 15% and Russia of 19%. Sales in Brazil were down as a result of generic competition for Crestor and Seroquel IR .

For more information regarding our products, see the Therapy Area Review from page 50. Details of material legal proceedings can be found in Note 25 to the Financial Statements from page 184

 

and details of relevant risks are set out in the Principal risks and uncertainties section from page 75. See the Market definitions table on page 209 for information about AstraZeneca’s market definitions. Sales figures in this Geographical Review are with reference to the customers’ location.

US

AstraZeneca is the fourth largest pharmaceutical company in the US, with a 5% market share of US pharmaceuticals by sales value.

Sales in the US decreased by 21% to $10,655 million (2011: $13,426 million; 2010: $13,727 million), as strong performance from our key brands, Brilinta , Crestor , Onglyza , Symbicort and Faslodex , was offset by loss of exclusivity on Seroquel IR in March 2012 as well as the impact of increased generic competition experienced by our other mature brands. Combined sales of our key brands, Brilinta , Crestor , Onglyza , Symbicort and Faslodex , were up by 9% to $4,733 million (2011: $4,351 million; 2010: $3,569 million). Other drivers of the sales decline include the reduction of sales for Zomig following the licensing of Zomig to Impax Pharmaceuticals Inc. in February 2012 down to $12 million (2011: $158 million; 2010: $176 million), additional generic competition affecting sales of Toprol-XL down to $320 million (2011: $404 million; 2010: $689 million), and loss of exclusivity of Atacand down to $150 million (2011: $182 million; 2010: $216 million).

Brilinta achieved sales of $19 million. Commercial preferred unrestricted managed markets access was 54%

 

Our financial performance

 

     2012     2011     2010  
    

Sales

$m

     Reported
growth
% 		    CER
growth
% 		    Sales
$m 		     Reported
growth
% 		    CER
growth
% 		    Sales
$m 		 

US

     10,655         (21     (21     13,426         (2     (2     13,727   

Western Europe

     6,486         (24     (19     8,501         (7     (11     9,168   

Canada

     1,090         (32     (31     1,604         6        1        1,510   

Japan

     2,904         (5     (5     3,064         17        6        2,617   

Other Established ROW

     1,086         (12     (12     1,233         18        4        1,049   

Established ROW

     5,080         (14     (14     5,901         14        4        5,176   

Emerging Europe

     1,165         (6     2        1,244         7        7        1,165   

China

     1,512         20        17        1,261         20        15        1,047   

Emerging Asia Pacific

     923         (5     (3     968         9        5        890   

Other Emerging ROW

     2,152         (6            2,290         9        12        2,096   

Emerging Markets

     5,752                4        5,763         11        10        5,198   

Total

       27,973         (17     (15       33,591         1        (2       33,269   

 

70   AstraZeneca Annual Report and Form 20-F Information 2012

LOGO

 

and trial among target interventional cardiologist initiators was 39% at the end of 2012. Crestor demonstrated resilience in the face of the November 2011 market entry of a generic version and, from May, multiple generic versions of atorvastatin, all competitors of Crestor. Crestor’s performance volume showed resilience in two of the largest and most profitable segments of the market, Commercial and Medicare. Crestor’s existing patient base remained solid, and continuing patients represented 94% of Crestor’s volume. Crestor achieved sales of $3,164 million (2011: $3,074 million; 2010: $2,640 million) and a total prescription share of 11.8% within the statin market. In 2012, Crestor became the most prescribed branded pharmaceutical in the US.

Symbicort pMDI continued to deliver steady growth in the US with sales up 19% to $1,003 million (2011: $846 million; 2010: $721 million) and prescription growth of 12.5%. It achieved a 21.3% total prescription share and a 22.5% new prescription share of the inhaled corticosteroid/long-acting beta 2 -agonist market.

Following the completion of BMS’s acquisition of Amylin, AstraZeneca and BMS have been developing and commercialising Amylin’s portfolio of products related to diabetes (and other metabolic diseases). Sales of GLP-1 agonists for the treatment of diabetes were $74 million for Byetta , $37 million for Bydureon and $17 million for Symlin.

Onglyza/Kombiglyze XR captured more than one in five new DPP-IV patient treatment decisions and achieved a 2.8% total prescription market share gain in 2012, ending the year with a total prescription market share of 17.1% of the rapidly growing DPP-IV inhibitor market. Onglyza revenues in the US were $237 million (2011: $156 million; 2010: $54 million).

The loss of exclusivity for Seroquel IR in March 2012 resulted in a decrease in sales of 79% to $697 million (2011: $3,344 million; 2010: $3,107 million). In 2012, generics accounted for 58.5% of quetiapine prescriptions in the US. The presence of generic competition impacted the prescription volume of Seroquel XR in 2012. However, sales of Seroquel XR were up 4% to $811 million (2011: $779 million; 2010: $640 million) because of higher prices.

Nexium was the third most prescribed branded pharmaceutical in the US. In the face of continuing generic, OTC and pricing pressures, Nexium sales declined 5% to $2,272 million (2011: $2,397 million; 2010: $2,695 million). Nexium remains the branded market leader retaining significant market share and volume within the proton pump inhibitor class.

In 2012, sales of Synagis were up 7% to $611 million (2011: $570 million; 2010: $646 million). Sales in the 2011 to 2012 RSV season experienced payer pressure, which was offset by heightened awareness efforts surrounding the RSV burden of disease, appropriate patient identification and enhanced efforts to ensure continuity of care for patients from the hospital to the paediatrician’s office.

In March 2010, the Affordable Care Act came into force. It has had, and is expected to continue to have, a significant impact on our US sales and the US healthcare industry as a whole. In 2012, the overall reduction in our profit before tax for the year due to higher minimum Medicaid rebates on prescription drugs, discounts on branded pharmaceutical sales to Medicare Part D beneficiaries and an industry-wide excise fee was $858 million. This amount reflects only those effects of the Affordable Care Act that we know have had or will have a direct impact on our financial condition or results of operations and which we are therefore able to quantify based on known and isolatable resulting changes in individual financial items within our Financial Statements. There are other potential indirect or associated consequences of these legislative developments, which continue to evolve and which cannot be estimated but could have similar impacts. These include broader changes in access to or eligibility for coverage under Medicare, Medicaid or similar governmental programmes, such as the recent proposals to limit Medicare benefits. These could indirectly impact our pricing or sales of prescription products within the private sector. By their nature and the fact that these potentially numerous consequences are not directly linked to a corresponding and quantifiable impact on our Financial Statements, it is not possible to accurately estimate the financial impact of these

potential consequences of the Affordable Care Act or related legislative changes when taken together with the number of other market and industry-related factors that can also result in similar impacts. Further details on the impact of the Affordable Care Act are contained in the Pricing pressure section from page 18 and the Principal risks and uncertainties section from page 75.

Currently, there is no direct governmental control of prices for commercial prescription drug sales in the US. However, some publicly funded programmes, such as Medicaid and TRICARE (Department of Veterans Affairs), have statutorily mandated rebates and discounts that have the effect of price controls for these programmes. Additionally, pressure on pricing, availability and utilisation of prescription drugs for both commercial and public payers continues to increase. This is driven by, among other things, an increased focus on generic alternatives. Primary drivers of increased generic use are budgetary policies within healthcare systems and providers, including the use of ‘generics only’ formularies, and increases in patient co-insurance or co-payments. In 2012, 84% of the prescriptions dispensed in the US were generic. While it is unlikely that there will be widespread adoption of a broad national price control scheme in the near future, there will continue to be increased attention to pharmaceutical prices and their impact on healthcare costs for the foreseeable future.

Rest of World

Sales performance outside the US in 2012 was down by 11% to $17,318 million (2011: $20,165 million; 2010: $19,542 million), due to loss of exclusivity, competition from generic products and the continuing challenging economic environment. Combined sales of key products ( Arimidex, Crestor, Nexium, Seroquel IR and Seroquel XR , and Symbicort ) were down 11% with sales of $8,769 million (2011: $10,301 million; 2010: $9,923 million). Emerging Markets delivered strong sales, up 4% with sales of $5,752 million (2011: $5,763 million; 2010: $5,198 million).

Western Europe

AstraZeneca is the eighth largest pharmaceutical company in Western Europe, with a 3.4% market share of prescription sales by value.

 

LOGO

 

AstraZeneca Annual Report and Form 20-F Information 2012   71

Performance  | Geographical Review

 

LOGO

 

The macro-economic situation has deteriorated, particularly in Greece, Italy, Portugal and Spain which have seen the implementation of new austerity measures, leading to increased pressure on healthcare budgets. Most governments in Europe intervene directly to control the price, volume and reimbursement of medicines. Several governments have imposed price reductions and increased the use of generic medicines as part of healthcare expenditure control. A number of countries are applying strict criteria for cost-effectiveness evaluations of medicines, which has delayed and reduced access to medicines for patients in areas of important unmet medical need. These and other measures all contribute to an increasingly difficult environment for branded pharmaceuticals in Europe.

Total sales in Western Europe were down 19% to $6,486 million (2011: $8,501 million; 2010: $9,168 million) due largely to volume erosion on Seroquel IR, Nexium, Arimidex and Meronem following generic entrants and the negative price and volume impact primarily related to government interventions, particularly in Greece, Italy, Portugal and Spain. The loss of exclusivity for Atacand in April 2012 resulted in a decrease in sales of 39% to $422 million (2011: $731 million; 2010: $736 million). Generics now account for 9.7% of candesartan prescriptions in Western Europe. This development was partially offset by revenue growth attributable to Brilique, Onglyza, Vimovo and Iressa.

Crestor outperformed the statin class with strong 2% sales growth. Generic versions of Seroquel IR are now available in Western Europe, with overall sales down 56% to $226 million (2011: $546 million; 2010: $560 million).

Brilique has been launched in all markets in Western Europe and sales reached $55 million in 2012 (2011: $9 million).

In Germany, sales fell by 30% to $775 million (2011: $1,189 million; 2010: $1,235 million), mainly driven by market entries of generic versions of Atacand (sales declined to $141 million; 2011: $255 million; 2010: $252 million), Seroquel IR (sales declined to $31 million; 2011: $127 million; 2010: $113 million) and Seroquel XR (sales declined to $93 million; 2011: $151 million; 2010: $100 million).

In the UK, a 22% decrease in sales to $668 million (2011: $866 million; 2010: $1,022 million) reflected strong volume erosion on Seroquel IR and Seroquel XR (sales declined to $58 million; 2011: $120 million; 2010: $124 million), following generic entrants. Sales of Nexium decreased by 59% to $17 million (2011: $41 million; 2010: $89 million) and sales of Arimidex decreased by 85% to $4 million (2011: $28 million; 2010: $114 million), both following the impact of a full year of generic penetration. The decrease in UK sales was partially offset by the solid performance of Symbicort , up 6% to $328 million (2011: $312 million; 2010: $272 million).

Sales in France decreased by 18% to $1,314 million (2011: $1,740 million; 2010: $1,889 million), driven largely by volume erosion on Nexium, Atacand, Zomig and Arimidex , following generic entrants, and the impact from the disposal of Astra Tech, which was not entirely offset by the strong growth of Crestor and the successful launch of Seroquel XR , which had sales of $37 million. Sales in Spain and Italy were down by 22% to $510 million (2011: $708 million; 2010: $788 million) and by 15% to $876 million (2011: $1,113 million; 2010: $1,198 million), respectively, mainly driven by generic entrants and the implementation of price and prescription controls associated with existing and new austerity measures.

Established ROW

Sales in Established ROW decreased by 14%. The key products with sales growth in 2012 were Symbicort, Seroquel XR, Onglyza, Faslodex and Iressa .

Canada

The trend in Canada indicates that provinces will continue to introduce policy changes that drive cost savings and exert pricing pressure on new and existing medicines (for example, conditional listings, product listing agreements and bulk purchasing), while providing reasonable patient access to innovative medicines.

Due to the loss of exclusivity for Crestor in Canada in April 2012, and the continued impact of the ‘at risk’ launch of a generic version of Nexium by a competitor in 2011, total Canadian sales decreased by 31% to $1,090 million (2011: $1,604 million; 2010: $1,510 million). Combined sales of Crestor ,

Nexium, Symbicort, Seroquel IR and Seroquel XR were $742 million (2011: $1,171 million; 2010: $1,055 million).

Japan

Sales in Japan decreased by 5% to $2,904 million (2011: $3,064 million; 2010: $2,617 million). Strong performance from Crestor, Symbicort, Faslodex and Iressa was largely offset by biennial price cuts imposed in April 2012.

Crestor sales grew by 4%, becoming the number one brand in the statin market in Japan. Symbicort sales grew 12%, backed by additional therapeutic indications for SMART and COPD.

Nexium achieved sales of $78 million in its first full year after launch, with sales accelerating following the lifting in October of the two week prescription limit imposed by the Japanese Ministry of Health, Labour and Welfare on new medicines during the first year from launch.

Our oncology business remains one of the leaders in Japan based on the performance of established brands including Iressa, Arimidex, Zoladex and Casodex . Faslodex , launched in November 2011, achieved sales of $58 million in its first full year in the market.

Other Established ROW

Our sales in Other Established ROW showed a decline of 12% to $1,086 million (2011: $1,233 million; 2010: $1,049 million). Australian sales were impacted by price cuts triggered by loss of exclusivity of Seroquel IR and Arimidex in April 2012, as well as by price reductions due to the Australian government’s therapeutic group policy, which impacted Crestor and Atacand. Price reductions were partially offset by performance of Crestor, Nexium and Symbicort , which all gained market share. Crestor achieved a 28.1% volume share in the statin class and became the number one drug in the statin market in Australia following loss of exclusivity of atorvastatin. Brilinta was successfully launched in Australia with reimbursement through the Australian pharmaceutical benefits scheme becoming available from August. Brilinta achieved formulary listing in the vast majority of hospitals in Australia in 2012. Marketing authorisation was obtained for Symbicort pMDI in Australia.

 

72   AstraZeneca Annual Report and Form 20-F Information 2012

LOGO

 

Crestor continues to face challenges from generic competitors. The patent protecting Crestor in Australia has been challenged. Details of this matter are included in Note 25 to the Financial Statements from page 184.

Emerging Markets

In Emerging Markets, our sales increased by 4% to $5,752 million (2011: $5,763 million; 2010: $5,198 million), which was principally driven by growth in China and Russia.

In many of the larger markets, such as Brazil and Mexico, patients tend to pay directly for prescription medicines and consequently these markets are at less risk of direct government interventions on pricing and reimbursement. In other markets such as South Korea, Taiwan and Turkey, where governments pay for medicines, we are seeing continued efforts to reduce the cost of prescriptions in line with the systems in Western Europe, Canada and Australia. Some strong growth markets such as Vietnam are also implementing price and volume controls in an attempt to control government spending.

Emerging Europe

Sales in Emerging Europe grew by 2% to $1,165 million (2011: $1,244 million; 2010: $1,165 million) driven by increased sales in Russia and Romania, which more than offset reduced sales in Turkey.

We have continued to build our presence in Russia, where sales increased by 17% to $314 million (2011: $284 million; 2010: $232 million) mainly due to increased sales of Symbicort by 24%, Nexium by 93%, Crestor by 14% and Seroquel XR by 154%, driven by growth in the retail segment. We have also consolidated our position among the growth leaders in the hospital and regional reimbursement segments.

In Romania, we delivered a strong performance with sales up 19% to $161 million (2011: $154 million; 2010: $119 million), largely as a result of sales of Atacand increasing by 34%, Seroquel XR increasing by 41%, Crestor increasing by 10% and Symbicort increasing by 4%. In Turkey, a decrease in sales to $252 million (2011: $297 million; 2010: $304 million) reflected the additional price and prescription controls imposed by the Turkish government in late 2011.

China

Our sales in China (excluding Hong Kong) increased by 17% to $1,512 million (2011: $1,261 million; 2010: $1,047 million). Sales of products in our Cardiovascular and Respiratory & Inflammation Therapy Areas continue to grow ahead of the market, driven by strong performances of Crestor, Betaloc Zok and Pulmicort Respules . Sales of Nexium and Symbicort grew strongly by 27% and 50% respectively, while our mature gastrointestinal and oncology brands experienced challenges from government pricing reductions. In 2012, we saw Zoladex 10.8mg successfully launched in China, the expansion of our co-promotion with BMS to achieve listing of Onglyza into key hospitals, and a new collaboration formed between AstraZeneca and Ironwood to co-develop and co-commercialise linaclotide in China. We continue to be one of the leading multinational pharmaceutical companies in China.

Emerging Asia Pacific

Sales in Emerging Asia Pacific decreased by 3% to $923 million (2011: $968 million; 2010: $890 million). This decline was driven by India, where sales decreased by 29% to $67 million (2011: $110 million; 2010: $92 million), due primarily to supply issues; continued government interventions on pricing in countries such as Thailand, where sales decreased by 7% to $97 million (2011: $106 million; 2010: $114 million); and by Vietnam, where sales decreased by 4% to $45 million (2011: $47 million; 2010: $37 million). This was partially offset by sales growth in Indonesia, up 7% to $39 million (2011: $39 million; 2010: $34 million); South Korea, up 4% to $239 million (2011: $235 million; 2010: $213 million); and Malaysia, up 6% to $73 million (2011: $70 million; 2010: $66 million).

Other Emerging ROW

Sales in Other Emerging ROW were flat at $2,152 million (2011: $2,290 million; 2010: $2,096 million), with increased sales in Latin America, Egypt, Maghreb, Saudi Arabia and the Gulf States balanced by reduced sales in South Africa and Israel.

The Latin American pharmaceutical market continues to grow, underpinned by a reasonably stable political and economic climate. However, in many of the countries, the majority of the growth in the market is being captured by generics, branded generics and private label product offerings, often from local, non-multinational, companies.

In Latin America, our sales were down 1% to $1,331 million (2011: $1,455 million; 2010: $1,392 million). This was driven by declines in Mexico, down 22%, and Brazil, down 5%. Brazil continued to feel the effects of the loss of exclusivity on Seroquel IR and Crestor with year-on-year declines of 54% and 39% respectively. Growth of Seloken, Faslodex and older products such as Diprivan and Meronem helped to compensate for this development. In Mexico, challenging market conditions and the impact of an ‘at risk’ generic version of Crestor , resulted in weak performance with sales in Mexico declining by 22%. This was partially offset by sales growth in Venezuela (up 41%) and Argentina (up 24%). All key brands achieved double digit growth in Argentina ( Nexium, Crestor, Atacand, Symbicort and Seroquel XR ) and growth of more than 40% in Venezuela ( Crestor, Symbicort, Seroquel XR, Atacand, Zoladex and Arimidex ).

Successful product launches in the year included Brilinta and Kombiglyze XR in Mexico, Colombia and Argentina, and Vimovo in Brazil, Colombia and Argentina. Faslodex 500mg was launched in the fourth quarter of 2012 in Argentina, and is expected to launch in the first half of 2013 in Brazil and Venezuela.

In the Middle East and Africa, despite political challenges arising from the ‘Arab Spring’ revolutions, we further accelerated our growth with sales up 3%. Our largest markets were South Africa, Saudi Arabia and the Gulf States.

 

LOGO

 

AstraZeneca Annual Report and Form 20-F Information 2012   73

Additional Information | Glossary

Glossary

Market definitions

 

United States of America

  Other Established Markets       Emerging Markets        

US

  Western Europe   Japan   Emerging Europe   China   Other Emerging ROW
    Austria       Albania*       Egypt
    Belgium   Canada   Belarus*   Emerging Asia Pacific   Gulf States
    Denmark       Bosnia and Herzegovina   Bangladesh*   Israel*
    Finland   Other Established ROW   Bulgaria   Cambodia*   Latin America
    France   Australia   Croatia   Hong Kong   Lebanon*
    Germany   New Zealand   Czech Republic   India   Maghreb
    Greece       Estonia*   Indonesia*   Saudi Arabia
    Iceland*       Georgia*   Laos*   South Africa
    Ireland       Hungary   Malaysia    
    Italy       Kazakhstan*   Philippines    
    Luxembourg*       Latvia*   Singapore    
    Netherlands       Lithuania*   South Korea    
    Norway       Macedonia*   Sri Lanka*    
    Portugal       Poland   Taiwan    
    Spain       Romania*   Thailand    
    Sweden       Russia   Vietnam*    
    Switzerland       Serbia and Montenegro*        
    UK       Slovakia        
           

Slovenia*

       
           

Turkey

       
           

Ukraine*

       

Rest of World means Other Established Markets and Emerging Markets.

Established Markets means the US and Other Established Markets.

Established ROW means Canada, Japan and Other Established ROW.

Latin America includes Argentina, Brazil, Chile, Colombia, Costa Rica*, El Salvador*, Guatemala*, Honduras*, Mexico, Nicaragua*, Panama*, Peru* and Venezuela.

Gulf States includes Bahrain*, Dubai*, Kuwait*, Oman*, Qatar* and UAE.

Maghreb means Algeria, Morocco and Tunisia*.

*IMS Health, IMS Midas Quantum Q3 2012 data is not available or AstraZeneca does not subscribe for IMS Health quarterly data for these countries.

The above table is not an exhaustive list of all the countries in which AstraZeneca operates.

US equivalents

 

Terms used in this Annual Report

   US equivalent or brief description

Accruals

   Accrued expenses

Allotted

   Issued

Called-up share capital

   Issued share capital

Creditors

   Liabilities/payables

Debtors

   Receivables and prepaid expenses

Earnings

   Net income

Employee share schemes

   Employee stock benefit plans

Fixed asset investments

   Non-current investments

Freehold

   Ownership with absolute rights in perpetuity

Interest payable

   Interest expense

Loans

   Long-term debt

Prepayments

   Prepaid expenses

Profit

   Income

Profit and loss account

   Income statement/consolidated statement of comprehensive income

Share premium account

   Premiums paid in excess of par value of Ordinary Shares

Short-term investments

   Redeemable securities and short-term deposits

 

LOGO

 

AstraZeneca Annual Report and Form 20-F Information 2012   209

 

Important information for readers of this Annual Report

Cautionary statement regarding forward-looking statements

The purpose of this Annual Report is to provide information to the members of the Company. The Company and its Directors, employees, agents and advisers do not accept or assume responsibility to any other person to whom this Annual Report is shown or into whose hands it may come and any such responsibility or liability is expressly disclaimed. In order, among other things, to utilise the ‘safe harbour’ provisions of the US Private Securities Litigation Reform Act of 1995 and the UK Companies Act 2006, we are providing the following cautionary statement: This Annual Report contains certain forward-looking statements with respect to the operations, performance and financial condition of the Group. Forward-looking statements are statements relating to the future which are based on information available at the time such statements are made, including information relating to risks and uncertainties. Although we believe that the forward-looking statements in this Annual Report are based on reasonable assumptions, the matters discussed in the forward-looking statements may be influenced by factors that could cause actual outcomes and results to be materially different from those expressed or implied by these statements. The forward-looking statements reflect knowledge and information available at the date of the preparation of this Annual Report and the Company undertakes no obligation to update these forward-looking statements. We identify the forward-looking statements by using the words ‘anticipates’, ‘believes’, ‘expects’, ‘intends’ and similar expressions in such statements. Important factors that could cause actual results to differ materially from those contained in forward-looking statements, certain of which are beyond our control, include, among other things, those factors identified in the Principal risks and uncertainties section from page 75 of this Annual Report. Nothing in this Annual Report should be construed as a profit forecast.

 

Inclusion of Reported performance, Core financial measures and constant exchange rate growth rates

AstraZeneca’s determination of non-GAAP measures together with our presentation of them within our financial information may differ from similarly titled non-GAAP measures of other companies.

 

Statements of competitive position, growth rates and sales

In this Annual Report, except as otherwise stated, market information regarding the position of our business or products relative to its or their competition is based upon published statistical sales data for the 12 months ended 30 September 2012 obtained from IMS Health, a leading supplier of statistical data to the pharmaceutical industry. For the US, dispensed new or total prescription data and audited sales data are taken, respectively, from IMS Health National Prescription Audit and IMS National Sales Perspectives for the 12 months ended 31 December 2012; such data is not adjusted for Medicaid and similar rebates. Except as otherwise stated, these market share and industry data from IMS Health have been derived by comparing our sales revenue to competitors’ and total market sales revenues for that period. Except as otherwise stated, growth rates are given at CER. For the purposes of this Annual Report, unless otherwise stated, references to the world pharmaceutical market or similar phrases are to the 54 countries contained in the IMS Health MIDAS Quantum database, which amounted to approximately 92% (in value) of the countries audited by IMS Health.

 

AstraZeneca websites

Information on or accessible through our websites, including astrazeneca.com, astrazenecaclinicaltrials.com and medimmune.com, does not form part of and is not incorporated into this Annual Report.

 

External/third party websites

Information on or accessible through any third party or external website does not form part of and is not incorporated into this Annual Report.

 

Figures

Figures in parentheses in tables and in the Financial Statements are used to represent negative numbers.

  LOGO

 

Exhibit 15.5

[LETTERHEAD OF BUREAU VERITAS UK LTD]


AstraZeneca PLC
Legal & Secretary’s Department
2 Kingdom Street
London
W2 6BD
For the attention of Adrian Kemp
By fax 020 7604 8151 & by post





25 March, 2013


Dear Ladies and Gentlemen

BUREAU VERITAS STATEMENT OF ASSURANCE FOR ANNUAL REPORT AND FORM 20-F INFORMATION 2012

In connection with the anticipated filing by AstraZeneca PLC (“AstraZeneca”) of a Form 20-F with the US Securities and Exchange Commission, Bureau Veritas hereby authorizes AstraZeneca to refer to Bureau Veritas’s external assurance on corporate responsibility related information as stated on page 49 and identified (highlighted in yellow) on the pages of the Annual Report and Form 20-F Information for the fiscal year ended December 31, 2012 (the “Annual Report”) annexed as Exhibit A, which is incorporated by reference in the registration statements No. 33-83774 for AstraZeneca and Zeneca Wilmington Inc. and No. 333-145848, No. 333-114165 and No. 333-171306 for AstraZeneca, each on Form F-3, and in the registration statements No. 333-09060, No. 333-09062, No. 33-65362, No, 33-65366, No. 333-12310, No. 333-12426, No. 333-12428, No. 333-13328, No. 333-13918, No. 333-124689, No. 333-152767 and No. 333-170381 on Form S-8 for AstraZeneca.

Our authorization is subject to AstraZeneca’s acknowledgement and agreement that: 

 
1)
Bureau Veritas has undertaken an independent review of the corporate responsibility information disclosed in the Annual Report and provided an opinion as to the accuracy and reliability of the information subject to the scope, objectives and limitations defined in the full assurance statement posted on AstraZeneca’s responsibility website;

 
2)
AstraZeneca acknowledges and agrees that Bureau Veritas shall not be deemed an “Expert” in respect of AstraZeneca’s securities filings, and AstraZeneca agrees that it shall not characterize Bureau Veritas as such; and

 
3)
AstraZeneca accepts full responsibility for the disclosure of all information and data, including that relating to Bureau Veritas, set forth in the Annual Report as filed with the SEC and agrees to indemnify Bureau Veritas from any third party claims that may arise therefrom.
 
 
 
 
 

 
Please indicate your agreement to the foregoing by signing in the space indicated below. Our authorization will not become effective until accepted and agreed by AstraZeneca.


Very truly yours,


/s/ Rachel Noel
Rachel Noel, Principal Consultant (Assurance Services)
For and on behalf of Bureau Veritas UK Ltd




ACCEPTED AND AGREED

this 25th day of March 2013

AstraZeneca PLC


/s/ Adrian Kemp
Name: Adrian Kemp
Title: Company Secretary
 
 
 
 
 
 
 

Exhibit A

LOGO

 

In 2012, there was Core R&D expenditure of $4.5 billion in our R&D organisation (2011: $5 billion; 2010: $4.2 billion). In addition, $5,228 million was spent on acquiring product rights (such as in-licensing) (2011: $189 million; 2010: $1,017 million) and we invested approximately $791 million on the implementation of our R&D restructuring strategy. The allocations of spend by early development and late-stage activities are presented in the R&D spend analysis table opposite.

R&D ethics

We want to be recognised for our high quality science and for the impact we can make on serious diseases, and to be trusted for the way we work. Our standards of R&D ethics are global and apply to all AstraZeneca research activity, in all locations, whether conducted by us or on our behalf by third parties.

Clinical trials

Our commitment: to deliver consistently high standards of ethical practice and scientific conduct in all our trials worldwide and to public transparency on registration and results of all clinical trials, whether positive or negative.

Our objective: to be recognised as an industry leader in the publication and sharing of clinical trial information.

We conduct clinical trials at multiple sites in several different countries/regions as shown in the chart above. A broad geographic span helps us to ensure that those taking part in our studies reflect the diversity of patients around the world for whom the new medicine is intended. This approach also helps to identify the types of people for whom the treatment may be most beneficial.

Our global governance process for determining where we place clinical trials provides the framework for ensuring a consistent approach worldwide. We take several factors into account, including the availability of experienced and independent ethics committees and a robust regulatory regime, as well as sufficient numbers of trained healthcare professionals and patients willing to participate in a trial.

Before a trial begins, we work to make sure that those taking part understand the nature and purpose of the research and that proper procedure for gaining informed consent is followed (including managing any special circumstances, such as different levels of literacy). Protecting participants throughout the trial process is a core priority and we have strict procedures in place to ensure that they are not exposed to any unnecessary risks.

All our clinical studies are conceptually designed and finally interpreted in-house but a percentage of them are run for us by contract research organisations (CROs). In 2012, around 31% of patients in our small molecule studies and around 87% of patients in our biologics studies were monitored by CROs on our behalf. We contractually require CROs to work to our global standards and we conduct risk-based audits to monitor compliance.

Animal research

Our commitment: to embrace, promote and embed scientific and technical best practice in animal research.

Our objective: to drive continuous improvement internally and engage with external providers on the implementation of AstraZeneca global standards for non-human primate housing and care. These include the following targets:

 

> roll-out of AstraZeneca Good Statistical Practice (GSP) global standard and associated compliance monitoring
> more than 80% of external providers of AstraZeneca non-human primate research studies are operating to AstraZeneca standards.

We remain committed to minimising our use of animals in our research without compromising the quality of the research data. Wherever possible, we use non-animal methods, such as computer modelling, that eliminate the need to use animals early in drug development or reduce the number required. We also work to refine our existing methods. This replacement, reduction and refinement of animal studies is known as ‘the 3Rs’. To support our drive for

continuous improvement, we work both within AstraZeneca and the wider scientific community to share the 3Rs knowledge and learning.

The number of animals we use will continue to vary because it depends on a number of factors, including the amount of pre-clinical research we are doing, the complexity of the diseases under investigation and regulatory requirements. We believe that, without our active commitment to the 3Rs, our animal use would be much greater. In 2012, we used approximately 304,000 animals in-house (2011: 381,000). In addition, approximately 14,000 animals were used by external CROs on our behalf (2011: 17,000). Against our 2012 target of more than 80%, 85% of our externally-placed non-human primate studies met AstraZeneca standards in 2012. We will continue to progress towards our 2013 target of 100% of our studies being conducted in facilities meeting AstraZeneca required standards.

The welfare of the animals we use continues to be a top priority and our Bioethics Policy applies worldwide. We routinely have inspections by government authorities of our internal animal research facilities. External CROs that conduct animal studies on our behalf are required to comply with our global standards and we undertake audits to ensure our expectations are being met.

During 2012, we developed, launched and began implementation of standard operating procedures and guidance documents to underpin our new GSP global standard, developed in 2011. These apply to our internal animal research and the launch included extensive training programmes for relevant scientists, technical staff and managers across the organisation.

 

Extract from 2012 Responsible Business Plan.

 

   Further information on AstraZeneca’s approach to responsible business can be found in the Responsible Business section from page 48 and on our website, astrazeneca.com/responsibility.

 

LOGO

 

AstraZeneca Annual Report and Form 20-F Information 2012   33

Performance | Business Review

 

LOGO

 

Patient safety

Our commitment: the safety of the patients who take our medicines is of fundamental importance to us.

Our objective: to enhance pharmacovigilance awareness – including the use of collaborative programmes to share and use our knowledge and best practice in order to improve reporting and patient safety in developing countries.

All drugs have potential side effects and we aim to minimise the risks and maximise the benefits of each of our medicines throughout the whole life-cycle of a medicine. We continually monitor the use of all our medicines to ensure that we become aware of any side effects not identified during the development process. This is known as pharmacovigilance and is core to our ongoing responsibility to patients. We have comprehensive and rigorous systems in place for detecting and rapidly evaluating such effects,

including mechanisms for highlighting those that require immediate attention. We also work to ensure that accurate, well-informed and up-to-date information concerning the safety profile of our drugs is provided to regulators, doctors, other healthcare professionals and, where appropriate, patients.

A pharmacovigilance awareness programme was developed in 2012 and circulated to marketing companies, together with guidance about how the information should be shared with regulatory authorities in readiness for external enquiry. One such opportunity arose when SFDA (the Chinese health authority) met UMC (WHO Uppsala Monitoring Centre) and we were able to share our experience and thoughts around signal management.

We have an experienced, in-house team of clinical patient safety professionals dedicated to the task of ensuring that we meet our commitment to patient safety.

At a global level, every medicine in development and on the market is allocated a Global Safety Physician and a team of patient safety scientists. In each of our markets we also have dedicated safety managers with responsibility for patient safety at a local level.

Our Chief Medical Officer has overall accountability for the benefit/risk profiles of the products we have in development and those on the market. He provides medical oversight and ensures that appropriate risk assessment processes are in place to enable informed decisions to be made about safety as quickly as possible.

 

Extract from 2012 Responsible Business Plan.

 

   Further information on AstraZeneca’s approach to responsible business can be found in the Responsible Business section from page 48 and on our website, astrazeneca.com/responsibility.

Clinical trial transparency

AstraZeneca has a long-standing commitment to making information about our clinical research publicly available to enhance the scientific understanding of how our medicines work and in the medical interest of patients. By the end of 2012, we had registered 2,050 clinical trials and posted the results of 1,360 trials on a range of public websites including our own dedicated clinical trials website, astrazenecaclinicaltrials.com.

We publish information on the registration and results of all new and ongoing AstraZeneca-sponsored clinical trials for all products in all phases, including marketed medicines, drugs in development and drugs whose further development has been discontinued. We post results, irrespective of whether they are favourable or unfavourable to AstraZeneca.

 

> Our disclosure policy goes beyond legal requirements, which currently require publication for Phase II studies onwards only.
> From 15 January 2013, we are voluntarily disclosing the research protocol for our clinical trials on astrazenecaclinicaltrials.com once a manuscript relating to an investigational or approved product is published in a peer-reviewed medical journal.

These disclosure requirements are set out in our Bioethics Policy and compliance is mandatory across the Group.

We consider requests for patient-level data from other parties on a case-by-case basis, following consistent criteria to establish if, and how, the information provided will be used for valid scientific purposes and to benefit patients.

Calls for ‘open access’ to clinical data raise complex practical, legal and ethical issues around full disclosure of patient information. Decision makers, as well as academia and industry, have a duty to consider all the implications that could arise from such proposals. These include ensuring scientific rigour, safeguarding patient privacy and protecting innovation and medical progress. We are engaging with regulators, legislators, industry, and medical and scientific bodies to discuss the issues raised by the proposals to routinely publish full clinical trial and patient data so we can collectively identify practicable solutions that deliver real benefits to medical science and patients.

 

34   AstraZeneca Annual Report and Form 20-F Information 2012

Performance | Business Review

 

LOGO

 

Global strategies tailored to meet local needs

We focus on developing global strategies tailored to meet local needs and recognise that our commercial capabilities must evolve to meet future market requirements. The pace and degree of change in global economies and intensifying regulatory and access challenges have led us to look at ways of better and more efficiently addressing the changing needs and preferences of payers, prescribers and patients. In 2012, this effort included completing the regional consolidation of our Commercial organisation announced in 2011. Our streamlined operating model includes integrating our smaller local marketing companies into area clusters, allowing them to benefit from global resources while staying local and concentrating on meeting local customer needs.

All our markets have a role to play in delivering our commercial strategy. We continue to prioritise investment and allocate our resources in the most cost-effective way. This allows us to identify those markets of major significance to us, those that will become more important drivers of our business in the future and highlight those Established Markets where we need to refocus our approach to deliver sustained success. Our footprint continues to evolve to reflect declining sales in Established Markets and increasing sales in Emerging Markets. For example, in 2012 we enhanced our presence in Asia with the opening of the Zhangjiang Park Regional Hub Headquarters in Shanghai.

Changing customer needs

In most countries, our sales are made through wholly-owned local marketing companies. In other countries, we sell through distributors or local representative offices. Our products are marketed primarily to primary care and specialist doctors. Our efforts are directed towards explaining the therapeutic as well as the economic benefits of our products to doctors, governments and others who pay for healthcare.

Historically, our commercial model has been based on the use of face-to-face marketing techniques. This is now changing to reflect the changing profile of the prescribers of our medicines. For example, primary care physicians tend to be younger on average than previously, a greater proportion is female, and more work part-time. Primary care physicians want to interact with pharmaceutical companies in different ways. Driven by experience from innovative approaches piloted and implemented in North America and Europe, we have changed the way we work. Improvements include the introduction of office-based sales teams, which include physicians and dedicated customer service staff, and expanded use of digital channels. These selling channels have now been rolled out in more than 30 countries and across a range of products. Evidence to date suggests these channels are appreciated by those who use them and are an efficient and effective way of driving value for our business. We are accelerating the roll-out and adoption of the new model in the majority of markets in which we operate.

Pricing our medicines

Our challenge is to deliver innovative medicines that improve health for patients, bring benefits to society and provide an appropriate return on our investment. Our global pricing policy provides the framework to ensure appropriate patient access while optimising the profitability of all our products in a sustainable way. When setting the price of a medicine, we take into consideration its full value to patients, to those who pay for healthcare and to society in general. We also pursue a flexible approach to the pricing of our medicines. For example, we support the concept of differential pricing, provided that appropriate safeguards are in place to ensure that differentially priced products are not diverted from patients who need them to be sold and used in more affluent markets.

Delivering value for payers

Our medicines play an important role in treating unmet medical need. In doing so, they bring economic as well as therapeutic benefits. Effective treatments can help to lower healthcare costs by reducing the need for more expensive care, such as hospital stays or surgery, or through preventing patients from developing more serious or debilitating diseases that are costly to treat. They also contribute to increased productivity by reducing or preventing the incidence of diseases that keep people away from work.

As outlined in the Pricing pressure section on page 18, there is continued downward pressure on drug pricing and, in the current difficult economic environment, payers expect us to be able to define the value our medicines create. We are acutely aware of the challenges facing those who pay for healthcare and are committed to delivering value, which will allow us to bring our medicines to the patients that need them. Therefore, we work with payers and healthcare providers to understand their priorities and requirements and generate evidence regarding how our products offer value and support cost-effective healthcare delivery.

Increasing access to healthcare

Our commitment: to increase access to healthcare for under-served patient populations in a sustainable way.

Our objective: to roll-out our access to healthcare strategy within the business and further develop the framework for implementation, including non-financial performance indicators for monitoring our performance across all our initiatives.

Sales of medicines in our Established Markets enable us to generate the revenue we need to provide our shareholders with a return, invest in continued innovation and pursue other opportunities to expand the availability of our medicines. Increasing that availability and increasing access to healthcare for under-served patient

 

38   AstraZeneca Annual Report and Form 20-F Information 2012

 

LOGO

 

populations in a sustainable way is a significant global challenge and, in March 2012, we announced our access to healthcare strategy to help in that process. The strategy framework is explained on our website, astrazeneca.com/responsibility. It seeks to take account of the different barriers to healthcare around the world and is tailored locally to meet the needs of different patient populations. We are pursuing a range of initiatives, including broadening affordability of our medicines, across these populations to understand what works best and in what context.

During the year, we rolled out our access to healthcare framework within our Global Sales and Marketing Organisation to support further development of our existing approach and to enable us to capture ongoing ‘broadening affordability’ commercial initiatives. For example, our work to expand patient access to healthcare in countries such as Brazil, Romania and Ukraine continues with a range of different commercial approaches being adopted. In China, we are pursuing our strategy to reach patients in the broader market, beyond the big hospitals in the big cities, by developing new commercial channels for reaching emerging hospitals and community health centres. Best practice will be shared and replicated. In addition, in 2012, we acquired Guangdong BeiKang Pharmaceutical Company Limited, a generics manufacturing company in China which gave us access to a portfolio of injectable medicines used to treat infections. First launches are planned for 2013 and underscore our intention to serve the health needs of Chinese patients through our innovative medicines and, increasingly, high quality branded generic treatments that are locally produced to global standards. You can read more about our strategy and the access initiatives we have under way on our website, astrazeneca.com.

We are making progress on the development of non-financial indicators for monitoring our performance and these are included in our 2013 Responsible Business Plan.

Sales and marketing ethics

Our commitment: to deliver consistently high ethical standards of sales and marketing practice worldwide.

Our objective: to focus on ensuring compliance with our Ethical Interactions Policy and report on the:

 

> number of confirmed breaches of external sales and marketing codes
> number of instances of failure to meet our standards in the Global Commercial Organisation, including contract staff
> number of corrective actions for breaches of our Code of Conduct or supporting policies by Commercial employees, including contract staff.

During 2012, we continued to provide training for employees on our global standards that govern the way that we conduct our business around the world. We have comprehensive processes in place for monitoring compliance with our Code of Conduct and global policies, including dedicated compliance professionals who support our line managers locally in monitoring their staff activities. We also have a network of nominated signatories who review our promotional materials against all applicable requirements. Additionally, in 2012, audit professionals have conducted compliance audits of a selection of our marketing companies.

As shown in the Global KPI: Disciplinary actions chart opposite, we identified a total of 10 confirmed breaches of external sales and marketing regulations or codes globally in 2012 (17 in 2011). There were 1,932 instances, including contract staff, of failure to comply with AstraZeneca’s Code of Conduct and global policies in our Global Commercial Organisation, the majority of which were minor (1,292 in 2011, including external breaches). We believe that the movement in both numbers reflects our enhanced management oversight and compliance monitoring.

As shown in the Corrective actions table above, in relation to these breaches (and it is important to note that a single breach can involve more than one person failing to meet the standards required), we removed 188 people from their role, formally warned 685 people and provided further guidance or coaching on our policies for 1,808 people. The most serious breaches are raised with the Audit Committee.

US Corporate Integrity Agreement reporting

In April 2010, AstraZeneca signed an agreement with the US Department of Justice to settle an investigation relating to the sales and marketing of Seroquel IR . The requirements of the associated Corporate Integrity Agreement between AstraZeneca and the Office of the Inspector General of the US Department of Health and Human Services (OIG) include a number of active monitoring and self-reporting obligations that differ from self-reporting required by authorities in the rest of the world. To meet these obligations, AstraZeneca provides notices to the OIG describing the outcomes of particular investigations potentially relating to violations of certain laws, as well as a separate annual report to the OIG summarising monitoring and investigation outcomes relevant to Corporate Integrity Agreement requirements.

 

Extract from 2012 Responsible Business Plan.

 

  Further information on AstraZeneca’s approach to responsible business can be found in the Responsible Business section from page 48 and on our website, astrazeneca.com/responsibility.

 

 

 

LOGO

 

AstraZeneca Annual Report and Form 20-F Information 2012   39

Performance | Business Review

 

LOGO

 

Working with suppliers

Our commitment: to integrate AstraZeneca ethical standards into our procurement activities and decisions worldwide.

Our objective: to monitor compliance through our ongoing assessment and programmes with focus on areas experiencing highest challenges; to address challenges with our suppliers and promote improvement through collaboration.

Our Global Responsible Procurement Standard defines one of the key business processes for integrating our ethical standards into our procurement activity and decision making worldwide. It includes detailed expectations of suppliers. The process is based on an escalating set of risk-based due diligence activities, applied in a pragmatic way. The same initial assessment process is used for all suppliers and more detailed, focused assessments are then made, relevant to the service provided. Since the programme began in 2009, we have completed 5,661 assessments of new and existing suppliers, which accounts for approximately two-thirds of our spend on suppliers.

We categorise suppliers as high, medium or low risk. We focus our auditing efforts on high and medium risk rated suppliers but we also audit some suppliers that we consider to be lower risk, to confirm our performance expectations across all suppliers we do business with. In 2012, we continued our audit activity with 482 audits across 52 countries (751 audits in 2011) as set out in the table on the previous page.

Forty-three percent of suppliers audited demonstrated standards that met our expectations, with a further 53% implementing improvements to address minor non-compliances. We monitor progress across all corrective actions and 4% of suppliers audited this year will require significant follow up to confirm they will make the improvements we require. We will not use suppliers who are unable or unwilling to meet our expectations in a timely way. During 2012, we removed eight suppliers from our supply chain.

Environmental impact

Our commitment: to minimise the environmental impact of our operations by reducing the carbon footprint and natural resource demands of our own and our suppliers’ business activities.

Our targets for 2012 included reducing:

> operational greenhouse gas footprint to 890 kilo tonnes CO 2 e/yr
> hazardous waste to 0.70 tonnes/$m sales and non-hazardous waste to 0.52 tonnes/employee
> water use to 4.0 million m 3 .

Our SHE strategy and associated objectives and targets for 2011 to 2015 provide the framework for driving our environmental sustainability going forward. This section includes summary information about certain key areas of the framework. Full details of our strategy, objectives and targets are available on our website, astrazeneca.com/responsibility.

We work to reduce our greenhouse gas emissions by, among other things, improving our energy efficiency and pursuing lower-carbon alternatives to fossil fuels at our sites. We strive to ensure that our travel and transport activities are as efficient as possible. Our carbon footprint is also affected by some of our respiratory therapies, specifically our pressurised metered-dose inhalers that rely on hydrofluoroalkane (HFA) propellants to deliver the medicine to a patient’s airways. While HFAs have no ozone depletion potential and a third or less of the global warming potential than the chlorofluorocarbons (CFCs) they replace, they are still greenhouse gases. Our target is to reduce our operational greenhouse gas footprint (excluding emissions from patient use of our inhaler therapies) by 20% from our 2011 levels by 2015. In 2012, our gross greenhouse gas emissions (from all sources) totalled 1.15 million tonnes (41 tonnes/$m indexed to Group revenue).

The management of waste is another key aspect of our commitment and we have a 2015 target of a 15% reduction in hazardous and non-hazardous waste from our 2011 levels. Our primary focus is waste prevention, but where this is not practical, we concentrate on waste minimisation and appropriate treatment or disposal to maximise the reuse and recycling of materials and minimise disposal to landfill. In 2012, our total waste was 47,000 tonnes with a tonnes/$m index of 1.7.

We recognise the need to use water responsibly and, where possible, to minimise the use of water in our facilities. To support the delivery of our target to reduce water use by 25% from our 2011 levels by 2015, we now have water conservation plans at our largest sites. In 2012, our water use was 3.6 million m 3 with a m 3 /$m index of 130.

We are also working to ensure that we measure and report the impact of our external manufacturing activity on the environment, and that our suppliers have appropriate environmental improvement targets.

Our continued commitment to product stewardship is underpinned by our ongoing work to integrate environmental considerations into a medicine’s complete life-cycle, from discovery and development, through manufacturing, marketing and to its ultimate disposal. Further information is available on our website, astrazeneca.com/ responsibility, including environmental risk assessment data for our medicines.

 

Extract from 2012 Responsible Business Plan.

 

   Further information on AstraZeneca’s approach to responsible business can be found in the Responsible Business section from page 48 and on our website, astrazeneca.com/responsibility.

 

The following figures have been revised from those previously published to incorporate our biologics capabilities into our targets.

 

 

42   AstraZeneca Annual Report and Form 20-F Information 2012

Performance | Business Review

 

LOGO

 

Further developing leadership and management capabilities

We encourage and support our people in achieving their full potential by providing a range of learning and development (L&D) programmes. These are designed to build the capabilities and encourage the behaviours needed to deliver our business strategy.

We have a global approach, supported by the creation of our global talent and development organisation, to ensure that high standards of L&D practice are applied across AstraZeneca. We continue to develop and deploy instructor-led and online development resources, which we aim to make available to all employees to increase access to learning and to support self-development.

We recognise the importance of good leadership and its critical role in stimulating high levels of performance and engagement. Our leadership development frameworks are focused on the core capabilities that we believe are essential for strong and effective leadership. These capabilities are defined for each level in the organisation and apply to all our employees. We complement our leadership capabilities with a set of manager accountabilities, which define what we expect from our managers. These manager accountabilities are further enabled across all markets through the deployment of our global HR platform.

Alongside judicious hiring of new leaders into critical senior roles, the development of an internal pipeline of future global leaders is a high priority. We identify individuals with

the potential for more senior and complex roles. These talent pools provide succession candidates for a range of leadership roles across

AstraZeneca. We regard these individuals as key assets to the organisation and we proactively support them to reach their potential through, for example, global talent development programmes and targeted development opportunities.

Changes to the Senior Executive Team announced in January 2013 included the promotion of six internal candidates and demonstrate our commitment to the development of senior leaders.

We remain committed to making full use of the talents and resource of all our people. We have policies in place to avoid discrimination, including on the grounds of disability. Our policies cover recruitment and selection, performance management, career development and promotion, transfer, and training (including re-training, if needed, for people who have become disabled) and reward.

Improving the strength and diversity of the talent pipeline

Our commitment: to build an inclusive, open and trusting organisation embracing the skills, knowledge and unique ability of our employees.

Our objective: to accelerate diversity and inclusion appropriately throughout the business, build accountability and track progress. Our target for 2015 is to improve female representation:

 

> at senior manager level and above from 38% (2010) to 43% (2015)
> in the global talent pool from 33% (2010) to 38% (2015).

Our global workforce provides a diversity of skills, capabilities and creativity, and we value the benefits that such diversity brings to our business. We aim to foster a culture of respect and fairness where individual success depends solely on ability, behaviour, work performance and demonstrated potential. As we continue to reshape our organisation and geographic footprint, our challenge is to ensure that diversity in its broadest sense is reflected in our workforce and leadership, and integrated into our business and people strategies. Within this context, we support the representation of women at the highe st

levels in our business. Women make up 50% of our global workforce, giving us a real opportunity to develop female leaders. Indeed, there are currently three women on our Board (25%) and, below Board level, women account for 40% of senior management.

Under the leadership of a global Diversity & Inclusion steering group chaired by a member of the SET and comprising senior leaders from across the business and geographies, we are driving change in three key areas: ‘leadership & management capability’; ‘transparency in talent management & career progression’; and ‘work-life challenges’. In March 2012, we launched our Global Insight Exchange programme as a direct result of the work of the steering group. This programme, which consists of peer-to-peer mentoring of over 30 ‘learning pairs’ of identified talent from different functional areas and geographies within our organisation, is designed to accelerate the development of our leadership culture and talent pipeline through the exchange of diversity of thought and experience. In addition, we track gender representation at different levels of the organisation and country of origin representation of our senior leaders to measure progress over the medium term.

Driving employee engagement

We use a variety of global leadership communication channels to engage employees in our business strategy. These include face-to-face meetings, video conferencing and Yammer (a social media tool) to encourage two-way dialogue to take place. For the third year in a row our annual global employee survey (FOCUS) included an open text feedback mechanism, with around 25,000 comments made on a variety of topics.

 

44   AstraZeneca Annual Report and Form 20-F Information 2012

 

LOGO

 

In 2012, 91% of our employees participated in the survey, which measures levels of employee engagement and considers the effectiveness of our organisational, leadership and management capabilities, and satisfaction in terms of employees’ working environment. Our employee engagement score decreased by three percentage points this year and our leadership communications and work-life balance scores also decreased. The survey took place at a challenging time for the Group and the scores were disappointing. We remained ahead of external pharmaceutical industry norms in areas such as motivation, willingness to put in more effort than would normally be expected, line management, and operating with integrity and ethics. However, we recognise that we have more work to do in important areas, such as strategic understanding and reducing organisational complexity, to ensure AstraZeneca is a great place to work. Local leadership teams have also identified actions designed to target any concerns specific to their organisational area.

A key element of our people strategy is the continued development of a performance culture across the organisation. By strengthening our focus on setting high quality objectives aligned to our business strategy, and ongoing coaching and feedback, we strive to ensure that performance at all levels of the organisation delivers value. The Board is responsible for setting our high-level strategic objectives and monitoring performance against them (see the Operation of the Board section on page 111). Managers across AstraZeneca are accountable for working with their teams to develop individual and team performance targets, and for ensuring that employees understand how they contribute to overall business objectives.

We will continue to empower our leaders to drive performance, to hold our managers accountable for understanding and delivering against the standards required, and to provide the tools necessary to reward outstanding contributions.

Our focus on optimising performance is reinforced by performance-related bonus and incentive plans. AstraZeneca also encourages employee share ownership by offering the opportunity to participate in various employee share plans, some of which are described in the Directors’ Remuneration Report from page 122 and also in Note 24 to the Financial Statements from page 179.

Human rights

Our commitment: to respect and promote international human rights in our operations and our sphere of influence.

Our objective: to ensure that human rights considerations are appropriately integrated into our policies, processes and practices.

As reported in 2011, we have carried out labour reviews in 106 countries in which we have employees. The reviews focused on International Labour Organization (ILO) core areas, including freedom of association and collective bargaining, child labour, discrimination, working hours and wages. The framework for the review was provided by an adaptation of the employment section of the Danish Institute for Human Rights assessment tool for pharmaceutical companies, which was developed with our industry’s help and launched in 2010. Results showed that our practices are generally consistent across all countries, based on our mandate that our global standards are applied when external national standards do not meet our minimum requirements. Some gaps to ILO standards have been identified and are being addressed as part of the review of our Global People Policy, which is planned for 2014.

Managing change

Recruitment in our Emerging Markets continues to be accompanied by headcount reductions in our Established Markets as a result of our continuing strategic drive to improve efficiency and effectiveness. Reductions have come about through restructuring in R&D, supply and manufacturing, support functions and our sales and marketing workforce. The net effect of these changes since the end of 2006 has been to reduce our total headcount by some 15,100 from 66,800 to 51,700. This decrease includes a reduction of 2,600 positions in 2010, 5,000 in 2011 and a further 6,300 in 2012, which resulted from our business change plans announced since 2010.

We are committed to ensuring that AstraZeneca’s core values, robust people policies, consultation infrastructure and prior experience were integrated into this multi-faceted business transformation. Trade unions and employee representative groups were involved throughout the restructuring process. With significant investment in outplacement support, high levels of success have been achieved in finding employees alternative opportunities outside AstraZeneca. Further details are set out in the Our strategy section from page 20.

 

Extract from 2012 Responsible Business Plan.

 

   Further information on AstraZeneca’s approach to responsible business can be found in the Responsible Business section from page 48 and on our website, astrazeneca.com/responsibility.

 

 

LOGO

 

AstraZeneca Annual Report and Form 20-F Information 2012   45

Performance | Business Review

 

LOGO

 

Managing employee relations

We work to ensure a level of global consistency in managing employee relations, while allowing enough flexibility to support the local markets in building good relations with their workforces, taking into account local laws and circumstances. To that end, relations with trade unions are nationally determined and managed locally in line with the applicable legal framework and standards of good practice. However, each change programme has its unique challenges and a standard solution may not always be appropriate. Where this is the case, the appropriate solution is developed through consultation with employee representatives or, where applicable, trade unions, with the aim of retaining key skills and mitigating job losses.

Early in 2012, we implemented our Global Employment Standards, which are linked to our Global People Policy. Our Global Employment Standards serve to provide common and consistent expectations concerning the way in which our employees will be managed globally and cover matters including attendance, employee concerns, flexible working, leaving AstraZeneca, misconduct, performance improvement, redeployment and redundancy, and work-life balance.

Safety, health and wellbeing

Our commitment: to promote a safe, healthy and energising work environment in which our people, and those from third parties working closely with us, are able to express their talents, drive innovation and improve business performance.

Our targets for 2012 included:

> 0 fatalities
> combined lost time injury/illness rate per million hours worked of 2.38
> 7.1 collisions per million kilometres driven.

Driver safety remains our highest priority for improvement and our focus is on promoting driver safety among our sales forces, collectively the single largest group of employees who drive on AstraZeneca business. Driver safety targets are included in regional and local scorecards. Performance is monitored centrally to assess progress and identify areas for improvement. In 2012, we missed our annual target for collisions per million kilometres driven. We remain on track to achieve our 2015 target.

We regret that during 2012, two members of the public were killed in two separate road traffic accidents involving AstraZeneca drivers in Russia and Turkey. Detailed investigations into both accidents have been carried out. For the Russian accident, an action plan was formulated to respond to the findings of the investigation and those actions are being tracked. The investigation report for the Turkish accident, which occurred in October, has not yet been finalised. Learning from the investigations into both accidents will be shared widely across the Group.

In 2012, the lost time injury/illness rate increased by 3% from 2011. However, we remain on track to achieve our 2015 target of a 25% reduction in the lost time injury/illness rate from the 2010 baseline, with an overall 21% reduction achieved so far.

Work-related stress has been a particular focus for us in recent years; in 2012 we achieved a significant (59%) reduction in the number of reportable cases compared to 2011. We are continuing our efforts in this area, using a risk-based approach, including wellbeing risk assessment tools, to identify high-risk areas and target interventions effectively.

 

Extract from 2012 Responsible Business Plan.

 

   Further information on AstraZeneca’s approach to responsible business can be found in the Responsible Business section from page 48 and on our website, astrazeneca.com/ responsibility.

 

46   AstraZeneca Annual Report and Form 20-F Information 2012

 

LOGO

 

of 23 criteria in 2011) including marketing practices, supply chain management and human capital development. While these scores are encouraging, we lost ground in some areas including innovation management and health outcomes contribution. To better understand these lower scores, we commissioned an in-depth external benchmark survey and the analysis will be used to inform our improvement planning.

Responsible business governance

The Board is responsible for our responsible business framework and Non-Executive Director, Nancy Rothwell, oversees implementation and reporting to the Board.

The SET and senior managers throughout the Group are accountable for operating responsibly within their areas taking into account national, functional and site issues and priorities. Line managers are accountable for ensuring that their teams understand the requirements and that people are clear about what is expected of them as they work to achieve AstraZeneca’s business goals.

Our Responsible Business Council (the Council) is chaired by our Executive Vice-President of Human Resources & Corporate Affairs, and members include senior leaders from each relevant SET area. Its agenda is focused on driving long-term value creation by agreeing, among other things:

 

> responsible business priorities for the Group in line with strategic business objectives
> managing and monitoring the annual process of setting responsible business objectives and targets recorded in the Responsible Business Plan, as well as reviewing performance against KPIs
> appropriate policy positions to support AstraZeneca’s business objectives and reputation management.

The Council is supported by a Responsible Business Working Group (the Working Group) of SET area representatives. Among other things, the Working Group continuously reviews external issues with the potential to impact AstraZeneca and, as appropriate, prepares management and measurement proposals for the Council’s consideration.

External assurance

Bureau Veritas has provided external assurance on the responsible business information contained within this Annual Report on pages 33-34, 38-39, 42, 44-46 and below, and of the performance related content of the Responsibility section of our website. Based on the evidence provided and subject to the scope, objectives and limitations defined in the full assurance statement, nothing has come to the attention of Bureau Veritas causing them to believe that the responsible business information included within this Annual Report is materially misstated. The full assurance statement, which contains detailed scope, methodology, overall opinion and recommendations can be found on our website, astrazeneca.com/responsibility. Bureau Veritas is an independent professional services company that specialises in quality, health, safety, social and environmental management with a long history of providing independent assurance services.

Community investment

Our commitment: to meet our responsibility as a global corporation to support the wider community, maximising the benefit of our investment for all stakeholders, through focused investment and by embracing current best practice.

Our objective: to extend the geographic reach of our Young

Health Programme (YHP). Our target was to have 15 YHP country programmes running by the end of 2012 with a total target reach of 500,000 adolescents by 2015.

In 2012, we spent a total of $1.18 billion (2011: $1.06 billion*) on community investment sponsorships, partnerships and charitable donations worldwide, including our product donation and patient assistance programmes which make our medicines available free of charge or at reduced prices. Through our three patient assistance programmes in the US we donated products valued at an average wholesale price of over $1.12 billion (2011: $938 million). We also donated products worth over $5.8 million, valued at average wholesale price, to charitable organisations Americares and Direct Relief International.

Our global community investment strategy focuses on two key areas, healthcare in the community and science in education. In 2012, we continued to expand our YHP country programme. This is designed to help young people in need around the world deal with the health issues they face so they can improve their chances of living a better life. We currently have 15 country programmes under way around the world.

Through YHP, we have reached over 250,000 young people in communities across five continents with health information. Over 3,000 of these young people have been trained to share this health information with their peers and with the community, and over 2,700 frontline health providers have completed training programmes in adolescent health. We are on track to meet our Clinton Global Initiative commitment to reach 500,000 young people by the end of 2015. Initial findings from the Wellbeing of Adolescents in Vulnerable Environments study being undertaken by Johns Hopkins Bloomberg School of Public Health as part of YHP were presented at the World Health Summit in Berlin, Germany in October. As part of our best practice sharing, our dedicated online resource (younghealthprogrammeYHP.com) enables those working with young people to access information and resources created by the YHP partners.

Our support for science education takes a number of forms. For example, in 2011, we entered a three year partnership with Career Academies UK to support increased participation by 16 to 19-year-olds in Science, Technology, Engineering and Maths (STEM) subjects, with a target that one-third of Career Academies have a STEM theme by the 2014/15 academic year. By the 2012/13 academic year, the proportion was almost one-quarter, representing 48 Career Academies. Our work with Career Academies UK complements the involvement we have had since 2003 with the STEM ambassador programme.

 

Extract from 2012 Responsible Business Plan.

 

   Further information on AstraZeneca’s approach to responsible business can be found above and on our website, astrazeneca.com/responsibility.

 

* Figures re-stated to correct product donation data capture error in 2011.

 

 

LOGO

 

AstraZeneca Annual Report and Form 20-F Information 2012   49