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1A. RISK FACTORS
An
investment in our securities is highly speculative and involves a high degree of
risk. Therefore, in evaluating us and our business you should carefully consider
the risks set forth below, which are only a few of the risks associated with
investing in our common stock. You should be in a position to risk the loss of
your entire investment.
RISKS RELATING TO OUR
BUSINESS
We are a
development stage company. We currently have no product revenues and will need
to raise additional capital to operate our business.
We are a
development stage company that has experienced significant losses since
inception and has a significant accumulated deficit. We expect to incur
additional operating losses in the future and expect our cumulative losses to
increase. To date, we have generated no product revenues. As of June 30, 2008,
we have expended approximately $21.4 million on a consolidated basis acquiring
and developing our current product candidates. Until such time as we receive
approval from the FDA and other regulatory authorities for our product
candidates, we will not be permitted to sell our drugs and will not have product
revenues. Therefore, for the foreseeable future we will have to fund all of our
operations and capital expenditures from equity and debt offerings, cash on
hand, licensing fees, and grants. We will need to seek additional sources of
financing and such additional financing may not be available on favorable terms,
if at all. If we do not succeed in raising additional funds on acceptable terms,
we may be unable to complete planned pre-clinical and clinical trials or obtain
approval of our product candidates from the FDA and other regulatory
authorities. In addition, we could be forced to discontinue product development,
reduce or forego sales and marketing efforts, and forego attractive business
opportunities. Any additional sources of financing will likely involve the
issuance of our equity or debt securities, which will have a dilutive effect on
our stockholders.
We
are not currently profitable and may never become profitable.
We have a
history of losses and expect to incur substantial losses and negative operating
cash flow for the foreseeable future. Even if we succeed in developing and
commercializing one or more of our product candidates, we expect to incur
substantial losses for the foreseeable future and may never become profitable.
We also expect to continue to incur significant operating and capital
expenditures and anticipate that our expenses will increase substantially in the
foreseeable future as we do the following:
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continue
to undertake pre-clinical development and clinical trials for our product
candidates;
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seek
regulatory approvals for our product candidates;
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implement
additional internal systems and infrastructure;
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lease
additional or alternative office facilities; and
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hire
additional personnel, including members of our management
team.
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We also
expect to experience negative cash flow for the foreseeable future as we fund
our technology development with capital expenditures. As a result, we will need
to generate significant revenues in order to achieve and maintain profitability.
We may not be able to generate these revenues or achieve profitability in the
future. Our failure to achieve or maintain profitability could negatively impact
the value of our common stock and underlying securities.
We
have a limited operating history on which investors can base an investment
decision.
We
are a development-stage company and have not demonstrated our ability to perform
the functions necessary for the successful commercialization of any of our
product candidates. The successful commercialization of our product candidates
will require us to perform a variety of functions, including:
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continuing
to undertake pre-clinical development and clinical
trials;
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participating
in regulatory approval processes;
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formulating
and manufacturing products; and
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conducting
sales and marketing activities.
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Our
operations have been limited to organizing and staffing our company, acquiring,
developing, and securing our proprietary technology, and undertaking
pre-clinical trials and Phase I/II, and Phase II and Phase III clinical trials
of our principal product candidates. These operations provide a limited basis
for you to assess our ability to commercialize our product candidates and the
advisability of investing in our securities.
Our NDA for oral
TTM has not been accepted for filing and/or we may not obtain the necessary U.S.
or worldwide regulatory approvals to commercialize oral TTM or one of our
product(s).
On
November 28, 2007, we filed a New Drug Application (NDA) with the Food and Drug
Administration (FDA) seeking approval to market oral TTM (oral
tetrathiomolybdate) for initially presenting neurologic Wilson's disease. On
January 28, 2008 representing sixty (60) days from the date of NDA filing we
received notification from the FDA that our NDA has not been accepted for
further review and the FDA issued a refusal to file letter ("RTF"). In the RTF
letter the FDA cited various deficiencies in the NDA filing, including, the
formatting and presentation of the data, preliminary assessments concerning the
adequacy and quality of the clinical evidence to support the safety and efficacy
of oral TTM, the necessity to conduct a Segment III preclinical reproductive
toxicology study as well as chemistry, manufacturing and controls issues
regarding the identity, strength and purity of oral TTM. Given the receipt of
the RTF letter, we will face substantial delays in our ability to prepare and
re-file a new NDA, if at all, and potential approval to market oral
TTM.
On
February 26, 2008, we completed a Type A meeting with the FDA to discuss the
deficiencies raised in the RTF letter. Based on this meeting with the FDA, Pipex
believes it reached an understanding with the FDA on a course of action to
resolve all of the filing issues raised in the RTF letter. Nevertheless, the FDA
raised concerns regarding the adequacy of the evidence of clinical efficacy,
safety, study quality, data collection and overall risk/benefit profile of oral
TTM for neurologic Wilson's disease as represented by the two completed clinical
trials of oral TTM for neurologic Wilson's disease that formed the basis of the
NDA. Even if Pipex is successful in preparing and filing a revised NDA, Pipex
cannot provide any assurances that a newly filed NDA will be accepted for filing
or that upon review of the NDA by the FDA, Pipex will be successful in
overcoming such FDA concerns and that oral TTM for initially presenting
neurologic Wilson's disease will be approved by the FDA. The clinical trials for
oral TTM which formed the basis of the NDA filing were conducted over a period
of 18 years from 1998 to 2005 prior to entering into our license agreement for
oral TTM and were conducted under an investigator initiated IND by our
scientific advisor and consultant, Dr. George Brewer under grant support from
various non-profit foundations and governmental agencies including the FDA’s
Orphan Products Group. In the event that we are able to prepare, file and obtain
FDA acceptance of a new NDA filing for oral TTM, we cannot provide any
assurances that after the FDA reviews our new submission, that the new NDA
submission will overcome the FDA's concerns raised in the RTF letter sufficient
for approval of oral TTM or that the FDA will not upon further review raise
additional concerns regarding manufacturing, clinical, or nonclinical which may
impact the potential approvability of oral TTM for the treatment of neurologic
Wilson’s disease.
We are
seeking potential business development corporate partners and potential
licensees that may support the further development of oral TTM for Wilson's
disease and other indications. In order to consider an enhanced resubmitted
NDA filing for oral TTM for the treatment of neurologic Wilson’s disease, at the
February 26, 2008 Type A meeting Pipex discussed with the FDA Pipex may intend
to schedule a Type B meeting with the FDA with potential corporate
partners, if any, in attendance to discuss the utility of providing the FDA with
additional efficacy data from an ongoing double-blind, comparator, dose
optimization clinical trial of oral TTM for the treatment of neurologic Wilson’s
disease. To date, this third study has enrolled and completed dosing in
approximately 40 neurologically presenting Wilson’s disease patients should
a Type B meeting be requested by Pipex and be scheduled, Pipex may
intend to present potential, available pharmacokinetic and pharmacodynamic
data (such as and including oral TTM's effects on lowering serum free copper
levels in patients) from this third clinical trial as well as a summarization of
the data from the previously completed clinical trials with oral TTM for
neurologic Wilson’s disease. The feedback from this Type B meeting with the FDA
will determine the timing of any potential NDA resubmission for oral TTM for
this indication and may result in Pipex discontinuing the NDA refiling process
for oral TTM as well as potentially our planned MAA filing in Europe.
Additionally, depending on the analysis of additional data, the FDA may request
a separate pharmacokinetic study or additional clinical studies.
On March
17, 2008, Dr. George Brewer informed us that pursuant to a teleconference
between Dr. Brewer and the FDA of the same date, Dr. Brewer's physician
sponsored investigational new drug application (IND) for oral tetrathiomolybdate
for Wilson's disease had been placed on clinical hold pending the potential
resolution, if any, of items described in the RTF. The IND that is
the subject of the clinical hold includes an active dose optimization comparator
protocol of oral tetrathiomolybdate that to date has enrolled and treated
approximately 40 neurologically presenting Wilson's disease patients the data
from which we intend to collect, analyze and present to the FDA at a Type B
meeting to be requested to discuss a potential revised New Drug Application
submission. We cannot provide any assurance that Dr. Brewer will be successful
in lifting the clinical hold imposed by the FDA, that we will be successful in
preparing and filing a revised NDA, that any such newly filed NDA will be
accepted for filing or that upon review of any such NDA by the FDA, we will be
successful in overcoming the concerns raised by the FDA and that oral
tetrathiomolybdate for initially presenting neurologic Wilson's disease will be
approved by the FDA. Based upon receipt of a written clinical hold letter
communicated to Dr. Brewer from the FDA and forwarded to us on March 26, 2008,
the FDA detailed its issues and concerns that are required to be addressed in
order to lift the clinical hold, including chemistry, manufacturing and control
(CMC) issues concerning the identity, strength and purity of oral TTM. We
presently intend to assist Dr. Brewer in resolving the CMC issues raised by the
FDA and do not presently intend to initiate patient dosing in our Italian
clinical trial of oral TTM for Alzheimer's disease until such issues are
resolved to the satisfaction of the FDA. We cannot provide any assurance that we
will be successful in overcoming such CMC issues to the satisfaction of the FDA.
Our license agreement with the University of Michigan required that we initiate
patient dosing for an additional clinical trial of oral TTM on or before August
5, 2008. Given our determination to withhold patient dosing of our
Italian Alzheimer's disease trial until the CMC issues raised by the FDA
are satisfied, we are currently renegotiating this provision of the license
agreement with the University of Michigan. We cannot assure you that our
negotiations will be successful. The written clinical hold letter also
provided feedback not related to the clinical hold per se including the
reference that the clinical endpoints, design and conduct of the dose comparator
clinical study that has enrolled 40 patients to date will most likely not be
sufficient for a NDA of oral TTM for neurologic Wilson's disease. Based on this
communication, Pipex may request a Type B meeting with the FDA with potential
corporate partners, if any, in attendance to discuss next steps for oral TTM
development in neurologic Wilson's disease. Given the issues raised by the FDA
in its RTF letter of January 28, 2008 as well as the FDA's written clinical hold
letter to Dr. George Brewer forwarded to us on March 26, 2008, at the present
time it appears that the FDA will not deem the three existing clinical trials of
oral TTM to be sufficient for a New Drug Application of oral TTM for initially
presenting neurologic Wilson's disease. Given the limited number of patients
afflicted by this disease, an additional clinical trial of oral TTM for this
indication will necessarily take a substantial amount of time and resources to
plan, enroll and complete. The design of such further study is also uncertain
given that existing drugs approved for Wilson's disease appear to be
contraindicated for initially presenting neurologic Wilson's disease or too slow
acting for this critically ill patient population. Should we elect to abandon
our efforts to seek U.S. and/or European approval of oral TTM for neurologically
presenting Wilson's disease we will most likely not have sufficient resources to
pursue all of the additional indications for oral TTM that are the subject of
our research and development, including, idiopathic pulmonary fibrosis,
Alzheimer's disease, primary biliary cirrhosis and Huntington's disease. If we
are are unable to identify interested corporate partners for oral TTM, we may
elect to abandon our efforts to develop oral TTM for any or all of these
indications, including, Wilson's disease.
We will
need FDA approval to commercialize our product candidates in the U.S. and
approvals from equivalent regulatory authorities in foreign jurisdictions to
commercialize our product candidates in those jurisdictions. In order to obtain
FDA approval for any of our product candidates, we must submit to the
FDA an NDA, demonstrating that the product candidate is safe for humans and
effective for its intended use and that the product candidate can be
consistently manufactured and is stable. This demonstration requires significant
research and animal tests, which are referred to as “pre-clinical studies,”
human tests, which are referred to as “clinical trials” as well as the ability
to manufacture the product candidate, referred to as “chemistry
manufacturing control” or “CMC.” We will also need to file additional
investigative new drug applications and protocols in order to initiate clinical
testing of our drug candidates in new therapeutic indications and delays in
obtaining required FDA and institutional review board approvals
to commence such studies may delay our initiation of such planned
additional studies.
Satisfying
the FDA’s regulatory requirements typically takes many years, depending on the
type, complexity, and novelty of the product candidate, and requires substantial
resources for research development, and testing. We cannot predict whether our
research and clinical approaches will result in drugs that the FDA considers
safe for humans and effective for indicated uses. The FDA has substantial
discretion in the drug approval process and may require us to conduct additional
pre-clinical and clinical testing or to perform post-marketing
studies.
The
approval process may also be delayed by changes in government regulation, future
legislation or administrative action, or changes in FDA policy that occur prior
to or during our regulatory review. Delays in obtaining regulatory approvals may
do the following:
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delay
commercialization of, and our ability to derive product revenues from, our
product candidates;
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impose
costly procedures on us; and
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diminish
any competitive advantages that we may otherwise
enjoy.
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Even if
we comply with all FDA requests, the FDA may ultimately reject one or more of
our NDAs. We cannot be sure that we will ever obtain regulatory clearance for
our product candidates. Failure to obtain FDA approval of any of our product
candidates will severely undermine our business by reducing our number of
salable products and, therefore, corresponding product revenues.
In
foreign jurisdictions, we must receive approval from the appropriate regulatory
authorities before we can commercialize our drugs. Foreign regulatory approval
processes generally include all of the risks associated with the FDA approval
procedures described above. We cannot assure you that we will receive the
approvals necessary to commercialize our product candidate for sale outside the
United States.
We may not be
able to retain rights licensed to us by others to commercialize key products and
may not be able to establish or maintain the relationships we need to develop,
manufacture, and market our products.
In
addition to our own patent applications, we also currently rely on an exclusive
worldwide license agreement with the University of Michigan relating to various
uses of oral TTM. We also have an exclusive license agreement with the McLean
Hospital relating to the use of EFFIRMA to treat fibromyalgia
syndrome; an exclusive license agreement with Thomas Jefferson University
relating to our CD4 inhibitor program; an exclusive license agreement
with the Regents of the University of California relating to our TRIMESTA
technology; an exclusive license agreement with the Children’s
Hospital-Boston relating to our CORRECTA technology; an exclusive license
agreement to license our T-cell vaccine program from the University
of Southern California (USC) an exclusive license to our oral immunotherapeutic
tolerance program from UCSD and an exclusive license agreement with Dr. Newsome
and Mr. Tate relating to our Zinthionein program. Each of these agreements
requires us to use our best efforts to commercialize each of the technologies as
well as meet certain diligence requirements and timelines in order to keep the
license agreement in effect. In the event we are not able to meet our diligence
requirements, we may not be able to retain the rights granted under our
agreements or renegotiate our arrangement with these institutions on reasonable
terms, or at all.
Furthermore,
we currently have very limited product development capabilities, and limited
marketing or sales capabilities. For us to research, develop, and test our
product candidates, we would need to contract with outside researchers, in most
cases those parties that did the original research and from whom we have
licensed the technologies.
We
can give no assurances that any of our issued patents licensed to us or any of
our other patent applications will provide us with significant proprietary
protection or be of commercial benefit to us. Furthermore, the issuance of a
patent is not conclusive as to its validity or enforceability, nor does the
issuance of a patent provide the patent holder with freedom to operate without
infringing the patent rights of others.
Developments by
competitors may render our products or technologies obsolete or
non-competitive.
Companies that currently sell or
are developing both generic and proprietary pharmaceutical compounds to treat
central-nervous-system and autoimmune diseases include: Pfizer, Inc., Aton
Pharma, GlaxoSmithKline Pharmaceuticals, Alcon, Inc., Shire Pharmaceuticals,
Plc., Schering-Plough, Organon NV, Merck & Co., Eli Lilly &
Co., Serono, SA, Biogen Idec, Inc., Achillion, Ltd., Active Biotech, Inc.,
Panteri Biosciences, Meda, Merrimack Pharmaceuticals, Inc., Schering
AG, Forest Laboratories, Inc., Attenuon, LLC, Cypress Biosciences, Inc.,
Novartis, Axcan Pharma, Inc., Teva Pharmaceuticals, Inc., Intermune,
Inc. Fibrogen, Inc., Active Biotech, CNSBio, Pty., Rare Disease
Therapeutics, Inc., Prana Biotechnology, Inc., Merz & Co., AstraZeneca
Pharmaceuticals, Inc., Chiesi Pharmaceuticals, Inc., Alcon, Inc.,
Bausch and Lomb, Inc., Targacept, Inc., and Johnson & Johnson, Inc.
Alternative technologies or alternative delivery or dosages of already approved
therapies are being developed to treat dry AMD, autoimmune
inflammatory, Fibromyalgia, MS, Huntington’s, Alzheimer’s and Wilson’s diseases,
several of which may be approved or are in early and advanced
clinical trials, such as zinc based combinations, FTY-720, Laquinimod,
pirfenidone, milnacipram, Lyrica, anti-depressant combinations, Cymbalta,
Effexor, Actimmune and other interferon preparations. Unlike us, many of our
competitors have significant financial and human resources. In addition,
academic research centers may develop technologies that compete with our
TRIMESTA, Zinthionein, CD4 inhibitors, EFFIRMA, CORRECTA and oral TTM
technologies. Should clinicians or regulatory authorities view these therapeutic
regiments as or more effective than our products, this might delay or prevent us
from obtaining regulatory approval for our products, or it might prevent us from
obtaining favorable reimbursement rates from payers, such as Medicare, Medicaid
and private insurers.
We may not
succeed in enforcing our orphan drug designations.
Oral
TTM has been designated by the FDA as an “orphan drug” for the treatment of
Wilson’s disease patients presenting with neurologic complications. CORRECTA
TM
has also been designated by the FDA as an “orphan drug” for the treatment of
pouchitis patients. We intend to file for “orphan drug” designations in the EMEA
(the European equivalent of the FDA) for both oral TTM and CORRECTA
TM
for
similar uses. Pursuant to our agreements with our scientific inventors and
universities, we have acquired these designations. Orphan drug designation is an
important element of our competitive strategy because there are no composition
of matter patents for oral TTM a designated orphan drug for a rare disease
generally receives marketing exclusivity for use of that drug for the designated
condition for a period of seven years in the United States and ten years in the
European Union.
To be
successful in enforcing this designation, our new drug application would need to
be the first NDA approved to use oral TTM to treat Wilson’s disease. While we
are not aware of any other companies that have sought orphan drug designation
for oral TTM or its active ingredient, tetrathiomolybdate, for this indication,
other companies may in the future seek it and may obtain FDA marketing approval
before we do. In addition, the FDA may permit other companies to market a form
of tetrathiomolybdate to treat Wilson’s disease patients with neurologic
complication if their product demonstrates clinical superiority. This could
create a more competitive market for us.
Competitors could
develop and gain FDA approval of our products for a different
indication.
Since we
do not have composition of matter patent claims for oral TTM, EFFIRMA, Solovax
and TRIMESTA, others may obtain approvals for other uses of these products which
are not covered by our issued or pending patents. For example, the active
ingredients in both EFFIRMA and TRIMESTA have been approved for marketing in
overseas countries for different uses. Other companies, including the original
developers or affiliates of these products may seek to develop EFFIRMA or
TRIMESTA for these uses in the US or any country we are seeking approval for. We
cannot provide any assurances that any other company may obtain FDA approval for
products that contain EFFIRMA or TRIMESTA in various formulations or delivery
systems that might adversely affect our ability to develop and market these
products in the US. Should a competitor obtain FDA approval for their
product prior to us, we might be precluded under the Waxman-Hatch Act to obtain
approval for our product candidates for a period of five years.
Other
companies could manufacture and develop oral TTM and its active ingredient,
tetrathiomolybdate, and secure approvals for different indications. We are aware
that a potential competitor has an exclusive license from the University of
Michigan (UM) to an issued U.S. patent that relates to the use of
tetrathiomolybdate to treat angiogenic diseases (the “Angiogenic
Patent”) and is currently in phase I and phase II clinical trials for the
treatment of various forms of cancer. To our knowledge, this competitor and UM
have filed additional patent applications claiming various analog structures and
formulations of tetrathiomolybdate to treat various diseases. Further, we cannot
predict whether our competitor might obtain approval in the U.S. or Europe to
market tetrathiomolybdate for cancer or another indication ahead of us. We also
cannot predict whether, if issued, any patent corresponding to the Angiogenic
Patent may prevent us from conducting our business or result in lengthy and
costly litigation or the need for a license. Furthermore, if we need to obtain a
license to these or other patents in order to conduct our business, we may find
that it is not available to us on commercially reasonable terms, or
is not available to us at all.
If
the FDA approves other tetrathiomolybdate products to treat indications other
than those covered by our issued or pending patent applications, physicians may
elect to prescribe a competitor’s tetrathiomolybdate to treat Wilson’s
disease—this is commonly referred to as “off-label” use. While under FDA
regulations a competitor is not allowed to promote off-label uses of its
product, the FDA does not regulate the practice of medicine and, as a result,
cannot direct physicians as to which source it should use for the
tetrathiomolybdate they prescribe to their patients. Consequently, we might be
limited in our ability to prevent off-label use of a competitor’s
tetrathiomolybdate to treat Wilson’s disease or inflammatory or fibrotic
disease, even if we have orphan drug exclusivity. Our competitor might seek FDA
or EMEA approval to market tetrathiomolybdate for any therapeutic indication,
including Wilson’s disease or idiopathic pulmonary fibrosis (IPF). If we are not
able to obtain and enforce these patents, a competitor could use
tetrathiomolybdate for a treatment or use not covered by any of our
patents.
We
rely primarily on method patents and patent applications and various regulatory
exclusivities to protect the development of our technologies, and our ability to
compete may decrease or be eliminated if we are not able to protect our
proprietary technology.
Our
competitiveness may be adversely affected if we are unable to protect our
proprietary technologies. Other than our CD4 inhibitor, oral tolerance and
Zinthionein program, we do not have composition of matter patents for TRIMESTA,
EFFIRMA, CORRECTA, Solovax, oral TTM or their respective active ingredients
estriol, flupirtine, clotrimazole and tetrathiomolybdate. We also
expect to rely on patent protection from an issued U.S. Patent for the use of
oral TTM and related compounds to treat inflammatory and fibrotic diseases (U.S.
Patent No 6,855,340). These patents have been exclusively licensed to us. We
have also filed various pending patent applications which cover various
formulations, packaging, distribution & monitoring methods for oral TTM. We
rely on issued patent and pending patent applications for use of TRIMESTA to
treat MS (issued U.S. Patent No. 6,936,599) and various other therapeutic
indications which have been exclusively licensed to us. We have also exclusively
licensed an issued patent for the treatment of fibromyalgia with EFFIRMA
TM
and
have pending patent applications for our uses of CORRECTA.
Our
Zinthionein product candidate is exclusively licensed from its inventors, David
A. Newsome, M.D. and David Tate, Jr. Zinthionein is the subject of
two issued U.S. patents, 7,164,035 and 6,586,611 and pending U.S. patent
application ser. no. 11/621,380 which cover composition of matter
claims.
In
our annual Form 10-KSB for the year ending December 31, 2007 filed March 31,
2008 (page 23), we described our receipt in March 2008 (and potential impact on
claim 1 of our exclusively licensed issued U.S. patent 7,164,035) of an English
translation of a Russian disclosure, Zegzhda et. al. Chemical Abstracts Vol. 85
Abstract No. 186052 (1976) that was cited by the U.S. patent examiner during our
prosecution of the pending divisional U.S. patent application Ser. No.
11/621,390. In April 2008, we analyzed the zinc-cysteine complex described by
Zegzhda and concluded that such complex describes an insoluble zinc salt
and does not describe a non-zinc salt zinc monocyteine complex and
therefore believe that such disclosure should not affect the validity of any of
our issued U.S. patent claims relating our zinc-monocysteine
composition-of-matter claims. We have filed a response and
declaration describing the results of our analysis with the U.S. Patent and
Trademark Office with respect to the Zegzhda reference with respect to U.S.
patent application ser. no. 11/621,380.
We also
expect to rely on regulatory exclusivities, such as the Orphan Drug Designation
with the FDA and EMEA (“Orphan Drug”) to protect oral TTM, CORRECTA
TM
and our other future products for certain therapeutic indications. Orphan Drug
protection provides for seven years of marketing exclusivity for that disease
indication in the U.S. and ten years of marketing exclusivity for that disease
indication in Europe. We have received an Orphan Drug Designation for the use of
CORRECTA to treat pouchitis as well as an Orphan Drug Designation for the use of
oral TTM to treat neurologically presenting Wilson’s disease and are in the
process of filing similar designations in Europe. Orphan Drug Designation is an
important element of our competitive strategy for oral TTM and CORRECTA. To be
successful in enforcing this designation, our NDA would need to be the first NDA
approved to use oral TTM and CORRECTA for that indication. While we are not
aware of any other companies that have sought orphan drug designation for oral
TTM and CORRECTA for any indication, other companies may in the future seek it
and may obtain FDA marketing approval before we do.
After
the Orphan Drug exclusivity period expires, assuming our patents are validly
issued, we still expect to rely on our issued and pending method of use patent
applications to protect our proprietary technology with respect to the
development of oral TTM and CORRECTA. The patent positions of pharmaceutical
companies are uncertain and may involve complex legal and factual questions. We
may incur significant expense in protecting our intellectual property and
defending or assessing claims with respect to intellectual property owned by
others. Any patent or other infringement litigation by or against us could cause
us to incur significant expense and divert the attention of our
management.
We may
also rely on the United States Drug Price Competition and Patent Term
Restoration Act, commonly known as the “Hatch-Waxman Amendments,” to protect
some of our current product candidates, specifically oral TTM, TRIMESTA,
zincmonocystine, Anti-CD4 802-2, EFFIRMA and other future product candidates we
may develop. Once a drug containing a new molecule is approved by the FDA, the
FDA cannot accept an abbreviated NDA for a generic drug containing that molecule
for five years, although the FDA may accept and approve a drug containing the
molecule pursuant to an NDA supported by independent clinical data. Recent
amendments have been proposed that would narrow the scope of Hatch-Waxman
exclusivity and permit generic drugs to compete with our drug.
In July
2007 our exclusively licensed European patent covering our multivalent T-cell
vaccine, Solovax, was opposed and revoked. In order to save resources, we have
elected not to appeal such ruling and may elect to abandon the license with
USC.
Others
may file patent applications or obtain patents on similar technologies or
compounds that compete with our products. We cannot predict how broad the claims
in any such patents or applications will be, and whether they will be allowed.
Once claims have been issued, we cannot predict how they will be construed or
enforced. We may infringe intellectual property rights of others without being
aware of it. If another party claims we are infringing their technology, we
could have to defend an expensive and time consuming lawsuit, pay a large sum if
we are found to be infringing, or be prohibited from selling or licensing our
products unless we obtain a license or redesign our product, which may not be
possible.
We
also rely on trade secrets and proprietary know-how to develop and maintain our
competitive position. Some of our current or former employees, consultants, or
scientific advisors, or current or prospective corporate collaborators, may
unintentionally or willfully disclose our confidential information to
competitors or use our proprietary technology for their own benefit.
Furthermore, enforcing a claim alleging the infringement of our trade secrets
would be expensive and difficult to prove, making the outcome uncertain. Our
competitors may also independently develop similar knowledge, methods, and
know-how or gain access to our proprietary information through some other
means.
We may fail to
retain or recruit necessary personnel, and we may be unable to secure the
services of consultants.
As
of July 29, 2008, we have 8 full-time employees. We have also engaged regulatory
consultants to advise us on our dealings with the FDA and other foreign
regulatory authorities. We intend to recruit certain key executive officers,
including a Chief Financial Officer and Vice President of Regulatory Affairs
during 2008. Our future performance will depend in part on our ability to
successfully integrate newly hired executive officers into our management team
and our ability to develop an effective working relationship among senior
management.
Certain
of our officers, directors, (including Jeffrey Kraws, a director and former VP
of Business Development, Jeffrey Wolf, a director and Dr. Kuo, a director)
scientific advisors, and consultants serve as officers, directors, scientific
advisors, or consultants of other biopharmaceutical or biotechnology companies
which might be developing competitive products to ours. None of our directors or
officers is obligated under any agreement or understanding with us to make any
additional products or technologies available to us. Similarly, we can give no
assurances, and we do not expect and stockholders should not expect, that any
biomedical or pharmaceutical product or technology identified by any of our
directors or affiliates in the future would be made available to
us.
We
can expect this to also be the case with personnel that we engage in the future.
We can give no assurances that any such other companies will not have interests
that are in conflict with our interests.
Losing
key personnel or failing to recruit necessary additional personnel would impede
our ability to attain our development objectives. There is intense competition
for qualified personnel in the drug-development field, and we may not be able to
attract and retain the qualified personnel we would need to develop our
business.
We
rely on independent organizations, advisors, and consultants to perform certain
services for us, including handling substantially all aspects of regulatory
approval, clinical management, manufacturing, marketing, and sales. We expect
that this will continue to be the case. Such services may not always be
available to us on a timely basis when we need them.
We
may experience difficulties in obtaining sufficient quantities of our products
or other compounds.
In
order to successfully commercialize our product candidates, we must be able to
manufacture our products in commercial quantities, in compliance with regulatory
requirements, at acceptable costs, and in a timely manner. Manufacture of the
types of biopharmaceutical products that we propose to develop present various
risks. For example, manufacture of the active ingredient in oral TTM and
Zinthionein is a complex process that can be difficult to scale up for purposes
of producing large quantities. This process can also be subject to delays,
inefficiencies, and poor or low yields of quality products. Furthermore, the
active ingredient of Zinthionein has been difficult to scale up at larger
quantities. As such, we can give no assurances that we will be able
to scale up the manufacturing of Zinthionein. Oral TTM is also known
to be subject to a loss of potency as a result of prolonged exposure to moisture
and other normal atmospheric conditions. We are developing proprietary
formulations and specialty packaging solutions to overcome this stability issue,
but we can give no assurances that we will be successful in meeting the
stability requirements required for approval by regulatory authorities such as
the FDA or the requirements that our new proprietary formulations and drug
product will demonstrate satisfactory comparability to less stable formulations
utilized in prior clinical trials. We may experience delays in demonstrating
satisfactory stability requirements and drug product comparability requirements
that could delay acceptance or approval of our planned NDA for oral
TTM.
For manufacturing and nonclinical information, we rely upon an
agreement with Organon, a division of Schering-Plough for access to clinical,
nonclinical, stability and drug supply relating to estriol, the active
ingredient in TRIMESTA which is currently in a phase II/III clinical trial for
MS. Should Organon terminate our agreement, this might delay enrollment and
commercialization plans for our TRIMESTA clinical trial program. Organon has
manufactured estriol for the European and Asian market for approximately 40
years.
Our
SOLOVAX T-cell vaccine technology is complex to manufacture. The vaccine is
manufactured through the procurement of a patient’s own T-cells derived from the
patient’s plasma. This manufacturing process involves incubation of T-cells,
irradiation and refrigeration of the cells. We plan to develop a revised
manufacturing procedure which will streamline quality control of the
vaccine.
Historically,
our manufacturing has been handled by contract manufacturers and compounding
pharmacies. We can give no assurances that we will be able to continue to use
our current manufacturer or be able to establish another relationship with a
manufacturer quickly enough so as not to disrupt commercialization of any of our
products, or that commercial quantities of any of our products, if approved for
marketing, will be available from contract manufacturers at acceptable
costs.
In
addition, any contract manufacturer that we select to manufacture our product
candidates might fail to maintain a
current “good
manufacturing practices” (cGMP) manufacturing facility. During February 2007, we
established a commercial manufacturing facility for oral
TTM product in Ann Arbor, MI and we have hired and trained our
employees to comply with the extensive regulations applicable to such a
facility. Upon FDA inspection our facility and/or cGMP procedures may require
changes that could delay our intended product launch of oral TTM and other
products that might develop.
The cost
of manufacturing certain product candidates may make them prohibitively
expensive. In order to successfully commercialize our product candidates we may
be required to reduce the costs of production, and we may find that we are
unable to do so. We may be unable to obtain, or may be required to pay high
prices for compounds manufactured or sold by others that we need for comparison
purposes in clinical trials and studies for our product candidates.
Clinical trials
are very expensive, time-consuming, and difficult to design and
implement.
Human
clinical trials are very expensive and difficult to design and implement, in
part because they are subject to rigorous regulatory requirements. The clinical
trial process is also time-consuming. We estimate that clinical trials of our
product candidates would take at least several years to complete. Furthermore,
failure can occur at any stage of the trials, and we could encounter problems
that cause us to abandon or repeat clinical trials. Commencement and completion
of clinical trials may be delayed by several factors,
including:
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unforeseen
safety issues;
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determination
of dosing;
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lack
of effectiveness during clinical trials;
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slower
than expected rates of patient recruitment;
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inability
to monitor patients adequately during or after treatment;
and
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inability
or unwillingness of medical investigators to follow our clinical
protocols.
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In
addition, we or the FDA may suspend our clinical trials at any time if it
appears that we are exposing participants to unacceptable health risks or if the
FDA finds deficiencies in our submissions or conduct of our trials.
The results of
our clinical trials may not support our product candidate
claims.
Even
if our clinical trials are completed as planned, we cannot be certain that the
results will support our product-candidate claims. Success in pre-clinical
testing and phase II clinical trials does not ensure that later phase II or
phase III clinical trials will be successful. We cannot be sure that the results
of later clinical trials would replicate the results of prior clinical trials
and pre-clinical testing. Clinical trials may fail to demonstrate that our
product candidates are safe for humans and effective for indicated uses. Any
such failure could cause us to abandon a product candidate and might delay
development of other product candidates. Any delay in, or termination of, our
clinical trials would delay our obtaining FDA approval for the affected product
candidate and, ultimately, our ability to commercialize that product
candidate.
Physicians and
patients may not accept and use our technologies.
Even
if the FDA approves our product candidates, physicians and patients may not
accept and use them. Acceptance and use of our product will depend upon a number
of factors, including the following:
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the
perception of members of the health care community, including physicians,
regarding the safety and effectiveness of our drugs;
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the
cost-effectiveness of our product relative to competing
products;
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availability
of reimbursement for our products from government or other healthcare
payers; and
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the
effectiveness of marketing and distribution efforts by us and our
licensees and distributors, if any.
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Because
we expect sales of our current product candidates, if approved, to generate
substantially all of our product revenues for the foreseeable future, the
failure of any of these drugs to find market acceptance would harm our business
and could require us to seek additional financing.
We depend on
researchers who are not under our control.
Since we
have in-licensed all of our product candidates, we depend upon independent
investigators and scientific collaborators, such as universities and medical
institutions or private physician scientists, to conduct our pre-clinical and
clinical trials under agreements with us. These collaborators are not our
employees and we cannot control the amount or timing of resources that they
devote to our programs or the timing of their procurement of clinical-trial
data. They may not assign as great a priority to our programs or pursue them as
diligently as we would if we were undertaking those programs ourselves. Failing
to devote sufficient time and resources to our drug-development programs, or
substandard performance, could result in delay of any FDA applications and our
commercialization of the drug candidate involved.
Our
oral TTM program is highly dependent on Dr. George Brewer, Professor Emeritus at
the University of Michigan. Dr. Brewer was the principal investigator and
conducted the clinical trials over an 18 year period on the oral TTM clinical
trials which formed the basis of our NDA filing. We have retained Dr. Brewer,
age 76 as an advisor and consultant to Pipex. In the event of Dr. Brewer’s
untimely death or disability, may significantly hamper our development
capabilities of oral TTM.
These
collaborators may also have relationships with other commercial entities, some
of which may compete with us. Our collaborators assisting our competitors at our
expense could harm our competitive position. For example, we depend on
scientific collaborators for our TRIMESTA, Zinthionein, SOLOVAX, CORRECTA, CD4
Inhibitor, EFFIRMA oral tolerance and oral TTM development programs.
Specifically, all of the clinical trials have been conducted under
physician-sponsored investigational new drug applications (INDs), not
corporate-sponsored INDs. Additionally, the clinical trials for oral TTM for the
treatment of neurologic Wilson’s disease have been conducted and completed prior
to us licensing this technology from the University of Michigan. Due to various
patient privacy regulations and other administrative matters, we have
experienced delays and/or an inability to obtain clinical trial data relating to
oral TTM. As such, this delay or inability to obtain any data might result
our inability to obtain regulatory approvals for oral TTM and our products. We
are also dependent on government and private grants to fund certain of our
clinical trials for our product candidates. For example, TRIMESTA has received a
$5 million grant from the Southern Chapter of the National Multiple Sclerosis
Society which funds a majority of our ongoing phase II/III clinical trial in
relapsing remitting multiple sclerosis. If we are unable to maintain
these grants, we might be forced to scale back development of these product
candidates. We have experienced difficulty in collecting the data or
transferring these programs to corporate-sponsored INDs. Additionally, we are
aware that all of our scientific collaborators may also act as advisors to our
competitors.
We have no
experience selling, marketing, or distributing products and do not have the
capability to do so.
We
currently have no sales, marketing, or distribution capabilities. We do not
anticipate having resources in the foreseeable future to allocate to selling and
marketing our proposed products. Our success will depend, in part, on whether we
are able to enter into and maintain collaborative relationships with a
pharmaceutical or a biotechnology company charged with marketing one or more of
our products. We may not be able to establish or maintain such collaborative
arrangements or to commercialize our products in foreign territories, and even
if we do, our collaborators may not have effective sales forces.
If we do not, or are unable to,
enter into collaborative arrangements to sell and market our proposed products,
we will need to devote significant capital, management resources, and time to
establishing and developing an in-house marketing and sales force with technical
expertise. We may be unsuccessful in doing so.
If we fail to
maintain positive relationships with particular individuals, we may be unable to
successfully develop our product candidates, conduct clinical trials, and obtain
financing.
If
we fail to maintain positive relationships with members of our management team
or if these individuals decrease their contributions to our company, our
business could be adversely impacted. We do not carry key employee insurance
policies for any of our key employees.
We
also rely greatly on employing and retaining other highly trained and
experienced senior management and scientific personnel. The competition for
these and other qualified personnel in the biotechnology field is intense. If we
are not able to attract and retain qualified scientific, technical, and
managerial personnel, we probably will be unable to achieve our business
objectives.
We may not be
able to compete successfully for market share against other drug
companies.
The
markets for our product candidates are characterized by intense competition and
rapid technological advances. If our product candidates receive FDA approval,
they will compete with existing and future drugs and therapies developed,
manufactured, and marketed by others. Competing products may provide greater
therapeutic convenience or clinical or other benefits for a specific indication
than our products, or may offer comparable performance at a lower cost. If our
products fail to capture and maintain market share, we may not achieve
sufficient product revenues and our business will suffer.
We will
compete against fully integrated pharmaceutical companies and smaller companies
that are collaborating with larger pharmaceutical companies, academic
institutions, government agencies, or other public and private research
organizations. Many of these competitors have therapies to treat autoimmune
fibrotic and central nervous system diseases already approved or in development.
In addition, many of these competitors, either alone or together with their
collaborative partners, operate larger research-and-development programs than we
do, have substantially greater financial resources than we do, and have
significantly greater experience in the following areas:
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developing
drugs;
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undertaking
pre-clinical testing and human clinical trials;
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obtaining
FDA and other regulatory approvals of drugs;
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formulating
and manufacturing drugs; and
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launching,
marketing and selling drugs.
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We
may incur substantial costs as a result of litigation or other proceedings
relating to patent and other intellectual property rights, as well as costs
associated with frivolous lawsuits.
If
any other person files patent applications, or is issued patents, claiming
technology also claimed by us in pending applications, we may be required to
participate in interference proceedings in the U.S. Patent and Trademark Office
to determine priority of invention. We, or our licensors, may also need to
participate in interference proceedings involving our issued patents and pending
applications of another entity.
We
cannot guarantee that the practice of our technologies will not conflict with
the rights of others. In some foreign jurisdictions, we could become involved in
opposition proceedings, either by opposing the validity of another’s foreign
patent or by persons opposing the validity of our foreign patents.
We may also face frivolous
litigation or lawsuits from various competitors or from litigious securities
attorneys. The cost to us of any litigation or other proceeding relating to
these areas, even if resolved in our favor, could be substantial and could
distract management from our business. Uncertainties resulting from initiation
and continuation of any litigation could have a material adverse effect on our
ability to continue our operations.
If we infringe
the rights of others we could be prevented from selling products or forced to
pay damages.
If our
products, methods, processes, and other technologies are found to infringe the
proprietary rights of other parties, we could be required to pay damages, or we
may be required to cease using the technology or to license rights from the
prevailing party. Any prevailing party may be unwilling to offer us a license on
commercially acceptable terms.
Our
ability to generate product revenues will be diminished if our drugs sell for
inadequate prices or patients are unable to obtain adequate levels of
reimbursement.
Our
ability to commercialize our drugs, alone or with collaborators, will depend in
part on the extent to which reimbursement is available from government and
health administration authorities, private health maintenance organizations,
health insurers, and other healthcare payers.
Significant
uncertainty exists as to the reimbursement status of newly approved healthcare
products. Healthcare payers, including Medicare, are challenging the prices
charged for medical products and services. Government and other healthcare
payers increasingly attempt to contain healthcare costs by limiting both
coverage and the level of reimbursement for drugs. Even if our product
candidates are approved by the FDA, insurance coverage may not be available, or
may be inadequate, to cover the cost of our drugs. This could affect our ability
to commercialize our products.
We
may not be able to obtain adequate insurance coverage against product liability
claims.
Our
business exposes us to the product liability risks inherent in the testing,
manufacturing, marketing, and sale of human therapeutic technologies and
products. Even if it is available, product liability insurance for the
pharmaceutical and biotechnology industry generally is expensive. Adequate
insurance coverage may not be available at a reasonable cost.
RISKS
RELATING TO OUR STOCK
We will seek to
raise additional funds in the future, which may be dilutive to stockholders or
impose operational restrictions.
We
expect to seek to raise additional capital in the future to help fund
development of our proposed products. If we raise additional capital through the
issuance of equity or debt securities, the percentage ownership of our current
stockholders will be reduced. We may also enter into strategic transactions,
issue equity as part of license issue fees to our licensors, compensate
consultants using equity that may be dilutive. Our stockholders may experience
additional dilution in net book value per share and any additional equity
securities may have rights, preferences and privileges senior to those of the
holders of our common stock. If we cannot raise additional funds, we will have
to delay development activities of our products candidates.
We are controlled
by our current officers, directors, and principal
stockholders.
Currently,
our directors, executive officers, and principal stockholders beneficially own a
majority of our common stock. As a result, they will be able to exert
substantial influence over the election of our board of directors and the vote
on issues submitted to our stockholders.
Our
shares of common stock are from time to time thinly traded, so stockholders may
be unable to sell at or near ask prices or at all if they need to sell shares to
raise money or otherwise desire to liquidate their shares.
Our
common stock has from time to time been “thinly-traded,” meaning that the number
of persons interested in purchasing our common stock at or near ask prices at
any given time may be relatively small or non-existent. This situation is
attributable to a number of factors, including the fact that we are a small
company that is relatively unknown to stock analysts, stock brokers,
institutional investors and others in the investment community that generate or
influence sales volume, and that even if we came to the attention of such
persons, they tend to be risk-averse and would be reluctant to follow an
unproven company such as ours or purchase or recommend the purchase of our
shares until such time as we became more seasoned and viable. As a consequence,
there may be periods of several days or more when trading activity in our shares
is minimal or nonexistent, as compared to a seasoned issuer which has a
large and steady volume of trading activity that will generally support
continuous sales without an adverse effect on share price. We cannot give
stockholders any assurance that a broader or more active public trading market
for our common shares will develop or be sustained, or that current trading
levels will be sustained.
Our compliance
with the Sarbanes-Oxley Act and SEC rules concerning internal controls may be
time consuming, difficult and costly.
Although
individual members of our management team have experience as officers of
publicly traded companies, much of that experience came prior to the adoption of
the Sarbanes-Oxley Act of 2002. It may be time consuming, difficult and costly
for us to develop and implement the internal controls and reporting procedures
required by Sarbanes-Oxley. We may need to hire additional financial reporting,
internal controls and other finance staff in order to develop and implement
appropriate internal controls and reporting procedures. If we are unable to
comply with Sarbanes-Oxley’s internal controls requirements, we may not be able
to obtain the independent accountant certifications that Sarbanes-Oxley Act
requires publicly-traded companies to obtain.
We cannot assure
you that the common stock will be liquid or that it will remain listed on a
securities exchange.
We
cannot assure you that we will be able to maintain the listing standards of the
American Stock Exchange. The American Stock Exchange requires companies to meet
certain listing criteria including certain minimum stockholders' equity and
equity prices per share. We may not be able to maintain such minimum
stockholders' equity or prices per share or may be required to effect a reverse
stock split to maintain such minimum prices and/or issue additional equity
securities in exchange for cash or other assets, if available, to maintain
certain minimum stockholders' equity required by the American Stock
Exchange.
There may be
issuances of shares of preferred stock in the future.
Although
we currently do not have preferred shares outstanding, the board of directors
could authorize the issuance of a series of preferred stock that would grant
holders preferred rights to our assets upon liquidation, the right to receive
dividends before dividends would be declared to common stockholders, and the
right to the redemption of such shares, possibly together with a premium, prior
to the redemption of the common stock. To the extent that we do issue preferred
stock, the rights of holders of common stock could be impaired thereby,
including without limitation, with respect to liquidation.
We have never
paid dividends.
We
have never paid cash dividends on our common stock and do not anticipate paying
any for the foreseeable future.
RISKS
RELATED TO OUR INDUSTRY
Government
Regulation
The
FDA, comparable foreign regulators and state and local pharmacy regulators
impose substantial requirements upon clinical development, manufacture and
marketing of pharmaceutical products. These and other entities regulate research
and development and the testing, manufacture, quality control, safety,
effectiveness, labeling, storage, record keeping, approval, advertising, and
promotion of our products. The drug approval process required by the FDA under
the Food, Drug, and Cosmetic Act generally involves:
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Preclinical
laboratory and animal tests;
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Submission
of an IND, prior to commencing human clinical trials;
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Adequate
and well-controlled human clinical trials to establish safety and efficacy
for intended use;
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Submission
to the FDA of a NDA; and
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FDA
review and approval of a NDA.
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The
testing and approval process requires substantial time, effort, and financial
resources, and we cannot be certain that any approval will be granted on a
timely basis, if at all.
Preclinical
tests include laboratory evaluation of the product candidate, its chemistry,
formulation and stability, and animal studies to assess potential safety and
efficacy. Certain preclinical tests must be conducted in compliance with good
laboratory practice regulations. Violations of these regulations can, in some
cases, lead to invalidation of the studies, requiring them to be replicated. In
some cases, long-term preclinical studies are conducted concurrently with
clinical studies.
We
will submit the preclinical test results, together with manufacturing
information and analytical data, to the FDA as part of an IND, which must become
effective before we begin human clinical trials. The IND automatically becomes
effective 30 days after filing, unless the FDA raises questions about conduct of
the trials outlined in the IND and imposes a clinical hold, in which case, the
IND sponsor and FDA must resolve the matters before clinical trials can begin.
It is possible that our submission may not result in FDA authorization to
commence clinical trials.
Clinical
trials must be supervised by a qualified investigator in accordance with good
clinical practice regulations, which include informed consent requirements. An
independent Institutional Review Board (“IRB”) at each medical center reviews
and approves and monitors the study, and is periodically informed of the study’s
progress, adverse events and changes in research. Progress reports are submitted
annually to the FDA and more frequently if adverse events occur.
Human
clinical trials typically have three sequential phases that may
overlap:
Phase
I: The drug is initially tested in healthy human subjects or patients for
safety, dosage tolerance, absorption, metabolism, distribution, and
excretion.
Phase
II: The drug is studied in a limited patient population to identify possible
adverse effects and safety risks, determine efficacy for specific diseases and
establish dosage tolerance and optimal dosage.
Phase
III: When phase II evaluations demonstrate that a dosage range is effective with
an acceptable safety profile, phase III trials to further evaluate dosage,
clinical efficacy and safety, are undertaken in an expanded patient population,
often at geographically dispersed sites.
We cannot
be certain that we will successfully complete phase I, phase II, or phase III
testing of our product candidates within any specific time period, if at all.
Furthermore, the FDA, an IRB or the IND sponsor may suspend clinical trials at
any time on various grounds, including a finding that subjects or patients are
exposed to unacceptable health risk. Concurrent with these trials and studies,
we also develop chemistry and physical characteristics data and finalize a
manufacturing process in accordance with good manufacturing practice (“GMP”)
requirements. The manufacturing process must conform to consistency and quality
standards, and we must develop methods for testing the quality, purity, and
potency of the final products. Appropriate packaging is selected and tested, and
chemistry stability studies are conducted to demonstrate that the product does
not undergo unacceptable deterioration over its shelf-life. Results of the
foregoing are submitted to the FDA as part of a NDA for marketing and commercial
shipment approval. The FDA reviews each NDA submitted and may request additional
information.
Once
the FDA accepts the NDA for filing, it begins its in-depth review. The FDA has
substantial discretion in the approval process and may disagree with our
interpretation of the data submitted. The process may be significantly extended
by requests for additional information or clarification regarding information
already provided. As part of this review, the FDA may refer the application to
an appropriate advisory committee, typically a panel of clinicians.
Manufacturing establishments often are inspected prior to NDA approval to assure
compliance with GMPs and with manufacturing commitments made in the
application.
Submission
of a NDA with clinical data requires payment of a fee (for fiscal year 2008,
$1,178,500). In return, the FDA assigns a goal of ten months for issuing its
“complete response,” in which the FDA may approve or deny the NDA, or require
additional clinical data. Even if these data are submitted, the FDA may
ultimately decide the NDA does not satisfy approval criteria. If the FDA
approves the NDA, the product becomes available for physicians prescription.
Product approval may be withdrawn if regulatory compliance is not maintained or
safety problems occur. The FDA may require post-marketing studies, also known as
phase IV studies, as a condition of approval, and requires surveillance programs
to monitor approved products that have been commercialized. The agency has the
power to require changes in labeling or prohibit further marketing based on the
results of post-marketing surveillance.
Satisfaction
of these and other regulatory requirements typically takes several years, and
the actual time required may vary substantially based upon the type, complexity
and novelty of the product. Government regulation may delay or prevent marketing
of potential products for a considerable period of time and impose costly
procedures on our activities. We cannot be certain that the FDA or other
regulatory agencies will approve any of our products on a timely basis, if at
all. Success in preclinical or early-stage clinical trials does not assure
success in later-stage clinical trials. Data obtained from pre-clinical and
clinical activities are not always conclusive and may be susceptible to varying
interpretations that could delay, limit or prevent regulatory approval. Even if
a product receives regulatory approval, the approval may be significantly
limited to specific indications or uses.
Even
after regulatory approval is obtained, later discovery of previously unknown
problems with a product may result in restrictions on the product or even
complete withdrawal of the product from the market. Delays in obtaining, or
failures to obtain regulatory approvals would have a material adverse effect on
our business.
Any
products manufactured or distributed by us pursuant to FDA approvals are subject
to pervasive and continuing FDA regulation, including record-keeping
requirements, reporting of adverse experiences, submitting periodic reports,
drug sampling and distribution requirements, manufacturing or labeling changes,
record-keeping requirements, and compliance with FDA promotion and advertising
requirements. Drug manufacturers and their subcontractors are required to
register their facilities with the FDA and state agencies, and are subject to
periodic unannounced inspections for GMP compliance, imposing procedural and
documentation requirements upon us and third-party manufacturers. Failure to
comply with these regulations could result, among other things, in suspension of
regulatory approval, recalls, suspension of production or injunctions, seizures,
or civil or criminal sanctions. We cannot be certain that we or our present or
future subcontractors will be able to comply with these
regulations.
The
FDA regulates drug labeling and promotion activities. The FDA has actively
enforced regulations prohibiting the marketing of products for unapproved uses.
The FDA permits the promotion of drugs for unapproved uses in certain
circumstances, subject to stringent requirements. We and our product candidates
are subject to a variety of state laws and regulations which may hinder our
ability to market our products. Whether or not FDA approval has been obtained,
approval by foreign regulatory authorities must be obtained prior to commencing
clinical trials, and sales and marketing efforts in those countries. These
approval procedures vary in complexity from country to country, and the
processes may be longer or shorter than that required for FDA approval. We may
incur significant costs to comply with these laws and regulations now or in the
future.
The FDA’s
policies may change, and additional government regulations may be enacted which
could prevent or delay regulatory approval of our potential products. Increased
attention to the containment of health care costs worldwide could result in new
government regulations materially adverse to our business. We cannot predict the
likelihood, nature or extent of adverse governmental regulation that might arise
from future legislative or administrative action, either in the U.S. or
abroad.
Other Regulatory
Requirements
The
U.S. Federal Trade Commission and the Office of the Inspector General of the
U.S. Department of Health and Human Services (“HHS”) also regulate certain
pharmaceutical marketing practices. Government reimbursement practices and
policies with respect to our products are important to our success.
We
are subject to numerous federal, state and local laws relating to safe working
conditions, manufacturing practices, environmental protection, fire hazard
control, and disposal of hazardous or potentially hazardous substances. We may
incur significant costs to comply with these laws and regulations. The
regulatory framework under which we operate will inevitably change in light of
scientific, economic, demographic and policy developments, and such changes may
have a material adverse effect on our business.
European
Product Approval
Prior
regulatory approval for human healthy volunteer studies (phase I studies) is
required in member states of the European Union (E.U.). Summary data from
successful phase I studies are submitted to regulatory authorities in member
states to support applications for phase II studies. E.U. authorities typically
have one to three months (which often may be extended in their discretion) to
raise objections to the proposed study. One or more independent ethics
committees (similar to U.S. IRBs) review relevant ethical issues.
For E.U.
marketing approval, we submit to the relevant authority for review a dossier, or
MAA (Market Authorization Application), providing information on the quality of
the chemistry, manufacturing and pharmaceutical aspects of the product as well
as non-clinical and clinical data.
Approval
can take several months to several years, and can be denied, depending on
whether additional studies or clinical trials are requested (which may delay
marketing approval and involve unbudgeted costs) or regulatory authorities
conduct facilities (including clinical investigation site) inspections and
review manufacturing procedures, operating systems and personnel qualifications.
In many cases, each drug manufacturing facility must be approved, and further
inspections may occur over the product’s life.
The
regulatory agency may require post-marketing surveillance to monitor for adverse
effects or other studies. Further clinical studies are usually necessary for
approval of additional indications. The terms of any approval, including
labeling content, may be more restrictive than expected and could affect the
marketability of a product.
Failure
to comply with these ongoing requirements can result in suspension of regulatory
approval and civil and criminal sanctions. European renewals may require
additional data, resulting in a license being withdrawn. E.U. regulators have
the authority to revoke, suspend or withdraw approvals, prevent companies and
individuals from participating in the drug approval process, request recalls,
seize violative products, obtain injunctions to close non-compliant
manufacturing plants and stop shipments of violative products.
Pricing
Controls
Pricing
for products under approval applications is also subject to regulation.
Requirements vary widely between countries and can be implemented disparately
intra-nationally. The E.U. generally provides options for member states to
control pricing of medicinal products for human use, ranging from specific
price-setting to systems of direct or indirect controls on the producer’s
profitability. U.K. regulation, for example, generally provides controls on
overall profits derived from sales to the U.K. National Health Service that are
based on profitability targets or a function of capital employed in servicing
the National Health Service market. Italy generally utilizes a price monitoring
system based on the European average price over the reference markets of France,
Spain, Germany and the U.K. Italy typically establishes price within a
therapeutic class based on the lowest price for a medicine belonging to that
category. Spain generally establishes selling price based on prime cost plus a
profit margin within a range established yearly by the Spanish Commission for
Economic Affairs.
There can
be no assurance that price controls or reimbursement limitations will result in
favorable arrangements for our products.
Third-Party
Reimbursements
In
the U.S., the E.U. and elsewhere, pharmaceutical sales are dependent in part on
the availability and adequacy of reimbursement from third party payers such as
governments and private insurance plans. Third party payers are increasingly
challenging established prices, and new products that are more expensive than
existing treatments may have difficulty finding ready acceptance unless there is
a clear therapeutic benefit.
In the
U.S., consumer willingness to choose a self-administered outpatient prescription
drug over a different drug or other form of treatment often depends on the
manufacturer’s success in placing the product on a health plan formulary or drug
list, which results in lower out-of-pocket costs. Favorable formulary placement
typically requires the product to be less expensive than what the health plan
determines to be therapeutically equivalent products, and often requires
manufacturers to offer rebates. Federal law also requires manufacturers to pay
rebates to state Medicaid programs in order to have their products reimbursed by
Medicaid. Medicare, which covers most Americans over age 65 and the disabled,
has adopted a new insurance regime that will offer eligible beneficiaries
limited coverage for outpatient prescription drugs effective January 1, 2006.
The prescription drugs that will be covered under this insurance will be
specified on a formulary published by Medicare. As part of these changes,
Medicare is adopting new payment formulas for prescription drugs administered by
providers, such as hospitals or physicians that are generally expected to lower
reimbursement.
The E.U.
generally provides options for member states to restrict the range of medicinal
products for which their national health insurance systems provide
reimbursement. Member states can opt for a “positive” or “negative” list, with
the former listing all covered medicinal products and the latter designating
those excluded from coverage. The E.U., the U.K. and Spain have negative lists,
while France uses a positive list. Canadian provinces establish their own
reimbursement measures. In some countries, products may also be subject to
clinical and cost effectiveness reviews by health technology assessment bodies.
Negative determinations in relation to our products could affect prescribing
practices. In the U.K., the National Institute for Clinical Excellence (“NICE”)
provides such guidance to the National Health Service, and doctors are expected
to take it into account when choosing drugs to prescribe. Health authorities may
withhold funding from drugs not given a positive recommendation by NICE. A
negative determination by NICE may mean fewer prescriptions. Although NICE
considers drugs with orphan status, there is a degree of tension on the
application of standard cost assessment for orphan drugs, which are often priced
higher to compensate for a limited market. It is unclear whether NICE will adopt
a more relaxed approach toward the assessment of orphan drugs.
We cannot
assure you that any of our products will be considered cost effective, or that
reimbursement will be available or sufficient to allow us to sell them
competitively and profitably.
Fraud and Abuse
Laws
The
U.S. federal Medicare/Medicaid anti-kickback law and similar state laws prohibit
remuneration intended to induce physicians or others either to refer patients,
or to acquire or arrange for or recommend the acquisition of health care
products or services. While the federal law applies only to referrals, products
or services receiving federal reimbursement, state laws often apply regardless
of whether federal funds are involved. Other federal and state laws prohibit
anyone from presenting or causing to be presented false or fraudulent payment
claims. Recent federal and state enforcement actions under these statutes have
targeted sales and marketing activities of prescription drug manufacturers. As
we begin to market our products to health care providers, the relationships we
form, such as compensating physicians for speaking or consulting services,
providing financial support for continuing medical education or research
programs, and assisting customers with third-party reimbursement claims, could
be challenged under these laws and lead to civil or criminal penalties,
including the exclusion of our products from federally-funded reimbursement.
Even an unsuccessful challenge could cause adverse publicity and be costly to
respond to, and thus could have a material adverse effect on our business,
results of operations and financial condition. We intend to consult counsel
concerning the potential application of these and other laws to our business and
to our sales, marketing and other activities to comply with them. Given their
broad reach and the increasing attention given them by law enforcement
authorities, however, we cannot assure you that some of our activities will not
be challenged.
Patent
Restoration and Marketing Exclusivity
The
U.S. Drug Price Competition and Patent Term Restoration Act of 1984
(Hatch-Waxman) permits the FDA to approve Abbreviated New Drug Applications
(“ANDAs”) for generic versions of innovator drugs, as well as NDAs with less
original clinical data, and provides patent restoration and exclusivity
protections to innovator drug manufacturers. The ANDA process permits competitor
companies to obtain marketing approval for drugs with the same active ingredient
and for the same uses as innovator drugs, but does not require the conduct and
submission of clinical studies demonstrating safety and efficacy. As a result, a
competitor could copy any of our drugs and only need to submit data
demonstrating that the copy is bioequivalent to gain marketing approval from the
FDA. Hatch-Waxman requires a competitor that submits an ANDA, or otherwise
relies on safety and efficacy data for one of our drugs, to notify us and/or our
business partners of potential infringement of our patent rights. We and/or our
business partners may sue the company for patent infringement, which would
result in a 30-month stay of approval of the competitor’s application. The
discovery, trial and appeals process in such suits can take several years. If
the litigation is resolved in favor of the generic applicant or the challenged
patent expires during the 30-month period, the stay is lifted and the FDA may
approve the application. Hatch-Waxman also allows competitors to market copies
of innovator products by submitting significantly less clinical data outside the
ANDA context. Such applications, known as “505(b)(2) NDAs” or “paper NDAs,” may
rely on clinical investigations not conducted by or for the applicant and for
which the applicant has not obtained a right of reference or use and are subject
to the ANDA notification procedures described above.
The
law also restores a portion of a product’s patent term that is lost during
clinical development and NDA review, and provides statutory protection, known as
exclusivity, against FDA approval or acceptance of certain competitor
applications. Restoration can return up to five years of patent term for a
patent covering a new product or its use to compensate for time lost during
product development and regulatory review. The restoration period is generally
one-half the time between the effective date of an IND and submission of an NDA,
plus the time between NDA submission and its approval (subject to the five-year
limit), and no extension can extend total patent life beyond 14 years after the
drug approval date. Applications for patent term extension are subject to U.S.
Patent and Trademark Office (“USPTO”) approval, in conjunction with FDA.
Approval of these applications takes at least six months, and there can be no
guarantee that it will be given at all.
Hatch-Waxman
also provides for differing periods of statutory protection for new drugs
approved under an NDA. Among the types of exclusivity are those for a “new
molecular entity” and those for a new formulation or indication for a
previously-approved drug. If granted, marketing exclusivity for the types of
products that we are developing, which include only drugs with innovative
changes to previously-approved products using the same active ingredient, would
prohibit the FDA from approving an ANDA or 505(b)(2) NDA relying on safety and
efficacy data for three years. This three-year exclusivity, however, covers only
the innovation associated with the original NDA. It does not prohibit the FDA
from approving applications for drugs with the same active ingredient but
without our new innovative change. These marketing exclusivity protections do
not prohibit FDA from approving a full NDA, even if it contains the innovative
change.