Initial Public Offering (IPO): Pre-Effective Amendment to Registration Statement (General Form) — Form S-1 Filing Table of Contents
Document/ExhibitDescriptionPagesSize 1: S-1/A Amendment No. 1 to Form S-1 HTML 1.40M
2: EX-3.5 Ex-3.5: Form of Amended and Restated Certificate 5 21K
of Incorporation
3: EX-3.6 Ex-3.6: Form of Amended and Restated Bylaws 15 56K
4: EX-5.1 Ex-5.1: Form of Opinion of Heller Ehrman LLP 1 8K
5: EX-23.1 Ex-23.1: Consent of Pricewaterhousecoopers LLP 1 5K
6: EX-23.2 Ex-23.2: Consent of Pricewaterhousecoopers LLP 1 5K
(Name, address, including zip code and telephone number,
including area code, of agent for service)
Copies to:
Stephen M. Davis, Esq.
Peter DiIorio, Esq.
Heller Ehrman LLP
Times Square Tower, 7 Times Square New York, New York10036
Phone: (212) 832-8300
Fax: (212) 763-7600
Jeffery M. Brinza, Esq.
QuatRx Pharmaceuticals Company
777 East Eisenhower Parkway, Suite 100 Ann Arbor, Michigan48108
Phone: (734) 913-9900
Fax: (734) 913-0743
Danielle Carbone, Esq.
Shearman & Sterling LLP
599 Lexington Avenue New York, New York10022
Phone: (212) 848-4000
Fax: (212) 848-7179
Approximate date of commencement of proposed sale to
public: As soon as practicable after this Registration
Statement becomes effective.
If any of the securities being registered on this Form are to be
offered on a delayed or continuous basis pursuant to
Rule 415 under the Securities Act of 1933, check the
following
box: o
If this Form is filed to register additional securities for an
offering pursuant to Rule 462(b) under the Securities Act,
please check the following box and list the Securities Act
registration statement number of the earlier effective
registration statement for the same
offering: o
If this Form is a post-effective amendment filed pursuant to
Rule 462(c) under the Securities Act, check the following
box and list the Securities Act registration statement number of
the earlier effective registration statement for the same
offering: o
If this Form is a post-effective amendment filed pursuant to
Rule 462(d) under the Securities Act, check the following
box and list the Securities Act registration statement number of
the earlier effective registration statement for the same
offering: o
The Registrant hereby amends this Registration Statement on
such date or dates as may be necessary to delay its effective
date until the Registrant shall file a further amendment which
specifically states that this Registration Statement shall
thereafter become effective in accordance with Section 8(a)
of the Securities Act of 1933 or until the Registration
Statement shall become effective on such date as the Commission,
acting pursuant to said Section 8(a), may determine.
The
information in this prospectus is not complete and may be
changed. We may not sell these securities until the registration
statement filed with the Securities and Exchange Commission is
effective. This prospectus is not an offer to sell these
securities and it is not soliciting an offer to buy these
securities in any jurisdiction where the offer or sale is not
permitted.
QuatRx Pharmaceuticals Company is
offering shares
of common stock. This is our initial public offering, and no
public market currently exists for our shares. We anticipate
that the initial public offering price will be between
$ and
$ per
share. After the offering, the market price for our shares may
be outside this range.
We have applied to list our common stock on the Nasdaq National
Market under the symbol “QTRX”.
Investing in our common stock involves a high degree of risk.
See “Risk Factors” beginning on page 7.
Per Share
Total
Offering price
$
$
Discounts and commissions to underwriters
$
$
Offering proceeds to QuatRx Pharmaceuticals Company, before
expenses
$
$
Neither the Securities and Exchange Commission nor any state
securities commission has approved or disapproved of these
securities or determined if this prospectus is accurate or
complete. Any representation to the contrary is a criminal
offense.
We have granted the underwriters the right to purchase up
to additional
shares of common stock to cover any over-allotments. The
underwriters can exercise this right at any time within
30 days after the offering. The underwriters expect to
deliver the shares on or
about ,
2006.
Sole Book-Running
Manager
Banc of America Securities LLC
Cowen & Company
Lazard Capital Markets
Pacific Growth Equities, LLC
,
2006
You should rely only on the information contained in this
prospectus. We have not, and the underwriters have not,
authorized anyone to provide you with different information. We
are not making offers to sell or seeking offers to buy these
securities in any jurisdiction where the offer or sale is not
permitted. You should assume that the information contained in
this prospectus is accurate as of the date in the front of this
prospectus only. Our business, financial condition, results of
operations and prospectus may have changed since that date.
Although this summary highlights information about us and our
business that we believe is important for you to read and
consider, you should read this entire prospectus carefully,
including “Risk Factors” beginning on page 7 and
our consolidated financial statements and the notes to those
financial statements beginning on page F-1, before you decide to
buy our common stock. In this prospectus, all references to
“QuatRx,”“the company,”“we,”“us” and “our” refer to QuatRx
Pharmaceuticals Company and its subsidiary, and all references
to “Hormos” refer to Hormos Medical Oy, our wholly
owned subsidiary, unless the context requires otherwise.
Our Business
Overview
We are a pharmaceutical company focused on discovering,
licensing, developing and commercializing compounds in the
endocrine, metabolic and cardiovascular therapeutic areas. We
currently have four product candidates in clinical development
and one compound that we expect to enter clinical development in
the first half of 2006. Our two lead product candidates treat
hormone deficiencies that result from aging in men and women.
Ospemifene, our treatment for vaginal atrophy, a common problem
associated with estrogen deficiency in post-menopausal women, is
in phase III clinical testing. Fispemifene, our treatment
for the symptoms of andropause in aging males, has recently
entered phase II clinical testing. We also have two product
candidates for the treatment of elevated cholesterol levels,
QRX-401 and QRX-431, in phase I clinical trials and
advanced preclinical development, respectively. Becocalcidiol,
our topical product candidate for the treatment of mild to
moderate psoriasis, has completed a phase IIb clinical
trial. Our management team has extensive experience in
pharmaceutical development, particularly in endocrine and
cardiovascular therapies, having participated in over
60 clinical development programs in their careers. This
team has contributed to over 30 programs involving approved
drugs, ten of which reached annual sales in excess of
$1 billion according to PharmaKey and include the
world’s best selling pharmaceutical product, Lipitor.
Ospemifene is our product candidate for the treatment of
post-menopausal vaginal atrophy. Vaginal atrophy is a chronic
condition resulting from a decline in estrogen levels. The
symptoms of vaginal atrophy include vaginal dryness, burning,
irritation, itching, pain during intercourse and vaginal
discharge. Scrip Reports estimates that in 2000 there were
145 million post-menopausal women in North America, Europe
and Japan, and the medical journal Clinical Geriatrics
estimates that between 10% and 40% of them suffer from vaginal
atrophy. Vaginal atrophy is typically treated with hormone
replacement therapies, including estrogen-based therapies.
U.S. sales of hormone replacement therapies for menopausal
symptoms were $1.7 billion in 2004 according to IMS Health,
but have been declining due to concerns that the long-term use
of these therapies increases the risk of breast and uterine
cancer. Ospemifene is a selective estrogen receptor modulator,
or SERM, an orally available small molecule that binds to
estrogen receptors and selectively stimulates or blocks
estrogen’s activity in different tissue types. We have
completed two phase II clinical trials of ospemifene in
which it has demonstrated beneficial effects on vaginal cell
maturation, indicating improvement in the symptoms of vaginal
atrophy. Based on our completed clinical trials, ospemifene has
demonstrated beneficial effects on the symptoms of vaginal
atrophy and, based on preclinical studies, positive effects on
bone density. In addition, in a completed phase II clinical
trial, ospemifene did not increase the frequency of hot flashes
when compared to placebo. In January 2006, we initiated our
first phase III clinical trial of ospemifene for the
treatment of vaginal atrophy. The trial is expected to take
place in approximately 60 sites in the U.S. and will enroll
approximately 800 patients.
Fispemifene is our product candidate for the treatment of the
symptoms of andropause. Andropause is a condition in men caused
by a gradual decline in testosterone levels that occurs
naturally as men age. The symptoms of andropause include muscle
wasting, enlarged breasts, urinary tract problems and sexual
dysfunction. Patients receiving treatment for andropause
typically utilize testosterone replacement therapy. According to
IMS Health, U.S. sales of testosterone replacement products
reached approximately $538 million in 2004, an increase of
40% versus the prior year. Unlike testosterone replacement
therapies that
are typically topical or injection therapies, fispemifene is an
oral treatment and is not a formulation of testosterone. Rather,
fispemifene is a novel SERM that utilizes the body’s normal
feedback mechanism to increase testosterone levels. In a
multiple dose phase I trial, subjects treated with
fispemifene demonstrated an increase in testosterone levels. In
the first quarter of 2006, we initiated a phase II trial
with fispemifene in older men with low testosterone levels.
QRX-401 and QRX-431 are our two product candidates for the oral
treatment of elevated levels of low-density lipoprotein
cholesterol, or LDL cholesterol, the so-called “bad
cholesterol.” Elevated LDL cholesterol levels have been
shown to increase a person’s risk of heart disease. In
2004, treatments for lowering cholesterol had worldwide sales of
approximately $26 billion. In preclinical studies with
monkeys, QRX-401 demonstrated the ability to lower LDL
cholesterol as well as lipoprotein(a), also referred to as
Lp(a), high levels of which are associated with an increased
risk of stroke and coronary artery disease. We are currently
conducting a phase I clinical program of QRX-401. In our
phase I studies to date, QRX-401 has been well-tolerated
and no safety issues have been observed. In the doses tested so
far, QRX-401 has not
demonstrated the ability to consistently and meaningfully lower
LDL levels in healthy volunteers. We are currently completing a
trial at a higher dose and a trial with
QRX-401 in combination
with a statin. We expect the results of these trials to be
available in the second quarter of 2006. Our second product
candidate for the treatment of elevated cholesterol levels,
QRX-431, has demonstrated the ability to reduce LDL cholesterol
and Lp(a) levels and cause weight loss in monkeys. We expect to
file an IND for QRX-431 in the first half of 2006.
Becocalcidiol is our topical product candidate for the treatment
of mild to moderate psoriasis. Psoriasis is a chronic disease of
the skin characterized by red patches covered with white scales
that can occur on any part of the body. Ten million people in
the United States, Japan, France, Germany, Italy, Spain and the
United Kingdom have been diagnosed with psoriasis and
approximately 81% of them are receiving treatment with a variety
of prescription and
over-the-counter
topical therapies, according to 2004 estimates published by
Datamonitor. Global sales of topical psoriasis therapies were
estimated at approximately $532 million for the twelve
months ended October 2005 according to IMS Health. We have
successfully completed a phase IIb trial of becocalcidiol
in which it demonstrated a statistically significant improvement
in both the Physicians’ Global Assessment of psoriasis and
the Psoriasis Symptom Score, two standard methods for assessing
efficacy of topical treatments for psoriasis in clinical trials.
Because becocalcidiol is outside our core therapeutic areas, we
are evaluating alternatives for continued development of this
product candidate, including seeking a partner for further
development and commercialization.
Our Strategy
Our goal is to build a successful pharmaceutical company that
develops and commercializes products in the endocrine, metabolic
and cardiovascular therapeutic areas. Our strategy is to
leverage our extensive management expertise in order to:
•
Build and maintain a portfolio of product candidates;
•
Utilize focused criteria to select product candidates that we
believe have a high likelihood of clinical success;
•
Focus on product candidates that have a large commercial
opportunity; and
•
Develop product opportunities in therapeutically aligned areas.
Risk Factors
We are subject to a number of risks of which you should be aware
before you decide to buy our common stock. These risks are more
fully described under the heading “Risk Factors.” All
of our product candidates are in the development stage. We have
not received regulatory approval for, or generated commercial
revenues from, any of our product candidates. If we do not
successfully obtain regulatory approval for, or commercialize
any of our product candidates, we will be unable to achieve our
business objectives. Since inception, we have incurred net
losses. As of December 31, 2005, we had an accumulated
deficit of $67.5 million. We expect to continue to incur
increasing losses over the next several years, and we may never
become profitable.
Corporate Information
We were incorporated in Delaware on November 20, 2000. In
May 2005, we acquired Hormos Medical Oy, a privately held
Finnish company. Our principal executive offices are located at
777 East Eisenhower Parkway, Suite 100, Ann Arbor, Michigan48108, and our telephone number is (734) 913-9900. Our
website address is www.quatrx.com. Information contained in our
website is not a part of this prospectus. We have included our
website address as a factual reference and do not intend it to
be an active link to our website.
“QUATRX” is our registered United States trademark.
Other service marks, trademarks and trade names referred to in
this prospectus are the property of their respective owners.
shares
( shares
if the underwriters’ over-allotment option is fully
exercised)
Common stock to be outstanding after this offering
shares
( shares
if the underwriters’ over-allotment option is fully
exercised)
Use of proceeds
We intend to use the net proceeds from this offering for the
development of our product candidates, research and development
of our preclinical programs and the remainder, if any, for
working capital and other general corporate purposes, which may
include in-licensing or acquiring additional product candidates.
See “Use of Proceeds.”
Proposed Nasdaq National Market symbol
QTRX
Risk factors
See “Risk Factors” and the other information in this
prospectus for information you should consider before deciding
whether to invest in shares of our common stock.
The number of shares of common stock to be outstanding after
this offering is based on 14,490,473 shares of common stock
outstanding as of December 31, 2005, and except as
otherwise indicated:
•
gives effect to a
1-for- reverse
stock split to be effected prior to the closing of this offering;
•
gives effect to our amended and restated certificate of
incorporation, which we will file immediately prior to the
closing of this offering;
•
gives effect to the automatic conversion of all outstanding
shares of our preferred stock into 61,230,251 shares of
common stock upon the closing of this offering;
•
gives effect to the required release upon the closing of this
offering of 3,446,305 shares of common stock held in escrow
in connection with the Hormos acquisition which are not
reflected in our outstanding shares, including
1,066,274 shares of common stock issued upon the conversion
of 1,066,274 shares of preferred stock held in such
escrow; and
•
assumes no exercise by the underwriters of their option to
purchase shares
of our common stock in this offering to cover over-allotments.
Except as otherwise indicated, all information in this
prospectus excludes:
•
5,576,671 shares of common stock issuable upon the exercise
of options outstanding as of December 31, 2005, with
exercise prices ranging from $0.20 to $0.35 per share and a
weighted average exercise price of $0.31 per share;
•
1,604,269 additional shares of common stock reserved for future
grants under our Amended and Restated 2005 Stock Incentive Plan
as of December 31, 2005; and
•
shares issuable upon the exercise of a warrant issued by us in
connection with a credit facility we entered into in January
2006, with respect to which the number of underlying shares and
exercise price will be established at the closing of this
offering pursuant to a formula agreed upon with the lender.
Under this formula, at an assumed initial public offering price
of
$ per
share and assuming a closing date
of ,
2006, this warrant would be exercisable
for shares
of common stock at an exercise price of
$ per
share.
You should read the summary consolidated financial data
presented below in conjunction with our consolidated financial
statements and the related notes, “Selected Consolidated
Financial Data,” and “Management’s Discussion and
Analysis of Financial Condition and Results of Operations”
included elsewhere in this prospectus. The summary consolidated
financial data presented below for the years ended
December 31, 2003, 2004 and 2005 and for the period from
inception (November 20, 2000) to December 31, 2005 and
as of December 31, 2005 have been derived from our audited
consolidated financial statements included elsewhere in this
prospectus. Historical results are not necessarily indicative of
the results of operations to be expected for future periods.
The pro forma consolidated statement of operations data for the
year ended December 31, 2005 gives effect to the
acquisition of Hormos as if the acquisition occurred on
January 1, 2005, and should be read in conjunction with our
Unaudited Pro Forma Condensed Combined Financial Statements
included elsewhere in this prospectus.
Accretion of redeemable convertible preferred stock
(1,504
)
(2,320
)
(13,210
)
(13,210
)
(17,571
)
Net loss available to common stockholders
$
(10,468
)
$
(11,624
)
$
(52,931
)
$
(29,028
)
$
(79,544
)
Net Loss Per Share, Basic and Diluted:
Loss per share available to common stockholders
$
(7.57
)
$
(4.79
)
$
(5.77
)
Shares used to compute basic and diluted net loss per share
1,382,723
2,425,592
9,179,723
Pro forma for conversion basic and diluted net loss per share
available to common stockholders(1)
$
(0.91
)
Shares used to compute pro forma basic and diluted net loss per
share
58,213,187
(1)
Pro forma for conversion basic and diluted net loss per common
shares is calculated to give effect to the conversion of all
outstanding shares of our preferred stock into
61,230,251 shares of common stock upon the completion of
this offering, excluding 1,066,274 shares of preferred
stock held in escrow in connection with the Hormos acquisition
that will convert into common stock upon the completion of this
offering.
The following table presents a summary of our balance sheet as
of December 31, 2005:
•
on an actual basis;
•
on a pro forma basis to give effect to the automatic conversion
of all of our outstanding preferred stock into
61,230,251 shares of our common stock upon the completion
of this offering; and
•
on a pro forma as adjusted basis to give further effect to
(1) the required release upon the closing of this offering
of 3,446,305 shares of common stock held in escrow in
connection with the Hormos acquisition, including
1,066,274 shares of common stock issued upon the conversion
of 1,066,274 shares of preferred stock held in such escrow,
and (2) the sale of shares of common stock by us in this
offering at an assumed initial public offering price of
$ per
share, after deducting underwriting discounts and commissions
and estimated offering costs to be paid by us.
Before you invest in our common stock, you should understand
the high degree of risk involved. You should consider carefully
the following risks and other information in this prospectus,
including our historical financial statements and related notes,
before you decide to purchase shares of our common stock. If any
of the following risks actually occur, our business, financial
condition and operating results could be adversely affected. As
a result, the trading price of our common stock could decline
and you could lose part or all of your investment.
Risks Related to Drug Discovery, Development and
Commercialization
Clinical trials may fail to adequately demonstrate the
safety or efficacy of our existing product candidates or any
future product candidates we may seek to develop, preventing or
significantly delaying their regulatory approval and
commercialization.
We will not be able to commercialize any of our product
candidates until we obtain applicable regulatory approvals. To
satisfy FDA or foreign regulatory approval standards for the
commercial sale of our product candidates, we must demonstrate
in adequate and controlled clinical trials that our product
candidates are safe and effective.
Clinical trial programs are expensive, time-consuming and
typically take years to complete. We do not expect to receive
approval for marketing of any of our product candidates for
several years, if at all. In connection with clinical trials, we
face the risks that:
•
the product candidate may not prove to be efficacious;
•
the results may not confirm positive results in earlier clinical
or preclinical trials;
•
the product candidate may not be well-tolerated, may cause
harmful side effects or may be subject to adverse or undesirable
interaction when used with other drugs;
•
patients may die or suffer other adverse medical events for
reasons that may or may not be related to the product candidate
being tested;
•
clinical research organizations or other suppliers we contract
with may not perform as we expect;
•
the results may not meet the level of statistical significance
required by the FDA or other regulatory agencies; and
•
the FDA or other regulatory agencies may place a clinical hold
on studies of our product candidates.
In 2006, we initiated a randomized, double-blind,
placebo-controlled, parallel group pivotal study of ospemifene
in the treatment of vaginal atrophy. The primary efficacy
endpoints will be assessed at week 12 and are a change in the
vaginal cell maturation index, change in vaginal pH and
improvement of the most bothersome symptom. Ospemifene is a
selective estrogen receptor modulator, or SERM. No SERM so far
has been approved by the FDA to treat vaginal atrophy. In
addition, some SERMs have been shown to increase the risk of
abnormal thickening of the endometrium, which is the lining of
the uterus, and of deep veinous thrombosis, which are blood
clots in a deep vein of an extremity. Some SERMs have also been
shown to cause increased incidence of hot flashes. We cannot
assure you that these side effects will not be demonstrated with
ospemifene. Lasofoxifene (Oporia), a SERM under development by
Pfizer for the treatment of osteoporosis and vaginal atrophy,
received a non-approvable letter from the FDA for the
osteoporosis indication. The reasons for the FDA’s decision
are not publicly known. The FDA has not yet publicly issued a
decision regarding the approval of Oporia for the treatment of
vaginal atrophy.
In the case of fispemifene, initial phase I trials have
demonstrated that fispemifene raises testosterone levels in
older men, but these trials were not specific to the target
population for this product candidate, men with low
testosterone. Testosterone replacement therapy increases
prostate size and may raise prostate specific
antigen, or PSA, levels, a marker for prostate cancer. We cannot
assure you that prostate enlargement and elevated PSA levels
will not be shown in any trials we may conduct with fispemifene.
There is no long-term safety data regarding administration of
SERMs in men, nor has the FDA ever approved a SERM for use in
men. In addition, fispemifene uses the body’s normal
feedback mechanism to increase testosterone levels. To date, our
clinical trials have only studied fispemifene in patients with
normal testosterone levels, and we have not yet confirmed that
fispemifene is effective in patients with low testosterone
levels. We cannot assure you that further clinical trials of
fispemifene will not raise safety or efficacy concerns.
QRX-401 is in phase I clinical trials to assess safety and
tolerability. Although phase I clinical trials are not
primarily designed to assess efficacy, in most products for the
treatment of elevated cholesterol levels, a cholesterol lowering
effect has been observed in phase I clinical trials. In a
phase I clinical trial of
QRX-401 in doses
between 75 mg/day and 150 mg/day for up to
14 days in healthy volunteers that had levels of LDL
cholesterol above 125 mg/dl, changes in LDL cholesterol
were not consistent within or between treatment groups, and as a
result these changes were not deemed to be meaningful. According
to the National Cholesterol Education Program, LDL cholesterol
levels between 130 and 159 mg/dl are considered borderline high,
LDL cholesterol levels between 100 and 129 mg/dl are considered
near optimal, and LDL cholesterol levels less than 100 mg/dl are
considered optimal. Our IND for QRX-401 permits us to dose
subjects in our clinical trials with doses up to 250 mg/day
of QRX-401. We have
recently completed dosing for a phase I clinical trial of
250 mg/day of QRX-401 for 14 days in healthy
volunteers with LDL cholesterol levels greater than
100 mg/dl. The treatment groups for this study have not
been unblinded to date, so we cannot draw any conclusions
regarding efficacy. We have also recently completed dosing of a
phase I clinical trial of 250 mg/day of QRX-401 in
combination with 10 mg/day of simvastatin for 14 days
in healthy volunteers with LDL cholesterol levels greater than
100 mg/dl. If we do not observe a meaningful and consistent
LDL cholesterol lowering effect in either of these two
phase I clinical studies, it is unlikely that we will
proceed with further development of QRX-401, which may
negatively affect our stock price.
QRX-431 is in
preclinical studies and has not yet been tested in human
clinical trials. In order to test
QRX-431 in humans, we
must file and the FDA must accept an IND for this product
candidate. The FDA may not accept our IND and allow us to test
QRX-431 in humans,
which would prevent us from further developing this product
candidate and assessing the potential safety or efficacy of
QRX-431 in humans.
Success in preclinical testing and early clinical trials
for any of our product candidates may not be demonstrated in
later clinical trials.
Success in preclinical testing and early clinical trials does
not ensure that later clinical trials will be successful. In
addition, our preclinical product candidates may not demonstrate
sufficient efficacy or safety to allow us to progress to
clinical testing. For instance, while we observed the effects of
QRX-401 on
LDL cholesterol and Lp(a) in animal models, we have not yet
observed that this mechanism is effective for lowering LDL
cholesterol in humans. A number of companies in the
pharmaceutical industry have suffered significant setbacks in
advanced clinical trials, even after obtaining promising results
in earlier clinical trials. Future clinical trials may indicate
previously undetected side effects or fail to demonstrate
efficacy in a statistically significant manner. If we fail to
achieve the primary endpoints in our clinical trials or the
results are ambiguous, we will have to determine whether to
redesign our trials and protocols and continue with additional
testing, or cease development of the product candidate.
Redesigning programs could be extremely costly and
time-consuming. Even if we are able to achieve the primary
endpoints of our trials, we may need positive results from
additional clinical trials to support the filing of a new drug
application, or NDA, with the FDA or a similar application with
regulatory authorities in other countries seeking marketing
approval for a product candidate. We cannot predict how long any
additional trial that might be required by the FDA or regulatory
authorities in other countries will take or what the cost will
be. If our clinical trials for our product candidates are not
completed, are significantly delayed or fail to demonstrate that
the product candidates are safe and effective, our business
prospects would be harmed and our stock price would likely
decline.
Delays in clinical trials could result in increased costs
to us and delay our ability to obtain regulatory approval and
commercialize our product candidates.
Significant delays in clinical trials could materially affect
our product development costs and delay regulatory approval of
our product candidates. We do not know whether planned clinical
trials will begin on time, will need to be redesigned or will be
completed on schedule, if at all. Clinical trials can be delayed
for a variety of reasons, including:
•
delays or failures in obtaining regulatory approval to commence
a trial, including, in the case of
QRX-431, any delays we
may experience in submitting an IND to the FDA or in receiving
FDA approval to commence clinical trials;
•
delays or failures in obtaining clinical materials and
manufacturing sufficient quantities of the product candidate for
use in trials;
•
an inability to find a sufficient number of clinical
investigators capable of running our clinical trials, or
clinical research organizations and other suppliers of materials
or services capable of providing support for our clinical trials;
•
delays or failures in reaching agreement on acceptable clinical
trial agreement terms with prospective sites;
•
delays or failures in obtaining approval of our clinical trial
protocol from an institutional review board to conduct a study
at a prospective site;
•
delays in recruiting patients to participate in a study;
•
failure of our clinical investigation sites and related
facilities to be in compliance with the applicable protocol or
applicable legal and regulatory requirements, including the
FDA’s Good Clinical Practices;
•
unforeseen safety issues;
•
inability to monitor patients adequately during or after
treatment;
•
difficulty monitoring multiple clinical sites; and
•
failure of our third-party clinical trial managers and other
suppliers of material or services to satisfy their contractual
duties, comply with regulations or meet expected deadlines.
Completion of clinical trials depends, among other things, on
our ability to enroll a sufficient number of patients who remain
in a study until its conclusion, which depends on many factors,
including:
•
the patient eligibility criteria defined in the applicable
protocol;
•
the size of the patient population required for analysis of the
trial’s therapeutic endpoints;
•
the proximity of patients to clinical sites;
•
the adherence of patients to the applicable protocol;
•
the design of the applicable protocol;
•
our ability to recruit clinical trial investigators with the
appropriate competencies and experience;
•
our ability to obtain and maintain patient consents; and
•
competition for patients by clinical trial programs for other
treatments.
For example, our current phase III clinical trial for
ospemifene and our current phase II clinical trial for
fispemifene require invasive monitoring procedures which may
result in difficulties in enrolling patients. Difficulties in
enrolling patients in our clinical trials could increase the
costs or affect the timing or outcome of clinical trials.
If we fail to obtain regulatory approvals in the United
States for our product candidates, we will not be able to
generate revenue in the United States market from the
commercialization of our product candidates.
We must receive FDA approval for our product candidates for an
indication at a particular dose before we can commercialize or
sell these product candidates in the United States for that
indication. The FDA can limit, delay or deny its approval for
many reasons, including:
•
a product candidate may be found to be unsafe or ineffective;
•
regulators may interpret data from preclinical testing and
clinical trials differently and less favorably than we do;
•
regulators may not approve the manufacturing processes or
facilities that we use; and
•
regulators may change or initiate new requirements for approval
at any time, many of which are unwritten.
We may incur additional costs from any significant delay in
obtaining FDA approval and delays may diminish any competitive
advantages that we have. Even if we obtain FDA approval, our
product candidates may not be approved for all indications that
we request, which could limit the uses of our products and
adversely impact our potential royalties and product sales. If
FDA approval of a product is granted, such approval will be
limited to the indicated uses for which the product may be
marketed and may require costly post-marketing
follow-up studies, and
the FDA approved labeling may carry warnings or restrictions
that detract from the market acceptance of the product.
If we fail to obtain regulatory approvals in countries
outside of the United States for our product candidates, we will
not be able to generate revenue in such countries from the
commercialization of product candidates.
In order to market our products outside of the United States, we
must comply with numerous and varying regulatory requirements of
other countries. Approval procedures vary among countries and
can involve additional product testing and additional
administrative review periods. Additional separate pricing
approval procedures may be required prior to commercialization
in such countries. The time required to obtain approval in other
countries might differ from that required to obtain FDA approval
in the United States. The regulatory approval process in other
countries may include all of the risks detailed above regarding
FDA approval as well as additional risks. Regulatory approval in
one country does not ensure regulatory approval in another, but
a failure or delay in obtaining regulatory approval in one
country may negatively impact the regulatory process in others.
Failure to obtain regulatory approval in other countries or any
delay or setback in obtaining such approval could have the same
adverse effects detailed above regarding FDA approval in the
United States.
Even if we obtain regulatory approval, our marketed
products will be subject to ongoing regulatory review. If we
fail to comply with continuing United States and foreign
regulations, we could lose approvals to market our products and
our business would be seriously harmed.
Following initial regulatory approval of any products we may
develop, we and our suppliers will be subject to continuing
regulatory review, including review of adverse drug experiences
and clinical results that are reported after our products become
commercially available. These post-approval clinical results
would include results from any post-marketing tests or vigilance
required as a condition of approval. The subsequent discovery of
previously unknown problems with the product, such as an adverse
side effect, may result in restrictions on the product or
withdrawal of the product from the market. The labeling,
packaging, storage, disposal, advertising, promotion and record
keeping related to the product will also continue to be subject
to extensive regulation. In addition, the manufacturer and
manufacturing facilities we use to make any of our product
candidates will be subject to periodic review and inspection by
the FDA and foreign regulatory agencies. If a previously unknown
problem or problems with a product or a manufacturing or
laboratory facility used by us is discovered, the FDA and any
foreign regulatory agency may impose restrictions on that
product or on the manufacturing facility, including requiring us
to withdraw the product from the market.
Any changes to an approved product, including the way it is
manufactured or promoted, often require regulatory approval
before the product, as modified, can be marketed. If we, our
contract manufacturers or any of our other suppliers fail to
comply with applicable regulatory requirements, a regulatory
agency may:
•
issue warning letters;
•
impose civil or criminal penalties;
•
suspend or withdraw our regulatory approval;
•
seize or detain products or require a product recall;
•
suspend any of our ongoing clinical trials;
•
impose restrictions on our operations;
•
refuse to approve pending applications or supplements to
approved applications filed by us; or
•
close the facilities of our contract manufacturers.
Even if we receive regulatory approval to market our
product candidates, the market may not be receptive to our
products, which would negatively affect our ability to achieve
profitability.
If approved for marketing, the commercial success of our product
candidates will depend upon their acceptance by physicians and
the medical community, patients, and private, government and
third-party payors as clinically useful, safe and cost-effective
therapeutics. The degree of market acceptance of any of our
approved products will depend upon a number of factors,
including:
•
the indication for which the product is approved, as well as its
approved labeling;
•
the establishment and demonstration in the medical community of
the safety and efficacy of our products;
•
the prevalence and severity of adverse side effects;
•
the potential advantages of such products over existing and
future treatment methods;
•
the relative convenience, tolerability and ease of
administration of our products;
•
the strength of sales, marketing and distribution support;
•
the price and cost-effectiveness of the product;
•
the willingness of third parties to include the product on their
drug formularies; and
•
sufficient third-party reimbursement.
We are aware that a significant number of product candidates are
currently under development and may become available in the
future for the treatment of endocrine diseases of aging,
elevated cholesterol levels and psoriasis, and may be approved
prior to any of our products coming to market. Even if our
products achieve market acceptance, we may not be able to
maintain that market acceptance over time if new therapeutics
are introduced that are safer or more effective than our
products or are more favorably received than our products.
Further, although we have not yet determined the pricing of any
of our product candidates if they were to be approved, market
acceptance of any of our approved products will depend in part
on the price and cost effectiveness of our products compared to
competing products. Companies with competing products may have
greater financial resources and a larger portfolio of products
which may allow them to price competing products at lower prices
relative to our approved products. Even competing products that
may not be as effective in treating the conditions targeted by
our approved products may affect the market acceptance of our
products if there are substantially less expensive. For
instance, there are several relatively inexpensive
over-the-counter
vaginal lubricants and moisturizers and over-the-counter
treatments for psoriasis which may affect the market acceptance
of our ospemifene and becocalcidiol product candidates,
respectively. In addition, market acceptance can be impacted if
previously unknown problems with our products are subsequently
discovered. If our products do not achieve and maintain market
acceptance, we will not be able to generate sufficient revenue
from product sales to attain profitability.
We have no experience selling, marketing or distributing
products and have minimal capabilities to do so.
If we receive regulatory approval to commence commercial sales
of any of our product candidates, we will need to establish a
sales and marketing organization with appropriate technical
expertise and distribution capability or identify collaborators
who have sales and marketing organizations. At present, we have
a Chief Business Officer who has marketing experience, but we
have no other sales or marketing employees. Factors that may
impede our efforts to commercialize our products through our own
sales and marketing organization include:
•
significant costs associated with building a sales, marketing
and distribution organization;
•
difficulty recruiting and retaining adequate numbers of
effective sales and marketing personnel;
•
the inability of sales personnel to obtain access to, or
persuade adequate numbers of, physicians to prescribe our
products; and
•
the lack of complementary products to be offered by sales
personnel, which may put us at a competitive disadvantage to
companies with broader product lines.
Even if we are able to develop our own sales and marketing
organization, we may not be able to compete effectively against
our competitors, many of which will include pharmaceutical
companies with substantially greater resources and larger sales
and marketing staffs than we are likely to have.
As an alternative to establishing our own sales and marketing
organization, we may attempt to engage pharmaceutical or other
health care companies with existing distribution systems and
direct sales and marketing organizations to assist us. If we
were to seek marketing partners or collaborators, we may not be
able to negotiate favorable distribution or partnering
arrangements, if at all. To the extent we enter co-promotion,
co-marketing or other licensing arrangements, the amount of
revenues we receive from the sale of our products will depend on
the efforts of third parties and will not be under our control.
Risks Related to Our Financial Performance and Operations
We have a history of losses, and we may never achieve
profitability.
Since our inception, we have incurred significant net losses,
including net losses of $39.7 million and $9.3 million
for years ended December 31, 2005 and 2004, respectively.
As of December 31, 2005, our cumulative net loss was
$62.0 million. We have not yet completed the development,
including obtaining regulatory approvals, of any of our product
candidates and, consequently, have not generated revenues from
the sale of products. 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. We also
anticipate that our expenses will increase substantially in the
foreseeable future as we:
•
continue the development of our product candidates and
preclinical programs;
•
begin clinical development of our preclinical programs;
•
prepare for commercialization of our product candidates;
•
expand our portfolio of product candidates;
•
increase our administrative functions; and
•
hire additional personnel.
We also expect to experience negative cash flow from operations
for the foreseeable future as we fund our operating losses. We
will need to generate significant revenues to achieve
profitability. We may not be able to generate significant
revenues, and we may never achieve profitability. Our failure to
fund our continuing losses or achieve profitability would
negatively impact the market price of our common stock.
Even if we do become profitable, we may not be able to sustain
or increase profitability on a quarterly or annual basis.
If we cannot raise additional capital on acceptable terms,
we may be unable to complete planned clinical and preclinical
trials, obtain regulatory approvals or commercialize our product
candidates.
We believe that our existing cash reserves, together with
available borrowings under our credit facility and proceeds from
this offering, will fund our planned activities for at least the
next 18 months. We will require substantial future capital
in order to continue to conduct the research and development,
preclinical and clinical programs and regulatory activities
necessary to bring our product candidates to market. During the
year ended December 31, 2005, our net cash used in
operating activities was $16.0 million. We expect our rate
of cash used in operating activities will increase as we
undertake large and costly phase III trials for ospemifene
and continue to advance other product candidates. Our future
capital requirements depend on many factors, including:
•
the progress of preclinical development and clinical trials;
•
the number of product candidates we pursue or the expansion of
existing product candidates to new indications;
•
the discovery, in-licensing or acquisition of additional product
candidates or technologies that require financial commitments;
•
the time and costs involved in obtaining regulatory approvals,
and the number of different regulatory agencies we seek approval
from;
•
delays that may be caused by evolving requirements of regulatory
agencies;
•
our plans to establish sales, marketing and distribution
capabilities;
•
the cost and timing of securing manufacturing capabilities for
our product candidates and commercial products, if any;
•
the terms and timing of any collaborative, licensing and other
arrangements we may establish;
•
the costs involved in filing, maintaining and prosecuting patent
applications and enforcing or defending patent claims;
•
our revenues, if any, from successful development and
commercialization of our products;
•
the costs of being a public company; and
•
the number of additional employees we hire.
We may seek additional funding through private or public sales
of our equity securities, debt financing or corporate
collaborations or licensing arrangements. To the extent that we
raise additional funds by issuing equity securities, our
existing stockholders may experience dilution. Debt financing
may subject us to restrictive covenants that could limit our
flexibility in conducting future business activities. To the
extent that we raise additional funds through collaboration or
licensing agreements, it will be necessary to relinquish some
commercial rights to our clinical product candidates. Our
ability to raise additional funds will depend on financial,
economic and market conditions in the pharmaceutical industry,
general market conditions and other factors, many of which are
beyond our control. We may not be able to obtain additional
funding on favorable terms, or at all. If we cannot obtain
adequate funds, we may:
•
delay, reduce the scope or eliminate some of our preclinical
development or clinical trials for one or more of our product
candidates;
•
delay establishment of, or decide not to establish,
manufacturing, sales, marketing and distribution capabilities;
•
curtail significant product development programs that are
designed to identify new product candidates;
be unable to acquire technologies or pursue other business
opportunities that require financial commitments; and/or
•
sublicense certain patents and patent applications, cease the
prosecution and maintenance of certain patents and applications
on a country-by-country basis, or otherwise relinquish some or
all rights to our product candidates.
Our research and development program is funded in part by
Finnish government agencies, and in order to maintain this
funding and obtain additional funding from these agencies, we
are required to comply with their requirements. If we fail to
comply, we may lose government funding for our research and
development programs in Finland.
Tekes, the National Technology Agency of Finland, is one of the
main public financers of technology research and development
programs in Finland. Tekes provides financial aid and loans on
favorable terms to qualifying companies in Finland. These loans
are granted on a project-by-project basis, generally carry
interest at below market rates and generally are not required to
be repaid for several years. Under Finnish law, interest and
principal on these loans are not repayable unless we have
adequate equity capital. As of December 31, 2005, we had
approximately $13.5 million in principal and accrued
interest outstanding with respect to these loans and
$2.2 million in outstanding advances from Tekes that relate
to several separate projects. The terms, conditions and
reporting requirements of the loans are set forth in loan
documents entered into with respect to each separate project
loan, and in the general terms and conditions published by
Tekes. Some of the loan terms may be subject to interpretation
by Tekes and us and may not provide definitive guidance as to
whether we are in compliance with them. Under the terms of the
loans, Tekes has the right to accelerate the loans in whole or
in part under a number of circumstances, including if:
•
significant changes in the funded programs occur;
•
changes in the conditions required by the research work occur
such that continuing the research work is not expedient;
•
we use the funding for purposes other than those for which they
were granted; or
•
we otherwise fail to comply with the loan terms.
We believe we are in compliance in all material respects with
all these requirements. However, if Tekes were to find that we
are not in compliance with the terms of the loans or the other
requirements, Tekes may have the right to stop funding loans and
to require repayment of outstanding loans. If Tekes were to
require us to repay all of the outstanding loans, it could have
a material adverse effect on us. If Tekes were to refuse to
provide additional funding, we would be required to seek
alternative funding for our research and development programs in
Finland and if such funding were not available, to reduce the
scope or eliminate some of our research and development
programs. Such alternative funding may not be available to us on
acceptable terms, or at all.
Our secured loan agreement contains various covenants that
may restrict our business and financing activities.
On January 26, 2006, we entered into an $18.0 million
secured loan agreement with Hercules Technology Growth Capital,
a third party lender. Loans under the agreement are secured by
substantially all of our assets other than our intellectual
property rights, and additionally, the agreement contains
covenants that, among other things, restrict our ability to:
•
borrow money;
•
pay cash dividends on our capital stock, including on the shares
of our common stock sold in this offering;
enter into certain transactions with our employees, officers or
directors.
These restrictions may limit our operational flexibility. Any
failure to comply with the restrictions of the secured loan
agreement may result in an event of default. Such default may
allow the lender to accelerate maturity of our obligations under
the agreement. If our debt were to be accelerated, we cannot
assure you that we would be able to repay it. In addition, our
default could give the lender the right to terminate any
commitments they have made to provide us with additional funds.
We may have difficulty managing the integration of Hormos
and we may be exposed to liabilities from its prior
operations.
In May 2005, we completed the acquisition of Hormos, a privately
held Finnish company focused on discovering and developing novel
hormonal therapies for age-related endocrine deficiencies in men
and women. The Hormos acquisition provided us with over 30
employees based in Finland, as well as multiple office locations
in Finland. The process of integrating Hormos has required and
continues to require a significant amount of resources and
management attention which detracts from attention to our
day-to-day business.
Our ability to manage the continued integration of Hormos will
require us to continue to improve our operational, financial and
management information systems and controls. If we fail to
manage the integration of Hormos effectively it could have a
material adverse effect on our results of operations.
In addition, as a result of the Hormos acquisition, we may be
subject to contingent liabilities resulting from Hormos’s
operations before we acquired it, including liabilities
resulting from the operation of Finnish law. Although we may
have some recourse to the sellers of the business under our
acquisition agreements, we may not be fully covered for
contingent liabilities.
If we are unable to retain any of our key executives or if
we are unable to recruit and retain other qualified personnel as
we grow our business, it may be more difficult for us to execute
our business strategy.
We believe that one of our strengths lies in the drug
development and commercialization skills and experience of our
senior management. Accordingly, we are highly dependent on our
four founders: Chief Executive Officer, Robert Zerbe, M.D.,
Chief Scientific and Regulatory Officer, Stuart
Dombey, M.B., F.R.C.P., Chief Medical Officer, Randall
Whitcomb, M.D. and Chief Business Officer, Christopher
Nicholas. We have key-man insurance on these members of our
management team, but we do not have employment agreements with
them and we cannot assure you that they will remain with us for
any specific period of time. The loss of any of our key
employees and our inability to fill these positions with equally
qualified employees could impede the achievement of our
development objectives. As we grow our business, our success
will also depend on our ability to hire additional qualified
personnel. We may be unable to attract and retain personnel on
acceptable terms given the competition for experienced
scientists among biotechnology, pharmaceutical and health care
companies, universities and non-profit research institutions. If
we are unsuccessful in our recruitment efforts, we may be unable
to execute our strategy.
We will need to increase the size of our organization, and
we may encounter difficulties managing our growth.
As of December 31, 2005, we had 19 employees in Ann Arbor
and 39 employees in Finland. We plan to hire several
additional employees as required each year to add depth and
specialized expertise to our scientific and management team. We
expect that any substantial growth would place a strain on our
administrative and operational infrastructure. If the product
candidates that we are developing continue to advance in
clinical trials, we will need to expand our development,
regulatory, manufacturing, quality, sales, marketing and
distribution capabilities or contract with third parties to
provide these capabilities for us. As
our operations expand, we expect that we will need to develop
additional relationships with various collaborators, contract
research organizations, suppliers, manufacturers and other
organizations. We may not be able to establish such
relationships or may incur significant costs to do so. Our
ability to manage our growth will also require us to continue to
improve our operational, financial and management controls,
reporting systems and procedures, which will further increase
our operating costs.
In addition to our operations in Ann Arbor, Michigan, we
operate two facilities in Finland. If we are unable to manage
the challenges associated with our international operations, the
growth of our business could be limited.
In May 2005, we acquired our wholly owned subsidiary Hormos, a
Finnish company. Prior to acquiring Hormos, we had never
conducted operations outside of the United States. We are
subject to a number of risks and challenges that specifically
relate to these international operations. Our international
operations may not be successful if we are unable to meet and
overcome these challenges, which could limit the growth of our
business and may have an adverse effect on our business and
operating results. These risks include:
•
difficulty managing operations in multiple locations;
•
local regulations that may make it more difficult to conduct our
research and development activities;
•
foreign protectionist laws and business practices that favor
local competition;
•
failure of local laws to provide the same degree of protection
against infringement of our intellectual property; and
•
understanding legal requirements that differ from those of the
United States and keeping abreast of changes in those
requirements.
Hormos conducts a portion of its business in Euros. However, we
fund a portion of the operations of Hormos through intercompany
financing denominated in United States dollars. We are exposed
to fluctuations in exchange rates, which could result in losses
and have an adverse impact on our results of operations. We have
no control over the factors that generally affect these risks,
such as economic, financial and political events and the supply
and demand for the applicable currencies. Because we have
foreign operations, fluctuations in foreign exchange rates could
have a material effect on our operating results.
Because we have operated as a private company, we have no
experience complying with public company obligations, including
the Sarbanes-Oxley Act. Complying with these requirements will
increase our costs and require additional management
resources.
We are a small company with limited resources. We have operated
as a private company, not subject to the requirements applicable
to public companies. We will need to expand our staff when we
become a public company, and we may encounter difficulty
attracting qualified staff with requisite experience due to the
high level of competition for experienced personnel.
As directed by Section 404 of the Sarbanes-Oxley Act, the
SEC adopted rules requiring public companies to include a report
of management on the company’s internal controls over
financial reporting in their annual reports on
Form 10-K. In
addition, the public accounting firm auditing the company’s
financial statements must attest to and report on
management’s assessment of the effectiveness of the
company’s internal controls over financial reporting. This
requirement will first apply to our annual report on
Form 10-K for our
fiscal year ending December 31, 2007. We may be unable to
comply with applicable deadlines. In addition, if we are unable
to conclude that we have effective internal controls over
financial reporting or, if our independent auditors are unable
to provide us with an unqualified report as to the effectiveness
of our internal controls over financial reporting as required by
Section 404 of the Sarbanes-Oxley Act, investors could lose
confidence in the reliability of our financial statements.
We rely on independent clinical investigators and contract
research organizations to conduct clinical trials, and they may
not be diligent, careful or timely, which may delay development
and commercialization of our product candidates.
We rely almost exclusively on independent clinical investigators
and contract research organizations (CROs) to conduct our
clinical trials and to perform data collection and analysis.
These investigators are not our employees, and we cannot control
the amount of time or resources that they devote to our product
development programs. These investigators may fail to devote
sufficient time and resources to our programs, fail to enroll
patients as rapidly as expected, or otherwise fail to perform in
a satisfactory manner, potentially delaying regulatory approval
of our product candidates. Failure of the CROs to meet their
obligations under our agreements could adversely affect clinical
development of our product candidates. These independent
investigators and CROs may also have relationships with other
commercial entities, some of which may compete with us. We
believe there are alternative independent investigators and
CROs. However, we may face delays if we are required to change
service providers. If identifying and contracting with
substitute providers causes significant delays in the progress
of our clinical trials, the commercial prospects for our product
candidates could be harmed and our ability to generate product
revenue from affected product candidates may be delayed or
prevented.
We rely on third party manufacturers to manufacture our
product candidates. If these third party manufacturers fail to
manufacture product candidates of satisfactory quality, in a
timely manner, in sufficient quantities or at acceptable costs,
development and commercialization of our product candidates
could be delayed.
We have no manufacturing facilities, and we have no experience
in the commercial manufacturing of drugs or in designing drug
manufacturing processes. We have contracted with third party
manufacturers to produce our product candidates for clinical
trials. We have limited supplies of our product candidates for
clinical trials. If our supplies are damaged or destroyed,
either during storage or shipping or otherwise, our clinical
trials may be delayed, which could have a material adverse
effect on our business. We intend to rely on third party
contract manufacturers to manufacture, supply, store and
distribute commercial quantities of our product candidates. In
the case of our product candidate ospemifene, our manufacturer,
Orion Corporation Fermion, owns all inventions made relating to
the synthesis of ospemifene and possesses a right of first
refusal to enter into an agreement to become our exclusive
supplier of commercial quantities of ospemifene. We will also
rely on our third party manufacturing partners to work with us
to complete the Chemistry, Manufacturing and Control, or CMC,
section of any NDAs or other marketing approval applications we
may file.
Contract manufacturers are obliged to operate in accordance with
government mandated obligations, including FDA-mandated current
good manufacturing practices, or cGMPs. A failure of any of our
contract manufacturers to establish and follow cGMPs or to
document their adherence to such practices may lead to
significant delays in the availability of material for clinical
trials and may delay or prevent filing or approval of marketing
applications for our products.
Changing contract manufacturers may be difficult, and the number
of potential manufacturers is limited. Changing manufacturers
requires re-validation of the manufacturing processes and
procedures in accordance with government mandated obligations,
including FDA-mandated cGMPs. Such re-validation may be costly
and time-consuming. It may be difficult or impossible for us to
find replacement manufacturers on acceptable terms quickly, if
at all. Any of these factors could delay or prevent the
completion of our clinical trials, the approval of our product
candidates by the FDA or other regulatory agencies, or the
commercialization of our products, result in higher costs, or
cause a decline in potential product revenues.
Drug manufacturers are subject to on-going, periodic unannounced
inspections by the FDA and corresponding state and foreign
agencies to ensure strict compliance with cGMPs, other
government regulations and corresponding foreign standards.
While we are obligated to audit the performance of third party
contractors, we do not have control over our third party
manufacturers’ compliance with these
regulations and standards. Failure by our third party
manufacturers or us to comply with applicable regulations could
result in sanctions being imposed on us, including fines,
injunctions, civil penalties, failure of the government to grant
market approval of drugs, delays, suspension of clinical trials,
withdrawal of approvals, seizures, detentions or recalls of
product, operating restrictions and criminal prosecution.
To date, our product candidates have been manufactured in small
quantities by third party manufacturers for preclinical and
clinical trials. In order to obtain marketing approval for any
of these product candidates, we will need to enter into
long-term supply agreements with our existing or new third party
manufacturers and demonstrate that we can manufacture sufficient
quantities for commercial sale. Our third party manufacturers
may not be able to successfully increase their manufacturing
capacity or apply at commercial scale the current manufacturing
process for any of our product candidates in a timely or
economic manner, or at all. For example, we are currently
working on improved synthetic manufacturing methods for
becocalcidiol to reduce the cost of manufacturing this product
candidate. If our third party manufacturers, for any reason, are
unable to manufacture our product candidates, we may need to
seek out additional manufacturing partners who may have
different equipment requiring additional validation studies,
which the relevant government regulator must review and approve.
If we are unable to successfully increase the manufacturing
capacity for a product candidate, the regulatory approval or
commercial launch of that product candidate may be delayed or
there may be a shortage in the supply of the product candidate.
Our product candidates require precise, high-quality
manufacturing. The failure of our third party manufacturers to
achieve and maintain these high manufacturing standards,
including the incidence of manufacturing errors, could result in
patient injury or death, product recalls or withdrawals, delays
or failures in product testing or delivery, cost overruns or
other problems that could seriously harm our business.
We may not succeed in entering into collaborations with
partners at the later stages of developing our product
candidates.
Our business strategy, in part, includes entering into
collaborations, licenses or marketing and distribution
arrangements with corporate partners, primarily pharmaceutical
companies, for later stage development, commercialization,
marketing and distribution of certain of our product candidates.
To date, we have not entered into any collaboration agreements.
We intend to seek collaborators in cases where a product
candidate is not within the endocrine, metabolic or
cardiovascular therapeutic areas or where we think the product
candidate would benefit from the resources of a larger
pharmaceutical company. For instance, because becocalcidiol is
outside our core therapeutic areas, we are evaluating
alternatives for further developing this product candidate,
including seeking a partner for further development and
commercialization. We have been in discussions with potential
partners for becocalcidiol, but have not yet reached an
agreement. We cannot assure you that we will be able to reach an
agreement on commercially reasonable terms, if at all. If we
fail to reach agreement with collaborators, we will have to
incur substantial additional costs to complete development of
our product candidates and begin commercialization. If we
determine that we do not have access to sufficient cash or
funding to meet these costs, we may be forced to stop developing
these product candidates, either temporarily or permanently,
which would adversely affect our business.
If we are successful in entering into collaborations, we will
face the following risks:
•
collaborators may under-fund or not commit sufficient resources
to the testing, marketing, distribution, development or
commercialization of our product candidates;
•
collaborators may fail to perform their obligations with respect
to the testing, marketing, distribution, development or
commercialization of our product candidates;
•
collaborators may not properly maintain or defend our
intellectual property rights, or they may utilize our
proprietary information in such a way as to invite litigation
that could jeopardize or potentially invalidate our proprietary
information or expose us to potential liability;
•
collaborators may encounter conflicts of interest, changes in
business strategy or other business issues, which could
adversely affect their willingness or ability to fulfill their
obligations to us; and
disputes may arise between us and our collaborators delaying or
terminating the research, development or commercialization of
our product candidates, resulting in significant litigation or
arbitration that could be time-consuming and expensive, or
causing collaborators to act in their own self-interest and not
in our interest.
Even if we are able to enter into collaboration arrangements for
our product candidates, we may not be able to maintain these
relationships. If we or a collaborator were to terminate a
collaboration, for breach or otherwise, it could be difficult
for us to attract new collaborators and it could also cause us
to incur additional costs and experience delays in the testing,
marketing, distribution, development or commercialization of our
product candidates. If we were to lose a key collaborator, it
could also adversely affect how we are perceived by the
scientific, business or financial communities.
If we fail to enter into additional in-licensing or
acquisition agreements or if these arrangements are
unsuccessful, our business and operations might be adversely
affected, and if we engage in any acquisition or in-licensing,
we will incur a variety of costs, and we may never realize the
anticipated benefits of the transaction.
Since our inception, we have in-licensed or acquired all of our
product candidates. One of our strategies for expanding our
business is the in-licensing and acquisition of products and
additional product candidates. The success of this strategy
depends upon our ability to identify, select and acquire the
right pharmaceutical product candidates and products. We may be
unable to enter into any additional in-licensing or acquisition
agreements because suitable products or product candidates that
are within our expertise may not be available to us on terms
that are acceptable to us or because competitors with greater
resources seek to in-license the same products or product
candidates. Product candidates that we would like to develop may
not be available to us because they are controlled by
competitors who are unwilling to license the rights to the
product or product candidate to us. If we are unable to enter
into additional agreements to license products or product
candidates, our ability to execute our business strategy could
be adversely affected. Even if we are able to enter into
additional license agreements, these agreements may be
unsuccessful. Further, these license agreements will typically
impose diligence, commercialization and other obligations on us.
If a licensor to any new agreement were to terminate the license
because of our failure to comply with the agreement’s
obligations, we may lose the rights to the product candidate
covered by the license, which could adversely affect our
business prospects.
Although we currently have no commitments or agreements with
respect to any acquisitions, if we undertake an acquisition, the
process of integrating the acquired business, technology,
services, product or programs may result in unforeseen operating
difficulties and expenditures and may divert significant
management attention from our on-going business operations.
Moreover, we may fail to realize the anticipated benefits of any
acquisition for a variety of reasons, such as an acquired
product candidate proving to not be safe or effective in later
clinical trials. We may fund any future acquisition by issuing
equity or equity-linked securities, which could dilute the
ownership percentage of our equity holders. We may also incur
debt to pay for an acquisition. The holders of the debt would
have priority over equity holders in the event of a subsequent
liquidation or bankruptcy, which would impair value for our
equity holders. Acquisition efforts can require substantial
expenditures, which could detract from our other programs. In
addition, we may devote resources to potential acquisitions that
are never completed.
Risks Related to Our Intellectual Property
If we are unable to protect our intellectual property
rights, our competitors may develop and market products with
similar features and our ability to commercialize our potential
products could suffer.
The following factors are important to our success:
•
receiving patent protection for our product candidates;
•
maintaining patent protection for products or product candidates
we have licensed and enforcing our license agreements;
•
preventing others from infringing our intellectual property
rights; and
maintaining our patent and trademark rights and trade secrets.
We will be able to protect our intellectual property rights from
unauthorized use by third parties only to the extent that such
intellectual property rights are covered by valid and
enforceable patents and trademarks or are effectively maintained
as trade secrets. The actual protection afforded by a patent
varies on a product by product basis, from country to country
and depends upon many factors, including the type of patent, the
scope of its coverage, the availability of regulatory related
extensions, the availability of legal remedies in a particular
country and the validity and enforceability of the patents. For
instance, in the case of our product candidate, ospemifene, the
compound is not covered by a composition of matter patent and we
must instead rely on patents covering its use. We have a license
from Orion under its patents covering the use of ospemifene in a
dosage formulation suitable for use in a variety of
pharmaceutical indications. We also have a patent covering the
use of ospemifene for the treatment of climacteric disorders in
women during or after menopause.
We try to protect our proprietary position by filing U.S. and
foreign patent applications related to our important proprietary
technology, inventions and improvements. Because the patent
position of pharmaceutical companies involves complex legal,
administrative and factual questions, the issuance, scope,
validity and enforceability of patents cannot be predicted with
certainty. Patents, if issued, may be challenged, invalidated,
circumvented or rendered unenforceable. U.S. patents and
patent applications may also be subject to interference
proceedings, U.S. patents may be subject to reexamination
or reissue proceedings in the U.S. Patent and Trademark
Office, or PTO, and foreign patents may be subject to opposition
or comparable proceedings in corresponding foreign patent
offices. These proceedings could result in either loss of the
patent or denial of the patent application or loss or reduction
in the scope of one or more of the claims of the patent or
patent application. In addition, such interference,
reexamination, reissue and opposition proceedings may be costly.
Thus, any patents that we own or license from others may not
provide any protection against competitors. Furthermore, an
adverse decision in an interference proceeding can result in a
third party receiving the patent rights sought by us, which in
turn could affect our ability to market a potential product to
which that patent filing was directed.
Our pending patent applications, those we may file in the
future, or those we may license from third parties, may not
result in patents being issued. The issuance of a patent is not
conclusive as to its validity or its enforceability and may not
provide us with proprietary protection or competitive advantages
against competitors with similar compounds. Furthermore, others
may independently develop more effective compounds, designs or
methods. We also rely on third party payment services for the
payment of patent annuities and other fees. Non-payment or delay
in payment of such fees, whether intentional or unintentional,
may result in loss of patents or patent rights important to our
business.
In addition, our ability to enforce our patent rights depends on
our ability to detect infringement. It is difficult to detect
infringers who do not advertise the compounds that are used in
their products. Moreover, it may be difficult or impossible to
detect infringement in a competitor’s or potential
competitor’s product. Any litigation to enforce or defend
our patent rights, even if we were to prevail, could be costly
and time-consuming and would divert the attention of our
management and key personnel from our business operations.
We also rely on our licensors to protect our intellectual
property rights, and if our licensors fail to adequately protect
this intellectual property or if we do not have exclusivity for
the marketing of our products, our ability to commercialize
products could suffer.
We are a party to a number of licenses that give us rights to
third party intellectual property that is necessary for our
business. In some of these cases, our licensors have retained
the right to prosecute and defend the intellectual property
rights licensed to us. In the case of ospemifene, our licensor,
Orion Corporation, has retained the right to prosecute and
maintain the patents licensed from Orion. In the case of
QRX-431, the Regents of the University of California, which
licensed the product candidate to our licensor, EndoChem, Inc.,
has retained the right to prosecute, maintain and jointly pursue
infringement claims against third parties for our licensed
patents. In the case of becocalcidiol, Wisconsin Alumni Research
Foundation,
which licensed the product candidate to our licensor, Deltanoid
Pharmaceuticals, Inc., has retained the right to prosecute,
maintain and pursue infringement claims against third parties
for our licensed patents. We depend in part on the ability of
our licensors to obtain, maintain and enforce patent protection
for our licensed intellectual property. Our licensors may not
successfully prosecute the patent applications that we have
licensed. Even if patents issue in respect of these patent
applications, our licensors may fail to maintain these patents,
may determine not to pursue litigation against other companies
that are infringing these patents, or may pursue such litigation
less aggressively than we would. Without protection for the
intellectual property we license, other companies might be able
to offer substantially identical products for sale, which could
adversely affect our competitive business position and harm our
business prospects.
We are dependent on patents and proprietary technology
licensed from others. If we lose our licenses for any of our
product candidates, we may not be able to continue developing
such product candidates.
We have obtained many of our product candidates pursuant to
licenses that give us rights to third party intellectual
property that is necessary or useful to our business. The
license agreements covering our product candidates impose
various diligence, commercialization, royalty and other
obligations on us. One or more of our licensors may allege that
we have breached our license agreement with them, and
accordingly seek to terminate our license. If we materially
breach the obligations in our license agreements, the licensor
typically has the right to terminate the license and we may not
be able to market products that were covered by the license,
which could adversely affect our competitive business position
and harm our business prospects. In addition, any claims brought
against us by our licensors could be costly and time-consuming
and would divert the attention of our management and key
personnel from our business operations.
Claims that we infringe a third party’s intellectual
property may give rise to burdensome litigation, result in
potential liability for damages or stop our development and
commercialization efforts.
Third parties may assert patent or other intellectual property
infringement claims against us with respect to technologies used
in our potential products. While we have conducted patent
searches to determine whether our product candidates infringe
patents held by third parties, due to the inherent uncertainty
in conducting patent searches, we cannot assure you that all
relevant patents were identified. In addition, we expect that
numerous patent applications are currently pending and may be
filed in the future for products generally related to our
product candidates, including many patent applications that
remain confidential after filing. Due to these factors, we
cannot assure you that our product candidates do not infringe
the patent rights of third parties.
A third party holds an issued United States patent related to
the use of an anti-estrogen for use in the treatment of androgen
deficiency and related disorders. Zonagen, Inc., a
pharmaceutical company also developing a treatment for
testosterone deficiency in men using a compound that is named in
the patent, requested a reexamination of this patent from the
PTO on the grounds that the claims of the third party’s
patent were invalid because they were disclosed in printed
publications before the date of the invention. In June 2005, the
PTO determined that the claims, as amended during this
reexamination, were patentable in view of the publications under
consideration. Zonagen has subsequently stated in its public
filings that it intends to seek further reexamination of this
third party patent based on additional prior art publications
not previously considered by the PTO. If, as a result of this
further reexamination, the patentability of the claims is
confirmed by the PTO, the patent’s scope could cover our
intended use of fispemifene. If Zonagen is not successful in its
attempt to invalidate all of the claims of the patent, our
intended use may be covered by any surviving claims. The patent
holder could bring a claim against us alleging that our
fispemifene product candidate infringes the patent. We believe
we would have valid defenses to any such claim; however,
notwithstanding any defenses we may assert, if such an
infringement claim were successful, we would need to obtain a
license from the patent holder in order to commercialize
fispemifene in the United States. If such a license were
necessary but not available to us on acceptable terms or at all,
we may not be able to commercialize fispemifene at all in the
United States.
The owners or licensees of this or other patents may file one or
more infringement actions against us. Patent litigation can
involve complex factual and legal questions, and its outcome is
uncertain. Any claim
relating to infringement of patents that is successfully
asserted against us may require us to pay substantial damages
for past use of the asserted intellectual property and a royalty
going forward if we are forced to take a license. Even if we
were to prevail, any litigation could be costly and
time-consuming and would divert the attention of our management
and key personnel from our business operations. As a result of a
patent infringement suit brought against us, we may be forced to
stop or delay developing, manufacturing or selling potential
products that are claimed to infringe a third party’s
intellectual property unless that party grants us rights to use
its intellectual property and we may be subject to damages. In
such cases, we may be required to obtain licenses to patents or
proprietary rights of others in order to continue to
commercialize our products. However, we may not be able to
obtain any required licenses on acceptable terms, or at all.
Even if we were able to obtain rights to the third party’s
intellectual property, these rights may be non-exclusive,
thereby giving our competitors access to the same intellectual
property, and any license may be royalty bearing. As a result of
third party claims, we may be forced to redesign or rename our
products to avoid infringing the intellectual property rights of
third parties, which may not be possible and could be costly and
time-consuming if it is possible to do. Ultimately, we may be
unable to commercialize some of our product candidates or may
have to discontinue development of product candidates or cease
some of our business operations as a result of patent
infringement claims or due to our failure to license essential
technology, which could severely diminish our commercial
prospects and harm our financial condition.
We are subject to the patent laws of countries other than
the United States, which may not offer the same level of patent
protection and may require us to pay royalties to employee
inventors that are not yet determinable.
Many countries, including certain countries in Europe, have
compulsory licensing laws under which a patent owner may be
compelled to grant licenses to third parties (for example, the
patent owner has failed to “work” the invention in
that country, or the third party has patented improvements). In
addition, many countries limit the enforceability of patents
against government agencies or government contractors. In these
countries, the patent owner may have limited remedies, which
could materially diminish the value of the patent. Moreover, the
legal systems of certain countries, particularly certain
developing countries, do not favor the aggressive enforcement of
patent and other intellectual property protection which makes it
difficult to stop infringement.
Under Finnish law, current and former employees of Hormos are
entitled to “fair and reasonable compensation” upon
commercialization of intellectual property developed by them and
transferred to Hormos. Hormos has a policy in place for the
calculation of the royalties due to employees that we believe
conforms to the statutory requirements. The potential royalty
payments depend on the type of assignment and the stage of
development of the invention, among other things. We believe
that all current employees of Hormos are bound by the policy of
Hormos which determines the amount of royalties due. However,
under Finnish law, an employee cannot be bound to accept a
certain level of compensation before the invention is made,
therefore Hormos may be required to negotiate “fair and
reasonable compensation” with its former employees if the
inventions of these former employees are ever commercialized. An
employee has a ten-year period, calculated from the date when
Hormos acquired the rights from the employee, to make claims
based on the employee’s inventions. Current and former
employees may seek royalties that are not acceptable to us, or
may refuse to accept our offer or may challenge the formula
itself. In case of an impasse in the negotiations, the parties
have the right under Finnish law to bring a claim in front of a
special “employee invention board” with
representatives of both employer and employee organizations. We
have no experience in these types of proceedings, and any
determination adverse to us, such as the imposition of a royalty
payment that we believe is excessive, could increase our
expenses.
We rely on trade secrets and other forms of non-patent
intellectual property protection. If we are unable to protect
our trade secrets, other companies may be able to compete more
effectively against us.
We also rely on trade secrets, know-how and technology, which
are not protected by patents, to maintain our competitive
position. We try to protect this information by entering into
confidentiality agreements with parties that have access to it,
such as our strategic partners, collaborators, employees and
consultants. Any of these parties may breach these agreements
and we may not have adequate remedies for any specific breach.
In addition, our trade secrets may otherwise become known or be
independently discovered by competitors. To the extent that our
commercial partners, collaborators, employees and consultants
use intellectual property owned by others in their work for us,
disputes may arise as to the rights in related or resulting
know-how and inventions. If any of our trade secrets, know-how
or other technologies not protected by a patent were to be
disclosed to or independently developed by a competitor, our
business, financial condition and results of operations could be
materially adversely affected.
We may be subject to damages resulting from claims that we
or our employees have wrongfully used or disclosed alleged trade
secrets of their former employers.
Many of our employees were previously employed at other
biotechnology or pharmaceutical companies, including our
competitors or potential competitors. Although no claims against
us are currently pending, we may be subject to claims that these
employees or we have inadvertently or otherwise used or
disclosed trade secrets or other proprietary information of
their former employers. Litigation may be necessary to defend
against these claims. Even if we are successful in defending
against these claims, litigation could result in substantial
costs and be a distraction to management. If we fail in
defending such claims, in addition to paying money claims, we
may lose valuable intellectual property rights or personnel. A
loss of key personnel or their work product could hamper or
prevent our ability to commercialize certain product candidates,
which would adversely affect our commercial development efforts.
Risks Related to Our Industry
Competition in the biotechnology and pharmaceutical
industries is intense, and even if our product candidates are
approved and commercialized, competitive products may impede
market acceptance of our products.
Our business is characterized by extensive research and
development efforts, rapid developments and intense competition.
Our competitors may have or may develop superior technologies or
approaches to treat the diseases or conditions targeted by our
product candidates, which may provide them with competitive
advantages. Our product candidates may not compete successfully.
The success of our product candidates will depend upon factors
such as product efficacy, safety, reliability, availability,
timing, scope of regulatory approval, acceptance and price,
among other things. If our competitors enter the marketplace
before we do with less expensive or favorably differentiated
drugs, our product candidates, if approved for
commercialization, may not be profitable to sell or continue to
develop.
Pharmaceutical technologies have undergone rapid and significant
change, and we expect that they will continue to do so. Any
compounds, products or processes that we develop may become
obsolete or uneconomical before we recover any expenses incurred
in connection with their development.
If ospemifene and fispemifene are approved and commercialized,
they will have significant competition. Vaginal atrophy is
generally treated with estrogen-based therapies, either oral or
topical, such as Premarin, Prempro and Premarin Vaginal Cream,
marketed by Wyeth, and Vagifem, marketed by Novo Nordisk. Other
products in development for this condition include bazedoxifene,
being developed by Wyeth, and Oporia, being developed by Pfizer,
which are both SERMs. Testosterone deficiency is most frequently
treated with topical gels or patches, such as Solvay
Pharmaceuticals’ Androgel and Watson Pharma’s
Androderm. Products in development include Acapodene and
Ostarine, both being developed by GTx and Androxal, being
developed by Zonagen.
If QRX-401 and
QRX-431 are approved
and commercialized, they will also have significant competition.
In the treatment of lipid disorders, statins are the most
frequently prescribed products, examples of which include
Lipitor, marketed by Pfizer, Zocor and Mevacor, both marketed by
Merck & Co., Crestor, marketed by AstraZeneca and
Pravachol, marketed by Bristol-Myers Squibb. Other competitors
include non-statin products, such as Zetia, marketed by
Merck/Schering-Plough, Tricor, marketed by Abbott, and Niaspan,
marketed by Kos; combinations of statins with other agents, for
example Vytorin, marketed by Merck/Schering-Plough and Advicor,
marketed by Kos; and new products in development, such as
KaroBio’s KB2115.
Becocalcidiol, if approved and commercialized, will face
competition from several marketed topical psoriasis products or
products under development, specifically topical calcitriol
analogues. These include Dovonex, marketed by Warner Chilcott,
Taclonex, to be marketed by Warner Chilcott,tisocalcitate, in development by Schering AG, and CTA018, in
development by Cytochroma.
Most of our competitors, including many of those listed above,
have substantially greater capital resources, research and
development staffs, facilities and experience in conducting
clinical trials and obtaining regulatory approvals, as well as
in manufacturing and marketing pharmaceutical products. As a
result, they may achieve earlier product commercialization or
patent protection. In addition to the branded competitive
products listed above, if our product candidates receive
regulatory approval they may face competition from generic
drugs, and the availability of generic drugs may adversely
affect the market for our products.
Any drugs we develop may become subject to unfavorable
third party reimbursement practice, pricing regulations or
health care reform initiatives, thereby harming our
business.
The commercial success of our product candidates is
substantially dependent on whether third party reimbursement is
available for our product candidates. Medicare, Medicaid, health
maintenance organizations and other third party payors may not
cover or provide adequate payment for our potential products.
They may not view our product candidates as cost-effective and
reimbursement may not be available to consumers or may not be
sufficient to allow our potential products to be marketed on a
competitive basis. Changes in reimbursement policies or health
care cost containment initiatives that limit or restrict
reimbursement for our products may cause our revenue to decline.
Legislative or regulatory efforts to control or reduce health
care costs or reform government health care programs could
result in lower prices or rejection of product candidates that
we may commercialize. Federal legislation enacted in December
2003 added an outpatient prescription drug benefit to Medicare,
effective January 2006. In the interim, Congress has established
a discount drug card program for Medicare beneficiaries. Both
benefits will be provided primarily through private entities,
which will attempt to negotiate price concessions from
pharmaceutical manufacturers. These negotiations may increase
pressure to lower prescription drug prices. While the new law
specifically prohibits the U.S. government from interfering
in price negotiations between manufacturers and Medicare drug
plan sponsors, some members of Congress are pursuing legislation
that would permit the U.S. government to use its enormous
purchasing power to demand discounts from pharmaceutical
companies, thereby creating de facto price controls on
prescription drugs. In addition, the new law contains triggers
for Congressional consideration of cost containment measures for
Medicare in the event Medicare cost increases exceed a certain
level. These cost containment measures could include limitations
on prescription drug prices. This Medicare prescription drug
coverage legislation, as well as additional healthcare
legislation that may be enacted at a future date, could reduce
our sales and adversely affect our results of operations.
Another development that may affect the pricing of drugs is
Congressional action regarding drug reimportation into the
United States. The Medicare Prescription Drug Plan legislation,
which became law in December 2003, requires the Secretary of
Health and Human Services to promulgate regulations for drug
reimportation from Canada into the United States under some
circumstances, including when the drugs are sold at a lower
price than in the United States. The Secretary retains the
discretion not to implement a drug reimportation plan if he
finds that the benefits do not outweigh the cost. Proponents of
drug reimportation may attempt to pass legislation that would
directly allow reimportation under certain circumstances. If
legislation or regulations were passed allowing the
reimportation of drugs, they could decrease the price we receive
for any products that we may develop, negatively affecting our
anticipated revenues and prospects for profitability.
State pharmaceutical marketing compliance and reporting
requirements may expose us to regulatory and legal action by
state governments or other government authorities.
In recent years, several states, including California, Maine,
Minnesota, New Mexico, Vermont and West Virginia, have enacted
legislation requiring pharmaceutical companies to establish
marketing compliance
programs and file periodic reports with the state on sales,
marketing, pricing and other activities. For example, California
has enacted a statute requiring pharmaceutical companies to
adopt a comprehensive compliance program that is in accordance
with the Office of Inspector General of the Department of Health
and Human Services Compliance Program Guidance for
Pharmaceutical Manufacturers. This compliance program must
include policies for compliance with the Pharmaceutical Research
and Manufacturers of America Code on Interactions with
Healthcare Professionals, as well as a specific annual dollar
limit on gifts or other items given to individual healthcare
professionals in California. The law requires posting policies
on a company’s public web site along with an annual
declaration of compliance.
Maine, Minnesota, New Mexico, Vermont and West Virginia have
also enacted statutes of varying scope that impose reporting and
disclosure requirements upon pharmaceutical companies pertaining
to drug pricing and payments and costs associated with
pharmaceutical marketing, advertising and promotional
activities, as well as restrictions upon the types of gifts that
may be provided to healthcare practitioners. Similar legislation
is being considered in other states. Many of these requirements
are new and uncertain and the penalties for failure to comply
with these requirements are unclear.
We face potential product liability exposure far in excess
of our limited insurance coverage.
The use of any of our product candidates in clinical trials, and
the sale of any approved products, may expose us to product
liability claims. These claims might be made directly by
consumers, health care providers, pharmaceutical companies or
others selling our products. We have obtained limited product
liability insurance coverage for our clinical trials. However,
our insurance may not reimburse us or may not be sufficient to
reimburse us for expenses or losses we may suffer. Moreover,
insurance coverage is becoming increasingly expensive, and we
may not be able to maintain insurance coverage at a reasonable
cost or in sufficient amounts to protect us against losses due
to liability. If we obtain marketing approval for any of our
product candidates, we intend to expand our insurance coverage
to include the sale of commercial products, but we may be unable
to obtain commercially reasonable product liability insurance
for any products approved for marketing. On occasion, juries
have awarded large judgments in class action lawsuits based on
drugs that had unanticipated side effects. In addition, the
pharmaceutical and biotechnology industries, in general, have
been subject to significant product liability litigation. A
product liability claim or series of claims brought against us
would decrease our cash reserves and could cause our stock price
to fall, and, if a claim against us is successful, it could have
a material adverse effect on our financial condition.
If we do not comply with laws regulating the protection of
the environment and health and human safety, our business could
be adversely affected.
Our research and development involves the use of hazardous
materials and chemical compounds. We maintain quantities of
various toxic chemicals in our facilities in Finland that are
required for our research and development activities. We believe
our procedures for storing, handling and disposing of these
materials in our Finnish facility comply with the standards
mandated by applicable Finnish laws and guidelines. Although we
believe that our safety procedures for handling and disposing of
these materials comply with the standards mandated by applicable
regulations, the risk of accidental contamination or injury from
these materials cannot be eliminated. If an accident occurs, we
could be held liable for resulting damages, which could be
substantial. We are also subject to numerous environmental,
health and workplace safety laws and regulations, including
those governing laboratory procedures, exposure to blood-borne
pathogens and the handling of biohazardous materials.
We may not be able to conduct, or contract with others to
conduct, animal testing in the future, which could harm our
research and development activities.
Certain laws and regulations relating to drug development
require us to test our product candidates on animals before
initiating clinical trials involving humans. The preclinical
trials for certain of our product candidates have involved, for
instance, experiments with monkeys,
mini-pigs, guinea pigs,
rabbits, mice, dogs and rats. Animal testing activities have
been the subject of controversy and adverse publicity. Animal
rights groups and other organizations and individuals have
attempted to stop animal testing activities by pressing for
legislation and regulation in these areas and by disrupting
these activities through protests and other means. To the extent
the activities of these groups are successful and we or our
contract research organizations are unable to conduct animal
testing, our research and development activities may be
interrupted or delayed.
Risks Related to Our Common Stock
We expect that our stock price will fluctuate
significantly.
Prior to this offering, you could not buy or sell our common
stock publicly. An active public market for our common stock may
not develop or be sustained after this offering. We will
negotiate and determine the initial public offering price with
the underwriters based on several factors. This price may vary
from the market price of our common stock after this offering.
You may be unable to sell your shares of common stock at or
above the initial offering price. The market price of
pharmaceutical and biotechnology stocks is subject to
significant volatility. The volatility of pharmaceutical and
biotechnology stocks often does not relate to the operating
performance of the companies represented by the stock. Factors
that could cause volatility in the market price of our common
stock include:
•
the timing and the results from our clinical trial programs;
•
the timing and results from our preclinical studies;
•
the discovery, in-licensing or acquisition of additional product
candidates;
•
FDA or international regulatory actions;
•
failure of any of our product candidates, if approved, to
achieve commercial success;
•
announcements of new products by our competitors;
•
market conditions in the pharmaceutical and biotechnology
sectors;
any public concern about the safety of our potential products;
•
comments by securities analysts;
•
actual and anticipated fluctuations in our quarterly operating
results;
•
deviations in our operating results from the estimates of
securities analysts;
•
rumors relating to us or our competitors;
•
additions or departures of key personnel;
•
third party reimbursement policies; and
•
developments concerning current or future strategic alliances.
These and other factors may cause the market price and demand
for our common stock to fluctuate substantially, which may limit
or prevent investors from readily selling their shares of common
stock and may otherwise negatively affect the liquidity of our
common stock. In addition, in the past, when the market price of
a stock has been volatile, holders of that stock have instituted
securities class action litigation against the company that
issued the stock. If any of our stockholders brought a lawsuit
against us, we could incur substantial costs defending the
lawsuit. Such a lawsuit could also divert the time and attention
of our management.
Upon the issuance of additional securities or the exercise
of outstanding options, the ownership interests of our existing
stockholders will be diluted. In addition, future sales of
common stock by us or our stockholders may cause our stock price
to fall.
We may issue additional securities to raise capital or make
acquisitions. We also have made and expect to continue to make
grants of stock options to retain and motivate employees,
officers and directors. Upon the issuance of additional
securities and options and the exercise of outstanding options,
your percentage ownership may be diluted both in terms of book
value and voting percentage. In addition, the market price of
our common stock could decline as a result of issuances by us,
or sales by our existing stockholders, of shares of common stock
in the market following the completion of this offering, or the
perception that these sales could occur. The
lock-up agreements with
Banc of America Securities LLC executed by us, our executive
officers and directors and substantially all of our stockholders
and optionholders, provide that Banc of America Securities LLC
may release those parties, at any time or from time to time and
without notice, from their obligation not to dispose of shares
of common stock for a period of 180 days after the date of
this prospectus (which period could be extended for up to an
additional 34 days under certain circumstances). Banc of
America Securities LLC has no pre-established conditions to
waiving the terms of the
lock-up agreements. Any
decision by it to waive those conditions would depend on a
number of factors, which may include market conditions, the
performance of our common stock in the market and our financial
condition at that time. Based on shares outstanding at
December 31, 2005, we will
have shares
of common stock outstanding upon the completion of this
offering. This includes
the shares
of common stock that we are selling in this offering, which may
be resold in the public market immediately. The
remaining shares,
or %
of our outstanding common stock upon completion of this
offering, will be restricted as a result of securities laws or
lock-up agreements.
Based on shares outstanding as of December 31, 2005, taking
into account the
lock-up agreements, and
assuming Banc of America Securities LLC does not release
stockholders from these agreements prior to the expiration of
the 180-day
lock-up period, the
following shares will be eligible for sale in the public market
at the following times:
•
shares
that are not subject to the
lock-up agreements
discussed above may be sold immediately after completion of this
offering;
•
additional
shares that are not subject to the
180-day
lock-up period
described above may be sold beginning 90 days after the
effective date of the offering; and
•
additional
shares may be sold upon expiration of the
180-day
lock-up period
described above.
Following the expiration of the
lock-up period, holders
of
approximately shares
of our common stock will have the right to require us to
register these shares under the Securities Act pursuant to a
registration rights agreement. See “Description of Capital
Stock — Registration Rights.”
Our directors and management will exercise significant
control over our company.
After this offering, our directors and executive officers and
their affiliates will collectively control
approximately %
of our outstanding common stock, assuming that the
underwriters’ over-allotment is not exercised. These
stockholders, if they act together, will be able to influence
our management and affairs and all matters requiring stockholder
approval, including the election of directors and approval of
significant corporate transactions. This concentration of
ownership may have the effect of delaying or preventing a change
in control of our company and might affect the market price of
our common stock.
We will have broad discretion in how we use the proceeds
of this offering, and we may not use these proceeds effectively,
which could affect our results of operations and cause our stock
price to decline.
We will have considerable discretion in the application of the
net proceeds of this offering. We currently intend to use the
net proceeds of this offering for general corporate purposes,
including clinical trials, research and development expenses,
general and administrative expenses, and potential acquisitions
of companies, products and technologies that complement our
business. We have not yet finalized the amount of
net proceeds that we will use specifically for each of these
purposes. We may use the net proceeds for corporate purposes
that do not yield a significant return or any return at all for
our stockholders.
Provisions of Delaware law or our charter documents could
delay or prevent an acquisition of our company, even if the
acquisition would be beneficial to our stockholders, and could
make it more difficult for you to change management.
Provisions of our certificate of incorporation and bylaws may
discourage, delay or prevent a merger, acquisition or other
change in control that stockholders may consider favorable,
including transactions in which stockholders might otherwise
receive a premium for their shares. This is because these
provisions may prevent or frustrate attempts by stockholders to
replace or remove our current management or members of our board
of directors.
These provisions include:
•
a classified board of directors;
•
a prohibition on stockholder action through written consent;
•
a requirement that special meetings of stockholders be called
only by the Chairman of the board of directors, the Chief
Executive Officer, or the board of directors pursuant to a
resolution adopted by a majority of the total number of
authorized directors;
•
advance notice requirements for stockholder proposals and
nominations;
•
a requirement that
662/3%
of stockholders approve certain amendments to our certificate of
incorporation and amendments to our bylaws; and
•
the authority of the board of directors to issue preferred stock
with such terms as the board of directors may determine.
As a result, these provisions and others available under
Delaware law could limit the price that investors are willing to
pay in the future for shares of our common stock.
We have never paid dividends on our capital stock, and we
do not anticipate paying any dividends in the foreseeable
future.
We have paid no dividends on any of our classes of capital stock
to date and we currently intend to retain our future earnings,
if any, to fund the development and growth of our businesses. In
addition, our secured loan agreement prohibits us from paying
cash dividends. As a result, capital appreciation, if any, of
our common stock will be your sole source of gain for the
foreseeable future.
Investors in this offering will pay a much higher price
than the book value of our common stock.
If you purchase common stock in this offering, you will pay more
for your shares than the amounts paid by existing stockholders
for their shares. You will incur immediate and substantial
dilution of
$ per
share, representing the difference between our pro forma as
adjusted net tangible book value per share after giving effect
to this offering and an assumed initial public offering price of
$ per
share. In the past, we issued options and warrants to acquire
common stock at prices significantly below the assumed initial
public offering price. To the extent these outstanding options
or warrants are ultimately exercised, you will sustain further
dilution.
This prospectus, including the sections entitled
“Prospectus Summary,”“Risk Factors,”“Management’s Discussion and Analysis of Financial
Condition and Results of Operations” and
“Business,” contains forward-looking statements.
Forward-looking statements include, but are not limited to,
statements about:
•
the progress, timing and completion of our research, development
and clinical trials for product candidates;
•
our ability to successfully complete preclinical studies;
•
our receipt of regulatory approvals;
•
our ability to market, commercialize and achieve market
acceptance for product candidates;
•
our ability to contract for and maintain third party
manufacturing services;
•
whether any product candidates we commercialize are safer or
more effective than other marketed products, treatments or
therapies;
•
our ability to enter into collaborative or strategic
relationships to assist in the clinical development or
commercialization of our product candidates;
•
our ability to maintain the licenses relating to our product
candidates or in-license or acquire new product candidates;
•
our ability to protect our intellectual property and operate our
business without infringing upon the intellectual property
rights of others;
•
our ability to build an internal sales and marketing
infrastructure;
•
implementation of our business strategy;
•
our use of the proceeds from this offering;
•
our estimates for future operating and financial
performance; and
•
our estimates regarding anticipated operating losses, future
revenues, capital requirements and our needs for additional
financing.
These statements relate to future events or our future financial
performance, and involve known and unknown risks, uncertainties
and other factors that may cause our actual results, levels of
activity, performance or achievements to be materially different
from any future results, levels of activity, performance or
achievements expressed or implied by these forward-looking
statements. These risks and other factors include those listed
under “Risk Factors” and elsewhere in this prospectus.
In some cases, you can identify forward-looking statements by
terminology such as “may,”“will,”“should,”“expects,”“intends,”“plans,”“anticipates,”“believes,”“estimates,”“predicts,”“potential,”“continue” or the negative of these terms or other
comparable terminology. Although we believe that the
expectations reflected in the forward-looking statements are
reasonable, we cannot guarantee future results, levels of
activity, performance or achievements. We undertake no duty to
update any of the forward-looking statements after the date of
this prospectus or to conform these statements to actual
results. Neither the Private Securities Litigation Reform Act of
1995 nor Section 27A of the Securities Act of 1933 provides
any protection for statements made in this prospectus.
We estimate that we will receive net proceeds from the sale of
shares of our common stock in this offering of approximately
$ million
($ million
if the underwriters exercise their over-allotment option in
full), based upon an assumed initial public offering price of
$ per
share and after deducting underwriting discounts and commissions
and estimated offering expenses payable by us.
We currently intend to use the proceeds of this offering to fund
the growth of our business and for general corporate purposes.
We estimate that we will use the proceeds of this offering as
follows:
•
approximately $20 million for continued phase III
clinical development of ospemifene
•
approximately $10 million for continued phase II
clinical development and initiation of phase III clinical
development of fispemifene
•
approximately $11 million for further clinical development
of becocalcidiol,
QRX-401 and
QRX-431.
•
the remainder for working capital and other general corporate
purposes, which may include the repayment of debt and
in-licensing or acquiring product candidates.
A $1.00 increase (decrease) in the assumed initial public
offering price of
$ per
share (the mid-point of the range on the cover page of this
prospectus) would increase (decrease) the net proceeds to us
from this offering by
$ million,
assuming the number of shares offered by us, as set forth on the
cover page of this prospectus, remains the same and after
deducting the estimated underwriting discounts and commissions
and estimated offering expenses payable by us.
As of the date of this prospectus, we cannot predict with
certainty all of the particular uses for the proceeds of this
offering or the amounts that we will actually spend on the uses
set forth above. The amounts that we actually expend for these
purposes may vary significantly depending on a number of
factors. The amounts and timing of our expenditures will depend
on numerous factors including the results of our research and
development efforts, the timing and success of preclinical
testing, the timing and success of clinical trials, the timing
of regulatory submissions, the amount of proceeds actually
raised in this offering and the amount of cash, if any,
generated by collaboration agreements. We may change the
allocation of use of proceeds as a result of contingencies such
as the progress and results of our clinical trials and other
research and development activities, the establishment of
collaborations and regulatory or competitive developments. As a
result, management will retain broad discretion over the
allocation of the net proceeds from this offering. We have no
current plans, agreements or commitments for acquisition of any
businesses, products, or technologies.
We do not expect the net proceeds from this offering to be
sufficient to fund the completion of the development of any of
our product candidates and we expect that we will need to raise
additional funds prior to being able to market any products.
Pending use of the net proceeds of this offering, we intend to
invest the net proceeds in accordance with our investment policy
guidelines, which provide for investment of funds in cash
equivalents, United States government obligations, high grade
municipal and corporate notes and commercial paper.
DIVIDEND POLICY
We have never declared or paid cash dividends on our capital
stock. We do not anticipate paying any cash dividends on our
capital stock in the foreseeable future. We currently intend to
retain all available funds and any future earnings to fund the
development and growth of our business.
The following table sets forth our capitalization as of
December 31, 2005:
•
on an actual basis;
•
on a pro forma basis, reflecting the conversion of all of our
preferred stock into an aggregate of 61,230,251 shares of
common stock immediately prior to the closing of this
offering; and
•
on a pro forma as adjusted basis, reflecting the pro forma
adjustment noted above and reflecting (1) the required
release upon the closing of this offering of
3,446,305 shares of common stock held in escrow in
connection with the Hormos acquisition, including
1,066,274 shares of common stock issued upon the conversion
of 1,066,274 shares of preferred stock held in such escrow,
and (2) the sale
of shares
of common stock in this offering at an assumed initial public
offering price of
$ per
share, after deducting underwriting discounts and commissions
and estimated offering expenses payable by us.
You should read this table in conjunction with the sections of
this prospectus entitled “Selected Consolidated Financial
Data” and “Management’s Discussion and Analysis
of Financial Condition and Results of Operations” and with
our financial statements and related notes.
Redeemable convertible preferred stock, $0.01 par value;
actual, 70,060,092 shares authorized,
60,422,374 shares issued and outstanding; pro forma and pro
forma as adjusted, no shares authorized, no shares issued and
outstanding
86,200
—
Stockholders’ equity (net capital deficiency):
Common stock, $0.01 par value; actual, 94,919,416 shares
authorized and 14,490,473 shares issued and outstanding;
pro forma, 94,919,416 shares authorized and
75,720,724 shares issued and outstanding; pro forma as
adjusted, shares authorized
and shares issued and outstanding
145
757
Additional paid-in capital
—
85,588
Deferred compensation
(285
)
(285
)
Deficit accumulated during the development stage
(67,522
)
(67,522
)
Accumulated other comprehensive income
872
872
Total stockholders’ equity (net capital deficiency)
The actual number of shares of common stock shown as issued and
outstanding in the table above excludes:
•
5,576,671 shares of common stock issuable upon the exercise
of options outstanding as of December 31, 2005, with
exercise prices ranging from $0.20 to $0.35 per share and a
weighted average exercise price of $0.31 per share;
•
1,604,269 additional shares of common stock reserved for future
grants under our Amended and Restated 2005 Stock Incentive Plan
as of December 31, 2005; and
•
shares issuable upon the exercise of a warrant issued by us in
connection with a credit facility we entered into in January
2006, with respect to which the number of underlying shares and
exercise price will be established at the closing of this
offering pursuant to a formula agreed upon with the lender.
Under this formula, at an assumed initial public offering price
of
$ per
share and assuming a closing date
of ,
2006, this warrant would be exercisable
for shares
of common stock at an exercise price of
$ per
share.
In addition, the amounts of cash and debt in the table above
exclude $6.0 million we borrowed pursuant to a credit
facility we entered into in January 2006.
Our historical net tangible book value as of December 31,2005 was approximately
$( ) million,
or
$ per
share, based
on shares
of common stock outstanding as of December 31, 2005.
Historical net tangible book value per share is determined by
dividing our total tangible assets less total liabilities and
convertible preferred stock by the actual number of outstanding
shares of our common stock. Our pro forma net tangible book
value as of December 31, 2005 was approximately
$ million,
or approximately
$ per
share, based
on shares
of common stock outstanding after giving effect to the
conversion of all outstanding shares of our convertible
preferred stock into common stock upon the closing of this
offering.
After giving effect to our sale
of shares
of common stock in this offering based on an assumed initial
public offering price of
$ per
share, less underwriting discounts and commissions and offering
expenses payable by us, the conversion of the outstanding shares
of convertible preferred stock into common stock and the release
of shares held in escrow in connection with our Hormos
acquisition, our pro forma as adjusted net tangible book value
as of December 31, 2005 would have been
$ per
share. This represents an immediate increase in net tangible
book value per share of
$ to
existing stockholders and immediate dilution in net tangible
book value of
$ per
share to new investors purchasing our common stock in the
offering at the initial public offering price. Dilution per
share to new investors is determined by subtracting pro forma as
adjusted net tangible book value per share after this offering
from the assumed initial public offering price per share paid by
a new investor. The following table illustrates the per share
dilution without giving effect to the over-allotment option
granted to the underwriters:
Assumed initial public offering price per share
$
Historical net tangible book value per share as of
December 31, 2005
$
( )
Increase per share due to the conversion of all shares of
preferred stock
Pro forma as adjusted net tangible book value per share after
the offering
Dilution per share to new investors
$
A $1.00 increase (decrease) in the assumed initial public
offering price of
$ per share (the
mid-point of the range on the cover page of this prospectus)
would increase (decrease) our pro forma as adjusted net tangible
book value by
$ million, the pro
forma as adjusted net tangible book value per share after this
offering by $ and the dilution per share to new investors
by $ , assuming the
number of shares offered by us, as set forth on the cover page
of this prospectus, remains the same and after deducting the
estimated underwriting discounts and commissions and estimated
offering expenses payable by us.
The following table summarizes on a pro forma basis, as of
December 31, 2005, the number of shares of our common stock
purchased from us, the total cash consideration paid to us and
the average price per share paid to us by existing stockholders
and to be paid by new investors purchasing shares of our common
stock
in this offering, before deducting underwriting discounts and
commissions and estimated offering expenses payable by us:
Total
Shares Purchased
Consideration
Average Price
Number
%
Amount
%
Per Share
Existing stockholders
$
%
$
%
$
New investors
Total
$
%
$
%
$
If the underwriters exercise their over-allotment option in
full, our existing shareholders will
own %
and our new investors will
own %
of our shares of common stock outstanding after this offering.
The above discussion and tables are based on
14,490,473 shares of common stock issued and outstanding as
of December 31, 2005 and excludes:
•
5,576,671 shares of common stock issuable upon the exercise
of options outstanding as of December 31, 2005, with
exercise prices ranging from $0.20 to $0.35 per share and a
weighted average exercise price of $0.31 per share;
•
1,604,269 additional shares of common stock reserved for future
grants under our Amended and Restated 2005 Stock Incentive Plan,
as of December 31, 2005; and
•
shares issuable upon the exercise of a warrant issued by us in
connection with a credit facility we entered into in January
2006, with respect to which the number of underlying shares and
exercise price will be established at the closing of this
offering pursuant to a formula agreed upon with the lender.
Under this formula, at an assumed initial public offering price
of
$ per
share and assuming a closing date
of ,
2006, this warrant would be exercisable
for shares
of common stock at an exercise price of
$ per
share.
To the extent the outstanding options are, or the warrant is,
exercised, you will experience further dilution. In addition, we
may choose to raise additional capital due to market conditions
or strategic considerations even if we believe we have
sufficient funds for our current or future operating plans. To
the extent that additional capital is raised through the sale of
equity or convertible debt securities, the issuance of these
securities could result in further dilution to our stockholders.
You should read the selected consolidated financial data
presented below in conjunction with our consolidated financial
statements and the related notes and “Management’s
Discussion and Analysis of Financial Condition and Results of
Operations” included elsewhere in this prospectus. The
selected consolidated financial data presented below for the
years ended December 31, 2003, 2004 and 2005 and for the
period from inception (November 20, 2000) to
December 31, 2005 and as of December 31, 2004 and
2005, have been derived from our audited consolidated financial
statements included elsewhere in this prospectus. The selected
consolidated financial data for the years ended
December 31, 2001 and 2002 and as of December 31,2001, 2002 and 2003, have been derived from our audited
consolidated financial statements not included in this
prospectus. Historical results are not necessarily indicative of
the results of operations to be expected for future periods.
The pro forma consolidated statement of operations data for the
year ended December 31, 2005 give effect to the acquisition
of Hormos as if the acquisition occurred on January 1, 2005
and should be read in conjunction with our Unaudited Pro Forma
Combined Financial Statements included elsewhere in this
prospectus.
Accretion of redeemable convertible preferred stock
(147
)
(390
)
(1,504
)
(2,320
)
(13,210
)
(13,210
)
(17,571
)
Net loss available to common stockholders
$
(741
)
$
(3,780
)
$
(10,468
)
$
(11,624
)
$
(52,931
)
$
(29,028
)
$
(79,544
)
Net Loss Per Share, Basic and Diluted:
Loss per share available to common stockholders
$
(1.25
)
$
(6.30
)
$
(7.57
)
$
(4.79
)
$
(5.77
)
Shares used to compute basic and diluted net loss per share
595,068
600,000
1,382,723
2,425,592
9,179,723
Pro forma basic and diluted net loss per share available to
common stockholders(1)
$
(0.91
)
Shares used to compute pro forma basic and diluted net loss per
share
58,213,187
(1)
Pro forma basic and diluted net loss per common shares is
calculated to give effect to the conversion of all outstanding
shares of our preferred stock into 61,230,251 shares of
common stock upon the completion of this offering, excluding
1,066,274 shares of preferred stock held in escrow in
connection with the Hormos acquisition that will convert into
common stock upon the completion of this offering.
You should read the following discussion of our financial
condition and results of operations in conjunction with the
financial statements and the notes to those statements included
elsewhere in this prospectus. This discussion contains
forward-looking statements that involve risks and uncertainties.
As a result of many factors, such as those set forth under the
section entitled “Risk Factors” and elsewhere in this
prospectus, our actual results may differ materially from those
anticipated in these forward-looking statements.
Overview
We are a pharmaceutical company focused on discovering,
licensing, developing and commercializing compounds in the
endocrine, metabolic and cardiovascular therapeutic areas. We
currently have four product candidates in clinical development
and one compound that we expect to enter clinical development in
the first half of 2006. Our two lead product candidates treat
hormone deficiencies that result from aging in men and women. We
also have two product candidates for the treatment of elevated
cholesterol levels, one in phase I and one in advanced
preclinical development. Becocalcidiol, our topical product
candidate for the treatment of mild to moderate psoriasis, has
completed a phase IIb clinical trial. In addition to our
drug development programs, we have two research programs for
targeted endocrine therapies.
Our strategy is to build and maintain a portfolio of product
candidates; utilize focused criteria to select product
candidates that we believe have a high likelihood of clinical
success; focus on product candidates that have a large
commercial opportunity; and develop product candidates in
therapeutically aligned areas. In certain cases, we expect that
we will build our own sales and marketing infrastructure to
market some of our products. In other cases, we expect that we
will enter into collaborations to develop and commercialize
product candidates that are either not in our core therapeutic
areas or for which the sales and marketing infrastructure
required to maximize the value of the product is larger than is
practical for a company of our size.
In May 2005, we completed the acquisition of Hormos Medical Oy,
a privately held Finnish company focused on discovering and
developing novel pharmaceutical compounds involving the tissue
specific regulation of estrogen effects for the treatment of
certain age-related diseases. In connection with the acquisition
of Hormos, which was accounted for as a purchase of assets and
assumption of liabilities, we assumed $20.3 million in
liabilities and debt and issued 857,145 shares of our
Series D Preferred Stock, 3,408,025 shares of our
Series D-1 Preferred Stock, and 9,520,154 shares of
our common stock, collectively valued at $8.8 million.
Contingent consideration associated with the acquisition
includes an additional 321,415 shares and
1,277,995 shares of Series D and
Series D-1
Preferred Stock, respectively, and 3,570,046 shares of
common stock, held in escrow and payable upon the occurrence of
certain future events. One-third of the contingent shares secure
indemnification obligations of the Hormos selling shareholders
and will be released to the Company in satisfaction of an
indemnification claim or to the Hormos shareholders one year
after the closing date of the acquisition. The remaining
contingent shares will generally be released to Hormos selling
shareholders upon the first to occur of the closing of a
qualified public offering of our common stock, including this
offering, or the dosing of the first patient in a second
phase III clinical trial of ospemifene. Additional purchase
consideration will be recorded as the contingent consideration
is released. The additional purchase consideration will be
allocated to the assets acquired based upon their relative fair
value and will result in additional expense for in-process
research and development and the accrued contingent
consideration totaling $1.6 million will be reclassified to
stockholders’ equity. The operating results of Hormos are
included in our results of operations as of the May 2005 date of
acquisition.
Most of our expenditures to date have been to license and
develop our product candidate portfolio. Research and
development expenditures through December 31, 2005
primarily were related to the licensing and development of
ospemifene and fispemifene, our product candidates for the
treatment of hormone deficiencies in aging women and men, and
QRX-401 and
QRX-431, our product
candidates for treating
elevated cholesterol levels, and becocalcidiol, our psoriasis
product candidate. We outsource a substantial portion of our
preclinical study efforts and our clinical trial and
manufacturing development activities to third parties to
maximize efficiency and minimize our internal overhead.
Since our inception in November 2000, we have generated
significant losses while we in-licensed, acquired and advanced
our product candidates and research programs. To date, we have
not generated significant product revenues and have funded our
operations primarily through proceeds of $71.2 million from
private placements of preferred stock. As of December 31,2005, we had an accumulated deficit of $67.5 million.
Historically, Hormos has used Finnish government sponsored loans
which bear below-market interest rates to help fund its
operations. We assumed these loans as part of our acquisition of
Hormos and we intend to continue to apply for additional loans
in the future.
We expect to incur substantial and increasing losses for the
next several years as we expand our research and development
activities and move our product candidates into later stages of
development and potential commercialization. These efforts
include:
•
our ongoing phase III clinical trials for ospemifene, our
product candidate for the treatment of vaginal atrophy, a
common, chronic condition of post-menopausal women;
•
our ongoing phase II clinical trials for fispemifene, our
product candidate for the treatment of the symptoms of
andropause;
•
continued clinical development of
QRX-401, a non-statin
compound for lowering LDL cholesterol and lipoprotein(a);
•
IND filing for and clinical development of
QRX-431, also a
non-statin compound for lowering LDL cholesterol and
lipoprotein(a), with phase I clinical trials expected to
begin in 2006;
•
additional development of becocalcidiol, a topical treatment for
mild to moderate psoriasis;
•
advancement of our preclinical research programs for targeted
endocrine therapies;
•
acquisition or in-licensing of additional technology or products
which complement our portfolio; and
•
preparations for commercialization.
International Operations
As of February 1, 2006, we had 58 employees located in
the United States and Finland. We coordinate program management,
drug development, clinical and regulatory activities from our
corporate offices in Ann Arbor, Michigan and our drug discovery
effort primarily is conducted in Turku and Oulu, Finland.
Research and Development
Since our inception, we have been focused primarily on drug
development programs. Our research and development expenses
include:
•
employee expenses, including salaries and benefits;
•
formulation and synthesis costs of our product candidates;
•
third-party manufacturing costs;
•
licensing payments;
•
preclinical study costs including toxicology study costs;
•
clinical trial costs;
•
costs related to the regulatory approvals process; and
Due to the significant risks and uncertainties inherent in the
research, clinical development and regulatory approval
processes, the cost and time to complete projects in research
and development is difficult to estimate. Our patient enrollment
may be slower than expected, the results from research and
clinical trials may not be favorable or the FDA, or other
regulatory agencies, may require additional trials. Further,
data from clinical trials is subject to varying interpretation
and may be deemed insufficient by the regulatory bodies
reviewing applications for marketing approvals. As such,
research, clinical development and regulatory programs are
subject to risks and changes that may significantly impact our
cost projections and development timelines.
Most of our product development programs are at an early stage;
therefore, the successful development of our product candidates
is highly uncertain and may not result in approved products.
Product candidates that may appear promising at early stages of
development may not reach the market for a number of reasons.
Product candidates may be found ineffective or cause harmful
side effects during clinical trials, may take longer to progress
through clinical trials than anticipated, may fail to receive
necessary regulatory approvals or may prove impractical to
manufacture in commercial quantities at reasonable cost and with
acceptable quality. We rely on third parties to conduct our
clinical trials. If these third parties do not perform as
contractually required or expected, we may not be able to obtain
regulatory approval for or commercialize our product candidates.
The lengthy process of seeking regulatory approvals requires the
expenditure of substantial resources. Any failure by us to
obtain, or any delay in obtaining, regulatory approvals could
materially adversely affect our product development efforts. Our
strategy includes entering into collaborations with third
parties to participate in the development and commercialization
of at least some of our product candidates. We cannot forecast
with certainty which of our product candidates, if any, will be
subject to future collaborations, when any such collaborations
may occur, or how such arrangements would affect our development
plans or capital requirements. As a result of these
uncertainties, we are unable to determine the timing, duration
and completion costs of our research and development projects or
when and to what extent we will generate revenues from the
commercialization and sale of any of our product candidates.
Research and Development Cost Allocations
We have many research and development projects ongoing at any
one time and we have the ability to utilize our financial and
human resources across several research and development
projects. Our internal resources, employees and infrastructure
are not directly tied to any individual research or development
project and are typically deployed across multiple projects. We
generally do not record or maintain information regarding
internal costs incurred for our research and development
programs on a program specific basis. Management generally
evaluates research and development projects based on outsourced
research and development costs. During the period from inception
through December 31, 2005, we incurred costs of
approximately $5.6 million for outsourced research and
development costs related to becocalcidiol, $11.0 million
for QRX-401,
$2.5 million for
QRX-431, and
$3.5 million for all other programs.
Critical Accounting Policies
The preparation of our consolidated financial statements
requires us to make estimates and assumptions that affect the
reported amounts of assets and liabilities and the disclosure of
contingent assets and liabilities at the date of our financial
statements as well as the reported revenues and expenses. We
base our estimates on historical experience and on various other
factors that we believe are reasonable under the circumstances,
the results of which form the basis for making judgments about
the carrying value of assets and liabilities that are not
readily apparent from other sources. Actual results may differ
from these estimates under different assumptions or conditions.
While our significant accounting policies are described in
Note 1 to our financial statements appearing at the end of
this prospectus, we believe the following critical accounting
policies are important to understanding and evaluating our
reported financial results.
Accrued Expenses. As part of the process of preparing
financial statements, we are required to estimate accrued
expenses. This process involves communicating with appropriate
personnel to identify services that
have been performed on our behalf and estimating the scope of
service performed and the associated cost incurred when we have
not yet been invoiced or otherwise notified of the actual cost.
The majority of our service providers invoice us monthly in
arrears for services performed. We make estimates of our accrued
expenses as of each balance sheet date in our financial
statements based on facts and circumstances known to us.
Examples of our estimated accrued expenses include:
•
fees paid to contract research organizations for preclinical and
toxicology studies and clinical trials;
•
fees paid to investigative sites in connection with clinical
trials;
•
fees paid to contract manufacturers in connection with the
production of clinical trial materials; and
•
professional service fees.
We base our expenses related to clinical trials on our estimates
of the services received and efforts expended pursuant to
contracts with multiple research institutions and clinical
research organizations that conduct and manage clinical trials
on our behalf. The financial terms of these agreements are
subject to negotiation, vary from contract to contract, and may
result in uneven payment flows. Payments under some of these
contracts depend on factors such as the successful enrollment of
patients and the completion of clinical trial milestones. In
accruing service fees, we estimate the time period over which
services will be performed and the level of effort to be
expended in each period. If the actual timing of the performance
of services or the level of effort varies from our estimate, we
will adjust the accrual accordingly. If we do not identify costs
that we have begun to incur or if we underestimate or
overestimate the level of services, our actual expenses could
differ from our estimates.
Valuation of Intangibles and Other Long-lived Assets. We
are required to periodically assess the impairment of
intangibles and other long-lived assets which requires us to
make assumptions and judgments regarding the carrying value of
these assets. The assets are considered to be impaired if we
determine that the carrying value may not be recoverable based
upon our assessment of the following events or changes in
circumstances:
•
a determination that the carrying value of such assets can not
be recovered through undiscounted cash flows;
•
loss of legal ownership or title to the assets;
•
significant changes in our strategic business objectives and
utilization of the assets; or
•
the impact of significant negative industry or economic trends.
If the assets are considered to be impaired, the impairment we
recognize is the amount by which the carrying value of the
assets exceeds the fair value of the assets. In addition, we
base the useful lives and related amortization or depreciation
expense on our estimate of the useful life of the assets. If a
change were to occur in any of the factors or estimates above,
the likelihood of a material change in our reported results
would increase.
Stock-based Compensation. We account for employee stock
options using the intrinsic-value method in accordance with
Accounting Principles Board, or APB, Opinion No. 25,
Accounting for Stock Issued to Employees, and Financial
Accounting Standards Board Interpretation, or FIN, No. 44,
Accounting for Certain Transactions Involving Stock
Compensation, an Interpretation of APB No. 25, and have
adopted the disclosure-only provisions of Statement of Financial
Accounting Standards, or SFAS No. 123, Accounting for
Stock-Based Compensation.
The information regarding net loss as required by
SFAS No. 123, presented in Note 1 to our
financial statements, has been determined as if we had accounted
for our employee stock options under the fair value method of
SFAS No. 123. The resulting effect on net loss to date
pursuant to SFAS No. 123 is not likely to be
representative of the effects on net loss pursuant to
SFAS No. 123(R), which will be effective for years
beginning January 1, 2006, since future years are likely to
include additional grants and the irregular impact of future
years’ vesting and because of the differing requirements of
SFAS No. 123(R).
Stock-based compensation for options granted to employees is
measured as the excess, if any, of the estimated fair value of
our common stock on the date the options were granted above the
exercise price of the option. Given the absence of an active
market for our common stock, the fair value of our common stock
has periodically been estimated using several criteria,
including progress and milestones achieved in our business
development and performance, the price per share of our
convertible redeemable preferred stock offerings, estimates of
the sale value of our company to a buyer, estimates of a
potential price per share in an initial public offering of our
common stock and, beginning in November 2004, periodic
contemporaneous independent valuations.
For stock options granted to non-employees, the fair value of
the stock options is estimated using the Black-Scholes valuation
model. This model utilizes the estimated fair value of common
stock and requires that, at the date of grant, we make
assumptions with respect to the expected life of the option, the
volatility of the fair value of our common stock, risk-free
interest rates and expected dividend yields of our common stock.
We have to date assumed that non-employee stock options have an
expected life of four years, representing about half of their
contractual life, and assumed common stock volatility of 70%.
Higher estimates of volatility and expected life of the option
increase the value of an option and the resulting expense.
Purchased In-process Research and Development. In our
acquisition of Hormos, we acquired technology that we expect to
utilize in our research and development activities. We account
for the costs associated with acquired technology in accordance
with FASB Statement No. 2, Accounting for Research and
Development Costs. Under this standard, we are required to
determine whether the technology relating to a particular
research and development project we acquire has an alternative
use. If we determine that the technology has no alternative
uses, the amount is expensed as incurred. Otherwise, the costs
are capitalized and amortized over their estimated useful life.
In conjunction with our acquisition of Hormos, we determined
that in-process research and development with respect to
ospemifene and fispemifene had no alternative use and we
recorded an expense of $25.8 million in the second quarter
of 2005 to write-off the fair value of this purchased in-process
research and development. The fair value of each of the
in-process research and development projects was determined on
an income-based approach which attempts to estimate the
income-producing capability of the asset.
Results of Operations
The comparisons which follow compare actual results for the
applicable periods and do not reflect any pro forma adjustments
for our acquisition of Hormos in May 2005. The results of Hormos
are included in our financial results from the date of
acquisition.
Research and Development Expenses. We group our research
and development activities into three major categories:
“outsourced research and development,”“research
and development operations,” and “license fees.”
Outsourced research and development costs include the cost of
clinical research organizations and third party manufacturing
costs. The costs from research and development operations
consist primarily of salaries and employee benefits for our
research and development staff and related travel and support
costs. License fees consist of fees and milestone payments due
to licensors of our product candidates. Of the total
research and development expenses for the year ended
December 31, 2005 and 2004, the costs associated with
outsourced research and development, research and development
operations and license fees were:
Outsourced research and development expenses increased
$6.7 million in 2005 compared to 2004. This increase is due
primarily to higher costs as
QRX-401 advanced in
phase I clinical trials,
QRX-431 entered
toxicology and other preclinical studies, and work began on
ospemifene and fispemifene in preparation for phase III and
phase II studies, respectively. We acquired ospemifene and
fispemifene as a result of the Hormos acquisition in May 2005.
Expenses in 2004 primarily consisted of clinical trials for
becocalcidiol and preclinical and clinical development of
QRX-401.
Expenses from our research and development operations increased
$1.7 million in 2005 compared to 2004. The increase in
expenses in 2005 is largely related to increased employee
expenses, particularly salaries and benefits, as we added
research and development operations personnel to work on and
manage the increased number and size of research projects and
development programs in 2005.
License fees paid by us decreased by $1.0 million in 2005
compared to 2004. License fees and milestone payments for
product candidates we have in-licensed vary widely from compound
to compound. Milestone payments usually are dependent on the
successful advancement of the licensed compound to
pre-determined milestones. License fees in 2005 relate to fees
for initial licensing of
QRX-431, while license
fees in 2004 are comprised of a milestone payment for
QRX-401.
General and Administrative Expenses. General and
administrative expenses consist primarily of salaries and
benefits for administrative, finance, business development and
legal personnel. In addition, general and administrative
expenses include insurance costs, professional services and
facilities costs. General and administrative expenses increased
$1.5 million to $3.2 million in 2005 compared to
$1.7 million in 2004. The increase in 2005 primarily
resulted from additional personnel and the related increase in
salaries, benefits and facilities expenses as the scope of our
operations expanded in 2005.
Purchased In-process Research and Development. In
connection with the acquisition of Hormos and in accordance with
the related valuation and purchase price allocation of Hormos,
we determined that $25.8 million of the purchase price
related to in-process research and development that had not
reached technological feasibility and had no alternative future
use. The principal technology we acquired related to ospemifene
and fispemifene. Accordingly, we recorded an expense of
$25.8 million in the second quarter of 2005 to write-off
the fair value of this acquired in-process research and
development. The fair value of each of the in-process research
and development projects was determined on an income-based
approach which attempts to estimate the income-producing
capability of the asset.
Contract Research Income.Contract research income of
$1.4 million in 2005 primarily consists of contract
research performed for a pharmaceutical company by Hormos. There
were no corresponding amounts for the same period in 2004.
Interest Income. Interest income increased by
$0.7 million to $0.8 million in 2005 compared to
$0.1 million in 2004. The increase was due to higher
average cash balances and higher prevailing interest rates in
2005.
Interest Expense. Interest expense of $0.6 million
in 2005 consists of interest incurred on debt held by Hormos.
Hormos holds loans from agencies of the Finnish government that
bear interest at below-market
rates. In connection with the acquisition of Hormos and in
accordance with the related purchase price allocation, the loans
were recorded at their estimated fair value which resulted in a
discount of $2.1 million. The discount is being amortized
over the lives of the underlying loans. Amortization expense
related to this discount totaled $0.3 million in 2005 and
is recorded as interest expense. There were no corresponding
amounts for the same period in 2004.
Forgiveness of Debt. Forgiveness of debt totalled
$2.7 million in 2005. In December 2005, loans to Hormos,
including principal and accrued interest, from two Finnish
government agencies were forgiven because the related research
project did not reach commercial feasibility. There were no
similar amounts in 2004.
Research and Development Expenses. Research and
development expenses decreased $0.6 million to
$7.7 million in 2004 from $8.4 million in 2003. The
decrease largely resulted from the $2.5 million initial
licensing fee paid for
QRX-401 and related
compounds in 2003. The following table summarizes the changes in
the components of research and development expense between 2003
and 2004.
Outsourced research and development expenses increased $21,000
in 2004. The increase reflects continuing clinical development
of becocalcidiol and preclinical and clinical work on
QRX-401 and related
compounds. Phase I clinical studies for
QRX-401 began in the
second quarter of 2004 with single-dose studies using a small
number of volunteers. Phase II clinical trials for
becocalcidiol began in 2003 and continued in 2004.
Expenses from our research and development operations increased
$0.3 million in 2004 compared to 2003. The increase in
expenses in 2004 was largely related to increased employee
related expenses, particularly salaries and benefits, as we
added research and development operations personnel to work on
and manage the increased number and size of research projects
and development programs in 2004.
License fees decreased by $1.0 million in 2004. License
fees in 2004 related to a milestone payment for
QRX-401, while license
fees in 2003 were comprised of initial in-licensing fees for
QRX-401 and related
compounds.
General and Administrative Expenses. General and
administrative expenses increased $0.8 million to
$1.7 million in 2004 compared to $0.9 million in 2003.
The increase in 2004 primarily resulted from additional
personnel and the related increase in salaries and benefits
expenses as the scope of our operations expanded in 2004.
Consulting Income. No consulting activity was undertaken
by us in 2004. Consulting income of $0.2 million in 2003
consisted of fees received for study design consultation we
performed for an unrelated company.
Interest Income. Interest income increased by $71,000 to
$144,000 in 2004 from $73,000 in 2003. The increase was due
largely to higher average cash balances.
Due to our significant research and development expenditures and
the lack of approved products to generate revenue, we have not
been profitable and have generated operating losses since we
were incorporated in November 2000. We have funded our
operations primarily through sales of our convertible preferred
stock. As of December 31, 2005, we had received aggregate
net proceeds of $71.2 million from sales of preferred
stock. As of December 31, 2005, we had unrestricted cash
and cash equivalents and short-term investments of
$36.0 million compared to $31.1 million as of
December 31, 2004. In addition, as of December 31,2005 we had $0.1 million of cash deposits with a financial
institution collateralizing a letter of credit in favor of our
landlord in the event of a breach of our Ann Arbor, Michigan
facility lease which expires in 2011.
Hormos historically has financed a portion of its research and
development activities with loans and grants from Finnish
governmental agencies, Tekes and Sitra, as well as contract
research, fees from a product license arrangement and interest
earned on investments. The Finnish government loans are granted
on a project-by-project basis and generally carry interest at
below-market rates. If a project fails or does not reach
commercial success, under certain circumstances repayment of the
loan can be forgiven. At the date of acquisition, Hormos had
$15.1 million in principal and accrued interest relating to
loans from Finnish governmental agencies and $2.4 million
in advances related to future loans, which we assumed. The loans
carry interest at 1% to 3% below the Finnish base rate as set by
the Bank of Finland at the date the loan was issued with a
minimum interest rate of 1% to 3%. The loans are unsecured and
generally are subordinated with a loan period of seven to ten
years. Generally, the first several years of the loan are free
of repayment. Under applicable Finnish law, interest or
principal related to the notes can only be repaid when the
company has adequate equity capital. Because Hormos lacks the
requisite equity capital, no amounts outstanding under these
loans are currently repayable. We intend to continue to pursue
this source of funding in the future though we cannot assure you
that the funding will continue to be available.
In December 2005, Tekes notified Hormos that repayment would not
be required for certain loans totaling $2.6 million,
including principal and accrued interest, associated with a
research project which did not reach commercial feasibility.
Also in December 2005, Sitra notified Hormos that a loan
totaling $0.1 million, including principal and accrued
interest, would not be required to be repaid. The forgiveness of
these loans has been included in other income in 2005.
In January 2006, we entered into an $18.0 million debt
agreement with Hercules Technology Growth Capital, a third-party
lender, and borrowed $6.0 million under the agreement with
$12.0 million available for future borrowings through the
end of 2006. Loans under the agreement bear interest at prime
plus 3% with interest-only payments due during the first
12 months of each loan. Principal is repaid over
36 months after the interest-only period, with a balloon
payment due at the end of the repayment period. Loans under the
agreement are collateralized by substantially all of our assets
other than our intellectual property rights. In addition, the
debt agreement contains covenants restricting our ability to
incur further indebtedness, pay dividends or make investments,
subject to exceptions specified in the agreement. In connection
with the debt agreement, we issued a warrant to the lender to
purchase shares of our preferred stock, which will convert to a
warrant for common stock upon the completion of this offering.
The number of shares and exercise price in the warrant will be
determined by a formula based on the timing and price of the
next round of equity invested in our company, which we expect to
be this offering. The warrant is exercisable for seven years
from the date of issue, or three years after an initial public
offering of our common stock.
Our policy is to invest in cash equivalents,
U.S. government obligations, high-grade municipal and
corporate notes and commercial paper. Our investment objectives
are, primarily, to assure liquidity and preservation of capital
and, secondarily, to obtain investment income. Wherever
possible, we seek to minimize the potential effects of
concentration and degrees of risk. All of our investments in
debt securities are recorded as available-for-sale and are
recorded at cost plus accrued interest which approximates fair
value due to their short duration.
Net cash used in operating activities increased
$7.0 million to $16.0 million in 2005 compared to
$9.0 million in 2004. The increase in cash used in
operations in 2005 is due to a higher net loss from increased
operating costs as QRX-401 advanced in phase I clinical
trials, QRX-431 was licensed and entered toxicology and other
preclinical trials and as work began on ospemifene and
fispemifene, in preparation for phase III and phase II
studies, respectively.
Net cash used in investing activities increased
$28.6 million to $28.7 million in 2005 compared to
2004. Underlying the increase in use of cash for investing
activities in 2005 were $28.5 million of net purchase of
short-term investments, $1.0 million used for acquisition
costs, $1.0 million acquired in the acquisition of Hormos
and $0.2 million used in the purchase of property and
equipment. Cash used in investing activities for the same period
in 2004 consisted of $39,000 for purchases of property and
equipment.
Net cash provided by financing activities decreased by
$8.9 million in 2005 compared to 2004. The decrease
resulted primarily from lower sales or issuances of preferred
stock in 2005.
Net cash used in operating activities increased
$0.9 million to $9.0 million in 2004 compared to
$8.2 million in 2003. The increase in cash used in
operations is due primarily to drug development and clinical
trial expenses associated with QRX-401 and becocalcidiol.
Net cash used in investing activities increased
$0.8 million to $39,000 in 2004 compared to net cash
provided by investing activities of $0.8 million in 2003.
This increase resulted primarily from reduced maturities of our
short-term investments in 2004 compared to 2003.
Net cash provided by financing activities increased
$13.1 million in 2004 compared to 2003. The increase in
2004 is due to proceeds of approximately $29.6 million from
the sale of shares of our Series C and D Preferred Stock in
2004 compared with proceeds of approximately $16.6 million
from the sale of shares of our Series B and C Preferred
Stock in 2003.
Our future contractual obligations at December 31, 2005
were as follows:
Payments Due by Period
Total
2006
2007-2008
2009-2010
After 2010
(in thousands)
Capital lease obligations
$
20
$
20
$
—
$
—
$
—
Operating lease obligations
5,808
1,025
2,000
1,999
784
Long-term debt
11,672
3,215
4,773
2,807
877
Total fixed contractual obligations
$
17,500
$
4,260
$
6,773
$
4,806
$
1,661
Our capital lease obligations include remaining payments due in
2006 on equipment acquired by Hormos through capital leases.
Our commitments under operating leases consist of payments
relating to our real estate leases in Ann Arbor, Michigan
and real estate leases in Finland, which generally expire in
2010 and 2011, respectively. Hormos is a party to five separate
real estate leases of office and laboratory space in Turku,
Finland and Oulu, Finland. Two of these Hormos leases are
long-term leases through 2011 which require monthly payments
totaling approximately $0.8 million annually. The remaining
Hormos facility leases require 15 months or less to
terminate and have monthly payments totaling approximately
$28,000 annually.
We have entered into a number of license agreements for our
product candidates. Generally these license agreements include
initial licensing payments, milestone payments, royalties on
future sales and patent maintenance costs. Future milestone
payments are generally due on the achievement of certain
development and regulatory milestones. Future milestone
obligations under licensing agreements total $59.2 million,
including a date-specific milestone payment of $0.1 million
due in 2006. The achievement and timing of reaching prescribed
milestones under these agreements and determination of royalties
on future sales is uncertain.
Our long-term debt consists of loans to Hormos from Finnish
governmental agencies. At the time of our acquisition of Hormos
in May 2005, it had $15.1 million in loans from Finnish
governmental agencies, Tekes and Sitra, and $2.4 million in
advances related to future Tekes loans, which we assumed. The
loans are unsecured and generally are subordinated with a loan
period of seven to ten years. Generally, the first several years
of the loan are free of repayment. Under applicable Finnish law,
interest or principal related to the notes can only be repaid
when the company has adequate equity capital. Because Hormos
lacks the requisite equity capital, no amounts outstanding under
these loans are currently repayable. In December 2005, Tekes
notified Hormos that repayment would not be required for certain
loans totaling $2.6 million, including principal and
accrued interest, associated with a research project which did
not reach commercial feasibility. Also in December 2005, Sitra
notified Hormos that a loan totaling $0.1 million,
including principal and accrued interest, would not be required
to be repaid.
Funding Requirements
We expect to devote substantial resources to continue our
research, development and commercialization efforts. Our funding
requirements will depend on a number of forward-looking factors.
These factors include, but are not limited to, the following:
•
the progress of preclinical development and clinical trials;
•
the number of product candidates we pursue or the expansion of
existing product candidates to new indications;
•
the discovery, in-licensing or acquisition of additional
technologies or product candidates that require financial
commitments;
•
the time and costs involved in obtaining regulatory approvals,
and the number of different regulatory agencies we seek approval
from;
delays that may be caused by evolving requirements of regulatory
agencies;
•
our plans to establish sales, marketing and distribution
capabilities;
•
the cost and timing of securing manufacturing capabilities for
our product candidates and commercial products, if any;
•
the terms and timing of any collaborative, licensing and other
arrangements we may establish;
•
the costs involved in filing, maintaining and prosecuting patent
applications and enforcing or defending patent claims;
•
our revenues, if any, from successful development and
commercialization of our products;
•
the costs of being a public company; and
•
the number of additional employees we hire.
Following completion of this offering we anticipate incurring
increased general and administrative expenses for directors and
officers insurance, investor relations and professional fees
associated with operating as a publicly traded company.
Increases in general and administrative expenses will also
likely include the hiring of additional personnel.
We believe that our existing capital resources, including
available borrowings of up to $12.0 million under our
existing debt facility, and the net proceeds from this offering,
together with interest thereon, will be sufficient to meet our
projected operating requirements for at least the next
18 months. We have based this estimate on assumptions that
may prove to be wrong, and we could utilize our available
capital resources sooner than we currently expect. Our
projection of financial requirements involves risks and
uncertainties and actual results could vary as a result of a
number of factors.
If we need to raise funds in the future, we may be required to
raise those funds through public or private financings,
strategic relationships or other arrangements. We also intend to
continue to pursue loans from Finnish government agencies. We
cannot assure you that these funding sources, if needed, will be
available on terms attractive to us, or at all. Furthermore, any
additional equity financing may be dilutive to stockholders and
debt financing, if available, may involve restrictive covenants.
To the extent that we raise additional capital through licensing
arrangements or arrangements with collaborative partners, we may
be required to relinquish, on terms that are not favorable to
us, rights to some of our technologies or product candidates
that we would otherwise seek to develop or commercialize
ourselves. Our failure to raise capital as and when needed could
have a negative impact on our financial condition and our
ability to pursue our business strategy.
Recent Accounting Pronouncements
In December 2004, the Financial Accounting Standards Board
issued SFAS No. 123(R), Share-based Payment,
which amends SFAS No. 123. The standard set forth in
SFAS No. 123(R) requires that all share-based payments
to employees, including grants of employee stock options, be
recognized in the consolidated financial statements of
operations based on their fair values. The pro forma disclosure
previously permitted under SFAS No. 123 will not be an
acceptable alternative to recognition of expenses in the
financial statements. The standard is effective for public
companies for annual periods beginning after June 15, 2005.
The adoption of SFAS No. 123(R) may have a material
impact on our results of operations and net loss per share. We
are currently in the process of evaluating the extent of such
impact.
Off-Balance Sheet Arrangements
Since inception, we have not engaged in any off-balance sheet
activities, including the use of structured finance, special
purpose entities, or variable interest entities.
Quantitative and Qualitative Disclosure About Market Risk
The primary objective of our investment activities is to
preserve principal. We also seek to maximize income from our
investments without incurring significant risk. Some of the
securities we invest in may have
market risk. This means that a change in prevailing interest
rates may cause the principal amount of the marketable
securities to fluctuate. To minimize this risk, we maintain our
portfolio of cash, cash equivalents, and short-term investments
in a variety of interest-bearing instruments, including United
States government and agency securities, high-grade corporate
bonds, commercial paper, and money market funds. We have not
used derivative financial instruments for speculation or trading
purposes. Due to the short duration of our investment portfolio,
we believe an immediate 10% change in interest rates would not
be material to our financial condition or results of operations.
Historically, our Finnish subsidiary’s costs and expenses
have been primarily denominated in Euros. Approximately 30% of
the projected costs and expenses for 2006 of our Finnish
subsidiary are denominated in Euros. If exchange rates
change 10%, the impact on our net loss and cash used in
operations would be $0.7 million. We do not hedge our
foreign currency exposures.
We are a pharmaceutical company focused on discovering,
licensing, developing and commercializing compounds in the
endocrine, metabolic and cardiovascular therapeutic areas. We
currently have four product candidates in clinical development
and one compound that we expect to enter clinical development in
the first half of 2006. Our two lead product candidates treat
hormone deficiencies that result from aging in men and women.
Ospemifene, our treatment for vaginal atrophy, a common problem
associated with estrogen deficiency in post-menopausal women, is
in phase III clinical testing. Fispemifene, our treatment
for the symptoms of andropause in aging males, has recently
entered phase II clinical testing. We also have two product
candidates for the treatment of elevated cholesterol levels,
QRX-401 and
QRX-431, in
phase I clinical trials and advanced preclinical
development, respectively. Becocalcidiol, our topical product
candidate for the treatment of mild to moderate psoriasis, has
completed a phase IIb clinical trial. Our management team
has extensive experience in pharmaceutical development,
particularly in endocrine and cardiovascular therapies, having
participated in over 60 clinical development programs in their
careers. This team has contributed to over 30 programs involving
approved drugs, ten of which reached annual sales in excess of
$1 billion according to PharmaKey and include the
world’s best selling pharmaceutical product, Lipitor.
Our Strategy
Our goal is to build a successful pharmaceutical company that
develops and commercializes products in the endocrine, metabolic
and cardiovascular therapeutic areas. Our strategy is to
leverage our extensive management expertise in order to:
•
Build and maintain a portfolio of product candidates. We
believe that taking a portfolio approach to drug development
balances risk by reducing our dependence on any one product
candidate’s clinical or commercial success. Our objective
is to have between three and five product candidates in clinical
development at any time. We also seek to maintain a portfolio of
product candidates at different stages of development in order
to ensure that our clinical pipeline continues to have multiple
product candidates.
•
Utilize focused criteria to select product candidates that we
believe have a high likelihood of clinical success. Our
management team has experience in all aspects of developing and
commercializing drugs, including preclinical development,
regulatory strategy, clinical trial management and
commercialization. Part of our strategy is to utilize these
skills to identify and in-license or acquire product candidates
that we believe will have a high likelihood of success. We seek
product candidates that:
•
have measurable, objective
clinical endpoints that provide the ability to demonstrate proof
of concept in human subjects early in the development process;
•
have established precedents for
regulatory approval; and
•
fall within the areas of expertise
of the management team.
•
Focus on product candidates that have a large commercial
opportunity. We seek product candidates that will provide a
substantial return on our investment. To achieve these returns
we seek to identify and develop product candidates that meet the
following criteria:
•
serve large markets with unmet
medical needs;
•
are favorably differentiated from
existing therapies; and
•
have a sufficiently long period of
exclusivity to justify development.
•
Develop product opportunities in therapeutically aligned
areas. We focus on developing treatments for endocrine,
metabolic and cardiovascular therapeutic diseases. We believe
that by having product candidates in therapeutically aligned
areas we will be best positioned to leverage our clinical
development expertise and regulatory knowledge. In addition,
concentration in therapeutically aligned areas gives us the
opportunity in the future to build sales and marketing
infrastructure that can be utilized to sell multiple products.
Using this strategy, we have built our current portfolio of four
clinical stage product candidates and an advanced preclinical
program. As we continue to build our company, we intend to
extend our strategy by:
•
Developing our current portfolio of product candidates;
•
Leveraging our management expertise to expand our product
pipeline;
•
Utilizing out-licensing and partnering opportunities, when
appropriate;
•
Continuing to build our management capacity and capabilities as
our needs expand; and
•
Developing sales and marketing capabilities, either on our own
or in partnership with others, in order to commercialize our
product candidates and maximize their value.
Our Product Pipeline
The following table summarizes our product pipeline:
Product Candidate
Initial Indication
Development Stage
Marketing Rights
Ospemifene
Vaginal Atrophy
Phase III
Worldwide*
Fispemifene
Symptoms of Andropause
Phase II
Worldwide*
QRX-401
Elevated LDL
Phase I
Worldwide
QRX-431
Elevated LDL
Preclinical
Worldwide
Becocalcidiol
Mild to Moderate Psoriasis
Phase II
Worldwide
*
Subject to our licensor’s right to negotiate exclusive
marketing rights in Denmark, Estonia, Finland, Iceland, Latvia,
Lithuania, Norway, Russia and Sweden.
Ospemifene — A Treatment for Vaginal
Atrophy
Description of Condition
In North America, Europe and Japan, Scrip Reports estimates that
in 2000 there were 145 million post-menopausal women, a
number that is projected to increase as the median age of the
population increases. Post-menopausal women suffer from a number
of conditions as a result of a decline in estrogen levels. These
conditions include decreased bone density, known as
osteoporosis, hot flashes and vaginal atrophy. It is estimated
that between 10% and 40% of post-menopausal women suffer from
vaginal atrophy according to the medical journal Clinical
Geriatrics.
Vaginal atrophy is a common, chronic condition of
post-menopausal women and is characterized by vaginal dryness,
burning, irritation, itching, vaginal discharge and feeling of
pressure. Dryness and irritation accompanying decreases in
vaginal secretions and lubrication can often cause pain and/or
bleeding during sexual intercourse. Associated urinary symptoms
can include urinary frequency, pain on urination, urinary tract
infections and incontinence. In contrast to hot flashes, which
eventually disappear, vaginal atrophy persists as women age.
Vaginal atrophy results from a decline in estrogen levels that
causes thinning of the vaginal cell lining. This condition leads
to a fragile vaginal mucous membrane characterized by decreased
elasticity, paleness and disappearance of the small folds found
in the vaginal wall. Vaginal secretions and blood flow to the
vagina decrease, resulting in decreased lubrication. The decline
in estrogen levels also leads to an increase in vaginal pH,
creating an environment more susceptible to infection.
Ospemifene is our product candidate for the treatment of vaginal
atrophy. We have completed two phase II clinical trials of
ospemifene in which it has demonstrated beneficial effects on
vaginal cell maturation, indicating improvement in vaginal
atrophy symptoms in post-menopausal women. Based on our
completed clinical studies, ospemifene demonstrated beneficial
effects on the symptoms of vaginal atrophy and, based on
preclinical studies, positive effects on bone density. In
addition, in a completed phase II clinical trial,
ospemifene did not increase the frequency of hot flashes when
compared to placebo. In January 2006, we initiated our first
phase III clinical trial of ospemifene for vaginal atrophy.
The trial is expected to take place in approximately 60 sites in
the U.S. and will enroll approximately 800 patients.
Ospemifene is differentiated from hormone replacement therapies
such as estrogen. Ospemifene is a next generation selective
estrogen receptor modulator, or SERM, which is a small molecule
that selectively binds to estrogen receptors and either
stimulates or blocks estrogen’s activity in different
tissue types. SERMs block the actions of estrogen in certain
tissues by occupying the estrogen receptors that transmit
signals for cells to grow and divide. SERMs in development have
been shown to mimic estrogen’s beneficial action in bone
tissue but do not stimulate estrogen’s harmful effects in
the breast and uterus which increases the risk of cancer.
Market Opportunity
Hormone replacement therapy has long been the standard treatment
for menopause related conditions, including vaginal atrophy.
Hormone replacement therapy consists of treatment using
medications containing one or more female hormones, most
commonly estrogen and progestin.
Hormone replacement therapy is effective in alleviating symptoms
of vaginal atrophy but, after long-term use, increases the risk
of breast and uterine cancer. In 1991, the National Heart, Lung
and Blood Institute of the National Institutes of Health
(NIH) launched the Women’s Health Initiative, a
15-year
U.S. national health study involving over 161,000 women
aged 50 to 79. The Women’s Health Initiative focused on
strategies for preventing heart disease, breast cancer,
colorectal cancer and osteoporosis in healthy post-menopausal
women and included two clinical trials designed to test the
effects of oral estrogen plus progestin and of oral estrogen
alone on heart disease, osteoporotic fractures and breast and
colorectal cancer risk. These studies were stopped early in July
2002 and February 2004, respectively, as the accumulated
evidence suggested the overall health risks of long-term hormone
replacement therapy outweighed the benefits from the therapy.
In 2004, U.S. hormone replacement therapies sales for
menopausal conditions were approximately $1.7 billion
according to IMS Health. This represents a 30% decline from the
level of sales prior to publication of the findings of the
clinical studies from the Women’s Health Initiative.
According to IMS Health, sales of hormone replacement products
containing estrogen alone dropped from $1.5 billion in 2002
to $1.1 billion in 2004 in the United States, although
still accounting for approximately 75% of total 2004 oral
hormone replacement prescriptions. Estrogen therapy is often
combined with other hormones, typically progestin, which is used
to decrease the estrogen-related risk of uterine cancer. These
combination therapies constituted approximately 25% of all U.S.
oral hormone replacement prescriptions and had U.S. sales
of $391 million in 2004, down from sales of approximately
$783 million in 2002 according to IMS Health.
Women and their physicians seeking alternatives to systemic
hormone replacement therapies to treat vaginal atrophy typically
turn to topical prescription-based hormone treatments. These
products include vaginal delivery of estrogen in the form of
creams, medicated vaginal suppositories and a hormone-releasing
ring. Sales in the U.S. of prescription topical treatments
for vaginal atrophy have increased by 35% to $232 million
from 2002 to 2004. Vaginal delivery of estrogen diminishes, but
does not eliminate, the risks of systemic exposure to estrogen.
Over-the-counter
topical vaginal lubricants and moisturizers are also commonly
used, but these therapies are messy to apply. Further, over the
counter topical treatments do not fundamentally change the
mucous membrane of the vagina, and as a result offer only
temporary relief of vaginal atrophy, little relief of associated
local urinary symptoms, and can actually increase vaginal
dryness after the lubricant dries.
SERMs may offer another alternative to hormone replacement
therapies because they have not been shown to increase the risk
of breast or uterine cancer. The therapeutic effects of SERMs
depend on the tissue
specificity of each compound. Raloxifene, marketed as Evista by
Eli Lilly, is the first and only approved SERM for
non-oncological treatment. Raloxifene is effective in treatment
of osteoporosis because it is selective to bone tissue, but it
has no effect on vaginal tissue and therefore does not treat
vaginal atrophy. Further, according to its product label,
raloxifene may increase the incidence of hot flashes.
Lasofoxifene (Oporia), currently in clinical development by
Pfizer for the treatment of vaginal atrophy, appears, based on
published clinical data, to effectively treat osteoporosis and
vaginal atrophy, but it also induces hot flashes. There are no
published data on the treatment of vaginal atrophy using
bazedoxifene, a SERM being developed by Wyeth.
Our product candidate, ospemifene, has been shown in
phase II studies to have beneficial effects on bone density
and vaginal atrophy and did not appear to induce hot flashes
when compared to placebo. As a result of the limitations of
current therapies, we believe that an oral therapeutic that
effectively treats the symptoms of post-menopausal vaginal
atrophy without increasing the risk of breast and uterine cancer
and which does not induce hot flashes would be an important
addition to the therapeutic choices of patients and their
physicians.
Completed Clinical Trials
Phase II Clinical Trial — Comparison with
Placebo
In February 2001, we completed a randomized, double-blind,
parallel group study of ospemifene versus placebo in
159 post-menopausal women at two study sites in Finland. In
this trial, three dose levels of ospemifene (30, 60 or
90 mg once daily) were compared to placebo when
administered for 12 weeks. This study was designed
primarily to examine the effect of ospemifene on bone markers in
blood and urine. We also measured other parameters including
change in the vaginal maturation index, thickness of the uterine
lining and blood hormone levels.
This trial demonstrated that ospemifene had an estrogen-like
effect on vaginal cells. Statistically significant changes were
observed in the decrease in parabasal cells
(p = 0.010, p = 0.005, and
p = 0.002 for 30, 60 and 90 mg versus placebo,
respectively) and increase in superficial cells
(p = 0.028 and p = 0.007 for 60 and
90 mg versus placebo, respectively) as reflected in the
vaginal maturation index compared to placebo for all doses
except the changes observed for superficial cells with the
30 mg dose which did not reach statistical significance
(p = 0.097). Statistical significance means that the
finding is unlikely to be the result of chance and is often
expressed as a
“p-value.” A
p-value is a
statistical term that indicates the probability that a
difference between treatment groups is random. The smaller the
p-value, the lower the
likelihood that the difference was random. Generally a
p-value of less than
0.05 is considered to represent a statistically significant
difference and means that there is a less than 5% chance that
the same result could have been produced by random fluctuations.
Further evidence of the positive effect of ospemifene was the
improvement in vaginal dryness, particularly in patients
receiving the 60 mg dose. In addition, ospemifene was found
to be superior to placebo in reducing bone turnover. Bone
turnover is the rate at which the bone builds up and breaks
down. After menopause, women generally experience an increase in
bone turnover, as bone is resorbed faster than it is replaced
resulting in an increased rate of bone loss and increased risk
of fractures. In this study, ospemifene was well-tolerated, no
safety issues were observed and the reported adverse events
represented an expected range of common symptoms and ailments
not significantly different than placebo. Ospemifene did not
increase the frequency of hot flashes or sweating when compared
to placebo. As with all clinical trials, statistically
significant results in our clinical trials may not necessarily
be demonstrated in later stage clinical trials we may conduct.
Phase II Clinical Trial — Comparison with
Raloxifene
In January 2000, we completed a randomized, double-blind study
of ospemifene versus raloxifene in 118 post-menopausal women at
seven study sites in Finland. In this trial, three dose levels
of ospemifene (30, 60 or 90 mg once daily) were compared to
raloxifene 60 mg once daily when administered for
12 weeks. This trial demonstrated that all ospemifene dose
levels had an estrogen-like effect on vaginal cells. Ospemifene
caused statistically significant relative decreases in parabasal
cells (p = 0.002 and p = 0.001 for 30 and
90 mg versus raloxifene, respectively) and increases in
superficial cells (p = 0.001, p = 0.041 and
p = 0.001 for 30, 60 and 90 mg versus raloxifene,
respectively), as reflected in the vaginal maturation index, as
compared to raloxifene for all dose levels except that no
statistically significant changes were observed for parabasal
cells with 60 mg of ospemifene (p = 0.057).
Raloxifene did not induce changes in the vaginal maturation
index. Ospemifene had similar effects on bone turnover to
raloxifene. In this study, ospemifene was well-tolerated and no
safety issues were observed.
Phase I Clinical Trials
Ospemifene has been the subject of five completed phase I
clinical trials with a total of 121 volunteers. These
trials included single and multi-dose escalating studies and
food effect studies. In these studies, ospemifene was well
tolerated and no safety issues were observed.
Ongoing Phase III Clinical Trials
In October 2005, we had an End of Phase II Meeting with the
Division of Reproductive and Urologic Drug Products of the FDA
to discuss the future development of ospemifene. Based on this
meeting, we are conducting a phase III program to seek FDA
approval of ospemifene for the treatment of vaginal atrophy. Our
phase III program will consist of at least two
phase III trials, the first of which was initiated in
January 2006. The phase III clinical trial program may also
include additional supportive trials examining bone markers and
the potential for treatment of hot flashes. In addition, in
order to file an NDA, we will be required to complete two
two-year carcinogenicity studies that we expect to initiate in
2006 and will run in parallel with our phase III trials.
Our first phase III clinical trial is a randomized,
double-blind, placebo-controlled, parallel group pivotal study
of ospemifene in the treatment of vaginal atrophy. We expect to
enroll approximately 800 post-menopausal women in this study at
approximately 60 study sites in the United States. Patients will
receive 30 or 60 mg of ospemifene or placebo for
12 weeks. Following the treatment phase of the study,
patients will be eligible to participate in a one-year extension
study.
In designing our phase III clinical program for ospemifene,
we have followed FDA published guidance for clinical evaluation
of estrogen/progestin drug products used for hormone replacement
therapy. This guidance is intended to provide recommendations
for studies of estrogen/progestin drug products for the
treatment of moderate to severe vaginal atrophy symptoms
associated with menopause. The guidance recommends that three
primary efficacy analyses demonstrate a statistically
significant improvement versus placebo from baseline to week 12
in all three of the following parameters:
(1) vaginal maturation index, with an improvement reflected
by a decrease of parabasal vaginal cells and increase in
superficial vaginal cells;
(2) vaginal pH, with an improvement reflected by a lowering
of vaginal pH; and
(3) the moderate to severe symptom identified by the
patient as being most bothersome to her.
In our meeting with the FDA, the FDA confirmed to us that these
endpoints would also apply to clinical trials involving SERMs,
and specifically to ospemifene. In our phase II studies, we
have shown a statistically significant improvement in the
vaginal maturation index as described above. In our
phase III studies, our goal is to confirm improvement in
the vaginal maturation index and achieve the vaginal pH and most
bothersome symptoms endpoints.
Fispemifene — A Treatment for the Symptoms of
Andropause
Description of Condition
Andropause is a result of a gradual decline in testosterone
levels that occurs naturally as men age, a phenomenon similar to
menopause in women. Testosterone, an androgen, is the
predominant male sex hormone. According to a recent World Health
Organization report, testosterone progressively declines as men
age, with 20% of men aged 60 to 80 and 33% of men over 80 having
lower than normal levels of testosterone. Andropause is linked
to a range of conditions including fatigue, reduced interest in
sexual activity, erectile dysfunction, reductions in muscle
mass, strength and agility, mood changes, hair loss, and breast
enlargement. Other longer term medical issues have also been
associated with low testosterone including reduced sperm
production and infertility, osteoporosis, depression and heart
disease. The severity and type of andropause symptoms and the
age at which symptoms first occur can differ greatly among men.
The production of testosterone in men is controlled by the
hypothalamus and pituitary gland. Under normal circumstances,
the release of two hormones, luteinizing hormone (LH) and
follicle stimulating hormone (FSH), stimulates production of
testosterone and estrogen from the testes. Testosterone and
estrogen in turn feedback to the hypothalamus and pituitary
gland. When adequate amounts of testosterone and estrogen have
been produced, the hypothalamus and pituitary recognize this and
decrease the release of LH and FSH. When either estrogen or
testosterone feedback is blocked, an increase in LH and FSH
occurs, stimulating the testes to produce more testosterone.
Product Candidate Characteristics
Fispemifene is our product candidate for the treatment of the
symptoms of andropause. Unlike testosterone replacement
therapies, fispemifene utilizes the body’s normal feedback
mechanism to increase testosterone levels into, but not beyond,
the normal range. Under normal circumstances, testosterone and
estrogen secretion from the testes are regulated by the
pituitary hormones, LH and FSH. Testosterone and estrogen in
turn feed back to the hypothalamus and pituitary to prevent
excessive secretion. By blocking estrogen feedback to the
pituitary with a drug like fispemifene, the pituitary increases
LH and FSH secretion which increases testosterone secretion. As
these rising testosterone levels feed back to the pituitary, LH
and FSH secretion return toward normal and testosterone reaches
a new, albeit higher, steady state level. Based on this
mechanism of action, fispemifene is being studied for the
treatment of androgen deficiency and associated symptoms in
aging men. We believe that increased production of testosterone
may treat many of the symptoms of andropause. In a multiple-dose
phase I study we conducted in healthy men, fispemifene
increased total testosterone levels after 28 days of
treatment.
Fispemifene’s direct effect on tissues other than the
hypothalamus and pituitary gland may provide additional benefits
in patients with andropause. Because fispemifene has selective
tissue effects, it has estrogen-blocking effects in some tissue,
while having estrogen-like effects in other tissue. For example,
fispemifene’s direct estrogen blocking effects on breast
may be useful in treatment of breast enlargement, while its
direct estrogen-like effect on bone may increase bone mass. In
addition, we have demonstrated preclinically the estrogen
blocking effects of fispemifene on the prostate, which may help
reduce certain risks associated with estrogen, including
prostate cancer and increase in prostate size.
Market Opportunity
Recent advances in the sensitivity of testing for bioavailable
testosterone have significantly enhanced the ability of
physicians to diagnose and treat andropause. In addition, the
growth of the aging population is driving a significant increase
in the number of older male patients that may benefit from
treatments for the symptoms of andropause. The symptoms of
andropause are most commonly treated with testosterone
replacement therapy. The current market for testosterone
replacement consists primarily of topical or injectable
products. Testosterone replacement products are designed to
provide exogenous testosterone to supplement the low levels of
testosterone seen in aging men but do not address the mechanism
which causes andropause.
Currently, gel and patch formulations of testosterone are the
most commonly prescribed replacement therapies. According to IMS
Health, in the United States alone, sales for this topical
category reached approximately $538 million in 2004, a
growth of 40% compared to 2003, and almost doubling since 2002.
In the same two-year period, U.S. prescriptions grew 25%,
from 1.9 million in 2002 to nearly 2.4 million in
2004. Androgel, marketed by Solvay, is the U.S. market
leader with a nearly 60% market share of prescriptions and sales
of almost $400 million in 2004 according to IMS Health.
Approximately half of
patients prescribed topical testosterone products are between 46
and 65 years old as reported by IMS Health. Topical
products have certain cosmetic and practical limitations, such
as messiness. Intramuscular injections of testosterone are
effective but are painful and inconvenient. Oral testosterone
therapy is rarely used because of the potential risk of
life-threatening liver toxicity.
The therapeutic goal of testosterone replacement therapy is to
normalize the blood serum testosterone concentration in men to
mid to low young adult serum levels and to avoid elevated
testosterone levels. In spite of this goal, elevated
testosterone levels do occur with replacement therapy and can
lead to problems including prostate enlargement and clinically
meaningful elevations in blood hemoglobin levels that can
increase the risk of vascular problems, including stroke. We
believe that an oral therapeutic option that could elevate
testosterone levels into the normal physiologic range without
increasing the risk of prostate enlargement and elevated blood
hemoglobin levels would be an important therapeutic option for
the treatment of the symptoms of andropause.
Completed Clinical Trials
Phase I Clinical Trial — Multiple Dose
Tolerance Study
In September 2002, we completed a randomized, double-blind,
placebo-controlled, ascending multiple-dose study of fispemifene
in 31 healthy older male subjects at a single site in Finland.
This study demonstrated that fispemifene was well tolerated at
doses of 10, 30, 100 and 300 mg administered once
daily for 28 days. As secondary objectives, the
pharmacokinetics and pharmacodynamics (serum hormone levels) of
fispemifene were also studied. The increase of the mean total
testosterone over baseline on days 15, 22 and 28 was
approximately 75% with 300 mg of fispemifene, which
constituted a statistically significant change
(p < 0.01) as indicated in Figure A below.
The increase of the mean total testosterone level with doses of
fispemifene lower than 300 mg was not statistically
significant and has been omitted from the graph.
Figure A. Testosterone Values Observed in Phase I
Clinical Trial
Multiple Dose Tolerance Study
* Measurements at days 15, 22 and 28 were
statistically significant (p < 0.01).
Phase I Clinical Trial — Single Dose Tolerance
Study
In November 2001, we completed a randomized, double-blind,
placebo-controlled, ascending single dose alternating group
study of fispemifene in 20 healthy male volunteers at a single
site in the United Kingdom. The primary objective was to study
the safety and tolerability of the drug. As secondary
objectives, the pharmacokinetics and pharmacodynamics of
fispemifene were studied. Six dose levels were included in the
study: 10 mg, 30 mg, 100 mg, 300 mg,
600 mg, and 1200 mg. Fispemifene was well tolerated at
all dose levels and there was no evidence of dose or
treatment-related trends in the number or severity of adverse
events.
Phase II Clinical Trial — Study of Patients
with Low Testosterone
To date, all clinical studies of fispemifene have occurred
outside of the United States. In November 2005, we submitted an
initial IND filing to the FDA for fispemifene in the treatment
of low testosterone in aging men. In the first quarter of 2006,
we initiated a randomized, double-blind, placebo-controlled,
parallel group phase II study of fispemifene in the
treatment of low testosterone in older men. This study will seek
to enroll approximately 100 older men with low testosterone
levels at approximately 20 study sites in the United States.
Patients will receive either 100, 200, or 300 mg
fispemifene or placebo for 28 days. The primary efficacy
parameter will be testosterone increases relative to baseline.
Safety parameters will include assessment of prostate volume in
addition to routine safety monitoring. Our phase II program
for fispemifene will include multiple phase II trials.
QRX-401 and
QRX-431 —
Treatments of Elevated LDL Cholesterol and Lp(a) Levels
Description of Condition
According to the American Heart Association (AHA), approximately
71 million people in the United States have one or more
forms of cardiovascular disease, including coronary heart
disease. Coronary heart disease is the leading cause of death in
the United States, responsible for over 479,000 deaths in 2003.
Coronary heart disease is caused by deposition of cholesterol, a
type of lipid, in the coronary arteries leading to coronary
arteriosclerosis, a condition that may lead to chest pain, heart
attack or debilitating and potentially fatal heart disease.
According to the AHA, at least 13.2 million Americans alive
today have suffered from such conditions. In addition,
arteriosclerosis can occur in other blood vessels, particularly
those supplying blood to the brain, leading to stroke and other
cerebrovascular conditions. High levels of LDL cholesterol, the
so-called “bad cholesterol,” which can result from
various factors including a genetic predisposition, a diet high
in saturated fats, lack of exercise or diabetes, have been
conclusively shown to be a major cause of coronary heart disease.
A series of recent landmark clinical trials using drugs that
inhibit cholesterol production in the liver, called statins,
confirmed that decreasing high LDL cholesterol reduces the risk
of coronary artery disease and stroke. In 1985, the United
States National Heart, Lung, and Blood Institute of the NIH
launched the National Cholesterol Education Program
(NCEP) with the goal of reducing coronary heart disease by
reducing the percentage of Americans with high cholesterol.
Treatment guidelines issued by the NCEP have advocated
increasingly lower LDL cholesterol treatment targets as new
scientific data has emerged. Despite this awareness, in the
major pharmaceuticals markets, over 300 million people have
cholesterol disorders and of these, almost 180 million
remain undiagnosed, and less than 32% are receiving any form of
lipid drug treatment, according to Datamonitor’s 2003
estimates. It is expected that the number of patients needing
cholesterol-lowering therapy will continue to grow because of an
aging population and the increasing number of people with
diabetes.
In addition to lowering LDL cholesterol levels, therapies are
being developed to lower triglycerides, a different form of fat,
to increase HDL cholesterol, the so-called “good
cholesterol,” and to lower other lipoproteins that may
contribute to coronary heart disease and strokes. Lipoproteins
are proteins which transport fatty substances in the blood
stream to and from the liver. One of these lipoproteins is
Lp(a), which has a shape similar to blood clotting proteins and
may encourage blood to clot when Lp(a) levels are high. Lp(a)
has been shown to be an important independent variable for
prediction of risk of cardiovascular disease
after LDL cholesterol and HDL cholesterol, as demonstrated in
patients with coronary heart disease, stroke and premature
peripheral vascular disease and in the aging. Epidemiological
studies indicate that high levels of Lp(a) are associated with
an increased frequency of stroke and coronary heart disease.
Large studies confirming the effect of lowering Lp(a) have not
yet been conducted. To date, there are no drugs approved for the
treatment of elevated Lp(a) levels. Nevertheless, it is
generally believed that lowering Lp(a) could be beneficial and
contribute to a further reduction of the incidence of stroke and
coronary heart disease.
Product Candidate Characteristics
QRX-401
We are developing
QRX-401 as a potential
new therapy for the treatment of patients with elevated LDL
cholesterol levels.
QRX-401 appears to be
unique in its mechanism for lowering LDL cholesterol and Lp(a).
The liver synthesizes cholesterol, converting it into either
bile acids or particles such as LDL cholesterol. The farnesyl X
receptor, or FXR, indirectly regulates this conversion of
cholesterol into bile acids by the liver.
QRX-401 has been shown
in preclinical studies to be an FXR antagonist, which means that
it blocks the stimulation of the FXR. Blocking the stimulation
of the FXR causes an increase in bile acid formation and a
consequent decrease in the amount of cholesterol available for
LDL cholesterol formation by the liver. Other mechanisms may
also contribute to the observed effects of
QRX-401 on LDL
cholesterol and Lp(a) in animal models. We have not yet
demonstrated that this mechanism for LDL cholesterol lowering is
effective in normal, healthy volunteers.
QRX-431
We are also developing
QRX-431 for the
treatment of elevated levels of LDL cholesterol and Lp(a).
QRX-431 activates the
thyroid beta receptor, which is a known mechanism for lowering
LDL cholesterol and Lp(a). The naturally occurring thyroid
hormone, T3, has been shown to lower LDL cholesterol and Lp(a)
through its effects on the thyroid beta receptor, but T3 also
stimulates the thyroid alpha receptor which produces potentially
harmful increases in heart rate. This lack of tissue specificity
renders T3 unacceptable as a therapy to lower cholesterol
because of the elevation in heart rate.
QRX-431 is selective to
the thyroid beta receptor and, as a result, has been shown in
our preclinical studies to lower LDL cholesterol and Lp(a) and
not affect heart rate. Further, in preclinical monkey studies,
QRX-431 was observed to
be selectively taken up by the liver relative to the heart. In
the monkey studies,
QRX-431 also caused an
average weight loss of 3% to 4% after seven days of treatment,
which may indicate the potential of QRX-431 to act as a weight
loss therapy.
In preclinical studies with
QRX-431, it was
observed that this product candidate stimulated reverse
cholesterol transport, or RCT, in mice. RCT is an important
protective mechanism involving the transport of cholesterol from
the arteries, including plaques which may cause strokes, back to
the liver. QRX-431
stimulates several steps in RCT including stimulation of the HDL
receptor SR-B1 and
increasing bile acid synthesis and removal. This suggests that
QRX-431 might be a
candidate for treatment and prevention of cardiovascular disease
in humans independent of its effects on LDL cholesterol and
Lp(a).
Market Opportunity
According to Datamonitor, in 2004, the market for prescription
lipid disorder treatments reached approximately $26 billion
worldwide, making it the single largest pharmaceutical category.
Much of this growth was driven by statins, which accounted for
approximately 87% of sales. Non-statin therapies, including
fibrates, niacin and cholesterol absorption inhibitors, have
also seen an increase in use, in particular in combination with
low dose statins, a recent example being Vytorin, a cholesterol
absorption inhibitor marketed by Merck/Schering-Plough.
The lowering of LDL cholesterol continues to be the primary
focus of current therapeutic strategies aimed at reducing the
risk of cardiovascular events in patients with elevated
cholesterol. A significant gap remains, however, between the
number of patients who would benefit from therapy and those who
are actually achieving treatment goals. For example, the results
of a recent survey in the United States, the Lipid Treatment
Assessment Project, published by the American Medical
Association reported that 37% of patients
at high risk of developing coronary heart disease and only 18%
of patients with established coronary heart disease actually
achieved the LDL cholesterol values recommended by the NCEP
guidelines.
Among currently available cholesterol lowering therapies,
statins are the most widely used because they are considered to
be the most effective. Troublesome or serious side effects may
limit the utility of statins in some patients. Muscle pain
resulting from statin therapy, while not considered a serious
complication, may affect quality of life and lead to lack of
compliance, treatment at less than optimal doses or withdrawal
from therapy. Rare serious side effects such as muscle damage, a
breakdown of skeletal muscle cells and liver toxicity preclude
the use of statins in older individuals or in patients with
kidney or liver disease.
Statins are sometimes combined with other therapies to limit the
statin dose in patients who cannot tolerate higher doses and to
achieve LDL cholesterol target levels in patients for whom use
of statins alone is not sufficient. Combining statin therapy
with some other types of cholesterol lowering drugs may cause
adverse side effects resulting from the interaction of statins
with the other drugs. In addition, certain of the drugs that are
used in combination with statins have adverse side effects
themselves, including adverse liver and gastrointestinal effects
and facial flushing. Because of these side effects, new
treatments to use in combination with statins are being sought.
While statin therapy has proven to be safe and effective in the
majority of patients for lowering LDL cholesterol, it does not
address all cardiovascular risk factors. Statins have only small
beneficial effects on elevated triglycerides and HDL cholesterol
and no effect on Lp(a). We believe a drug that reduces LDL
cholesterol and Lp(a) and that can be used either alone or in
combination with statins would produce additional benefits over
existing therapies.
Development Program —
QRX-401
Phase I Clinical Trials — Single and Multiple
Dose Tolerance Studies
In June 2004 we began our initial single dose tolerance
phase I study with
QRX-401. Since that
time, we have completed a total of three single and multiple
dose tolerance studies with a total of 152 normal volunteers
with doses of up to 150 mg/day for 14 days. In all of
these studies, QRX-401
has been well-tolerated and no safety issues were observed. In
one of these studies, a phase I study of QRX-401 in doses
between 75 mg/day and 150 mg/day for 14 days in healthy
volunteers, there did not appear to be any meaningful
differences in any overall lipid parameter between treatment
groups at doses of 75 mg/day up to 150 mg/day and placebo,
although we are still analyzing data from these studies, which
were not rigorously designed to demonstrate efficacy.
Phase I Clinical Trial — Food Effect Study
In June 2005, we completed a single-center, randomized,
balanced, single-dose, crossover study of the pharmacokinetics
of 150 mg QRX-401
in fed and fasted healthy male subjects. This trial demonstrated
that QRX-401 was
rapidly absorbed and metabolized. In addition, the trial showed
that safety and tolerability parameters were similar between the
fasted and fed states.
Ongoing Phase I Clinical Trial — Multiple Dose
Tolerance Study
We are currently conducting a multiple-dose tolerance study of
250 mg in healthy male volunteers to assess the safety and
tolerance of QRX-401 when administered once daily for two weeks.
All subjects have been dosed to date. The results from this
study are expected in the second quarter of 2006.
Ongoing Phase I Clinical Trial — Statin
Interaction Study
We are currently conducting a multiple-dose pharmacokinetic drug
interaction between
QRX-401 and
simvastatin, a commonly used statin marketed as Zocor by
Merck & Co., in healthy male volunteers to evaluate the
potential for a pharmacokinetic drug interaction of
QRX-401 on simvastatin
as well as to assess the safety, tolerance and pharmacodynamic
effects of the co-administration of
QRX-401 and simvastatin
when administered once daily for two weeks. A secondary
objective is to evaluate the potential for a
pharmacokinetic drug interaction of simvastatin on
QRX-401 as compared to
historical single dose 250 mg
QRX-401 pharmacokinetic
data. All subjects have been dosed to date. The results from
this study are expected in the second quarter of 2006.
Development Program —
QRX-431
Preclinical Studies
A preclinical study of
QRX-431 in cynomolgus
monkeys was published in Endocrinology in 2004. The
monkeys were treated either with the natural T3 hormone or
QRX-431 once daily for
seven days. The group treated with
QRX-431 demonstrated no
statistically significant increase in heart rate
(p < 0.05). Reductions in LDL cholesterol and
Lp(a) levels and a 3% to 4% weight reduction in this group were
observed. The differences between the
QRX-431 group and the
T3 group were statistically significant for each of the markers
(p < 0.05). The results of the study are shown in
Figure B below comparing T3 to
QRX-431 (referred to as
GC-1 in the graph).
Figure B. 7 Day Treatment in
Cynomolgus Monkeys
* Measurements were statistically significant
(p<0.05)
G. J. Grover, D.M. Egan, P.G. Sleph,
B.C. Beehler, G. Chiellini, N. Nguyen,
J.D. Baxter and T.S. Scanlan, “Effects of the
Thyroid Hormone Receptor Agonist
GC-1 on Metabolic Rate
and Cholesterol in Rats and Primates: Selective Actions Relative
to 3,5,39- Triiodo-L-Thyronine,” Endocrinology, April
2004 (4), 145, 1656 -1661. Copyright 2004 by The Endocrine
Society.
Planned Clinical Trial
We plan to submit an initial IND filing for
QRX-431 in the
treatment of lipid disorders in the first half of 2006 and
initiate a phase I trial shortly thereafter. Supportive
toxicology and safety pharmacology studies have been conducted
and are currently being summarized. The phase I clinical
program will consist of single and multiple rising dose
tolerance studies, a food effect study, and a drug interaction
study with a statin product.
Becocalcidiol — A Topical Treatment for
Psoriasis
Description of Condition
Psoriasis is a chronic disease of the skin characterized by red
patches covered with white scales, or plaques, that can occur on
any part of the body. Psoriasis usually develops in individuals
between 15 and 35 years of age, but can develop at any
time. In addition to its cosmetic aspect, psoriasis can have a
profound effect on quality of life depending on location on the
body and how much of the body is affected. Psoriasis is a very
common condition. According to a 2004 Datamonitor publication,
it is estimated that 1% to 3% of the
adult population have the disease with various forms of severity
and that over 18 million people in the United States,
Japan, France, Germany, Italy, Spain and the United Kingdom
suffer from the disease. In these markets, Datamonitor estimates
that that approximately 10 million patients are currently
diagnosed with psoriasis and that approximately 81% of these
patients receive treatment with topical therapies. In the United
States, approximately 4.1 million patients are currently
diagnosed with psoriasis and that approximately 87% of these
patients receive topical therapy treatments according to
Datamonitor estimates.
Product Candidate Characteristics
Becocalcidiol is our product candidate for the treatment of mild
to moderate psoriasis. Becocalcidiol is a novel topical
calcitriol analog. Topical calcitriol and its analogs have been
shown for many years to be effective in the treatment of
psoriasis. Based on our completed phase IIb study,
becocalcidiol was statistically superior to vehicle in reducing
plaque (p < 0.001 PGA; p = 0.005 PSS) and did
not result in excessive blood calcium levels, a side effect of
existing calcitriol topical treatments for psoriasis. This
allows the potential for use of becocalcidiol at higher doses
and/or on larger body surface areas than can be achieved with
existing calcitriol topical products. We believe that the
ability to treat patients with higher doses may in turn offer
the potential for enhanced efficacy. In our clinical and
preclinical studies, becocalcidiol has been well tolerated with
a low incidence of skin irritation.
Becocalcidiol has been formulated into an ointment, and has
undergone preliminary formulation work for cream, mousse and
lotion forms that all appear feasible and which could provide a
range of presentation options to address different patient
needs. Becocalcidiol has also successfully undergone
pre-formulation feasibility work for combination with a topical
steroid and a topical retinoid, two existing treatments for
psoriasis.
Market Opportunity
Global sales of topical products for the treatment of psoriasis
were approximately $532 million for the twelve month period
ended October 2005, with almost 70% of these sales coming from
existing topical vitamin D-based products according to IMS
Health. Other available topical agents include corticosteroids,
keratolytics, anthralin, coal tar and retinoids. While each of
these existing topical treatments has been shown to produce some
clinical benefit, each has also been associated with undesirable
side effects, including skin irritation, odor and staining of
the skin. Physicians often switch or rotate therapies to try to
avoid such problems or improve efficacy. Topical products are
mainly used for mild to moderate psoriasis; recently, new
systemic products have been approved for the treatment of
moderate to severe psoriasis. As use of these much more
expensive therapies increases, the overall value of the total
market for psoriasis products is projected to grow significantly.
Corticosteroids and calcitriol analogs, either alone or in
combination, are the most popular of topical treatments.
Steroids can quickly clear lesions, but they typically do not
produce long remissions and repeated use can be associated with
a thinning of the outer layers of the skin and other undesired
skin changes. All currently marketed calcitriol based products
have reported cases of excessive blood levels of calcium, which
can result in kidney and other potentially serious problems.
These existing products are also reported to exhibit frequent
skin irritation that may reduce patient compliance and encourage
switching of therapies. Calcipotriol, a topical calcitriol
analog marketed by Warner Chilcott as Dovonex, and
calcipotriene/betamethason dipropionate, a calcipotrol with a
topical steroid to be marketed by Warner Chilcott as Taclonex,
are the only topical calcitriol products available in the United
States. In Europe, other topical calcitriol agents are also
available, as is a combination of calcipotriol with a topical
steroid.
Completed Clinical Trials
Phase IIb Clinical Trial — Whole Body Proof of
Concept Study
In March 2005, we completed a randomized, double-blind, parallel
group, vehicle-controlled study of becocalcidiol in
185 patients with mild to moderate chronic psoriasis at 12
centers in the United States. In this trial, two dose regimens
of becocalcidiol ointment, 75 mg/g ointment applied once daily
(low dose) and
75 mg/g ointment applied twice daily (high dose), were compared
to a vehicle ointment not containing any drug. The primary study
endpoints were a Physician’s Global Assessment
(PGA) reflecting the percentage of patients with all
plaques on body cleared or almost cleared, and a Psoriasis
Symptom Score (PSS) based on two to four target plaques
selected at baseline. Efficacy was assessed following eight
weeks of therapy.
This trial demonstrated that treatment with high dose and low
dose becocalcidiol resulted in a statistically significant
improvement in PGA score compared to vehicle
(p < 0.001 high dose; p = 0.027 low
dose). In addition, all plaques were cleared or almost cleared
in 31% and 20% of patients treated in this trial with high and
low dose becocalcidiol, respectively, compared to 6% patients
treated with vehicle. Patients in the high dose becocalcidiol
group achieved a statistically significant improvement in PSS
score (p = 0.005) from baseline as compared to
patients in the vehicle group (p < 0.001 high
dose; p = 0.027 low dose). Becocalcidiol was generally
well-tolerated in this study with a low incidence of skin
irritation and no change in blood calcium levels.
Phase IIa Clinical Trials
In October 2003, we completed two phase IIa clinical
trials. These two trials enrolled a total of 152 patients.
Patients were treated for two weeks in one study and
12 weeks in the other study. These studies were conducted
at low doses compared to our phase IIb trial described
above. We observed initial indications of efficacy that
demonstrated the need to proceed to the higher doses. We have
now studied higher doses in our phase IIb trial.
Becocalcidiol was generally well-tolerated in both of these
phase IIa studies. No clinically significant changes in
blood or urine calcium levels were observed.
Planned Development
Because becocalcidiol is outside our core therapeutic areas, we
are evaluating alternatives for continued development of this
product candidate, including seeking a partner for further
development and commercialization. We are also currently working
on improved synthetic manufacturing methods for becocalcidiol.
Our Preclinical and Discovery Programs
Our preclinical and discovery programs are primarily conducted
by Hormos, our wholly owned Finnish subsidiary which we acquired
in May 2005. Over the last seven years, Hormos has built a drug
discovery capability that is focused on discovering and
developing novel pharmaceutical compounds involving the tissue
specific regulation of estrogen effects for the treatment of
certain age-related diseases. Hormos’s discovery efforts
are aided by the potential for Finnish government research loans
and grants offered for drug discovery in Finland.
We are focusing our research on SERMs and
17b hydroxysteroid dehydrogenases, or HSDs. We are
enhancing and following the work already completed with
ospemifene and fispemifene in the SERM area, and particularly
focusing on the treatment of hot flashes in women. We have built
up a SERM library in which several molecules show no
estrogen-like effect in breast or uterine tissue, but
estrogen-like effect in the central nervous system, which should
have a positive effect in treating hot flashes in menopausal
women. HSDs are selective inhibitors to prevent the conversion
of estrone to estradiol and therefore cause relative estrogen
deficiency in selected tissues. We believe HSDs could be useful
for endometriosis and uterine fibroids in women and may have
applications for shrinking prostate size in men.
We have nine scientists and eight technicians working in our
chemistry and pharmacology laboratories at our research division
in Finland. Senior members of our research division have
extensive experience in drug discovery and development at
companies such as Farmos, Orion and Schering and with a wide
variety of products, including hormonal products. Prior to
joining Hormos, certain members of this research team
participated in the discovery of the SERM compound toremifene,
marketed as Fareston by GTx, and participated in its worldwide
development for the treatment of breast cancer. Our resources in
Finland enable us to focus on the most critical elements of drug
discovery, namely developing and running key high
throughput screening of compound libraries and optimizing lead
compounds. We also have access to a state of the art animal
facility allowing key small scale in vivo experiments to be done
in a timely manner.
Hormos also supports our clinical development activities by
providing expertise and resources in pharmacokinetics,
pharmaceutical product development and project management. The
development staff consists of ten members, eight of whom are
scientists. Bioanalytics is done in our
GLP-approved
laboratory. Our GMP approved
in-house resource
allows tablet development and stability studies and release of
products for clinical studies. The team leader for our GMP work
has extensive experience in product development, outsourcing of
manufacturing and NDA filings relating to hormonal products.
Sales and Marketing
We do not have sales or marketing personnel. In order to
commercialize any products that are approved for commercial
sale, we must either build a sales and marketing infrastructure
or collaborate with third parties with sales and marketing
experience. We expect that we may build our own sales and
marketing infrastructure to market some of our product
candidates. We expect that we will
out-license or enter
into collaboration agreements for the commercialization of other
product candidates, particularly in the case of product
candidates, such as our product candidates for treating elevated
cholesterol levels, where the sales and marketing infrastructure
required to maximize their value is larger than is practical for
a company of our size.
Intellectual Property
Our policy is to protect the technology that we consider
important to our business. We will be able to protect our
technology from unauthorized use by third parties only to the
extent it is effectively maintained as a trade secret or is
covered by valid and enforceable patents and trademarks.
Individual patents extend for varying periods depending on the
date of filing of the patent application or the date of patent
issuance and the legal term of patents in the countries in which
they are obtained. Generally, patents issued in the United
States are effective for: (a) 20 years from the
earliest effective filing date, if the patent application was
filed on or after June 8, 1995, or (b) 17 years
from the issue date or 20 years from the earliest effective
filing date, whichever is later, if the patent application was
filed prior to June 8, 1995. The length of these effective
terms assume all maintenance fees are paid.
In addition, in certain instances, a patent term can be extended
to recapture a portion of the term effectively lost as a result
of the FDA regulatory review period. The duration of foreign
patents varies in accordance with provisions of applicable local
law.
The actual protection afforded by a patent varies on a product
by product basis, from country to country and depends upon many
factors, including the type of patent, the scope of its
coverage, the availability of regulatory related extensions, the
availability of legal remedies in a particular country and the
validity and enforceability of the patents.
We actively seek to obtain patent protection on the technology
that we consider important to our business, including chemical
species, compositions and forms, their methods of use and
processes for their manufacture. In addition to seeking patent
protection in the United States, we generally file patent
applications in Australia, Canada, Western European countries,
Japan, Mexico and additional foreign countries on a selective
basis in order to further protect the inventions that we
consider potentially important to the development of our
business.
For ospemifene, we have obtained an issued patent covering the
use of ospemifene for the treatment of climacteric disorders in
women during or after menopause. The patent will expire,
assuming all maintenance fees or annuities are paid, in the
United States in 2020, in Australia in 2021, in New Zealand in
2021 and in South Africa in 2021. A patent on the subject matter
has also been approved for issue in Europe.
We also have a license from Orion under its patents covering the
use of ospemifene in a dosage formulation suitable for use in a
variety of indications. The patent will expire, assuming all
maintenance fees or annuities are paid, in the United States in
2015, in Europe in 2015, in Australia in 2015, in Israel in 2015,
in Norway in 2015, in New Zealand in 2015 and in South Africa in
2015. The license from Orion also grants us rights under
Orion’s patent claiming the use of ospemifene as a serum
cholesterol lowering agent. This patent expires, assuming all
maintenance fees or annuities are paid, in the United States in
2017, in Australia in 2017, in Europe in 2017 and in New Zealand
in 2017. Our license rights from Orion are exclusive worldwide,
subject to a right of first refusal retained by Orion for
Denmark, Estonia, Finland, Iceland, Latvia, Lithuania, Norway,
Russia and Sweden.
For fispemifene, we have obtained an issued patent covering
triphenylalkene derivatives (including fispemifene) and their
use as selective estrogen receptor modulators. Orion owns an
undivided interest in this patent and we have entered into a
license agreement with Orion under this patent. Our license
rights from Orion are exclusive worldwide, subject to a right of
first refusal retained by Orion for Denmark, Estonia, Finland,
Iceland, Latvia, Lithuania, Norway, Russia and Sweden. This
patent will expire, assuming all maintenance fees or annuities
are paid, in the United States on November 15, 2020. This
patent will also expire, assuming all maintenance fees or
annuities are paid, in Indonesia in 2020, in New Zealand in
2020, in Singapore in 2020, in Taiwan in 2020 and in South
Africa in 2020.
A third party holds an issued United States patent related to
the use of an anti-estrogen for use in the treatment of androgen
deficiency and related disorders. Zonagen, Inc., a
pharmaceutical company also developing a treatment for
testosterone deficiency in men using a compound that is named in
the patent, requested a reexamination of this patent from the
PTO on the grounds that the claims of the third party’s
patent were invalid because they were disclosed in printed
publications before the date of the invention. In June 2005, the
PTO determined that the claims, as amended during this
reexamination, were patentable in view of the publications under
consideration. Zonagen has subsequently stated in its public
filings that it intends to seek further reexamination of this
third party patent based on additional prior art publications
not previously considered by the PTO. If, as a result of this
further reexamination, the patentability of the claims is
confirmed by the PTO, the patent’s scope could cover our
intended use of fispemifene. Even if Zonagen is not successful
in its attempt to invalidate all of the claims of the patent,
our intended use may be covered by any surviving claims. The
patent holder could bring a claim against us alleging that our
fispemifene product candidate infringes the patent. We believe
we would have valid defenses to any such claim; however,
notwithstanding any defenses we may assert, if such an
infringement claim were successful, we would need to obtain a
license from the patent-holder in order to commercialize
fispemifene in the United States. If such a license were
necessary but not available to us on acceptable terms or at all,
we may not be able to commercialize fispemifene at all in the
United States.
For QRX-401, we have a
license from Genzyme Corporation (formerly Ilex Products, Inc.)
under its patent claiming the composition of matter of
QRX-401 and its use as
a cholesterol lowering agent. This patent expires in the United
States in 2021. Our rights under this patent are worldwide and
exclusive in the field of lipid disorders, atherosclerosis and
all other cardiovascular related diseases.
For QRX-431, we have a
license from EndoChem, Inc. under patents it licensed from the
University of California claiming the composition of
QRX-431 and its use in
the treatment of hyperlipidemia, obesity and diabetes. This
patent expires in 2017. Our rights under this patent are
exclusive and worldwide for all therapeutic applications.
For becocalcidiol, we have a license from Deltanoid
Pharmaceuticals, Inc. under its patent rights obtained from the
Wisconsin Alumni Research Foundation claiming the composition of
becocalcidiol and its use in the treatment of psoriasis. Our
rights under these patents are worldwide. These patents expire
in 2022. Our license rights under these patents are limited to
this compound and are for topical treatments of skin diseases.
In addition to the foregoing patents, we or our licensors, have
also filed various patent applications in certain countries to
obtain additional patent protection relating to ospemifene,
fispemifene, QRX-401,
QRX-431 and
becocalcidiol.
In addition to patents, we rely upon unpatented trade secrets
and know-how to develop
and maintain our competitive position. We also have
confidentiality agreements or invention assignment agreements
with some
of our commercial partners and consultants. These agreements are
designed to protect our proprietary information and, in the case
of the invention assignment agreements, to grant us ownership of
technologies that are developed through a relationship with a
third party.
Licenses and Collaborative Relationships
We have established and intend to continue to pursue licenses
from and collaborative relationships with pharmaceutical and
biotechnology companies and academic institutions.
Orion
We have two license agreements with Orion Corporation, one
relating to ospemifene and one relating to fispemifene.
Under a license agreement with Orion relating to ospemifene, we
received an exclusive, worldwide license to Orion’s
undivided interest in patents with respect to osteoporosis,
vaginal atrophy and cholesterol lowering in women. We separately
own an undivided interest in such patents. This license to
Orion’s interest in the patents is limited to
pharmaceutical products containing ospemifene as its sole active
ingredient. The agreement includes the right to grant
sublicenses to third parties. Orion retained a right of first
refusal to become the exclusive importer and market seller and
distributor of ospemifene in Denmark, Estonia, Finland, Iceland,
Latvia, Lithuania, Norway, Russia and Sweden. Under the terms of
the agreement, we paid Orion a license fee of 400,000 Euros
and also agreed to pay Orion development milestone payments of
up to $750,000 for two milestones, and of up to an additional
1,100,000 Euros for the remaining milestones, plus a
royalty based on net sales of products resulting under the
agreement. The term of our license from Orion continues on a
country-by-country basis until the expiration or invalidation of
the last to expire or be invalidated of the licensed patents, or
15 years from the date of the agreement, whichever is
longer. In the case of a payment default, Orion has the right to
terminate the license upon 15 days prior written notice and
failure to cure within such 15 day period. In all other
cases, each party has the right to terminate the license upon
30 days prior written notice in the case of material breach
and failure to take action to cure such a breach within such
30 day period. Orion also has the right to terminate the
agreement immediately in the event that we fail to launch
ospemifene in the United States, Germany, the United Kingdom and
France before December 31, 2015.
Under a license agreement with Orion relating to fispemifene, we
received an exclusive, worldwide license to Orion’s
undivided interest in patents with respect to fispemifene. We
separately own an undivided interest in such patents. The
agreement includes the right to grant sublicenses to third
parties. Orion retained a right of first refusal to become the
exclusive importer and market seller and distributor of
fispemifene in Denmark, Estonia, Finland, Iceland, Latvia,
Lithuania, Norway, Russia and Sweden. Under the terms of the
agreement, we paid Orion an initial license fee of
50,000 Euros and also agreed to pay Orion combined
development milestone payments of up to 900,000 Euros and a
royalty based on net sales of products resulting under the
agreement. The term of the license from Orion continues on a
country-by-country basis until the expiration or invalidation of
the last to expire or be invalidated of the licensed patents.
Each party has the right to terminate the license upon
30 days prior written notice in the case of material breach
and failure to take action to cure such a breach within such
30 day period.
Tess Diagnostics and Pharmaceuticals
Our former development partner for ospemifene, Tess Diagnostics
and Pharmaceuticals, Inc. has assigned to us all of its license
rights under certain patents for the use of ospemifene. In
consideration for that assignment and Tess’ earlier
contribution to the development of ospemifene, we made a payment
of $700,000 to Tess. We have also agreed to pay a royalty out of
ospemifene net sales of each product and a share of milestones
received from third parties depending on the implemented
commercialization model. Our requirement to pay royalties
continues on a country-by-country basis until the expiration of
the last to expire of an ospemifene patent covering such
product. If we have a change in control and we determine to
develop and commercialize ospemifene without giving an exclusive
license to a third party, then we must pay to Tess
combined milestone payments of up to $8.5 million. If we
have a change in control and we grant royalty bearing licenses
to third parties, we must pay to Tess a share of the payments
received from third parties. If we decide to permanently
discontinue our development and commercialization of ospemifene,
we have the right to terminate our license from Tess upon
written notice to Tess.
Genzyme Corporation
Under an exclusive license agreement with Genzyme Corporation
(formerly Ilex Products, Inc.), we have a license to develop and
market certain compounds for the treatment of lipid disorders,
atherosclerosis and all other cardiovascular related disorders
on a worldwide basis. These compounds include
QRX-401. We have the
right to grant sublicenses to third parties. Under the terms of
the agreement, we paid Genzyme Corporation an initial license
fee of $2.5 million. With respect to
QRX-401, we have agreed
to pay Genzyme Corporation combined development milestone
payments of up to $39 million, a share of sublicense
revenue and a royalty based on net sales of products resulting
under the agreement. Milestone payments made to date have
totaled $1.5 million. Our requirement to pay royalties
continues on a country-by-country basis until the expiration of
the last to expire of the licensed patents that claim the
products or for the period of non-patent marketing exclusivity
in that country. We may terminate the agreement for any reason
upon 90 days written notice. Genzyme Corporation may
terminate the agreement if we are in material breach and fail to
cure such a breach within 60 days of written notice of such
breach by Genzyme.
EndoChem
Under an exclusive license agreement with EndoChem, Inc., we
have a license to develop and market
QRX-431 for all human
therapeutic applications on a worldwide basis. We have the right
to grant sublicenses to third parties, however this right may
only be granted to the extent reasonably necessary for the
development and commercialization of products and sublicensees
who have received a direct sublicense from us may grant further
sublicenses without further rights to sublicense. Under the
terms of the agreement, we owe EndoChem an initial license fee
of $800,000, of which $550,000 has been paid, and $250,000 is
due within seven days of the filing of an Investigational
New Drug application for commencement of phase I clinical
trials with the FDA. We have also agreed to pay EndoChem
combined development milestone payments of up to
$3.25 million, a royalty based on net sales of products
resulting under the agreement and a percentage of sublicensing
revenues other than net sales. This agreement also requires us
to make specified minimum annual royalty payments of $100,000
beginning in the first year of sales, and in any event,
beginning in 2012, even if sales have not occurred by then. Our
requirement to pay royalties continues on a country-by-country
basis until the expiration of the last to expire of the licensed
patents that covers the sale of the product in such country. We
may terminate the agreement for any reason upon 90 days
written notice. EndoChem may terminate the agreement upon
written notice if we are in material breach and fail to cure
such a breach within 45 days of the notice for monetary
defaults and 75 days of the notice for any other default.
The rights licensed to us by EndoChem were licensed by EndoChem
from the Regents of the University of California and our rights
are therefore subject to the continuation of the license between
EndoChem and the University of California. We have received an
affirmation from the University of California providing that
notwithstanding the termination or expiration of the license
between EndoChem and the University of California, the
University shall permit us to exercise all rights granted to
EndoChem under its license with EndoChem and sublicensed to us
provided that we are not in default in our license with EndoChem
at the time of termination or expiration, and that we agree in
writing to the terms of the University’s license with
EndoChem.
Deltanoid Pharmaceuticals
Under an exclusive license agreement with Deltanoid
Pharmaceuticals, Inc., we have a license to develop and market
becocalcidiol for topical treatments of skin diseases, including
psoriasis, on a worldwide basis. We have the right to grant
sublicenses to third parties. Under the terms of the agreement,
we have paid Deltanoid Pharmaceuticals an initial license fee
and have agreed to pay Deltanoid Pharmaceuticals development
milestone payments up to $3.5 million and a royalty based
on net sales of products resulting
under the agreement. Our requirement to pay royalties continues
on a country-by-country basis until the expiration of the last
to expire of the licensed patents that covers the sale of the
products in that country. We may terminate the agreement for any
reason upon 90 days written notice. Deltanoid
Pharmaceuticals may terminate the agreement if we are in breach
and fail to cure such a breach within 30 days of written
notice of such breach. The rights licensed to us by Deltanoid
Pharmaceuticals were licensed by Deltanoid Pharmaceuticals from
the Wisconsin Alumni Research Foundation and our rights are
therefore subject to the continuation of the license between
Deltanoid and the Wisconsin Alumni Research Foundation. As such,
we have entered into an agreement with the Foundation providing
that if the license between the Foundation and Deltanoid
Pharmaceuticals is terminated, and we are not in default in our
license with Deltanoid Pharmaceuticals, then we will be deemed
to have entered into a license directly with the Foundation on
the same terms and conditions as those set forth in our license
with Deltanoid.
University of Turku
Under a patent assignment agreement with the University of
Turku, we have rights to a patent relating to the method of use
of fispemifene for treatments for lower urinary tract symptoms
or pelvic pain. Under the terms of the agreement, we paid patent
application and patent approval fees to the inventors and a
signing fee to the University that totaled 11,400 Euros. We
have also agreed to pay a 10,000 Euros milestone payment
and to pay a royalty based on net income. Our requirement to pay
royalties continues on a country-by-country basis until the
expiration of the licensed patent in that country. We have
further agreed to pay a percentage of any purchase price we
receive for the outright license or assignment to a third party
of the applicable patent. Each party has the right to terminate
the license on 30 days prior written notice in the case of
breach and failure to cure such a breach within such 30 day
period.
Orion Corporation Fermion
On May 1, 1999, Hormos entered into an agreement with Orion
Corporation Fermion to develop a synthetic process for
manufacturing at commercial scale our product candidate
ospemifene. The parties agreed to conduct a development program
for such synthesis, with the term of the program ending on
May 28, 2004. Under the terms of this agreement, Fermion
shall own all inventions relating to the synthesis of ospemifene
made as a result of Fermion’s efforts. Fermion has granted
Hormos a worldwide, personal, non-exclusive, non-transferable
license, with the right to grant one sublicense, to such
inventions. In addition, Fermion has a right of first refusal to
enter into an agreement with Hormos to become the exclusive
supplier of commercial quantities of ospemifene. If the parties
enter into any such agreement and Fermion discontinues
manufacture of ospemifene, Fermion is obligated to deliver to
Hormos the manufacturing and quality control technology and
methodology owned by Fermion and indicated in the drug master
file for ospemifene and related analytical methods so that
Hormos may transfer such technology to a third party
manufacturer.
Linnea
We entered into a Manufacturing, Sales and Distribution License
Agreement with Linnea S.A. whereby Linnea received an exclusive,
worldwide license to our HMRlignan technology for nutraceutical
use. Under this agreement, Linnea has the right to develop,
manufacture and commercialize HMRlignan as an active ingredient
in dietary supplement products. Linnea has the right to grant
sublicenses to third parties. We retained a non-exclusive right
to market HMRlignan in finished forms in the United States. We
also retained the right to develop, manufacture, commercialize
and license to third parties HMRlignan for prescription
pharmaceutical applications. Under the terms of the agreement,
Linnea is required to pay a royalty on sales of HMR bulk
ingredient by Linnea to its customers after April 1, 2007
and on revenues for sublicenses granted by Linnea. Linnea must
maintain certain minimum sales volumes in order to maintain its
exclusive rights under the agreement. We granted Linnea an
option to the right to sell HMRlignan products approved under
(i) the Generally Recognized As Safe regulatory clearance
by the FDA and (ii) the criteria stated in the European
Union for sale of novel food items, upon payment of an option
fee of $500,000 for each such use. Linnea has paid an initial
signing fee of 400,000 Euros. Linnea has the right to
terminate the agreement at
any time upon 4 months prior written notice. Either party
has the right to terminate the agreement if the other party is
in material breach and fails to cure such breach within
30 days from the date the written notice of breach is
dispatched. The term of this agreement expires on the expiration
of US patent 6,451,849 which expires in 2019.
Competition
Our major competitors are public and private pharmaceutical and
biotechnology companies, both in the United States and abroad,
which are engaged in the discovery and development of products
that would compete directly with our therapeutic compound
candidates in the fields of endocrine, metabolic and
cardiovascular diseases, as well as psoriasis. Many of these
companies have greater financial resources and expertise than we
have in research and development, manufacturing, preclinical
testing, conducting clinical trials, obtaining regulatory
approvals and marketing. These entities also compete with us in
recruiting and retaining qualified scientific and management
personnel, as well as in acquiring technologies complementary
to, or necessary for, our programs.
Any compound candidates that we successfully develop and
commercialize will compete with existing therapies and new
therapies that are likely to become available in the future. It
is possible that competing companies will develop drug
candidates and market drugs that are less expensive and more
effective than any drugs we may successfully develop or that
will render any drugs we develop obsolete. It is also possible
that these companies will commercialize competing drugs before
we or any of our partners can launch any drugs developed from
our product candidates. In addition to branded competitive
products, if our product candidates receive regulatory approval
they may face competition from generic drugs and the
availability of generic drugs may adversely affect the market
for our products.
Vaginal atrophy is generally treated with estrogen-based
therapies either oral or topical, such as Premarin, Prempro and
Premarin Vaginal Cream, marketed by Wyeth, and Vagifem, marketed
by Novo Nordisk. Other products in development for this
condition include bazedoxifene, being developed by Wyeth, and
Oporia, being developed by Pfizer, which are both SERMs.
Testosterone deficiency is most frequently treated with topical
gels or patches, such as Solvay Pharmaceuticals’ Androgel
and Watson Pharma’s Androderm. Products in development
include Acapodene and Ostarine, both being developed by GTx, and
Androxal, being developed by Zonagen.
In the treatment of lipid disorders, statins are the most
frequently prescribed products, examples of which include
Lipitor, marketed by Pfizer, Zocor and Mevacor, both marketed by
Merck & Co., Crestor, marketed by AstraZeneca and
Pravachol, marketed by Bristol-Myers Squibb. Other competitors
include non-statin products, such as Zetia, marketed by Merck/
Schering-Plough, Tricor, marketed by Abbott, and Niaspan,
marketed by Kos; combinations of statins with other agents, for
example Merck/ Schering-Plough’s Vytorin and Kos’
Advicor; and new products in development, such as KaroBio’s
KB2115.
Competing marketed topical psoriasis products or products under
development, specifically topical calcitriol analogues, include
Dovonex marketed by Warner Chilcott, Taclonex to be marketed by
Warner Chilcott, tisocalcitate, in development by Schering AG,
and CTA018 in development by Cytochroma.
Regulatory
The FDA and comparable regulatory agencies in foreign countries,
as well as local and state or other regional governmental
agencies, impose substantial requirements upon the clinical
development, manufacture and marketing of pharmaceutical
products. These agencies and other federal, state and local
entities regulate research and development activities and the
testing, manufacture, quality control, safety, effectiveness,
labeling, storage, record keeping, approval, advertising and
promotion of our products.
The process required by the FDA before product candidates may be
marketed in the United States generally involves the following:
submission of an investigational new drug application, or IND
application, which must become effective before clinical trials
may begin;
•
adequate and well-controlled human clinical trials to establish
the safety and efficacy of the proposed drug for its intended
use;
•
pre-approval inspection of manufacturing facilities, company
regulatory files, and selected clinical investigators; and
•
FDA approval of a new drug application, or NDA, or FDA approval
of an NDA supplement in the case of a new indication if the
product is already approved for another indication.
The testing and approval process requires substantial time,
effort and financial resources, and we cannot be certain that
any new approvals for our product candidates will be granted on
a timely basis, if at all.
Prior to commencing the first human clinical trial, we must
submit an IND application to the FDA. The IND application
automatically becomes effective 30 days after receipt by
the FDA, unless the FDA, within the
30-day time period,
raises concerns or questions about the preclinical drug testing
or nonclinical safety evaluation in animals, or the design or
conduct of the first proposed clinical trial, and places the
study on clinical hold. In such a case, the IND sponsor and the
FDA must resolve any outstanding concerns before the clinical
trial may begin. Our submission of an IND application may result
in the FDA’s denial of authorization to commence a clinical
trial. A separate submission to the existing IND application
must be made for each successive clinical trial conducted during
product development, and the FDA must not object to the
submission before each clinical trial may start and continue.
Further, an independent institutional review board for
investigation in human subjects within each medical center in
which the clinical trial will be conducted must review and
approve the preclinical drug testing and nonclinical safety
evaluation and efficacy in animals or prior human trials as well
as the design and goals of the proposed clinical trial before
the clinical trial commences at that center. Regulatory
authorities or an institutional review board or the sponsor may
suspend a clinical trial at any time on various grounds,
including a finding that the subjects or patients are being
exposed to an unacceptable health risk.
For purposes of NDA approval, human clinical trials are
typically conducted in three sequential phases that may overlap.
Phase I: Phase I clinical studies are initially
conducted in a limited population to evaluate the product
candidate for safety, dosage tolerance, absorption, metabolism,
distribution and excretion in healthy subjects.
Phase II: Phase II clinical studies are
conducted in a limited patient population to further identify
and measure possible adverse effects or other safety risks, to
determine the initial efficacy of the product for specific
targeted diseases and to determine dosage tolerance and optimal
dosage. Multiple phase II clinical trials may be conducted
by the sponsor to obtain information prior to beginning larger
and more expensive phase III clinical trials. The first,
limited phase II clinical trials may be termed
“phase IIa” trials to denote that only a few
patients are enrolled in order to obtain preliminary safety and
efficacy data. Later, larger phase II clinical trials may
be termed “phase IIb” trials to denote that
preliminary evidence of safety and efficacy has already been
obtained, and the current trial is intended to confirm the
finding of the earlier trial, as well as to enroll additional
patients in order to further refine the estimate of the optimal
dose and to detect less common side effects. In some instances,
a phase IIb trial may be declared acceptable by a
regulatory agency, such as the FDA, as one of the
“pivotal” trials necessary for purposes of obtaining
marketing authorization for a drug.
Phase III: When phase II clinical evaluations
demonstrate that a dosage range of the product appears to be
effective and has an acceptable safety profile, phase III
clinical trials are undertaken in large patient populations to
further evaluate dosage, to confirm clinical efficacy and to
evaluate safety in yet larger and more diverse patient
populations at multiple clinical trial sites.
The FDA may require, or companies may pursue, additional
clinical trials after a product is approved. These so-called
phase IV clinical studies may be made a condition to be
satisfied after a drug receives approval. The results of
phase IV clinical studies may confirm the effectiveness of
a product and may provide important safety information to
augment the FDA’s voluntary adverse drug reaction reporting
system.
The results of product development, preclinical studies and
clinical trials are submitted to the FDA as part of an NDA, or
as part of an NDA supplement. The FDA may deny approval of an
NDA or NDA supplement if the applicable regulatory criteria are
not satisfied, or it may require additional clinical data or an
additional pivotal phase III clinical trial. Even if such
data are submitted, the FDA may ultimately decide that the NDA
or NDA supplement does not satisfy the criteria for approval.
The FDA may move to withdraw product approval, once issued, if
ongoing regulatory standards are not met or if safety problems
occur after the product reaches the market. In addition, the FDA
may require testing and surveillance programs to monitor the
effect of approved products that have been commercialized, and
the FDA may move to prevent or limit further marketing of a
product based on the results of these post-marketing programs.
Satisfaction of FDA requirements or similar requirements of
state, local and foreign regulatory agencies typically takes
several years and the actual time required may vary
substantially based upon the type, complexity and novelty of the
product or disease. Typically, if a drug product is intended to
treat a chronic condition, as is the case with some of the
product candidates we are developing, safety and efficacy data
must be gathered over an extended period of time, which can
range from one to three years or more. Government regulation may
delay or prevent marketing of product candidates for new
indications for a considerable period of time and impose costly
procedures upon our activities. The FDA or any other regulatory
agency may not grant approvals for new indications for our
product candidates on a timely basis, if at all. Success in
preclinical testing and early clinical trials does not ensure
that later clinical trials will be successful. A number of
companies in the pharmaceutical industry have suffered
significant setbacks in advanced clinical trials, even after
obtaining promising results in earlier clinical trials. Future
clinical trials may indicate previously undetected side effects
or fail to demonstrate efficacy in a statistically significant
manner. Data obtained from clinical activities is not always
conclusive and may be susceptible to varying interpretations,
which could delay, limit or prevent regulatory approval. Even if
a product candidate receives regulatory approval, the approval
may be significantly limited to specific disease states, patient
populations and dosages. Further, 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, additional regulatory
approvals for our products would harm our business. In addition,
we cannot predict what adverse governmental regulations may
arise from future U.S. or foreign governmental action.
Any products manufactured or distributed by us pursuant to FDA
approvals are subject to continuing regulation by the FDA,
including record-keeping requirements and reporting of adverse
experiences with the drug. Drug manufacturers and their
subcontractors are required to register their establishments
with the FDA and certain state agencies, and are subject to
periodic unannounced inspections by the FDA and certain state
agencies for compliance with good manufacturing practices, which
impose certain procedural and documentation requirements upon us
and our third party manufacturers. We cannot be certain that we
or our present or future suppliers will be able to comply with
the good manufacturing practices regulations and other FDA
regulatory requirements. If our present or future suppliers are
not able to comply with these requirements, the FDA may halt our
clinical trials, require us to recall a drug from distribution,
or withdraw approval of the NDA for that drug.
The FDA closely regulates the marketing and promotion of drugs.
A company is permitted to make only those claims relating to
safety and efficacy that are approved by the FDA. Failure to
comply with these requirements can result in adverse publicity,
warning letters, corrective advertising and potential civil and
criminal penalties. Physicians may prescribe legally available
drugs for uses that are not described in the product’s
labeling and that differ from those tested by us and approved by
the FDA. Such off-label uses are common across medical
specialties. Physicians may believe that such off-label uses are
the best treatment for many patients in varied circumstances.
The FDA does not regulate the behavior of physicians in their
choice of treatments. The FDA does, however, restrict
manufacturers’ communications on the subject of off-label
use.
The FDA’s policies may change, and additional government
regulations may be enacted which could prevent or delay
regulatory approval of our product candidates or approval of new
diseases for our product candidates. We cannot predict the
likelihood, nature or extent of adverse governmental regulation
that might arise from future legislative or administrative
action, either in the United States or abroad.
We have no manufacturing facilities and we do not intend to
build manufacturing facilities of our own in the foreseeable
future. We have entered into arrangements with various third
parties for the formulation and manufacture of our clinical
supplies. These suppliers and their manufacturing facilities
must comply with regulations, current good laboratory practices,
or cGLPs, and current good manufacturing practices, or cGMPs,
enforced by the FDA. We currently have sufficient drug supplies
to complete our ongoing and planned clinical trials. We plan to
continue to outsource the formulation and manufacturing of our
clinical supplies. Although we have no long-term drug supply
contracts for our clinical trial supplies, we maintain good
relationships with the suppliers of our current drug supply and
we believe there are alternative manufacturers available to
produce clinical trial supplies if necessary. Prior to seeking
approval for any of our product candidates, we will need to
enter into a long-term supply agreement with a third-party
manufacturer who can formulate and manufacture supplies of our
product candidate on a commercial scale and who will work with
us to complete the Chemistry, Manufacturing and Controls, or
CMC, section of our NDA filing.
Legal Proceedings
We are not involved in any material legal proceedings.
Facilities
We currently lease and occupy approximately 9,742 square
feet of office space in Ann Arbor, Michigan under a lease
expiring in May, 2011. We also lease a total of approximately
3,111 square meters of office and laboratory space in
Turku, Finland and Oulu, Finland under five separate leases, two
of which expire in 2011 and the other three of which allow us to
terminate them upon prior notice of 15 months or less. We
believe our facilities are adequate for our present operations.
Employees
As of February 1, 2006, we had 19 employees in the
United States and 39 employees in Finland. Certain of our
employees in Finland are covered by a collective bargaining
agreement. We believe our relations with our employees are good.
Member of the nominating and corporate governance committee.
Executive Officers
Robert L. Zerbe, M.D. co-founded QuatRx in
November 2000 and has served as our Chief Executive Officer
and President and as a member of our board of directors since
inception. Dr. Zerbe has extensive experience in regulatory
affairs and global clinical development at Eli Lilly in the
United States and the United Kingdom, where he held a variety of
research and development positions, including Managing Director,
Lilly Research Center U.K., and Vice President of Clinical
Investigation and Regulatory Affairs, from 1982 to 1993. He
joined Parke-Davis in 1993, becoming Senior Vice President of
Worldwide Clinical Research and Development, during which time
he oversaw the successful development programs for Lipitor,
Neurontin and other key products. He serves on the boards of AP
Pharma, Corgentech and Aastrom Bioscience. Dr. Zerbe earned
his medical degree at Indiana University in 1975 and did post
graduate training in internal medicine, endocrinology and
neuroendocrinology at Indiana University and the National
Institutes of Mental Health.
Stuart Dombey, M.B., F.R.C.P. co-founded QuatRx in
November 2000 and has served as our Chief Scientific and
Regulatory Officer since inception. Dr. Dombey is a
U.K.-trained physician
with more than 25 years of experience in the pharmaceutical
industry and 13 years of international regulatory
experience. He initially worked for Hoechst as Medical Advisor
in the United Kingdom and then for Squibb, first as
U.K. Medical Director and then transferred to the United
States in 1987 as Vice President, Regulatory Liaison. He joined
Parke-Davis in the United States in 1990 as Vice President of
International Regulatory Affairs, where he had responsibility
for all regulatory activities on Parke-Davis products outside
the United States and the development and implementation of
innovative regulatory strategies for Parke-Davis
compounds. Most recently, he was Vice President of R&D in
Japan. Dr. Dombey received his M.B. and Ch.B. degrees from
the University of Liverpool Medical School in 1971.
Randall Whitcomb, M.D. joined QuatRx in
January 2001 as a co-founder and has served as our Chief
Medical Officer since that time. Dr. Whitcomb came to
QuatRx from Parke-Davis, where he was a Senior Director and
subsequently Vice President within Worldwide Clinical Research
and Drug Development from 1992 to 2000. His work involved the
development and approval of products for women’s health
care and diabetes, and the oversight of earlier-stage compounds
for diabetic neuropathy, osteoporosis, inflammation and
gastrointestinal diseases. Dr. Whitcomb serves on the board
of Insmed. He was on the faculty of Massachusetts General
Hospital and Harvard Medical School prior to joining Parke-Davis
in 1992. Dr. Whitcomb received his medical degree at the
University of Kansas and research training at the National
Institutes of Health.
Christopher Nicholas co-founded QuatRx in November 2000
and has served as our Chief Business Officer since inception.
Mr. Nicholas has more than 25 years of global
pharmaceutical marketing, business development and general
management experience at companies such as Bayer,
Hoechst/Roussel and Parke-Davis. He joined Parke-Davis in the
U.K. in 1980, and was ultimately responsible for the United
Kingdom marketing team before moving to the United States
headquarters in 1987. As Vice President of Global Marketing at
Parke-Davis, he was responsible for several major products,
notably the worldwide launch of Lipitor, and he chaired the
co-promotion/co-development partnership on Lipitor with Pfizer.
He also had responsibility for Parke-Davis business development.
He held Vice President and General Manager positions for
Parke-Davis in Benelux from April 1997 to April 1999
and Japan from April 1999 to September 2000.
Mr. Nicholas received B.Sc. honors degrees in chemistry and
business administration and a diploma in industrial studies in
chemistry and biology from Loughborough University in 1976.
Gary Onnhas served as our Chief Financial Officer since
November 2003. Mr. Onn is a Certified Public
Accountant in the state of Washington with over 20 years of
finance and management experience. From January 2003 to
November 2003, Mr. Onn served as a financial
consultant to early-stage businesses. From June 2001 to
January 2003, he served as the Chief Financial Officer and
interim Chief Executive Officer of Aculight Corporation, a laser
development company, and from July 2000 to June 2001,
he was the Chief Financial Officer of RevX.net, a software
developer. In 1994, Mr. Onn joined Heartstream, a publicly
listed developer of automatic external defibrillators, where he
served in the position of director of finance and later, Chief
Financial Officer. In 1990 he joined publicly listed software
developer Aldus Corporation as Financial Reporting Manager
responsible for external and internal financial reporting from
Aldus’s domestic, European, and Asia-Pacific operations.
Prior to that, Mr. Onn spent nearly seven years as an
auditor with the public accounting firm of Ernst &
Young, including two years as an audit manager. Mr. Onn
received his B.A. in business administration from the University
of Washington in 1983.
Key Employees
Jeffery Brinza has served as our General Counsel since
June 2005. Mr. Brinza has 19 years of experience
as a corporate and transactional attorney. In 1993, he joined
Warner-Lambert Company as associate counsel. From 1998 to 2000,
he served as vice president and assistant general counsel at
Warner-Lambert Company. From February 2001 to
September 2001, Mr. Brinza served as a Senior
Associate at the law firm of Butzel Long. From
September 2001 to June 2005, Mr. Brinza served as
a partner at Brinza & Associates, providing legal
representation for various pharmaceutical, life science and
technology companies. Mr. Brinza received his B.A. in
Economics and Computer Science from the University of Michigan
in 1983 and his J.D. from the University of Michigan in 1986.
Constance Keyserling has served as our Head of
Development Operations since April 2002.
Ms. Keyserling has nearly 20 years of global clinical
development experience at Parke-Davis, Pfizer and Esperion
Therapeutics. As Director of Clinical Operations from December
2000 to October 2001 and Senior Director of Operations at
Esperion from October 2001 to April 2002, her responsibilities
included clinical program design and management, project
management, clinical outsourcing, regulatory operations and SOP
systems development, in addition to co-chairing one of three
product development teams. Her roles at Parke-
Davis from October 1986 to November 2000 spanned biometrics and
anti-infective clinical development in the United States and
Europe, and she was the Director of Clinical Operations for
Pfizer Global Research and Development from December 1998 to
November 2000. Ms. Keyserling received her M.S. in
Biostatistics from Harvard University in 1984. Prior to joining
the pharmaceutical industry in 1986, she performed biomedical
research at the Dana-Farber Cancer Institute and the University
of Michigan.
Risto Lammintausta, M.D., Ph.D. co-founded
Hormos Medical Oy in 1997 and has served as its Chief Executive
Officer since that time. Mr. Lammintausta joined us in
May 2005 in connection with our acquisition of Hormos.
Previously, he was Vice President for new drug development at
Orion Corporation from 1992 to 1997 and Research Director at
Farmos Group Ltd. from 1981 to 1991. In these positions he had
responsibility for new compound discovery and development.
Dr. Lammintausta served as a member of the Medical Research
Council of the Academy of Finland between 1995 and 2000 and is
Chairman of the Pharma Cluster Finland. He serves as a member of
the board of directors of Juvantia Pharma, Innomedica and the
Finnish Cancer Research Foundation. Dr. Lammintausta is a
medical doctor and holds a Ph.D. in Pharmacology from the
University of Turku.
Non-Management Directors
Caley Castelein, M.D. has served as a member of our
board of directors since October 2004. Dr. Castelein became
a founding member of Thomas Weisel Healthcare Venture Partners
in March 2003. Since October 2000, Dr. Castelein has served
as a principal at ABS Ventures. Prior to that,
Dr. Castelein received a medical degree from the University
of California San Francisco in 1999, and was a resident in
the general surgery program from 1999 to 2000. He began his
career in corporate finance at Hambrecht & Quist, where
he served in the position of analyst from 1993 to 1994.
Dr. Castelein graduated Magna Cum Laude from Harvard
College in 1993.
Christopher B. Ehrlich has served as a member of our
board of directors since October 2004. He is currently a partner
at InterWest Partners, a diversified venture capital firm, which
he joined in August 2000. Before InterWest, Mr. Ehrlich was
Director, Licensing & Business Development at Purdue
Pharma, a private pharmaceutical firm based in Stamford, CT.
Mr. Ehrlich worked in business development at Genentech,
Inc., in venture capital at The U.S. Russia Investment
Fund, and in biotechnology strategy development at LEK
Consulting. He also currently serves on the boards of BioMimetic
Pharmaceuticals, KAI Pharmaceuticals, Carbylan BioSurgery,
TransOral Pharmaceuticals and Xenon Pharmaceuticals. Mr. Ehrlich
earned his Bachelor’s degree from Dartmouth College, cum
laude and an M.B.A. from the J.L. Kellogg Graduate School of
Management where he serves as an instructor and advisor to the
Biotech Program.
Richard P. Fox has served as a member of our board of
directors since January 2006. Since October 2001, Mr. Fox
has served as a consultant and outside board member to
entrepreneurs and the financial services industry. From April
2000 to September 2001, he was an officer of CyberSafe, an IT
security company, serving as President and Chief Operating
Officer from January 2001 to September 2001. Mr. Fox spent
28 years with Ernst & Young, last serving as
Managing Partner of the Seattle office. He serves on the board
of directors of Premera, a Blue Cross managed care provider,
aQuantive, an online marketing company, Flow International, a
machine tool manufacturer, Isothermal Systems, and Shurgard
Storage Centers, Inc., a real estate investment trust. In
addition, he serves as Treasurer and is on the Board of Trustees
of the Seattle Foundation and is on the Board of Visitors of the
Fuqua School of Business, Duke University. Mr. Fox received
a B.B.A. degree from Ohio University and an M.B.A. from the
Fuqua School of Business, Duke University. He is a Certified
Public Accountant in Washington State.
William Greene, M.D. has served on our board of
directors since May 2003. Dr. Greene joined MPM Capital in
January 2002, and is a General Partner. From June 1998
to January 2002, Dr. Greene was a senior Clinical
Scientist at Genentech, where he had responsibility for drug
development activities in several therapeutic areas. Previously,
from 1991 to 1998, he was in academic medicine at Yale Medical
School. He currently serves on the board of directors of Alsius
Corporation, Archus Orthopedics, EndoGastric Solutions and
Synergia Pharma. Dr. Greene received his medical degree at
the University of California San Francisco, where he is an
assistant professor of medicine and a B.A., with honors, from
Wesleyan University.
Patrick Heron helped found QuatRx and has served as a
member of our board of directors since our inception in November
2000. Through Frazier Healthcare Ventures, he was a founding
investor in QuatRx. Mr. Heron has held various positions
with Frazier Healthcare Ventures since September 1999, and is
currently a general partner. Frazier Healthcare Ventures manages
venture capital funds that invest in early, mid and late stage
biopharma, medical device and healthcare service companies.
Prior to Frazier Healthcare Ventures, Mr. Heron was with
McKinsey & Co.’s biotechnology consulting practice
from 1992 to 1999, working on corporate strategy, M&A,
product launch, corporate partnering and research
prioritization. Mr. Heron obtained a B.A. from, and was a
Morehead Scholar at, the University of North Carolina at Chapel
Hill and holds an M.B.A. from Harvard Business School. In
addition to QuatRx, he also serves on the boards of Avera
Pharmaceuticals, Chimerix, Cerexa Pharmaceuticals, GenoSpectra,
Informed Medical Communications and Trubion Pharmaceuticals.
Christopher Moller, Ph.D. has served as a member of
our board of directors since December 2000 and, through
TL Ventures, was a founding investor in QuatRx. In 1990,
Dr. Moller joined Radnor Venture Partners, a
TL Ventures predecessor fund, and has been leading the
biotechnology group since 1992, having responsibility for
selecting, evaluating and managing all the biotechnology
companies in TL Ventures’ portfolio. Dr. Moller
currently serves as a director of Sopherion Therapeutics,
PharmaStem Therapeutics and CombinatoRx. Dr. Moller holds a
Ph.D. in immunology from the University of Pennsylvania.
Dr. Moller has informed us that he intends to resign from
our board of directors upon consummation of this offering.
Nicholas Simon III has served as a member of our
board of directors since May 2003. Mr. Simon has been a
Managing Director of Clarus Ventures, a life sciences focused
venture capital firm, since February 2005. Mr. Simon has
also been a General Partner in MPM Bioventures III since October
2001. From 2000 to July 2001, Mr. Simon was the Chief
Executive Officer, founder and a director of Collabra Pharma, a
pharmaceutical development company. From 1989 to March 2000,
Mr. Simon served in various management positions with
Genentech including Vice President of Business and Corporate
Development. He currently serves on the board of directors of
several biopharmaceutical companies, including ARYx
Therapeutics, Barrier Therapeutics, Inc. and CoTherix, Inc., as
well as several private companies. He also serves on the
Advisory Board of Gladstone Foundation, a private
not-for-profit research
institute affiliated with UCSF. Mr. Simon holds a B.S. in
microbiology from the University of Maryland and an M.B.A. from
Loyola College.
August M. Watanabe, M.D. has served on our board of
directors since September 2003. From March 1990 to his
retirement in June 2003, Dr. Watanabe was with Eli Lilly
and Company, where he served as the Director and Executive Vice
President of Science and Technology at Eli Lilly and President
of Lilly Research Laboratories from 1994 to 2003. Prior to Eli
Lilly, from July 1971 to March 1990, Dr. Watanabe was a
full-time faculty member of the Department of Medicine of
Indiana University School of Medicine, and Professor and
Chairman of the Department of Internal Medicine at Indiana
University School of Medicine. He has co-authored more than 100
scientific publications. Dr. Watanabe has served as an
officer in several national academic organizations, including
the American College of Cardiology and the American Heart
Association, and as a consultant to the U.S. Food and Drug
Administration and the U.S. Public Health Service’s
National Institutes of Health. Dr. Watanabe serves on the
boards of other biopharmaceutical companies, including Guidant
Corporation, Reliant, Endocyte, Kalypsys and Ambrx.
Dr. Watanabe received his medical degree from the Indiana
University School of Medicine.
Anders Wiklund has served on our board of directors since
October 2005. Mr. Wiklund has been a principal of Wiklund
International Inc., a biotechnology advisory firm, since January
1997, and serves on the boards of several other
biopharmaceutical companies, including Medivir AB, EffRx, Gyros
AB and Insite Vision Inc. Mr. Wiklund was also on the board
and was a co-founder of Esperion Therapeutics. Previously, from
January 1996 to December 1996, Mr. Wiklund led corporate
business development at Pharmacia Inc. (later
Pharmacia & Upjohn). Prior to that, Mr. Wiklund
was chief executive officer and president of KabiVitrum Inc. and
Kabi Pharmacia Inc., as well as president of KabiVitrum
International in Stockholm, Sweden. Mr. Wiklund received
his Masters of Pharmacy from the Pharmaceutical Institute in
Stockholm, Sweden and studied business administration at the
University of Stockholm.
Our Scientific Advisory Board was initially formed in early
2004. The purpose of this Board is to provide input on our
compounds in development. As such, we ask them to review and
comment on data as requested. We have met with them as
individuals and as a group on several occasions since that time.
When the Board was originally formed, the focus of the portfolio
was lipids and therefore the Board is heavily weighted with
expertise in the lipid area. We are currently meeting with
additional experts and will be adding additional expertise in
the endocrine area consistent with our current portfolio of
product candidates.
The following individuals are members of our Scientific Advisory
Board:
Name
Current Positions
Christie M. Ballantyne, M.D.
Director, Center for Cardiovascular Disease Prevention,
Methodist DeBakey Center; Professor, Section of Atherosclerosis,
Department of Medicine, Baylor College of Medicine
Robert H. Knopp, M.D.
Director, the Northwest Lipid Research Clinic; Professor of
Medicine, University of Washington School of Medicine
Daniel J. Rader, M.D.
Director, Preventive Cardiology and Lipid Clinic; Associate
Professor of Medicine, University of Pennsylvania School of
Medicine.
Alan R. Saltiel, Ph.D.
Director, Life Sciences Institute, Professor of Internal
Medicine and Physiology, University of Michigan School of
Medicine
August M. Watanabe, M.D.
Retired Executive Vice President of Science and Technology,
Director of Eli Lilly and Company, and President of Lilly
Research Laboratories
Composition of our Board of Directors
Immediately prior to this offering, our board of directors will
be divided into three staggered classes of directors of the same
or nearly the same number and each of our directors will be
assigned to one of the three classes. At each annual meeting of
stockholders, a class of directors will be elected for a
three-year term to succeed the directors of the same class whose
terms are then expiring. The terms of the directors will expire
upon election and qualification of successor directors at the
annual meeting of stockholders to be held during the years 2007
for the Class I directors, 2008 for the Class II
directors and 2009 for the Class III directors.
Our certificate of incorporation and bylaws provide that the
number of our directors shall be fixed from time to time by a
resolution of the majority of our board of directors. Any
additional directorships resulting from an increase in the
number of directors will be distributed among the three classes
so that, as nearly as possible, each class shall consist of one
third of the directors. There are no family relationships among
any of our directors or executive officers.
The division of our board of directors into three classes with
staggered three-year terms may delay or prevent stockholder
efforts to effect a change of our management or a change in
control.
Each of our directors currently serves on the board of directors
pursuant to a voting agreement. The voting agreement will
terminate upon the closing of this offering.
Committees of our Board of Directors
Our board of directors has established a compensation committee,
an audit committee and a nominating and corporate governance
committee.
Compensation Committee. Our compensation committee is a
standing committee of, and operates under a written charter
adopted by, our board of directors. Our compensation committee
consists of Patrick Heron, August Watanabe and Richard Fox. The
compensation committee makes decisions and recommendations
regarding cash and other compensation for our directors and
executive officers other than the compensation of
our Chief Executive Officer, which is recommended to and
determined by our board, and administers our incentive
compensation and benefit plans, including our Amended and
Restated 2005 Stock Incentive Plan.
Audit Committee. Our audit committee is a standing
committee of, and operates under a written charter adopted by,
our board of directors. Our audit committee consists of Patrick
Heron, Caley Castelein and Richard Fox. The audit committee
reviews and monitors our accounting practices and financial
statements; appoints, determines funding for, and oversees our
independent auditors; reviews the results and scope of audits;
approves the retention of the independent auditors to perform
any proposed permissible non-audit services; and reviews and
evaluates our audit and control functions. We believe that each
member of our audit committee satisfies the requirements for
members established by the Nasdaq National Market and the
Securities and Exchange Commission. Our board of directors has
determined that Mr. Fox is an audit committee financial
expert as currently defined under SEC rules.
Nominating and Corporate Governance Committee. Our
nominating and corporate governance committee is a standing
committee of, and operates under a written charter adopted by,
our board of directors. Our nominating and corporate governance
committee consists of Nicholas Simon, Anders Wiklund and William
Greene. The nominating and corporate governance committee is
authorized to identify and approve individuals qualified to
serve as members of our board of directors, select director
nominees for our annual meetings of stockholders, evaluate our
board’s performance and develop and recommend to our board
corporate governance guidelines and provide oversight with
respect to corporate governance and ethical conduct.
Other Committees. Our board of directors may establish
other committees as it deems necessary or appropriate from time
to time.
Compensation Committee Interlocks and Insider
Participation
None of the members of our compensation committee has at any
time been one of our officers or employees. None of our
executive officers currently serves, or in the past fiscal year
has served, as a member of the board of directors or
compensation committee of any entity that has one or more
executive officers serving on our board of directors or
compensation committee.
Director Compensation
We reimburse our directors who are not employees for their
reasonable expenses incurred in attending meetings of the board
of directors. Our directors are eligible to participate in our
Amended and Restated 2005 Stock Incentive Plan. Our outside
directors, Anders Wiklund, August Watanabe and Richard Fox,
receive payments of $1,500 for each meeting of our board of
directors attended in person, and $750 for each meeting of our
board attended telephonically.
Limitation of Liability and Indemnification of Officers and
Directors
Our certificate of incorporation limits the liability of
directors to the maximum extent permitted by Delaware law.
Delaware law provides that directors of a corporation will not
be personally liable for monetary damages for breach of their
fiduciary duties as directors, except liability for:
•
any breach of their duty of loyalty to the corporation or its
stockholders;
•
acts or omissions not in good faith or which involve intentional
misconduct or a knowing violation of law;
•
unlawful payments of dividends or unlawful stock repurchases or
redemptions; or
•
any transaction from which the director derived an improper
personal benefit.
Our bylaws provide that we will indemnify our directors and
officers to the fullest extent permitted by law, including if he
or she is serving as a director, officer, employee or agent of
another company at our request. We believe that indemnification
under our bylaws covers at least negligence and gross negligence
on
the part of indemnified parties. Our bylaws also permit us to
secure insurance on behalf of any officer, director, employee or
other agent for any liability arising out of his or her actions
in connection with their services to us, regardless of whether
our bylaws permit such indemnification.
In conjunction with this offering, we intend to enter into
separate indemnification agreements with our directors and
executive officers, in addition to the indemnification provided
for in our bylaws. These agreements, among other things, will
provide that we will indemnify our directors and executive
officers for certain expenses (including attorneys’ fees),
judgments, fines and settlement amounts incurred by a director
or executive officer in any action or proceeding arising out of
such person’s services as one of our directors or executive
officers, or any of our subsidiaries or any other company or
enterprise to which the person provides services at our request.
We believe that these provisions and agreements are necessary to
attract and retain qualified persons as directors and executive
officers.
There is no pending litigation or proceeding involving any of
our directors or executive officers as to which indemnification
is required or permitted, and we are not aware of any threatened
litigation or proceeding that may result in a claim for
indemnification.
Executive Compensation
The following table sets forth information regarding the
compensation that we paid to our Chief Executive Officer and
each of our other four most highly compensated executive
officers during the year ended December 31, 2005. We refer
to these officers in this prospectus as the “named
executive officers.”
In accordance with the rules of the SEC, the compensation
described in this table does not include medical, group life
insurance or other benefits which are available generally to all
of our salaried employees and certain perquisites and other
personal benefits received which do not exceed the lesser of
$50,000 or 10% of any named executive officer’s salary and
bonus disclosed in this table.
The following table sets forth information regarding grants of
stock options to each of our named executive officers during the
fiscal year ended December 31, 2005. The percentage of
options granted was based on aggregate grants of options to
purchase common stock totaling 4,187,710 shares granted to
employees during 2005. Potential realizable values are net of
exercise price before taxes, and are based on the assumption
that our common stock appreciates at the annual rate shown,
compounded annually, from the date of grant until expiration of
the ten-year term.
There was no public trading market for our common stock during
fiscal 2005. Accordingly, these exercise prices are based on our
board of directors’ determination of the fair market value
of the underlying shares as of the dates of grant.
(2)
A total of 25% of these options vested on May 20, 2005 and
the remaining options vest monthly in equal installments over
the following 36 months.
(3)
41,517.5 of these options vested on the date of grant;
6,156.50 options vested on July 20, 2005;
513.04 options vest monthly on and after August 20,2005; and 1,710.13 options vest monthly on and after
May 1, 2005.
(4)
4,229 of these options vested on the date of grant and the
remaining 31,720 options vested on May 20, 2005.
(5)
A total of
5/36
of these options vested on the date of grant and the remaining
options vest monthly in equal installments over the following
31 months.
(6)
12,585.67 of these options vested on the date of grant;
1,209.75 options vested on July 20, 2005;
100.81 options vest monthly on and after August 20,2005; and 336.08 options vest monthly on and after
May 1, 2005.
(7)
1,841 of these options vested on the date of grant and the
remaining 24,543 options vested on May 20, 2005.
(8)
27,336.5 of these options vested on the date of grant;
3,865 options vested on July 20, 2005;
322.08 options vest monthly on and after August 20,2005; and 1,073.63 options vest monthly on and after
May 1, 2005.
(9)
12,822.67 of these options vested on the date of grant;
1,209.75 options vested on July 20, 2005;
100.81 options vest monthly on and after August 20,2005; and 336.08 options vest monthly on and after
May 1, 2005.
(10)
1,916 of these options vested on the date of grant and the
remaining 31,935 options vested on May 20, 2005.
(11)
21,250 of these options vested on the date of grant and
1/48
of the total number of options vest monthly on and after
May 1, 2005.
(12)
10,449 of these options vested on the date of grant and the
remaining 17,415 options vested on May 20, 2005.
The potential realizable value is calculated based on the
ten-year term of the stock option at the time of grant. The
assumed 5% and 10% rates of stock price appreciation are
provided in accordance with the rules of the SEC based on an
assumed initial public offering price of
$ per
share and do not represent our estimate or projection of our
future stock price. The potential realizable values at 5% and
10% appreciation are calculated by:
•
multiplying the number of shares of common stock subject to a
given stock option by the assumed initial public offering price
of
$ per
share;
•
assuming that the aggregate stock value derived from that
calculation compounds at the annual 5% or 10% rate shown in the
table until the expiration of the option; and
•
subtracting from that result the aggregate option exercise price.
Aggregated Option Exercises in Last Fiscal Year and Fiscal
Year-End Option Values
The following table sets forth the number and value of
securities underlying options held as of December 31, 2005
by each of our named executive officers. Options shown as
exercisable in the table below are immediately exercisable.
These values have been calculated based on an assumed initial
public offering price of
$ per share, less
the applicable exercise price per share, multiplied by the
underlying shares, without taking into account any taxes that
may be payable in connection with the transaction.
Employment Agreements and Change of Control Arrangements
We have entered into an employment agreement dated as of
September 29, 2003 with Gary Onn, our Chief Financial
Officer. The agreement provides for an employment at-will
arrangement and can be terminated by Mr. Onn or us at any
time. Pursuant to his employment agreement, Mr. Onn is
entitled to a base salary of $175,000 per year. In 2004,
our board of directors authorized an increase in
Mr. Onn’s annual salary to $187,250. Under the
agreement, we granted Mr. Onn an option to purchase up to
400,000 shares of our common stock at a price of
$0.20 per share. According to the vesting schedule in
Mr. Onn’s employment agreement, 100,000 shares of
the option vested on November 1, 2004, and an additional
8,333.34 shares vested or will vest in each subsequent
month of Mr. Onn’s employment. The vesting schedule
will accelerate if Mr. Onn’s employment is terminated
without cause, or upon a dissolution or liquidation or change of
control involving us or sale of all or substantially all of our
assets. Under Mr. Onn’s employment agreement, if we
terminate Mr. Onn’s employment without cause, he is
entitled to his then annual salary for nine months.
Benefit Plans
Amended and Restated 2005 Stock Incentive Plan
We maintain a stock incentive plan which allows for the grant of
incentive stock options, nonqualified stock options, stock
bonuses, stock appreciation rights and rights to acquire
restricted stock to our employees, directors and consultants.
The plan has a ten year term that commenced on April 18,2005 and terminates on April 17,
2015, unless it is terminated earlier as approved by our
stockholders. The plan may be administered by our board of
directors or any committee of one or more members of the board
appointed by the board. We have reserved 5,851,979 shares
of our common stock, increased by up to 2,323,280 shares
issued under our 2000 Equity Incentive Plan that are forfeited
to us (i.e., in connection with the termination of the
holder’s employment) or that were subject to options
granted by us pursuant to the 2000 Equity Incentive Plan which
terminate or expire or become unexercisable for any reason
without having been exercised in full after April 14, 2005,
for issuance pursuant to awards under this plan. As of
December 31, 2005, options to purchase a total of
5,576,671 shares of common stock, with a weighted average
price of $0.31 per share, were outstanding under this plan. The
Board has authorized the grant to management of options to
purchase 4,375,000 shares of Company common stock upon the
attainment of Company milestones, 1,625,000 of which will be
granted upon the success of a phase II study as determined
by the board and 2,750,000 of which will be granted upon the
success of a phase III study to be determined by the board.
The allocations of the options will be determined prior to grant
and the exercise price will be the fair market value of the
Company’s common stock on the date of grant. The Company
plans to seek board and stockholder approval to increase the
number of shares underlying the stock incentive plan to provide
for these options.
Administration. The administrative committee selects the
individuals to receive awards under the stock incentive plan and
sets the terms and conditions of each award. The administrative
committee has plenary authority to interpret the stock incentive
plan and to make all determinations relating to the plan. After
the date that awards under this plan are no longer exempt from
the provisions of Section 162(m) of the Internal Revenue
Code, the maximum number of shares of our common stock that may
be subject to awards of options or stock appreciation rights for
any single individual in any year cannot exceed 1.5 million
shares, except that awards covering up to an additional
1 million shares may be granted to an individual during
their first year of service as an employee, director or
consultant.
Term of Awards; Transferability. The term of each award
is set by the administrative committee, provided that, in the
case of an option, no term can exceed ten years, or ten and
one-half years (or a shorter period) in the case of options
granted to employees in certain jurisdictions outside the United
States, from the date of grant. Awards may expire earlier upon
an optionee’s termination of employment. Awards under the
plan are non-assignable and otherwise non-transferable except as
determined by the administrative committee or by will or the
laws of descent and distribution.
Stock Options. Options granted under the stock incentive
plan may be “incentive stock options” as defined under
Section 422 of the Internal Revenue Code or nonqualified
stock options. Incentive stock options may only be granted to
employees. The exercise price and vesting schedule for options
will be set by the administrative committee at the time of
grant, provided that the per share exercise price for incentive
stock options and nonqualified stock options intended to be
exempt from the provisions of Section 162(m) of the
Internal Revenue Code cannot be less than the fair market value
of a share of our common stock on the date of grant. Fair market
value is defined in the stock incentive plan as the closing
price of our common stock on the Nasdaq Stock Market, or such
national securities exchange upon which our common stock is
listed, on the date of determination. If our common stock is not
publicly traded, the administrative committee determines the
fair market value in a manner it deems reasonable in good faith.
The exercise price of an option may be reduced, or options
cancelled and regranted in order to reduce the applicable
exercise price, without stockholder approval. Upon exercise, the
exercise price for an option may be paid in cash, by bank check
or wire transfer or, in the discretion of the administrative
committee, through delivery of shares of our common stock having
an aggregate value equal to the aggregate exercise price, or
through a brokered exercise procedure or other procedure not in
violation of any law.
Other Stock-based Awards. The administrative committee
may grant other cash, stock or stock-related awards under the
stock incentive plan, including stock appreciation rights and
stock units. The terms and conditions of any such other
stock-based awards will be determined by the administrative
committee, in its sole discretion. Shares of restricted stock
granted under the stock incentive plan will be subject to
forfeiture upon the termination of employment. The holder of a
restricted stock award will generally have the rights and
privileges of a stockholder after the shares are issued,
including the right to vote such shares. Cash and stock
dividends on such shares, if any, may be distributed to the
holder of a restricted stock award or held for the account of
the holder, as determined by the administrative committee.
Adjustments. All outstanding awards under the stock
incentive plan, the maximum number of shares available under the
stock incentive plan and the maximum number of shares of our
common stock available pursuant to the grant of options and
stock appreciation rights to any single person in any year, if
applicable, are subject to adjustment or substitution, as
determined by the administrative committee in the event of
certain corporate transactions.
Restrictions on Shares. In an award agreement, we may
reserve a right of first refusal to purchase all shares that a
participant proposes to transfer to a third party. Our right of
first refusal terminates upon the initial public offering of our
common stock.
Amendment. The stock incentive plan may be terminated or
amended at any time by the administrative committee, subject to
the approval of our stockholders as required by law, provided
that without stockholder approval no such amendment may:
•
materially increase the number of shares of our common stock for
which awards may be granted under the stock incentive plan;
•
reduce the minimum exercise price at which options may be
granted under the incentive stock plan; or
•
change the class of persons eligible to receive awards under the
plan without stockholder approval.
Except for adjustments subject to certain corporate transactions
and amendments, suspensions or termination of the plan that do
not impair the rights of an award, alterations to outstanding
awards under the stock incentive plan may be made only with the
consent of the award recipient.
2000 Equity Incentive Plan
Our 2000 Equity Incentive Plan, or the 2000 Plan, was adopted by
our board of directors. The 2000 Plan has a ten-year term that
commenced on December 19, 2000 and terminates on
December 18, 2010 unless it is terminated earlier as
approved by our stockholders. We no longer expect to grant
options under this plan, but as of December 31, 2005,
non-qualified options to purchase a total of
1,328,961 shares of common stock, with a weighted average
exercise price of $0.20 per share, were outstanding under this
plan. The 2000 Plan allowed for the grant or sale of stock
options and restricted stock awards to employees, officers,
directors and consultants.
Administration. The 2000 Plan is administered by the
committee appointed by our board of directors or administered by
our board of directors acting as the committee. The
administrative committee selected individuals to receive awards
under the 2000 Plan and sets the terms and conditions of each
award. The administrative committee also has the authority to
interpret the 2000 Plan, set rules and regulations relating to
it, and make all other determinations for the administration of
the 2000 Plan.
Payment for Share Purchase. Payment for shares purchased
under the 2000 Plan may be made in cash by check, or, where
expressly approved for the participant by the administrative
committee and where permitted by law, by cancellation of any
debt owned by us, shares of our common stock (with some
restriction), full recourse promissory note having such terms as
approved by the administrative committee, waiver of compensation
or, if the shares are purchased on exercise of an option, the
2000 Plan also permits payment to be made by broker-assisted
same day sales or margin commitment, or by surrender of shares
then issuable upon exercise of the option. The administrative
committee may help the participant pay for shares purchased
under the 2000 Plan by authorizing a guarantee by us of a third
party loan to the participant.
Rights and Privileges; Transferability. No participant
will have any rights of a shareholder until the shares are
issued to the participant. After the issuance, the participant
will be a shareholder and have all the rights of a shareholder
with respect to such shares, including the right to vote and
receive dividends or other distributions. If the shares issued
are restricted stock, then any new, additional or different
securities the participant receives by virtue of stock dividend,
stock split or any other changes in our corporate or capital
structure will be subject to the same restrictions as the
restricted stock. Awards granted under the 2000 Plan are not
transferable or assignable by participant, and may not be made
subject to execution, attachment or similar process, otherwise
than by will or by the laws of descent and distribution.
However, the administrative committee may provide that the
awards granted under the 2000 Plan (other than an incentive
stock option) be transferable, without consideration, to a
participant’s immediate family members.
Restrictions on Shares. In an award agreement, we may
reserve a right of first refusal to purchase all shares that a
participant proposes to transfer to a third party. Our right of
first refusal terminates upon the initial public offering of our
common stock. In an award agreement, we may also reserve a right
to repurchase the unvested shares held by a participant for cash
and/or cancellation of purchase money indebtedness, following
such participant’s termination at any time within
90 days after his termination date and the date the
participant purchases shares, whichever is later.
Exchange and Buyout. With the consent of participants,
the administrative committee may authorize us to issue new
awards in exchange for the surrender and cancellation of
outstanding awards. The administrative committee may buy from a
participant an award previously granted with payment in cash,
shares of our common stock (including restricted stock) or other
consideration, based on the terms and conditions agreed by the
administrative committee and the participant.
Amendment. The 2000 Plan may be amended by the
administrative committee. However, without stockholder approval,
no such amendment may increase the number of shares reserved for
issuance under the 2000 Plan. Our board of directors may suspend
the 2000 Plan at any time; however, such suspension must not
adversely affect any outstanding benefit.
Vesting and Exercise Price of Stock Options. The vesting
schedule and exercise price for options granted under the 2000
Plan were determined by the administrative committee and set
forth in a stock option agreement. In no event is an option
exercisable after 10 years from the grant date. The
exercise price of the non-qualified options was not less than
85% of the fair market value of the shares on the date of grant.
Since our common stock was not publicly traded at the time of
the grants under the 2000 Plan, the administrative committee
determined the fair market value in a manner it deemed
reasonable and in good faith.
Termination. If a participant of the 2000 Plan is
terminated because of death or disability, then the
participant’s option is exercisable only to the extent that
it is exercisable on the termination date, and the option must
be exercised by the participant no later than 12 months
after the termination date. If a participant is terminated for
cause, then the participant’s option will expire on the
termination date, or at such later time determined by the
administrative committee. If a participant is terminated for any
reason except death, disability or for cause, then the
participant’s option is exercisable only to the extent that
it is exercisable on the termination date, and the option must
be excised no later than 3 months after the termination
date. In any event, no option may be exercised after the
expiration date of the options.
Modification, Extension or Renewal. The administrative
committee may modify, extend or renew outstanding options and
authorize the grant of new options in substitution for the
outstanding options, however, such action may not, without the
written consent of a participant, impair the participant’s
rights under any option previously granted. The administrative
committee may reduce the exercise price of outstanding options
without the consent of participants affected by a written notice
to them; however, the exercise price may not be reduced below
the minimum exercise price that would be permitted under the
2000 Plan.
401(k) Plan
We have established a tax-qualified employee savings and
retirement plan for all employees who satisfy certain
eligibility requirements, including requirements relating to age
and length of service. Under our 401(k) plan, employees may
elect to reduce their current compensation by up to 15% or the
statutory limit, $13,000 in 2004, whichever is less, and have us
contribute the amount of this reduction to the 401(k) plan. In
addition, we contribute an amount equal to 3% of certain
eligible employees’ compensation as a nonelective
contribution to our 401(k) plan. As of December 31, 2005 we
had 12 employees eligible for participation in our 401(k) plan.
We will make contributions of approximately $28,000 for 2005 to
the plan for certain eligible employees.
We intend for the 401(k) plan to qualify under Section 401
of the Internal Revenue Code so that contributions by employees
or by us to the 401(k) plan, and income earned on plan
contributions, are not taxable to employees until withdrawn from
the 401(k) plan. Our contributions, if any, will be deducted by
us when made.
CERTAIN RELATIONSHIPS AND RELATED PARTY TRANSACTIONS
The following is a description of transactions since
January 1, 2003 to which we were or are a party in which
the amount involved exceeds $60,000 and in which any director,
executive officer or holder of more than 5% of our capital stock
or any member of such person’s immediate family had or will
have a direct or indirect material interest, other than
compensation agreements, which are described under the caption
“Management”.
Purchases of Securities
Since January 1, 2003, the following executive officers,
directors, holders of more than 5% of our capital stock and
members of such person’s immediate family purchased
securities in the amounts and as of the dates shown below.
Number of
Number of
Number of
Number of
Number of
Shares of
Shares of
Shares of
Shares of
Shares of
Series B
Series C
Series D
Series D-1
Common
Preferred
Preferred
Preferred
Preferred
Name of Purchaser
Stock
Stock
Stock
Stock
Stock
5% Stockholders affiliated with Directors:
Entities associated with Fraizer Healthcare Ventures(1)
—
700,000
3,070,176
1,428,571
—
Entities associated with InterWest Partners(2)
—
—
4,385,964
4,285,714
—
Entities associated with MPM BioVentures III(3)
—
—
13,456,140
7,857,142
—
Thomas Weisel Healthcare Venture Partners, L.P.(4)
—
—
—
5,000,000
—
Entities associated with TL Ventures(5)
—
700,000
3,508,772
2,500,000
—
Other 5% Stockholders:
Biomedical Venture III Ltd.(6)
1,920,827
—
—
1,271,432
795,217
Directors and Executive Officers:
Caley Castelein, M.D.(4)
—
—
—
—
—
Christopher B. Ehrlich(2)
—
—
—
—
—
William Greene, M.D.(3)
—
—
—
—
—
Patrick Heron(1)
—
—
—
—
—
Christopher Moller, Ph.D.(5)
—
—
—
—
—
Robert Zerbe, M.D.(7)
452,357
—
—
—
—
(1)
Represents shares held by Frazier Healthcare, III L.P. and
Frazier Affiliates, III, L.P. Patrick Heron, a member of
our board of directors, is a venture capitalist with Frazier
Healthcare Ventures where he holds the title of General Partner.
Entities affiliated with Frazier Healthcare Ventures serve as
the general partners of Frazier Healthcare III, LP and
Frazier Affiliates III, LP. During 2003, entities
associated with Frazier Healthcare Ventures purchased
700,000 shares of our Series B Preferred Stock at
$1.50 per share. During 2003 and 2004, entities associated
with Frazier Healthcare Ventures purchased 3,070,176 shares
of our Series C Preferred Stock at $1.14 per share,
and in 2004 and 2005, entities associated with Frazier
Healthcare Ventures purchased 1,428,571 shares of our
Series D Preferred Stock at $1.40 per share.
(2)
Represents shares held by InterWest Investors VIII, L.P.,
InterWest Investors Q VIII, L.P. and InterWest Partners VIII,
L.P. Christopher Ehrlich, a member of our board of directors, is
a Partner at InterWest Partners. During 2003 and 2004, entities
associated with InterWest Partners purchased
4,385,964 shares of our Series C Preferred Stock at
$1.14 per share. During 2004 and 2005, entities associated
with InterWest Partners purchased 4,285,714 shares of our
Series D Preferred Stock at $1.40 per share.
(3)
Represents shares held by MPM Asset Management Investors 2003
BVIII LLC, MPM Bioventures III GmbH & Co.
Beteiligungs KG, MPM Bioventures III Parallel Fund, L.P.,
MPM Bioventures III, L.P., MPM Bioventures III-QP, L.P.,
MPM Bioventures Strategic Fund, L.P. William Greene, M.D.
and Nicholas Simon III, members of our board of directors,
are General Partners of MPM Bioventures III. During 2003
and 2004, entities associated with MPM Bioventures III
purchased 13,456,140 shares of our Series C Preferred
Stock at $1.14 per share and 7,857,142 shares of our
Series D Preferred Stock at $1.40 per share.
Caley Castelein, M.D., a member of our board of directors,
is a Managing Partner of Thomas Weisel Healthcare Partners LLC,
the General Partner of Thomas Weisel Healthcare Venture
Partners, L.P. During 2004 and 2005, Thomas Weisel Healthcare
Venture Partners LLC purchased 5,000,000 shares of our
Series D Preferred Stock at $1.40 per share.
(5)
Represents shares held by TL Ventures V Interfund, L.P. and TL
Ventures V L.P. Christopher Moller, Ph.D., a member of our
board of directors, is a member and on the board of directors of
TL Ventures V LLC, the General Partner of TL
Ventures V Interfund L.P. and TL Ventures V Management
L.P., the General Partner of TL Ventures V L.P. During
2003, entities associated with TL Ventures purchased
700,000 shares of our Series B Preferred Stock at
$1.50 per share. During 2003 and 2004, entities associated
with TL Ventures purchased 3,508,772 shares of our
Series C Preferred Stock at $1.14 per share, and in
2004 and 2005, entities associated with TL Ventures purchased
2,500,000 shares of our Series D Preferred Stock at
$1.40 per share.
(6)
In May 2005, we issued 200,003 shares of our Series D
Preferred Stock, 795,217 shares of our Series D-1
Preferred Stock and 1,920,827 shares of our common stock to
Biomedical Venture III Ltd. in exchange for shares of
Hormos representing all the outstanding capital stock of Hormos
and all securities or other instruments convertible into or
exercisable for capital stock of Hormos held by Biomedical
Venture III Ltd. Between June 2005 and October 2005,
Biomedical Venture III Ltd. purchased
1,071,428.57 shares of our Series D Preferred Stock at
$1.40 per share.
(7)
During 2005, Robert Zerbe, M.D., our Chief Executive
Officer, exercised options to purchase 407,893 shares
of our common stock at an exercise price of $0.20 per
share. During 2006, Dr. Zerbe exercised options to purchase
an additional 44,464 shares at an exercise price of $0.20
per share.
Indemnification Agreements
As permitted by the Delaware General Corporation Law, we have
adopted provisions in our certificate of incorporation and
bylaws that authorize and require us to indemnify our officers
and directors to the full extent permitted under Delaware law,
subject to limited exceptions. See “Management —
Limitation of Liability and Indemnification of Officers and
Directors.” In addition, in conjunction with this offering,
we intend to enter into separate indemnification agreements with
our directors and executive officers, in addition to the
indemnification provided for in our bylaws.
Fourth Amended and Restated Investor Rights Agreement, as
amended
We and our preferred stockholders have entered into an investor
rights agreement under which our preferred stockholders have
registration rights with respect to their shares of common
stock, rights of first refusal on certain new issues of our
capital stock and rights to purchase shares in this offering.
These rights have been waived with respect to this offering and
the rights of first refusal shall terminate immediately prior to
the closing of this offering. Upon closing of this offering, all
our currently outstanding shares of preferred stock will be
converted into shares of our common stock. See “Description
of Capital Stock — Registration Rights” for a
further description of the terms of this agreement.
The following table presents information concerning the
beneficial ownership of the shares of our common stock as of
February 28, 2006, by:
•
each person we know to be the beneficial owner of 5% or more of
our outstanding shares of our capital stock;
•
each of our named executive officers listed on the Summary
Compensation Table;
•
each of our directors; and
•
all of our executive officers and directors as a group.
The information set forth in the table gives effect to the
conversion of all of our preferred stock.
Beneficial ownership is determined under the rules of the SEC
and generally includes voting or investment power over
securities. Except in cases where community property laws apply
or as indicated in the footnotes to this table, we believe that
each stockholder identified in the table possesses sole voting
and investment power over all shares of common stock shown as
beneficially owned by the stockholder. Percentage of beneficial
ownership is based on 77,573,662 shares of common stock
outstanding as of February 28, 2006 (as adjusted to reflect
as of that date the conversion of all shares of our preferred
stock outstanding into common stock),
and shares
of common stock outstanding after the completion of this
offering. Shares of common stock subject to options that are
currently exercisable or exercisable within 60 days of
February 28, 2006, are considered outstanding and
beneficially owned by the person holding the options for the
purpose of computing the percentage ownership of that person but
are not treated as outstanding for the purpose of computing the
percentage ownership of any other person. Unless indicated
below, the address of each individual listed below is
c/o QuatRx Pharmaceuticals Company, 777 East Eisenhower
Parkway, Suite 100, Ann Arbor, Michigan48108.
Percentage of Shares
Number of
Outstanding
Shares
Beneficially
Prior to the
After the
Name of Beneficial Owner
Owned(1)
Offering
Offering
Stockholders owning 5% or more:
Entities affiliated with MPM Bioventures III(2)
21,313,282
27.47
%
Entities affiliated with TL Ventures(3)
9,362,711
12.07
Entities affiliated with InterWest Partners(4)
8,671,678
11.18
Entities affiliated with Frazier Healthcare(5)
8,252,686
10.64
Entities affiliated with Thomas Weisel Healthcare Venture
Partners, L.P.(6)
Includes shares of common stock issuable pursuant to options
exercisable within 60 days of February 28, 2005.
(2)
Includes 326,238 shares held by MPM Asset Management
Investors 2003 BVIII LLC, 1,424,013 shares held by MPM
Bioventures III GmbH & Co. Beteiligungs KG,
508,879 shares held by MPM Bioventures III Parallel
Fund, L.P., 1,132,937 shares held by MPM
Bioventures III, L.P., 16,849,787 shares held by MPM
Bioventures III-QP,
L.P. and 1,071,428 shares held by MPM Bioventures Strategic
Fund, L.P., collectively, the MPM Funds. William
Greene, M.D. and Nicholas Simon III, members of our
board of directors, are General Partners of
MPM Bioventures III. Dr. Greene and
Mr. Simon have shared voting and dispositive powers over
the shares held by the MPM Funds. They disclaim beneficial
ownership of the shares held by the MPM Funds, except to the
extent of their pecuniary interest therein. The address for MPM
BioVentures III LLC is 200 Clarendon St.,
54th Floor, Boston, MA02116.
(3)
Includes 159,185 shares held by TL Ventures V Interfund,
L.P. and 9,203,526 shares held by TL Ventures V L.P.,
collectively, the TL Ventures Funds. Christopher
Moller, Ph.D., a member of our board of directors, is a
member and on the board of directors of TL Ventures V LLC,
the general partner of TL Ventures V Interfund L.P.
and TL Ventures V Management L.P., the general partner of TL
Ventures V L.P. Dr. Moller may be deemed to have
shared voting and dispositive powers over the shares held by the
TL Ventures Funds. He disclaims beneficial ownership of the
shares held by the TL Ventures Funds, except to the extent of
his pecuniary interest therein. The address for the TL Ventures
Funds is 700 Building, 435 Devon Park Drive, Wayne, PA19087.
(4)
Includes 66,772 shares held by InterWest Investors VIII,
L.P., 239,338 shares held by InterWest Investors Q VIII,
L.P. and 8,365,568 shares held by InterWest Partners VIII,
L.P, collectively, the InterWest Funds. Christopher Ehrlich, a
member of our board of directors, is a Venture Member of
InterWest Management Partners VIII, LLC, the general partner of
the InterWest Funds. Mr. Ehrlich has shared voting and
dispositive powers over the shares held by the InterWest Funds.
He disclaims beneficial ownership of the shares held by the
InterWest Funds, except to the extent of his pecuniary interest
therein. The address for InterWest Partners is 2710 Sand Hill
Road, Menlo Park, CA94025.
(5)
Includes 8,191,086 shares held by Frazier
Healthcare III, L.P. and 61,600 shares held by Frazier
Affiliates, III, L.P., collectively, the Frazier III
Funds. Patrick Heron, a member of our board of directors, is a
venture capitalist with Frazier Healthcare Ventures where he
holds the title of General Partner. Entities affiliated with
Frazier Healthcare Ventures serve as the general partners of the
Frazier III Funds. Mr. Heron may be deemed to have
shared voting and dispositive powers over the shares held by the
Frazier III Funds. He disclaims beneficial ownership of the
shares held by the Frazier III Funds, except to the extent
of his pecuniary interest therein. The address for the
Frazier III Funds and Frazier Healthcare Ventures is
601 Union Street, Suite 3200, Seattle, WA98101.
(6)
Caley Castelein, M.D., a member of our board of directors,
is a Managing Partner of Thomas Weisel Healthcare Partners LLC,
the general partner of Thomas Weisel Healthcare Venture
Partners, L.P. Mr. Castelein has shared voting and
dispositive powers over the shares held by Thomas Weisel
Healthcare Venture Partners, L.P. He disclaims beneficial
ownership of the shares held by the Thomas Weisel Healthcare
Venture Partners, L.P., except to the extent of his pecuniary
interest therein. The address for Thomas Weisel Healthcare
Venture Partners is One Montgomery Street, San Francisco,
CA94101.
(7)
The address for Biomedical Venture III Ltd. is
Sundkrogsgade 7, DK-2100, Copenhagen, Denmark.
(8)
Includes 5,000 shares of common stock issuable upon the
exercise of stock options exercisable within 60 days of
February 28, 2006.
(9)
Includes 583,597 shares of common stock issuable upon the
exercise of stock options exercisable within 60 days of
February 28, 2006. Also includes an aggregate of
955,000 shares held by trusts established by Dr. Zerbe
for the benefit of his children and of which he and his wife,
Linda Zerbe, are the trustees.
(10)
Includes 290,020 shares of common stock issuable upon the
exercise of stock options exercisable within 60 days of
February 28, 2006. Also includes an aggregate of
925,000 shares held by trusts established by
Dr. Dombey for the benefit of his children and of which he
and his wife, Heather Jane Dombey, are the trustees and
40,000 shares held by a trust established by
Dr. Dombey as trustee of the Stuart Lionel Dombey Trust
u/a/d.
(11)
Includes 297,438 shares of common stock issuable upon the
exercise of stock options exercisable within 60 days of
February 28, 2006. Also includes 20,000 shares held by
Christine L. Nicholas, Mr. Nicholas’s wife and an
aggregate of 450,000 shares held by trusts established by
Mr. Nicholas for the benefit of his children.
(12)
Includes 219,533 shares of common stock issuable upon the
exercise of stock options exercisable within 60 days of
February 28, 2006.
(13)
Includes 343,654 shares of common stock issuable upon the
exercise of stock options exercisable within 60 days of
February 28, 2006. Also includes an aggregate of
400,000 shares held by trusts established by
Dr. Whitcomb of which he and his wife, Rita K. Whitcomb,
are the trustees.
Upon the completion of this offering, our authorized capital
stock will consist
of shares
of common stock, par value $0.01 per share,
and shares
of preferred stock, par value $0.01 per share, and there
will
be shares
of common stock outstanding and no shares of preferred stock
outstanding. As of December 31, 2005, we had
approximately record
holders of our capital stock. All of our outstanding shares of
preferred stock will automatically convert into shares of our
common stock upon the completion of this offering. In addition,
upon completion of this offering, options to
purchase shares
of our common stock will be outstanding
and shares
of our common stock will be reserved for future grants under our
Amended and Restated 2005 Stock Incentive Plan.
The following description of our capital stock and provisions of
our certificate of incorporation and bylaws are summaries of
material terms and provisions and are qualified by reference to
our certificate of incorporation and bylaws, copies of which
have been filed with the SEC as exhibits to the registration
statement of which this prospectus is a part. The descriptions
of the common stock and preferred stock reflect amendments to
our certificate of incorporation and bylaws that will become
effective upon closing of this offering.
Common Stock
Upon the closing of this offering, we will be authorized to
issue one class of common stock. Stockholders will be entitled
to one vote for each share of our common stock held of record on
all matters on which stockholders are entitled or permitted to
vote. Our common stock will not have cumulative voting rights in
the election of directors. As a result, holders of a majority of
the shares of our common stock voting for the election of
directors can elect all the directors standing for election.
Holders of our common stock will be entitled to receive
dividends out of legally available funds when and if declared
from time to time by our board of directors. See “Dividend
Policy.” In the event of our liquidation, dissolution or
winding up, the holders of our common stock will be entitled to
share ratably in all assets remaining after payment of
liabilities, subject to the rights of any then outstanding
preferred stock. The rights, preferences and privileges of
holders of our common stock will be subject to, and may be
adversely affected by, the rights of holders of shares of any
series of preferred stock that we may designate and issue in the
future. All outstanding shares of our common stock are fully
paid and nonassessable, and the shares of common stock offered
hereby will be fully paid and nonassessable.
Preferred Stock
Upon the closing of this offering, all outstanding shares of our
preferred stock, including shares of preferred stock held in the
escrow established in connection with our acquisition of Hormos,
will be converted into an aggregate of 62,296,525 shares of
common stock. Under our certificate of incorporation, upon the
closing of this offering, we will be authorized, subject to the
limits imposed by the Delaware General Corporation Law, to
issue shares
of preferred stock in one or more series, to establish from time
to time the number of shares to be included in each series, to
fix the rights, preferences and privileges of the shares of each
wholly unissued series and any of its qualifications,
limitations, restrictions. Our board of directors can also
increase or decrease the number of shares of any series of our
preferred stock, but not below the number of shares of that
series then outstanding, without any further vote or action by
our stockholders.
Our board of directors may authorize the issuance of preferred
stock with voting or conversion rights that could adversely
affect the voting power or other rights of our common
stockholders. The issuance of preferred stock, while providing
flexibility in connection with possible acquisitions and other
corporate purposes, could have the effect of delaying or
preventing our change in control and may cause the market price
of our common stock to decline or impair the voting and other
rights of the holders of our common stock. We have no current
plans to issue any shares of preferred stock.
Upon completion of this offering, the holders of
approximately shares
of common stock will be entitled to rights with respect to the
registration of these shares under the Securities Act as
described below.
Demand Registration Rights
At any time beginning 180 days after the closing of this
offering, the holders of at least fifty percent (50%) of the
shares having registration rights can demand that we file a
registration statement for those shares so long as the demand
covers at least fifty percent (50%) of the shares subject to the
registration rights. We will use our best efforts to effect the
registration as requested, unless the underwriters if any,
decide to limit the number of shares that may be included in the
registration due to marketing factors. We are only obligated to
satisfy two demand registrations (provided that at least eighty
percent (80%) of the shares requested to be registered must be
registered in order for such demand to qualify as a demand
registration), and we may defer a registration by up to
90 days under specified circumstances not more than once in
any 12-month period. We
are not obligated to satisfy a demand registration if the
registrable shares may be immediately registered pursuant to a
registration statement on
Form S-3, as
described below.
Piggyback Registration Rights
If we register any securities for public sale, the holders of
the shares having registration rights may include their shares
in the registration statement. The underwriters have the right
to limit the number of shares having registration rights that
may be included in the registration statement, but not below 20%
of the total number of shares included in the registration
statement. These piggyback registration rights have been waived
with respect to this offering on behalf of the holders of these
rights.
Form S-3
Registration Rights
If we are eligible to file a registration statement on
Form S-3, any
holders of the shares having registration rights can demand that
we file a registration statement on
Form S-3 or any
similar short-form registration statement, so long as
(i) the aggregate amount of securities to be sold under the
registration statement on
Form S-3 is at
least $1.0 million and (ii) we have not already
effected two registrations on
Form S-3 in any
12-month period.
Expenses of Registration
We will pay for all registration expenses, including the
reasonable legal expenses of a single counsel for the holders,
relating to any demand, piggyback or
Form S-3
registration, other than the underwriting discount and selling
commissions applicable to the shares of common stock held by the
holders with registration rights.
Expiration of Registration Rights
If shares having registration rights are sold either to the
public, sold pursuant to Rule 144 or sold by a holder in a
transaction in which those rights are not assigned, then the
shares will no longer be considered registrable shares.
We are subject to Section 203 of the Delaware General
Corporation Law. This statute regulating corporate takeovers
prohibits a Delaware corporation from engaging in any business
combination with any
interested stockholder for three years following the date that
the stockholder became an interested stockholder, unless:
•
prior to the date of the transaction that resulted in the
interested stockholder becoming an interested stockholder, the
board of directors of the corporation approved either the
business combination or the transaction which resulted in the
stockholder becoming an interested stockholder;
•
upon completion of the transaction that resulted in the
interested stockholder becoming an interested stockholder, the
interested stockholder owned at least 85% of the voting stock of
the corporation outstanding at the time the transaction
commenced, excluding for purposes of determining the number of
shares outstanding (a) shares owned by persons who are
directors and also officers, and (b) shares owned by
employee stock plans in which employee participants do not have
the right to determine confidentially whether shares held
subject to the plan will be tendered in a tender or exchange
offer; or
•
on or subsequent to the date of the transaction that resulted in
the interested stockholder becoming an interested stockholder,
the business combination is approved by the board and authorized
at an annual or special meeting of stockholders, and not by
written consent, by the affirmative vote of at least
662/3%
of the outstanding voting stock which is not owned by the
interested stockholder.
Generally, a business combination includes a merger, asset or
stock sale, or other transaction resulting in a financial
benefit to the interested stockholder. An interested stockholder
is a person who, together with affiliates and associates, owns
or, within three years prior to the determination of interested
stockholder status, did own 15% or more of a corporation’s
outstanding voting securities. We expect the existence of this
provision to have an anti-takeover effect with respect to
transactions our board of directors does not approve in advance.
We also anticipate that Section 203 may discourage takeover
attempts that might result in a premium over the market price
for the shares of common stock held by stockholders.
Provisions of our certificate of incorporation and bylaws, which
will become effective upon the closing of this offering, may
have the effect of making it more difficult for a third party to
acquire, or discourage a third party from attempting to acquire,
control of our company by means of a tender offer, a proxy
contest or otherwise. These provisions may also make the removal
of incumbent officers and directors more difficult. These
provisions are intended to discourage certain types of coercive
takeover practices and inadequate takeover bids and to encourage
persons seeking to acquire control of QuatRx to first negotiate
with us. These provisions could also limit the price that
investors might be willing to pay in the future for shares of
our common stock. These provisions may make it more difficult
for stockholders to take specific corporate actions and could
have the effect of delaying or preventing a change in control.
Staggered Board of Directors. Our board of directors is
divided into three classes of the same or nearly the same number
of directors, each serving staggered three-year terms, which
means that only one class of directors may be elected at each
annual meeting or special meeting in lieu of such annual
meeting. These provisions may make the removal of incumbent
directors difficult and may discourage third parties from
attempting to circumvent the anti-takeover effects of our
certificate of incorporation and bylaws by removing our
incumbent directors.
No Written Consent of Stockholders. Any action to be
taken by our stockholders must be effected at a duly called
annual or special meeting and may not be effected by written
consent.
Special Meetings of Stockholders. Special meetings of our
stockholders may be called only by (i) the Chairman of the
board of directors, (ii) the Chief Executive Officer, or
(iii) the board of directors pursuant to a resolution
adopted by a majority of the total number of authorized
directors.
Advance Notice Requirement. Stockholder proposals to be
brought before an annual meeting of our stockholders must comply
with advance notice procedures. These advance notice procedures
require timely
notice and apply in several situations, including stockholder
proposals relating to the nominations of persons for election to
the board of directors. Generally, to be timely, notice must be
received at our principal executive offices not less than
90 days nor more than 120 days prior to the first
anniversary date of the annual meeting for the preceding year.
Issuance of Undesignated Preferred Stock. Our board of
directors is authorized to issue, without further action by the
stockholders, up
to shares
of undesignated preferred stock with rights and preferences,
including voting rights, designated from time to time by the
board of directors. The existence of authorized but unissued
shares of preferred stock enables our board of directors to
render more difficult or to discourage an attempt to obtain
control of us by means of a merger, tender offer, proxy contest
or otherwise.
Transfer Agent and Registrar
The transfer agent and registrar for our common stock
is .
Listing
We have applied for our common stock to be quoted on the Nasdaq
National Market under the trading symbol “QTRX”.
The following is a general discussion of certain United States
federal income tax consequences of the ownership and disposition
of our common stock to a non-United States holder. For the
purpose of this discussion, a non-United States holder is any
beneficial holder of our common stock that for United States
federal income tax purposes is not a United States person. For
United States federal income tax purposes, person means:
•
an individual citizen or resident of the United States;
•
a corporation or other entity taxable as a corporation or a
partnership or entity taxable as a partnership created or
organized in the United States or under the laws of the United
States or any state thereof;
•
an estate whose income is subject to United States federal
income tax regardless of its source; or
•
a trust (i) whose administration is subject to the primary
supervision of a United States court and which has one or more
United States persons who have the authority to control all
substantial decisions of the trust or (ii) which has made
an election to be treated as a United States person.
If a partnership holds common stock, the tax treatment of a
partner will generally depend on the status of the partner and
upon the activities of the partnership. Accordingly, we urge
partnerships which hold our common stock and partners in such
partnerships to consult their tax advisors.
This discussion assumes that non-United States holders will hold
our common stock issued pursuant to the offering as a capital
asset (generally, property held for investment). This discussion
does not address all aspects of United States federal income
taxation that may be relevant in light of a non-United States
holder’s special tax status or special tax situations.
United States expatriates, life insurance companies, tax-exempt
organizations, dealers in securities or currency, banks or other
financial institutions, holders whose functional currency is
other than the United States dollar, “controlled foreign
corporations,”“passive foreign investment
companies,” and investors that hold common stock as part of
a hedge, straddle or conversion transaction are among those
categories of potential investors that are subject to special
rules not covered in this discussion. This discussion does not
address any tax consequences arising under the laws of any
state, local or non-United States taxing jurisdiction.
Furthermore, the following discussion is based on current
provisions of the Internal Revenue Code of 1986, as amended (the
“Code”), legislative history and Treasury Regulations
and administrative and judicial interpretations thereof, all as
in effect on the date hereof, and all of which are subject to
change, possibly with retroactive effect. Accordingly, we urge
each non-United States Holder to consult a tax advisor regarding
the United States federal, state, local and non-United States
income and other tax consequences of acquiring, holding and
disposing of shares of our common stock.
Prospective purchasers are urged to consult their own tax
advisors regarding United States federal income tax
consequences, as well as other United States federal, state, and
local income and estate tax consequences, and non-United States
tax consequences, to them of acquiring, owning, and disposing of
our common stock.
Dividends
We have not paid any distributions on our common stock and we do
not plan to pay any distributions for the foreseeable future.
However if we do make distributions on our common stock, those
payments will constitute dividends for United States tax
purposes to the extent paid from our current or accumulated
earnings and profits, as determined under United States federal
income tax principles. To the extent those distributions exceed
our current or accumulated earnings and profits, the
distributions will constitute a return of capital and will first
reduce a holder’s basis, but not below zero, and then will
be treated as gain from the sale of stock.
Any dividend paid from our current or accumulated earnings and
profits paid to a non-United States holder of common stock
generally will be subject to United States withholding tax
either at a rate of 30% of the gross amount of the dividend or
such lower rate as may be specified by an applicable tax treaty.
In order
to receive a reduced treaty rate, a non-United States holder
must provide us with an IRS
Form W-8BEN (or
successor form) certifying, under penalty of perjury, the
holder’s status as a
non-U.S. person as
defined under the Code and qualification for the reduced rate.
Dividends received by a non-United States holder that are
effectively connected with a United States trade or business
conducted by the non-United States holder are exempt from such
withholding tax. In order to obtain this exemption, a non-United
States holder must provide us with an IRS
Form W-8ECI (or
successor form) properly certifying such exemption. Such
effectively connected dividends, although not subject to
withholding tax, are taxed at the same graduated rates
applicable to United States persons, net of certain deductions
and credits. In addition to the graduated tax described above,
dividends received by a corporate non-United States holder that
are effectively connected with a United States trade or business
of the corporate non-United States holder may also be subject to
a branch profits tax at a rate of 30% or such lower rate as may
be specified by an applicable tax treaty.
A non-United States holder of common stock that is eligible for
a reduced rate of withholding tax pursuant to a tax treaty may
obtain a refund of any excess amounts currently withheld if an
appropriate claim for refund is filed with the Internal Revenue
Service, or IRS. If a non-United States holder holds common
stock through a foreign partnership or foreign intermediary, the
foreign partnership or foreign intermediary will also be
required to comply with additional certification requirements.
Gain on Disposition of Common Stock
A non-United States holder generally will not be subject to
United States federal income tax on any gain realized upon the
sale or other disposition of our common stock unless:
•
the gain is effectively connected with a United States trade or
business of the non-United States holder (and if required by an
applicable income tax treaty, is attributable to a United States
permanent establishment of the non-United States holder);
•
the non-United States holder is an individual who holds his or
her common stock as a capital asset (generally, an asset held
for investment purposes) and who is present in the United States
for a period or periods aggregating 183 days or more during
the calendar year in which the sale or disposition occurs and
certain other conditions are met; or
•
our common stock constitutes a United States real property
interest by reason of our status as a “United States real
property holding corporation” (“USRPHC”) for
United States federal income tax purposes at any time within the
shorter of the five-year period preceding the disposition or the
holder’s holding period for our common stock.
We believe that we are not currently, and that we will not
become, a USRPHC for United States federal income tax purposes.
If we are determined to be a USRPHC, the United States federal
income and withholding taxes relating to interests in USRPHCs
nevertheless will not apply to gains derived from the sale or
other disposition of the common stock by a non-United States
holder whose shareholdings, actual and constructive, at all
times during the applicable period, amount to 5% or less of our
common stock, provided that our common stock is regularly traded
on an established securities market. However, no assurance can
be given that we will not be a USRPHC, or that our common stock
will be considered regularly traded, when a non-United States
holder sells its shares of our common stock.
Unless an applicable treaty provides otherwise, gain described
in the first bullet point above will be subject to the United
States federal income tax imposed on net income on the same
basis that applies to United States persons, as defined under
the Code, generally and, for corporate holders under certain
circumstances, the branch profits tax, but will generally not be
subject to withholding, provided any certification requirements
are met. Gain described in the second bullet point above will be
subject to a flat 30% United States federal income tax and may
be offset by United States source capital losses. Non-United
States holders should consult any applicable income tax treaties
that may alter the applicable rules.
Generally, we must report annually to the IRS the amount of
dividends paid, the name and address of the recipient, and the
amount, if any, of tax withheld. A similar report is sent to the
holder. Pursuant to tax treaties or other agreements, the IRS
may make its reports available to tax authorities in the
recipient’s country of residence.
Payments of dividends or of proceeds on the disposition of stock
made to a non-United States holder may be subject to backup
withholding (currently at a rate of 28%) unless the non-United
States holder establishes an exemption, for example, by properly
certifying its non-United States status on a
Form W-8BEN or
another appropriate version of
Form W-8.
Notwithstanding the foregoing, backup withholding may apply if
either we or our paying agent has actual knowledge, or reason to
know, that the holder is a United States person as defined under
the Code.
Information reporting and, depending on the circumstances,
backup withholding will apply to the proceeds of a sale of our
common stock within the United States or conducted through
certain United States-related financial intermediaries, unless
the beneficial owner certifies under penalty of perjury that it
is a non-United States holder (and the payor does not have
actual knowledge or reason to know that the beneficial owner is
a United States person as defined under the Code), or such owner
otherwise establishes an exemption.
Backup withholding is not an additional tax. Rather, the United
States income tax liability of persons subject to backup
withholding will be reduced by the amount of tax withheld. If
withholding results in an overpayment of taxes, a refund may be
obtained, provided that the required information is timely
furnished to the IRS.
Prior to this offering, there has been no public market for our
common stock, and there can be no assurance that a significant
public market for the common stock will develop or be sustained
after this offering. Future sales of substantial amounts of our
common stock, including shares issued upon exercise of
outstanding options, in the public market following this
offering could adversely affect market prices prevailing from
time to time and could impair our ability to raise capital
through the sale of our equity securities.
Upon completion of this offering and based on shares outstanding
at December 31, 2005 and the conversion of all shares of
preferred stock into shares of common stock, we will have
outstanding shares
of common stock. All the shares sold in this offering, plus any
shares issued upon exercise of the underwriters’ option to
purchase additional shares from us, will be freely tradable
without restriction under the Securities Act, unless purchased
by our “affiliates” as that term is defined in
Rule 144 under the Securities Act.
The
remaining shares
of common stock outstanding are “restricted
securities” within the meaning of Rule 144 under the
Securities Act. Restricted securities may be sold in the public
market only if registered or if they qualify for an exemption
from registration under Rule 701 or another exemption or
meet the safe harbor qualifications under Rule 144 under
the Securities Act as summarized below.
Our directors, officers and substantially all of our
stockholders, who combined hold
approximately %
of our stock, have entered into
lock-up agreements with
the underwriters of this offering generally providing that they
will not offer, sell, contract or grant any option to sell,
pledge, transfer, establish an open put equivalent position or
liquidate or decrease a call equivalent position or otherwise
dispose of or transfer any shares of common stock, options or
warrants to acquire shares of common stock, or securities
exchangeable or exercisable for or convertible into shares of
common stock owned by them prior to this offering for a period
of 180 days after the date of this prospectus without the
prior written consent of Banc of America Securities LLC, on
behalf of our underwriters. The
lock-up agreements do
not prohibit transfers or dispositions by our officers,
directors and stockholders as a gift or by will or intestacy, to
immediate family members or affiliates, and to any trust for the
direct or indirect benefit of the holder or his or her
immediately family. As a result of these contractual
restrictions, notwithstanding possible earlier eligibility for
sale under the provisions of Rules 144, 144(k) and 701,
shares subject to
lock-up agreements may
not be sold until such agreements expire or are waived by Banc
of America Securities LLC, on behalf of our underwriters. Banc
of America Securities LLC has advised us that it has no current
intention to shorten or release any of the shares subject to the
lock-up agreements
prior to the expiration of the
lock-up period. Based
on shares outstanding as of December 31, 2005, taking into
account the lock-up
agreements, and assuming Banc of America Securities LLC does not
release stockholders from these agreements prior to the
expiration of the
180-day
lock-up period, the
following shares will be eligible for sale in the public market
at the following times:
•
shares
that are not subject to the
lock-up agreements
discussed above may be sold immediately after completion of this
offering;
•
additional
shares that are not subject to the
180-day
lock-up period
described above may be sold beginning 90 days after the
effective date of the offering; and
•
additional
shares may be sold upon expiration of the
180-day
lock-up period
described above.
In general, under Rule 144 as currently in effect, a person
who has beneficially owned restricted shares for at least one
year, including the holding period of any prior owner except an
affiliate, would be entitled to sell within any three-month
period a number of shares that does not exceed the greater of:
•
1% of the number of shares of common stock then outstanding,
which will equal
approximately shares
immediately after this offering; or
•
the average weekly trading volume of our common stock during the
four calendar weeks preceding the date on which notice of the
sale is filed.
Sales under Rule 144 are also subject to certain manner of
sale provisions and notice requirements and to the availability
of current public information about us. Under Rule 144(k),
a person who is not deemed to have been an affiliate of us at
any time during the three months preceding a sale, and who has
beneficially owned the shares proposed to be sold for at least
two years, including the holding period of any prior owner
except an affiliate, is entitled to sell such shares without
complying with the manner of sale, public information, volume
limitation or notice provisions of Rule 144.
Rule 701
Any of our employees, officers, directors or consultants who
purchased shares under a written compensatory plan or contract
may be entitled to rely on the resale provisions of
Rule 701. Rule 701 permits affiliates to sell their
Rule 701 shares under Rule 144 without complying
with the holding period requirements of Rule 144.
Rule 701 further provides that non-affiliates may sell such
shares in reliance on Rule 144 without having to comply
with the holding period, public information, volume limitation
or notice provisions of Rule 144. All holders of
Rule 701 shares are required to wait until
90 days after the effective date of this offering before
selling such shares.
Registration Rights
Upon completion of this offering, the holders
of shares
of our common stock, or their transferees, have rights to
require or participate in the registration of those shares under
the Securities Act pursuant to our amended and restated investor
rights agreement. For a detailed description of these
registration rights see “Description of Capital
Stock — Registration Rights.”
Stock Options
We intend to file a registration statement under the Securities
Act covering shares of common stock reserved for issuance under
our 2005 Equity Incentive Plan. That registration statement is
expected to become effective upon filing with the SEC.
Accordingly, common stock registered under that registration
statement will, subject to vesting provisions and limitations as
to the volume of shares that may be sold by our affiliates under
Rule 144 described above, be available for sale in the open
market unless the holder is subject to the
180-day
lock-up period.
As of December 31, 2005, options to purchase
5,576,671 shares of common stock were issued and
outstanding at a weighted average exercise price of $0.31 per
share. Upon the expiration of the
lock-up period
described above, at
least shares
of common stock will be subject to vested options.
Upon completion of this offering, there will be outstanding a
warrant to purchase shares of common stock issued in connection
with a credit facility we entered into in January 2006. The
number of shares subject to the warrant and the exercise price
will be established at the closing of this offering pursuant to
a formula agreed upon with the lender. Under this formula, at an
assumed initial public offering price of
$ per
share and assuming a closing date
of ,
2006, this warrant would be exercisable
for shares
of common stock at an exercise price of the $ per share.
The shares issuable upon exercise of the warrant are subject to
a lock-up agreement
with Banc of America Securities LLC. Such shares are also
entitled to the registration rights discussed above. In
addition, any shares purchased pursuant to the warrant may be
sold pursuant to the requirements of Rule 144.
We are offering the shares of common stock described in this
prospectus through a number of underwriters. Banc of America
Securities LLC, Cowen & Co., LLC, Lazard Capital
Markets LLC and Pacific Growth Equities, LLC are the
representatives of the underwriters. We have entered into a firm
commitment underwriting agreement with the representatives.
Subject to the terms and conditions of the underwriting
agreement, we have agreed to sell to the underwriters, and each
underwriter has agreed to purchase, the number of shares of
common stock listed next to its name in the following table:
Underwriter
Number of Shares
Banc of America Securities LLC
Cowen & Co., LLC
Lazard Capital Markets LLC
Pacific Growth Equities, LLC
Total
The underwriting agreement is subject to a number of terms and
conditions and provides that the underwriters must buy all of
the shares if they buy any of them. The underwriters will sell
the shares to the public when and if the underwriters buy the
shares from us.
The underwriters initially will offer the shares to the public
at the price specified on the cover page of this prospectus. The
underwriters may allow a concession of not more than
$ per
share to selected dealers. The underwriters may also allow, and
those dealers may reallow, a concession of not more than
$ per
share to some other dealers. If all the shares are not sold at
the public offering price, the underwriters may change the
public offering price and the other selling terms. Our common
stock is offered subject to a number of conditions, including:
•
receipt and acceptance of the common stock by the
underwriters; and
•
the underwriters’ right to reject orders in whole or in
part.
Over-Allotment Options. We have granted the underwriters
an over-allotment option to buy up to additional shares of our
common stock at the same price per share as they are paying for
the shares shown in the table above. These additional shares
would cover sales of shares by the underwriters that exceed the
total number of shares shown in the table above. The
underwriters may exercise this option at any time within
30 days after the date of this prospectus. To the extent
that the underwriters exercise this option, each underwriter
will purchase additional shares from us in approximately the
same proportion as it purchased the shares shown in the table
above. If purchased, the additional shares will be sold by the
underwriters on the same terms as those on which the other
shares are sold.
Discount and Commissions. The following table shows the
per share and total underwriting discounts and commissions to be
paid to the underwriters by us. These amounts are shown assuming
no exercise and full exercise of the underwriters’ option
to purchase additional shares.
We estimate that the expenses of the offering to be paid by us,
not including the underwriting discounts and commissions, will
be approximately
$ .
Paid by Us
No Exercise
Full Exercise
Per Share
$
$
Total
$
$
Listing. We have applied to have our common stock
included for quotation on the Nasdaq National Market under the
symbol “QTRX”.
Stabilization. In connection with this offering, the
underwriters may engage in activities that stabilize, maintain
or otherwise affect the price of our common stock, including:
•
stabilizing transactions;
•
short sales;
•
syndicate covering transactions;
•
imposition of penalty bids; and
•
purchases to cover positions created by short sales.
Stabilizing transactions consist of bids or purchases made for
the purpose of preventing or retarding a decline in the market
price of our common stock while this offering is in progress.
Stabilizing transactions may include making short sales of our
common stock, which involves the sale by the underwriters of a
greater number of shares of common stock than they are required
to purchase in this offering, and purchasing shares of common
stock from us or in the open market to cover positions created
by short sales. Short sales may be “covered” shorts,
which are short positions in an amount not greater than the
underwriters’ over-allotment option referred to above, or
may be “naked” shorts, which are short positions in
excess of that amount. Syndicate covering transactions involve
purchases of our common stock in the open market after the
distribution has been completed in order to cover syndicate
short positions.
The underwriters may close out any covered short position either
by exercising their over-allotment option, in whole or in part,
or by purchasing shares in the open market. In making this
determination, the underwriters will consider, among other
things, the price of shares available for purchase in the open
market compared to the price at which the underwriters may
purchase shares pursuant to the over-allotment option.
A naked short position is more likely to be created if the
underwriters are concerned that there may be downward pressure
on the price of the common stock in the open market that could
adversely affect investors who purchased in this offering. To
the extent that the underwriters create a naked short position,
they will purchase shares in the open market to cover the
position.
The representatives also may impose a penalty bid on
underwriters and dealers participating in the offering. This
means that the representatives may reclaim from any syndicate
members or other dealers participating in the offering the
underwriting discounts on shares sold by them and purchased by
the representatives in stabilizing or short covering
transactions.
These activities may have the effect of raising or maintaining
the market price of our common stock or preventing or retarding
a decline in the market price of our common stock. As a result
of these activities, the price of our common stock may be higher
than the price that otherwise might exist in the open market. If
the underwriters commence these activities, they may discontinue
them at any time. The underwriters may carry out these
transactions on the Nasdaq National Market, in the
over-the-counter market
or otherwise.
Discretionary Accounts. The underwriters have informed us
that they do not expect to make sales to accounts over which
they exercise discretionary authority in excess of 5% of the
shares of common stock being offered.
IPO Pricing. Prior to this offering, there has been no
public market for our common stock. The initial public offering
price will be negotiated between us and the representatives of
the underwriters. Among the factors to be considered in these
negotiations are:
•
the history of, and prospects for, our company and the industry
in which we compete;
the prevailing conditions of the applicable United States
securities market at the time of this offering;
•
market valuations of publicly traded companies that we and the
representatives of the underwriters believe to be comparable to
us; and
•
other factors deemed relevant.
Lock-up
Agreement. We, our executive officers and directors and
substantially all of our stockholders have entered into or will,
prior to the completion of this offering, enter into
lock-up agreements with
the underwriters. Under these agreements, subject to exceptions,
we may not issue any new shares of common stock, and those
holders of stock and options may not, directly or indirectly,
sell, offer, contract or grant any option to sell, pledge,
transfer or otherwise dispose of or hedge any common stock or
securities convertible into or exchangeable for shares of common
stock, or publicly announce the intention to do any of the
foregoing, without the prior written consent of Banc of America
Securities LLC for a period of 180 days from the date of
this prospectus, subject to a potential extension of up to an
additional 34 days under certain circumstances. This
consent may be given at any time without public notice. In
addition, during this period, we have also agreed not to file
any registration statement for any shares of our common stock
without the prior written consent of Banc of America Securities
LLC. Pursuant to the
lock-up agreements
holders of greater
than %
of the “registrable securities” under our registration
rights agreement have also agreed not to make any demand for, or
exercise any right to registration of any shares of common stock
or any securities convertible into or exercisable or
exchangeable for common stock, without the prior written consent
of Banc of America Securities LLC.
Indemnification. We will indemnify the underwriters
against some liabilities, including liabilities under the
Securities Act. If we are unable to provide this
indemnification, we will contribute to payments the underwriters
may be required to make in respect of those liabilities.
Conflicts/ Affiliates. The underwriters and their
affiliates have provided, or may in the future provide, various
investment banking, commercial banking and other financial
services for us.
Compliance with
Non-U.S. Laws and
Regulations
Each underwriter intends to comply with all applicable laws and
regulations in each jurisdiction in which it acquires, offers,
sells or delivers shares of our common stock or has in its
possession or distributes the prospectus.
European Economic Area
In relation to each Member State of the European Economic Area
which has implemented the Prospectus Directive (each, a Relevant
Member State), with effect from and including the date on which
the Prospectus Directive is implemented in that Relevant Member
State (the Relevant Implementation Date) an offer of shares to
the public may not be made in that Relevant Member State prior
to the publication of a prospectus in relation to shares which
has been approved by the competent authority in that Relevant
Member State or, where appropriate, approved in another Relevant
Member State and notified to the competent authority in that
Relevant Member State, all in accordance with the Prospectus
Directive, except that it may, with effect from and including
the Relevant Implementation Date, make an offer of shares to the
public in that Relevant Member State at any time:
•
to legal entities which are authorized or regulated to operate
in the financial markets or, if not so authorized or regulated,
whose corporate purpose is solely to invest in securities;
•
to any legal entity which has two or more of (1) an average
of at least 250 employees during the last financial year;
(2) a total balance sheet of more than
43,000,000 Euros and (3) an annual net turnover of
more than 50,000,000 Euros, as shown in its last annual or
consolidated accounts; or
•
in any other circumstances which do not require the publication
by the Issuer of a prospectus pursuant to Article 3 of the
Prospectus Directive.
For the purposes of this provision, the expression an
“offer of shares to the public” in relation to any
shares in any Relevant Member State means the communication in
any form and by any means of sufficient information on the terms
of the offer and the shares to be offered so as to enable an
investor to decide to purchase or subscribe the shares, as the
same may be varied in that Member State by any measure
implementing the Prospectus Directive in that Member State and
the expression Prospectus Directive means Directive 2003/71/ EC
and includes any relevant implementing measure in each Relevant
Member State.
France
No prospectus (including any amendment, supplement or
replacement thereto) has been prepared in connection with the
offering of the shares that has been approved by the
Autorité des marchés financiers or by the
competent authority of another State that is a contracting party
to the Agreement on the European Economic Area and notified to
the Autorité des marchés financiers; no shares
have been offered or sold and will be offered or sold, directly
or indirectly, to the public in France except to permitted
investors (“Permitted Investors”) consisting of
persons licensed to provide the investment service of portfolio
management for the account of third parties, qualified investors
(investisseurs qualifiés) acting for their own
account and/or corporate investors meeting one of the four
criteria provided in Article 1 of Decree N o
2004-1019 of
September 28, 2004 and belonging to a limited circle of
investors (cercle restreint d’investisseurs) acting
for their own account, with “qualified investors” and
“limited circle of investors” having the meaning
ascribed to them in Article L.
411-2 ,
D.411-1,
D.411-2,
D.734-1,
D.744-1,
D754-1 and
D.764-1 of the French
Code Monétaire et Financier and applicable
regulations thereunder; neither this prospectus, nor any other
materials related to the offering or information contained
therein relating to the shares has been released, issued or
distributed to the public in France except to Permitted
Investors; and the direct or indirect resale to the public in
France of any shares acquired by any Permitted Investors may be
made only as provided by
Articles L.411-1,
L.411-2,
L.412-1 and
L.621-8 to
L.621-8-3 of the French
Code Monétaire et Financier and applicable
regulations thereunder.
United Kingdom
Each underwriter acknowledges and agrees that:
•
it has not offered or sold and will not offer or sell any shares
other than to persons whose ordinary activities involve them in
acquiring, holding, managing or disposing of investments (as
principal or as agent) for the purposes of their businesses or
who it is reasonable to expect will acquire, hold, manage or
dispose of investments (as principal or agent) for the purposes
of their businesses where the issue of the shares would
otherwise constitute a contravention of Section 19 of the
Financial Services and Markets Act 2000 (the “FSMA”)
by the issuer;
•
it has only communicated or caused to be communicated and will
only communicate or cause to be communicated an invitation or
inducement to engage in investment activity (within the meaning
of Section 21 of the FSMA) received by it in connection
with the issue or sale of the shares in circumstances in which
Section 21(1) of the FSMA does not apply to the
Issuer; and
•
it has complied and will comply with all applicable provisions
of the FSMA with respect to anything done by it in relation to
the shares in, from or otherwise involving the United Kingdom.
This document is only being distributed to and is only directed
at (i) persons who are outside the United Kingdom or
(ii) to investment professionals falling within
Article 19(5) of the Financial Services and Markets Act
2000 (Financial Promotion) Order 2005 (the “Order”) or
(iii) high net worth entities, and other persons to whom it
may lawfully be communicated, falling within
Article 49(2)(a) to (d) of the Order (all such persons
together being referred to as “relevant persons”). The
shares are only available to, and any invitation, offer or
agreement to subscribe, purchase or otherwise acquire such
shares will be engaged in only with, relevant persons. Any
person who is not a relevant person should not act or rely on
this document or any of its contents.
Each underwriter acknowledges and agrees that the offering of
the shares has not been cleared by the Italian Securities
Exchange Commission (Commissione Nazionale per le Società e
la Borsa, the “CONSOB”) pursuant to Italian securities
legislation and, accordingly, acknowledges and agrees that the
shares may not and will not be offered, sold or delivered, nor
may or will copies of the prospectus or any other documents
relating to the shares or the prospectus be distributed in Italy
other than to professional investors (investitori
professionali), as defined in Article 31, paragraph 2
of CONSOB Regulation No. 11522 of July 1, 1998,
as amended (“Regulation No. 11522”) or
pursuant to another exemption from the requirements of
Articles 94 and seq. of Legislative Decree No. 58 of
February 24, 1998 (the “Italian Finance Law”) and
CONSOB Regulation No. 11971 of May 14, 1999
(“Regulation No. 11971”).
Each underwriter acknowledges and agrees that any offer, sale or
delivery of the shares or distribution of copies of the
prospectus or any other document relating to the shares or the
prospectus in Italy may and will be effected in accordance with
all Italian securities, tax, exchange control and other
applicable laws and regulations, and, in particular, will be:
•
made by an investment firm, bank or financial intermediary
permitted to conduct such activities in Italy in accordance with
the Legislative Decree No. 385 of September 1, 1993,
as amended (the “Italian Banking Law”), Legislative
Decree No. 58 of February 24, 1998, as amended, CONSOB
Regulation No. 11522 of July 1, 1998, and any
other applicable laws and regulations;
•
in compliance with Article 129 of the Italian Banking Law
and the implementing guidelines of the Bank of Italy; and
•
in compliance with any other applicable notification requirement
or limitation which may be imposed upon the offer of shares by
CONSOB or the Bank of Italy.
Any investor purchasing the shares in this offering is solely
responsible for ensuring that any offer or resale of the shares
it purchased in this offering occurs in compliance with
applicable laws and regulations.
This prospectus and the information contained herein are
intended only for the use of its recipient and are not to be
distributed to any third party resident or located in Italy for
any reason. No person resident or located in Italy other than
the original recipients of this document may rely on it or its
content.
In addition to the above (which shall continue to apply to the
extent not inconsistent with the implementing measures of the
Prospectus Directive in Italy), after the implementation of the
Prospectus Directive in Italy, the restrictions, acknowledgments
and agreements set out under the heading “European Economic
Area” above shall apply to Italy.
LEGAL MATTERS
The validity of the common stock offered hereby will be passed
upon for us by Heller Ehrman LLP and certain matters will be
passed upon for the underwriters by Shearman & Sterling
LLP.
EXPERTS
The financial statements as of December 31, 2004 and
December 31, 2005 and for each of the three years in the
period ended December 31, 2005 and cumulative for the
period of inception (November 20, 2000) through
December 31, 2005 included in this prospectus have been so
included in reliance on the report of PricewaterhouseCoopers
LLP, an independent registered public accounting firm, given on
the authority of said firm as experts in auditing and accounting.
The financial statements as of December 31, 2003 and
December 31, 2004 and for each of the two years then ended
for Hormos Medical Oy included in this prospectus have been so
included in reliance on the report of PricewaterhouseCoopers Oy,
independent accountants, given on authority of said firm as
experts in auditing and accounting.
We have filed with the SEC a registration statement on
Form S-1 under the
Securities Act that registers the shares of our common stock to
be sold in this offering. This prospectus does not contain all
of the information set forth in the registration statement and
the exhibits and schedules filed as part of the registration
statement. For further information with respect to us and our
common stock, we refer you to the registration statement and the
exhibits and schedules filed as a part of the registration
statement. Statements contained in this prospectus concerning
the contents of any contract or any other document are not
necessarily complete. If a contract or document has been filed
as an exhibit to the registration statement, we refer you to the
copy of the contract or document that has been filed. Each
statement in this prospectus relating to a contract or document
filed as an exhibit is qualified in all respects by the filed
exhibit. The reports and other information we file with the SEC
can be read and copied at the SEC’s Public Reference Room
at 100 F Street, NE, Washington D.C. 20549. Copies of these
materials can be obtained at prescribed rates from the Public
Reference Section of the SEC at the principal offices of the
SEC, 100 F Street, NE, Washington D.C. 20549. You may
obtain information regarding the operation of the Public
Reference Room by calling
1(800) SEC-0330.
The SEC also maintains a web site (http://www.sec.gov) that
contains reports, proxy and information statements and other
information regarding issuers that file electronically with the
SEC.
Upon completion of this offering, we will become subject to the
reporting and information requirements of the Exchange Act and,
as a result, will file periodic reports, proxy statements and
other information with the SEC. These periodic reports, proxy
statements and other information will be available for
inspection and copying at the SEC’s public reference room
and the web site of the SEC referred to above.
Report of Independent Registered Public Accounting Firm
To the Board of Directors and Stockholders of
QuatRx Pharmaceuticals Company
In our opinion, the accompanying consolidated balance sheets and
the related consolidated statements of operations,
stockholders’ equity and cash flows present fairly, in all
material respects, the financial position of QuatRx
Pharmaceuticals Company and its subsidiary at December 31,2005 and 2004 and the results of their operations and their cash
flows for each of the three years in the period ended
December 31, 2005 and, cumulatively, for the period from
November 20, 2000 (date of inception) to December 31,2005 in conformity with accounting principles generally accepted
in the United States of America. These financial statements are
the responsibility of the Company’s management. Our
responsibility is to express an opinion on these financial
statements based on our audits. We conducted our audits of these
statements in accordance with the standards of the Public
Company Accounting Oversight Board (United States). 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, assessing the accounting principles
used and significant estimates made by management, and
evaluating the overall financial statement presentation. We
believe that our audits provide a reasonable basis for our
opinion.
Redeemable convertible preferred stock, liquidation value of
$56,697,445 and $86,681,742 at December 31, 2004 and 2005,
respectively, no shares outstanding pro forma (unaudited)
55,907,373
86,200,020
$
—
Stockholders’ Equity (Deficit):
Common stock, $0.01 par value; 72,502,056 and
94,919,416 shares authorized at December 31, 2004 and
2005 respectively; 3,976,000 and 14,490,473 shares issued
and outstanding at December 31, 2004 and 2005 respectively;
75,720,724 shares outstanding pro forma (unaudited)
39,760
144,905
757,207
Additional paid-in capital
—
—
85,587,718
Deferred compensation
—
(284,594
)
(284,594
)
Deficit accumulated during the development stage
(26,055,834
)
(67,522,185
)
(67,522,185
)
Accumulated other comprehensive income
—
872,315
872,315
Total stockholders’ equity (deficit)
(26,016,074
)
(66,789,559
)
$
19,410,461
Total liabilities, redeemable convertible preferred stock and
stockholders’ equity (deficit)
$
31,494,623
$
38,361,409
The accompanying notes are an integral part of these
consolidated financial statements.
Organization and Summary of Significant Accounting
Policies
Organization and Business
QuatRx Pharmaceuticals Company (“QuatRx” or the
“Company”) was incorporated in Delaware in November
2000, and is engaged in the discovery, licensing, development
and commercialization of compounds in the endocrine, metabolic
and cardiovascular therapeutic areas. QuatRx has four product
candidates in clinical development and one product candidate
expected to enter clinical development in the first half of
2006. QuatRx’s two lead product candidates treat hormone
deficiencies that result from aging in men and women.
Ospemifene, a treatment for vaginal atrophy in post-menopausal
women, is in phase III clinical testing, and fispemifene, a
treatment for the symptoms of andropause in aging males, has
recently entered phase II clinical testing in the first
half of 2006. QuatRx also has two product candidates for the
treatment of elevated cholesterol levels,
QRX-401 and
QRX-431, in
phase I clinical trials and preclinical development,
respectively. Becocalcidiol, our topical product candidate for
the treatment of mild to moderate psoriasis, has completed a
phase IIb clinical trial. In addition, QuatRx has two
research programs for targeted endocrine therapies.
On May 25, 2005, QuatRx completed the acquisition of Hormos
Medical Oy (“Hormos”), a privately held Finnish
development-stage pharmaceuticals company. Hormos focuses on the
discovery and development of novel pharmaceutical compounds
involving the tissue specific regulation of estrogen effects for
the treatment of certain age-related diseases. The acquisition
allowed QuatRx to expand its existing pipeline and technologies
to include potential therapies for endocrine deficiencies
associated with aging in men and women, including ospemifene and
fispemifene. The accompanying financial statements include the
operating results of Hormos since the date of acquisition.
QuatRx complements its internal drug development expertise by
entering into collaborations and agreements with third parties
including pharmaceutical companies, academic laboratories, and
contract service providers. In the course of its activities,
QuatRx has sustained significant operating losses and expects
such losses, which will likely increase as QuatRx expands its
research and development activities, to continue for at least
the next several years. QuatRx has not generated any product
sales or any significant revenues and has not achieved
profitable operations or positive cash flows from operations.
QuatRx’s cumulative net loss during the development stage
totaled $61,972,941 through December 31, 2005. QuatRx plans
to finance its operations with a combination of stock issuances,
Finnish government sponsored loans and grants, borrowings under
long-term debt arrangements, payments from license and other
strategic research and development arrangements and, if its
product candidates are commercialized, with revenues from
product sales. There are no assurances that QuatRx will be
successful in obtaining an adequate level of financing needed
for the long-term development and commercialization of its
planned products.
Basis of Presentation
QuatRx has generated no revenue to date and its activities have
consisted primarily of raising capital, acquiring compounds,
planning and conducting clinical trials, recruiting personnel,
and negotiating licensing arrangements. Accordingly, QuatRx is
considered to be in the development stage as of
December 31, 2005 as defined in Statement of Financial
Accounting Standards (“SFAS”) No. 7,
Accounting and Reporting by Development Stage Enterprises.
Principles of Consolidation
The consolidated financial statements include the accounts of
the Company and its wholly owned subsidiary, Hormos, from the
date of acquisition, May 25, 2005. All significant
intercompany balances and transactions have been eliminated.
Notes to Consolidated Financial
Statements — (Continued)
Unaudited Pro Forma Presentation
The unaudited pro forma stockholders’ equity as of
December 31, 2005 and net loss per share available to
common stockholders for the year ended December 31, 2005
reflect the automatic conversion of all outstanding shares of
Series A, Series B, Series C, Series D and
Series D-1 Redeemable Convertible Preferred Stock into
43,143,653 and 61,230,251 shares of common stock,
respectively, upon the closing of the Company’s initial
public offering.
Foreign Currency Translation
The financial statements of QuatRx’s foreign subsidiary are
translated from Euros to U.S. dollars using exchange rates
in effect at period end for assets and liabilities and at
average rates during the period for results of operations. The
resulting foreign currency translation adjustment is reflected
as a separate component of stockholders’ equity (deficit).
Foreign currency transaction loss resulting from intercompany
debt denominated in foreign currencies totaled approximately
$93,850 for the year ended December 31, 2005, and is
included in general and administrative expense in the
accompanying consolidated statements of operations.
Use of Estimates
The preparation of financial statements in conformity with
accounting principles generally accepted in the United States of
America requires management to make estimates and assumptions
that affect the amounts reported in the financial statements and
accompanying notes. Actual results could differ from those
estimates.
Cash and Cash Equivalents
QuatRx considers all highly liquid investments with an original
maturity of three months or less at the date of purchase to be
cash equivalents.
Short-term Investments
Investments with an original maturity of more than three months
and less than one year are considered short-term investments and
have been classified by QuatRx as securities available-for-sale.
Such investments are carried at fair value, with unrealized
gains and losses included as a separate component of
stockholders’ equity.
Fair Value Financial Instruments
The carrying amount of cash and cash equivalents, short-term
investments, accounts receivable, accounts payable, accrued
liabilities are considered to be representative of their
respective fair values because of the short-term nature of those
instruments and obligations. Because the Company’s loans
bear interest generally at below-market rates, an adjustment
related to the carrying value of the loans has been recorded to
approximate fair value (see note 2). No significant change
in value has occurred since May 2005, the revaluation date.
Concentration of Credit Risk
Financial instruments that potentially subject QuatRx to a
significant concentration of credit risk consist primarily of
cash and cash equivalents and short-term investments. QuatRx
maintains deposits in federally insured financial institutions
in excess of federally insured limits. Management, however,
believes the Company is not exposed to significant credit risk
due to the financial position of the depository institutions in
which those deposits are held. The Company’s credit risk
from short-term investments is managed through
Notes to Consolidated Financial
Statements — (Continued)
the purchase of investment-grade securities and diversification
of the investment portfolio among issuers, industries, and
maturities.
Property and Equipment
Property and equipment are stated at cost and are depreciated
over the estimated useful lives of the assets (ranging from
three to five years) using the straight-line method. Equipment
under capital leases is amortized over their estimated useful
lives or the remaining lease term, whichever is shorter. Repairs
and maintenance are expensed as incurred.
Impairment of Long-Lived Assets
In accordance with SFAS No. 144, Accounting for the
Impairment or Disposal of Long-Lived Assets, if indicators
of impairment exist, QuatRx assesses the recoverability of the
affected long-lived assets by determining whether the carrying
value of such assets can be recovered through undiscounted
future operating cash flows. If impairment is indicated, QuatRx
measures the amount of such impairment by comparing the fair
value to the carrying value and reduces the carrying value
accordingly.
Contract research income consists of quarterly payments to
Hormos for research performed and reimbursement of outsourced
costs incurred by Hormos on the contracted research project. The
agreement expired January 2006.
Deferred Income
Certain non-core technology has been out-licensed to others. The
upfront payment of approximately $480,000 is being amortized
into income over the period of the agreement.
Consulting Income
Consulting fee income consists of fees paid by a pharmaceutical
company to QuatRx for consultation on design, implementation,
and assessment of certain clinical trials. There has been no
consulting fee income since 2003.
Forgiveness of Debt
Loans from Finnish governmental agencies to Hormos for specified
research and development projects may be forgiven at the
discretion of the Finnish governmental agencies if the project
fails to reach technological or commercial success. Forgiveness
of debt is recorded upon notification from the Finnish
governmental agencies that repayment is not required. Debt
forgiveness is recorded as other income in the consolidated
financial statements.
Research and Development
Research and development expenses consist primarily of costs
associated with the clinical trials of QuatRx’s product
candidates, up-front license fees and milestone obligations for
access to technology, compensation and other expenses for
research and development personnel, and supplies and development
materials, costs for clinical research organizations and
contract manufacturers. Expenditures relating to research and
development, including up-front license fees and milestone
obligations, are expensed as incurred.
Notes to Consolidated Financial
Statements — (Continued)
Clinical Trials
QuatRx accrues and expenses costs for clinical trial activities
performed by third parties based upon estimates of the
percentage of work completed over the life of the individual
study in accordance with agreements established with contract
research organizations and clinical trial sites. QuatRx
determines the estimates through discussion with internal
clinical personnel and outside service providers as to progress
or stage of completion of trials or services and the agreed upon
fee to be paid for such services. Costs of setting up clinical
trial sites for participation in the trials are expensed
immediately as research and development expenses. Clinical trial
site costs related to patient enrollment are accrued as patients
are entered into the trial and reduced by any initial payment
made to the clinical trial site when the first patient is
enrolled.
Comprehensive Income (Loss)
In accordance with SFAS No. 130, Reporting
Comprehensive Income, all components of comprehensive
income (loss), including, net income (loss), are
reported in the financial statements in the period in which they
are recognized. Comprehensive income (loss) is defined as
the change in equity during the period from transactions and
other events and circumstances from non-owner sources. Net
income (loss) and other comprehensive income (loss)
are reported net of their related tax effect to arrive at
comprehensive income (loss). For the period from inception
(November 20, 2000) to December 31, 2005, the
comprehensive loss is equal to the net loss, unrealized loss on
investments and cumulative translation adjustment as presented
in the statement of stockholders’ equity.
Stock-Based Compensation
QuatRx has elected to follow Accounting Principles Board
Opinion (“APB”) No. 25, Accounting for
Stock Issued to Employees, and related interpretations in
accounting for its employee stock options. Under APB 25, if
the exercise price of the Company’s employee stock options
equals or exceeds the estimated fair value of the underlying
stock on the date of grant, no compensation expense is
recognized. Since November 2004, the Company has used
independent contemporaneous valuations to determine the fair
value of the Company’s common stock.
The fair value of common stock for stock options granted through
December 31, 2005 was determined by the Company’s
board of directors in consultation with management. During the
year ended December 31, 2005, the Company granted common
stock options to employees and directors with exercise prices
ranging from $0.20 to $0.35 per share primarily using periodic
independent contemporaneous valuations of the Company’s
common stock.
Based on market estimates for the Company’s proposed
initial public offering, the Company has subsequently determined
that certain stock options were granted with exercise prices
below the estimated fair market value of the common stock at the
date of grant. Options for 182,500 shares granted in
October 2005 were determined to have a fair value of $2.04 per
share resulting in an intrinsic value of $1.69 per share at
the date of grant. Significant factors contributing to the
difference between the fair value as of the date of grant and
the exercise price for the October 2005 grants include:
increased company enterprise value late in 2005 with a
successful end of phase II FDA meeting for ospemifene,
receipt of the second tranche of Series D preferred stock
financing in late 2005, advance of other clinical programs, and
the increased likelihood of an initial public offering. The
Company recorded non-cash deferred compensation of $308,744
during the year ended December 31, 2005 in accordance with
APB 25 for these options, which is being amortized on a
straight-line basis over the related vesting period of the
options. The Company recorded non-cash employee stock
compensation expense associated with the amortization of
deferred stock compensation of $24,150 for the year ended
December 31, 2005.
As required under SFAS No. 123 (amended by
SFAS No. 148), the pro forma effects of stock-based
compensation on net loss are estimated at the date of grant
based on the fair value method using the Black-Scholes
option-pricing model.
The fair value of these options was estimated at the date of
grant using the Black-Scholes option valuation model with the
following weighted average assumptions for the years ended
December 31, 2003, 2004 and 2005; risk-free interest rate
of 2.97%, 3.43% and 4.00%, respectively; no dividend yield,
expected volatility of 70%, and weighted-average expected lives
of the options of 4 years. The estimated fair value of
stock options granted during 2003, 2004 and 2005 was $0.11,
$0.11 and $0.25, respectively. Risk-free interest rates were
determined using government securities with original maturities
similar to the respective expected option life at the date of
grant.
Had employee and director compensation cost for QuatRx’s
stock-based compensation plans been determined based on the fair
value at the grant dates for awards using the fair value method
prescribed by SFAS No. 123, QuatRx’s pro forma
net loss would be as follows:
Net loss available to common stockholders as reported
$
(10,468,330
)
$
(11,623,560
)
$
(52,930,573
)
Add stock-based employee compensation expense included in
reported net loss available to common stockholders
—
—
24,150
Deduct total stock-based employee compensation expense
determined under the fair value method for all awards
(47,038
)
(76,596
)
(205,361
)
Pro forma net loss available to common stockholders
$
(10,515,368
)
$
(11,700,156
)
$
(53,111,784
)
Net loss per share available to common stockholders (basic and
diluted)
As reported
$
(7.57
)
$
(4.79
)
$
(5.77
)
Pro forma
$
(7.60
)
$
(4.82
)
$
(5.79
)
Beneficial Conversion Feature
The issuance of Series D manditorily redeemable preferred stock
in October 2005 resulted in a beneficial conversion
amounting to $8,205,714 in accordance with EITF No. 98-5,
Accounting for Convertible Securities with Beneficial
Conversion Features or Contingently Adjustable Conversion
Ratios and EITF No. 00-27, Application of Issue No. 98-5
to Certain Convertible Instruments. The beneficial
conversion is
Notes to Consolidated Financial
Statements — (Continued)
calculated based on the estimated fair value per share of the
Company’s common stock at the date of issuance of the
Series D Preferred Stock in October 2005. The estimated fair
value of the common stock was approximately $2.04 per share
based on estimates of the projected initial public offering
price of the Company’s common stock which is planned in
mid-2006. The beneficial conversion charge related to the
October 2005 issuance of Series D mandatorily redeemable
preferred stock, which may be converted at any time at the
option of the holders to common stock, has been recorded as an
immediate charge to additional paid-in capital.
Income Taxes
QuatRx utilizes the liability method of accounting for income
taxes as required by SFAS No. 109, Accounting for
Income Taxes. Under this method, deferred tax assets and
liabilities are determined based on differences between
financial reporting and tax reporting bases of assets and
liabilities and are measured using enacted tax rates and laws
that are expected to be in effect when the differences are
expected to reverse. Valuation allowances are established when
necessary to reduce deferred tax assets to the amounts expected
to be realized.
Net Loss Per Share
Basic and diluted net loss per share amounts have been presented
in conformity with SFAS No. 128, Earnings Per
Share, for all periods presented. The Company has excluded
all common stock subject to repurchase by the Company,
convertible preferred stock and outstanding stock options from
the calculation of diluted net loss per share because all of
these securities are anti-dilutive due to the net loss for each
period. The total number of shares excluded from the
calculations of diluted net loss per share was 15,910,830,
24,966,797, and 49,739,110 in 2003, 2004 and 2005, respectively.
Accretion of redeemable convertible preferred stock
(1,503,791
)
(2,319,484
)
(13,210,271
)
Net loss available to common stockholders
$
(10,468,330
)
$
(11,623,560
)
$
(52,930,573
)
Basic and diluted —
Weighted average common shares outstanding
3,976,000
3,976,000
9,885,369
Weighted average unvested common shares subject to repurchase
(2,593,277
)
(1,550,408
)
(705,646
)
Net weighted average common shares outstanding
1,382,723
2,425,592
9,179,723
Net loss per share available to common stockholders
$
(7.57
)
$
(4.79
)
$
(5.77
)
Pro forma for Conversion (unaudited):
Pro forma net loss
$
(52,930,573
)
Basic and diluted —
Net weighted average common shares used above
9,179,723
Pro forma adjustment to reflect assumed weighted average effect
of conversion of preferred stock
49,033,464
Pro forma shares used to compute basic and diluted net loss per
share
58,213,187
Pro forma basic and diluted net loss per share
$
(0.91
)
Pro Forma
The shares used to compute basic and diluted net loss per share
represent the weighted average common shares outstanding,
reduced by the weighted average unvested common shares subject
to repurchase, and including the assumed conversion of all
outstanding shares of preferred stock into shares of common
stock using the as-if
converted method as of January 1, 2005 or the date of
issuance, if later.
Recent Accounting Pronouncements
In December 2004, the Financial Accounting Standards Board
issued SFAS No. 123(R) “Share-Based
Payment,”which amends SFAS No. 123. The
standard set forth in SFAS No. 123(R) requires that
all share-based payments to employees, including grants of
employee stock options, be recognized in the consolidated
statements of operations based on their fair values. The pro
forma disclosure previously permitted under
SFAS No. 123 will not be an acceptable alternative to
recognition of expenses in the financial statements. The
standard is effective for public companies for annual periods
beginning after June 15, 2005. The Company expects adoption
of SFAS No. 123(R) may have a material impact on its
results of operations and net loss per share. The Company is
currently in the process of evaluating the extent of such impact.
2.
Hormos Medical Oy Acquisition
On May 25, 2005, the Company completed the acquisition of
Hormos, a Finnish development-stage pharmaceuticals company.
Hormos is in the development stage and is presumed not to be a
business according to the Emerging Issues Task Force
(“EITF”) 98-3,
Determining Whether a Nonmonetary Transaction Involves
Receipt of Productive Assets or of a Business. The
transaction therefore was accounted
Notes to Consolidated Financial
Statements — (Continued)
for as a purchase of assets and assumption of liabilities. In
connection with the acquisition, the Company acquired all of the
outstanding capital stock of Hormos in exchange for
857,145 shares of Series D and 3,408,025 shares
of Series D-1
Preferred Stock and 9,520,154 shares of common stock and
assumed current liabilities and notes payable totaling
$20,289,423. The Company also incurred $1,000,000 in
acquisition-related costs.
Adjustments were made to record the acquired net assets of
Hormos at fair value, including allocating a portion of the
total purchase price to in-process research and development.
Based on management’s review of the analysis of the
tangible and intangible assets and liabilities of Hormos, the
purchase price has been allocated as follows:
Total acquisition costs:
Issuance of Series D Preferred Stock
$
1,200,003
Issuance of Series D-1 Preferred Stock
4,771,235
Issuance of common stock
2,856,047
Acquisition-related costs
1,000,000
Assumed liabilities and notes payable
20,289,423
$
30,116,708
Allocated to assets and liabilities as follows:
Current assets
$
1,170,596
Property and equipment acquired
776,995
In-process research and development
25,800,000
Work force
480,000
Favorable loan discount
2,101,923
Note receivable
1,380,219
Accrued contingent consideration
(1,593,025
)
$
30,116,708
Contingent consideration associated with the acquisition
includes an additional 321,415 shares and
1,277,995 shares of Series D and Series D-1
Preferred Stock, respectively, and 3,570,046 shares of
common stock held in escrow and payable upon the occurrence of
certain future events. One-third of the contingent shares secure
indemnification obligations of the Hormos selling shareholders
and will be released to the Company in satisfaction of an
indemnification claim or to the Hormos shareholders one year
after the closing date of the acquisition. The remaining
contingent shares will generally be released to Hormos selling
shareholders upon the first to occur of: the closing of a
qualified public offering of QuatRx’s common stock or the
dosing of the first patient in a second phase III clinical
trial of ospemifene. Additional purchase consideration will be
recorded as the contingent consideration is released. The
additional purchase consideration will be allocated to the
assets acquired based upon their relative fair value and will
result in additional expense for in-process research and
development, and the accrued contingent consideration totaling
$1,593,000 will be reclassified to stockholders’ equity.
The principal technology acquired in the acquisition of Hormos
consisted of two clinical-stage compounds which were under
development for the treatment of endocrine diseases of aging. In
accordance with FASB Interpretation No. 4, Applicability
of FASB Statement No. 2 to Business Combinations Accounted
for by the Purchase Method, purchased in-process research
and development of $25,800,000 related to these two
clinical-stage compounds was expensed since ultimate
commercialization of the compounds is uncertain and the
technology has no alternative uses. The fair value of each of
the in-process research and development projects was determined
based on an income approach which attempts to estimate the
income-producing capability of the asset.
Notes to Consolidated Financial
Statements — (Continued)
At the date of the acquisition, Hormos had $15,078,514 in loans,
including principal and accrued interest, from agencies of the
Finnish government. These loans include below-market interest
rates ranging from 1% to 5.25% annually. The loans were revalued
using both the favorable contractual interest rates as well as
the fair market yields. The difference in value under both
interest rate assumptions is $2,101,923 related to these loans
and has been recorded as a discount to long-term debt. This
discount is being amortized, using the effective interest
method, over the remaining lives of the underlying loans,
generally one to six years. Amortization expense of $265,974 is
included in interest expense in the accompanying statement of
operations for the year ended December 31, 2005.
In connection with the acquisition, Hormos’s workforce of
37 people joined the Company. Using estimated costs primarily of
recruitment and training, it was determined the fair value of
the assembled workforce represents an intangible asset of
$480,000. This asset is being amortized over approximately
4 years based on historical employee turnover rates.
Amortization expense of $50,827 and $22,218 is included in
research and development expense and general and administrative
expense, respectively, in the accompanying statement of
operations for the year ended December 31, 2005.
Management was primarily responsible for the estimates and
assumptions used in determining each of the above factors and
believes that the analysis was performed based on the most
relevant available data.
The following pro forma unaudited financial data illustrates the
estimated effects of the Hormos acquisition as if it had
occurred on January 1, 2005. For the year ended
December 31, 2005, pro forma net loss available to common
stockholders and basic and diluted net loss per share would have
been $29,028,553 and $2.24, respectively.
3.
Short-term Investments
Short-term investments consists of corporate debt securities and
are classified as available-for-sale securities. The
Company’s investments in these securities are recorded at
cost, which approximates fair market value due to their accrued
interest and contractual lives of less than one year. As a
result, the Company has no gross unrealized holding gains
(losses) or gross realized gains (losses) from these current
investments. The Company’s securities available-for-sale
consisted of the following:
Office equipment and furniture (depreciable life –
5 years)
38,051
281,797
116,410
1,073,192
Less: Accumulated depreciation
56,501
362,634
Total property and equipment
$
59,909
$
710,558
Equipment under capital leases totaled approximately $300,327
and the related accumulated depreciation totaled approximately
$79,731 at December 31, 2005.
Total depreciation expense for property and equipment totaled
$16,894, $19,663, $323,323 and $379,824 for the years ended
December 31, 2003, 2004 and 2005, and the period from
inception (November 20, 2000) to December 31, 2005,
respectively.
Subordinated notes payable, due in varying amounts with stated
interest rate of 3% and effective interest rate ranging from
4.6% to 7.1%, net of unamortized discount of $1,767,761 at
December 31, 2005
$
—
$
10,896,963
Note payable, with stated interest rate of 1% and effective
interest rate of approximately 5%, net of unamortized discount
of $68,187 at December 31, 2005
—
775,139
Capital lease obligation by Hormos, payable in monthly
installments of approximately $5,400, plus interest at 9.5%,
through February 2006
Hormos finances a portion of its research and development
activities with loans from Finnish governmental agencies. These
loans are granted on a project-by-project basis and generally
carry interest at below-market rates. If a project fails or does
not reach commercial success, under certain circumstances and at
the discretion of the Finnish governmental agencies, the loan
can be forgiven. In December 2005, Tekes notified Hormos that
repayment would not be required for certain loans totaling
$2,558,214, including principal and accrued interest, associated
with a research project which did not reach commercial
feasibility. Also in December 2005, Sitra notified Hormos that a
loan totaling $123,353, including principal and accrued
interest, would not be required to be repaid. The forgiveness of
debt has been recorded in other income (expense) in the
Consolidated Statements of Operations.
Subordinated Notes Payable
Subordinated notes payable consists of 17 notes with Tekes, the
National Technology Agency in Finland. As of December 31,2005, Hormos had subordinated notes payable of $10,896,963,
including accrued interest of $1,262,687.
The terms of these unsecured subordinated loans generally
include interest at 1% below the Finnish base interest rate as
set by the Bank of Finland, but at a minimum of 3%, a loan
period of six to eight years, with no payments of principal or
interest due for the first three to five years. Repayment of
principal and accrued interest begins after the repayment-free
period. Under applicable Finnish law, interest or principal
related to subordinated notes can only be repaid when the
company has distributable retained earnings or adequate equity
capital. Because Hormos lacks the requisite retained earnings or
equity capital, no amounts outstanding under these loans are
considered currently payable.
Note Payable
Note payable consists of an industrial research and development
note with Tekes. The terms of the unsecured note payable
includes interest at 3% below the Finnish base interest rate as
set by the Bank of Finland, but a minimum of 1%, a loan period
of 10 years, with no payment of principle due for the first
five years. Repayment of principal and accrued interest begins
after the repayment-free period. Accrued interest is payable
annually.
Notes to Consolidated Financial
Statements — (Continued)
7.
Commitments and Contingencies
Leases
The Company leases its office facilities under various
noncancelable operating lease agreements. Rent expense was
$44,205, $44,457, $473,562 and $616,714 for the years ended
December 31, 2003, 2004 and 2005, and the period from
inception (November 20, 2000) to December 31, 2005,
respectively.
In connection with the acquisition of Hormos in May 2005, the
Company assumed additional operating leases for facilities in
Finland. Hormos is party to five separate real estate leases of
office and laboratory space in Turku, Finland and Oulu, Finland.
Two of these leases are long-term leases through 2011 which
require monthly payments totaling approximately $750,000
annually. The remaining facility leases require 15 months
or less to terminate and have monthly payments totaling
approximately $28,000 annually.
In 2004, the Company put in place a letter of credit from a
financial institution for $120,000 in favor of the
Company’s landlord in the event of a breach of the
Company’s Ann Arbor, Michigan facility lease, which expires
in 2011. The letter of credit is collateralized by $120,000 of
QuatRx’s deposits with the issuing financial institution.
Future minimum lease payments under these noncancelable capital
and operating leases at December 31, 2005 are approximately
as follows:
In July 2001, QuatRx entered into a license agreement with
Temple University for certain pharmaceutical delivery methods.
In consideration for this license, QuatRx paid an upfront
license fee of $10,000. QuatRx is obligated to pay certain
amounts for patent maintenance costs, a payment of $20,000 for a
patent improvement milestone and royalties on future net sales
of products incorporating technology covered by this license. As
of December 31, 2005 patent maintenance costs totaled
$1,825. No patent improvement milestones or sales royalties have
been incurred under this license through December 31, 2005.
The license agreement terminates upon expiration of the last of
any patent rights to licensed products that are developed under
the agreement. This agreement was terminated by QuatRx in
November 2005.
Notes to Consolidated Financial
Statements — (Continued)
Deltanoid Pharmaceuticals
In November 2001, QuatRx entered into a license agreement with
Deltanoid Pharmaceuticals, Inc. for certain pharmaceutical
compounds for the topical treatment of skin disease. QuatRx is
obligated to make certain future payments of up to $3,500,000
based on reaching certain clinical and regulatory milestones. No
milestone or royalty expense has been incurred under this
license through December 31, 2005. The royalty provision
under this license agreement terminates upon expiration of the
last to expire licensed patent under this agreement. QuatRx may
terminate this agreement at any time upon 90 days’
written notice.
Topical Pharmaceutical Compounds
In November 2001, QuatRx entered into a license with a research
organization for certain pharmaceutical compounds for topical
application. QuatRx paid upfront license fees of $50,000 in
connection with this license and is obligated to future
milestone payments of up to $2,750,000 based on achieving
certain clinical and regulatory milestones. QuatRx also is
obligated to royalty payments on net sales of products
incorporating the licensed compound. In addition, QuatRx has
agreed to pay from $5,000 to $20,000 per patent for costs
associated with domestic and foreign patents filed by the
research organization relating to the licensed compound.
Research and development costs incurred under this agreement in
2004 were $10,000. No costs were incurred for the year ended
December 31, 2005. Total amounts paid under this agreement
through December 31, 2005 are $50,000 in upfront license
fees and $25,000 in patent filing costs. The license agreement
terminates upon the earlier of the date that no licensed patent
under the agreement remains enforceable or the payment of earned
royalties, once begun, ceases for more than eight calendar
quarters. QuatRx has sent notification of its intent to
terminate this agreement.
In May 2003, QuatRx entered into a license agreement with
Genzyme Corporation (formerly Ilex Products, Inc.) for exclusive
rights to two novel classes of orally active compounds for the
treatment of lipid disorders and other cardiovascular diseases.
QuatRx paid a $2,500,000 upfront license fee under the agreement
which is included in research and development expense and is
obligated to future milestone and royalty payments. In 2004,
QuatRx paid $1,500,000, in milestone payments under this
agreement, which is included in research and development
expense. Future milestone payments are based on achievement of
certain clinical and regulatory milestones and total up to
$37,500,000. Royalty payments are based on net sales of products
incorporating the licensed compounds. No royalty payments have
been incurred under the agreement. The agreement provides that
patent maintenance costs are shared equally between the licensor
and QuatRx during the first two years and 100% by QuatRx
thereafter. Patent maintenance costs paid by QuatRx under this
agreement totaled $59,792, $101,045, none and $160,837 for the
years ended December 31, 2003, 2004 and 2005, and the
period from inception (November 30, 2000) to
December 31, 2005, respectively. The royalty provision
under the license terminates when all valid claims under any
patent included in the license have expired or are no longer
enforceable. QuatRx may terminate the agreement at any time with
90 days’ written notice.
EndoChem, Inc.
In February 2005, QuatRx entered into a license agreement with
EndoChem, Inc. for exclusive worldwide rights to certain
compounds for all human therapeutic applications including the
treatment of lipid disorders and obesity. QuatRx paid a $450,000
upfront license fee under the agreement in 2005, which is
included in research and development expense, and is obligated
to future license fee, milestone and royalty payments. A future
license fee of $100,000 is due within seven days of the one year
anniversary date of the agreement. Future development and
regulatory milestone payments total up to $3,500,000. Royalty
payments
Notes to Consolidated Financial
Statements — (Continued)
are based on net sales of products incorporating the licensed
compounds. No royalty payments have been incurred under the
agreement. Under terms of the agreement, maintenance costs of
the licensed patents are the responsibility of QuatRx. Patent
maintenance costs paid by QuatRx under this agreement totaled
$196,812 for the year ended December 31, 2005. The royalty
provision under the license terminates when all valid claims
under any patent included in the license have expired or are no
longer enforceable. QuatRx may terminate the agreement at any
time with 90 days’ written notice.
Orion and Tess Diagnostics and Pharmaceuticals for
Ospemifene
In December 2002, Hormos entered into two agreements with
pharmaceutical products companies for pharmaceutical compounds
involved in the treatment of certain endocrine deficiencies of
aging in women. Under an agreement with Orion, Hormos paid an
upfront license fee of approximately $482,000 and is obligated
to pay future milestones and royalties. Future milestones are
based on achievement of certain clinical and regulatory
milestones and total up to approximately $2,053,000. Royalty
payments are based on net sales of products incorporating the
licensed compounds. No royalty payments have been incurred under
the agreement. Under terms of the agreement, maintenance costs
of the licensed patents are the responsibility of Orion. The
license terminates at the later of 19 years from date of
agreement or when all valid claims under any patent included in
the license have expired or are no longer enforceable.
Under an agreement with Tess Diagnostics and Pharmaceuticals,
Hormos paid a $700,000 upfront license fee and is obligated to
future milestone and royalty payments. Future milestone payments
are based on achievement of certain clinical and regulatory
milestones and total up to $8,500,000. Royalty payments are
based on net sales of products incorporating the licensed
compounds. No royalty payments have been incurred under the
agreement. QuatRx has the right, in its sole discretion, to
terminate this agreement upon written notice.
Orion for Fispemifene
In March 2004, Hormos entered into a license agreement with
Orion for triphenylalkene derivatives and their use as selective
estrogen receptor modulators. Under the agreement, Hormos paid
an upfront license fee of approximately $60,000 and is obligated
to future milestone and royalty payments. Future milestone
payments are based on achievement of certain clinical and
regulatory milestones and total up to approximately $1,066,000.
Royalty payments are based on net sales of products
incorporating the licensed compounds. No royalty payments have
been incurred under the agreement. Under terms of the agreement,
maintenance costs of the licensed patents are the responsibility
of Hormos. No patent maintenance costs have been incurred under
the agreement. The license terminates on a country by country
basis when all valid claims under any patent included in the
license have expired or are no longer enforceable.
University of Turku
Under a June 2004 patent assignment agreement with the
University of Turku, the Company was assigned rights to a patent
relating to the method of use of fispemifene for treatments for
lower urinary tract symptoms or pelvic pain. Under the terms of
the agreement, Hormos paid patent application and patent
approval fees to the inventors and a signing fee to the
University of Turku totaling approximately $13,700. The Company
has agreed to pay a milestone payment of approximately $11,800
and to pay a royalty based on net income. The requirement to pay
royalties continues on a country-by-country basis until the
expiration of the licensed patent in that country. The Company
has further agreed to pay a percentage of any purchase price
received for the outright license or assignment to a third party
of the applicable patent. The license terminates on a country by
country basis when all valid claims under any patent included in
the license have expired or are no longer enforceable.
Notes to Consolidated Financial
Statements — (Continued)
Royalties and Research and Development Expense
Aggregate minimum royalties under licensing and research
agreements range from $250,000 to $450,000 on net sales of
products incorporating compounds under these agreements. There
were no minimum royalty payments required for the years ended
December 31, 2003, 2004, and 2005.
The amount charged to research and development expense in
connection with these agreements was $2,561,617, $1,611,045,
$646,812, and $4,944,474 for the years ended December 31,2003, 2004 and 2005, and for the period from inception
(November 20, 2000) to December 31, 2005, respectively.
Commitments and Contingencies
In the ordinary course of its business, QuatRx makes certain
indemnities, commitments and guarantees under which it may be
required to make payments in relation to certain transactions.
These include indemnities of clinical investigators,
consultants, and contract research organizations involved in the
development of QuatRx’s pre-clinical and clinical stage
products and indemnities to QuatRx’s directors and officers
to the maximum extent permitted under the laws of the State of
Delaware. The duration of these indemnities, commitments and
guarantees varies, and in certain cases is indefinite. The
majority of these indemnities, commitments and guarantees do not
provide for any limitation of the maximum potential future
payments the Company could be obligated to make. QuatRx has not
recorded any liability for these indemnities, commitments and
guarantees in the accompanying balance sheets. However, QuatRx
accrues for losses for any known contingent liability, including
those that may arise from indemnification provisions, when
future payment is probable. No such losses have been recorded to
date.
The par value for all shares of Preferred Stock is $0.01.
During 2000, QuatRx issued 1,575,000 shares of
Series A Preferred Stock at $1.00 per share for
proceeds of $1,546,259, net of issuance costs of $28,741.
During 2001, QuatRx issued 1,400,000 shares of
Series B Preferred Stock at $1.50 per share for
proceeds of $2,070,661, net of issuance costs of $29,339.
During 2002, QuatRx issued 1,400,000 shares of
Series B Preferred Stock at $1.50 per share for
proceeds of $2,078,671 net of issuance costs of $21,329.
Notes to Consolidated Financial
Statements — (Continued)
During 2003, QuatRx issued 1,400,000 shares of
Series B Preferred Stock at $1.50 per share for
proceeds of $2,084,977, net of issuance costs of $15,023. Also
during 2003, QuatRx issued 12,885,963 shares of
Series C Preferred Stock at $1.14 per share for
proceeds of $14,485,395, net of $204,603 of issuance costs.
During 2004, QuatRx issued 12,710,528 shares of
Series C Preferred Stock at $1.14 per share for
proceeds of $14,448,873, net of issuance costs of $41,129. Also
during 2004, QuatRx issued 10,964,285 shares of
Series D Preferred Stock at $1.40 per share for
proceeds of $15,183,204, net of issuance costs of $166,796.
During 2005, QuatRx issued 13,821,428 shares of
Series D Preferred Stock at $1.40 per share for
proceeds of $19,316,851, net of issuance costs of $33,148. In
addition, in connection with the acquisition of Hormos, QuatRx
issued 857,145 shares of Series D and
3,408,025 shares of Series D-1 Preferred Stock.
The holders of Preferred Stock have the following rights and
preferences:
Voting Rights
The holders of shares of all series of preferred stock are
entitled to one vote for each share of common stock into which
each share of preferred stock could be converted. The holders of
preferred stock, voting equally with shares of common stock, are
entitled to vote upon any matters submitted to stockholders.
Election of Directors
The holders of Series A Preferred Stock, as a class, the
holders of Series B Preferred Stock, as a class, and the
holders of Series D-1 Preferred Stock, as a class, each are
entitled to elect one director to QuatRx’s Board of
Directors. The holders of Series C Preferred Stock, as a
class, and the holders of Series D Preferred Stock, as a
class, each are entitled to elect two directors to QuatRx’s
Board of Directors. The holders of Series A Preferred
Stock, Series B Preferred Stock, Series C Preferred
Stock, Series D Preferred Stock, and
Series D-1
Preferred Stock, voting together as a single class, are entitled
to elect one director to QuatRx’s Board of Directors. The
holders of the QuatRx common stock, voting as a single class,
are entitled to elect one member to QuatRx’s Board of
Directors.
Dividends
The holders of Series D Preferred Stock and
Series D-1
Preferred Stock are entitled to receive dividends, prior and in
preference to any declaration or payment of any dividend on
Series A, Series B or Series C Preferred Stock,
or common stock of QuatRx, at the rate of 8% per annum on
the original issue price of $1.40.
The holders of Series C Preferred Stock are entitled to
receive dividends, prior and in preference to any declaration or
payment of any dividend on Series A or Series B
Preferred Stock, or common stock of QuatRx, at the rate of
8% per annum on the original issue price of $1.14.
The holders of Series A and Series B Preferred Stock
are entitled to receive dividends, prior and in preference to
any declaration or payment of any dividend on common stock of
QuatRx, at the rate of 9% per annum for the period prior to
the issuance of the Series C shares and 8% per annum
subsequent to the issuance of the Series C shares on the
original issue price of $1.00 and $1.50, respectively.
Dividends are payable only when, as and if declared by the Board
of Directors. As of December 31, 2005, no dividends have
been declared.
Notes to Consolidated Financial
Statements — (Continued)
Liquidation
In the event of any liquidation, dissolution or winding up of
QuatRx, after payment of the full liquidation preference, any
remaining assets shall be distributed ratably to the holders of
all preferred stock, on an as-converted to common stock basis,
and common stock until the holders of all preferred stock have
received an aggregate amount per share equal to three times the
applicable original issue price; thereafter, the holders of
common stock shall receive all of the remaining assets in
proportion to their applicable share.
The liquidation preference is $1.00, $1.50, $1.14, $1.40 and
$1.40 per share for Series A, Series B,
Series C, Series D and
Series D-1
Preferred Stock, respectively, plus 9% per annum for
Series A and Series B shares prior to the issuance of
Series C Preferred Stock and 8% per annum thereafter,
plus 8% per annum from the date of issuance for
Series C, Series D and
Series D-1
Preferred Stock, shares less any dividends declared and paid to
the respective shareholders.
Redemption
The redemption provisions of the preferred stock stipulate that
at any time on or after December 31, 2008, upon request of
at least 65% of the then outstanding shares of Series D
Preferred Stock and a majority of the then outstanding shares of
Series C Preferred Stock, QuatRx is required to redeem the
Series A, Series B, Series C, Series D and
Series D-1
Preferred Stock. The redemption price is equal to the
liquidation preference. During the years ended December 31,2003, 2004 and 2005, and the period from inception
(November 30, 2000) to December 31, 2005 accretion of
$1,503,791, $2,319,484, $13,210,271 and $17,570,604
respectively, was recorded to adjust the carrying amounts of the
preferred stock to their redemption value.
Conversion
All series of preferred stock are convertible, at the option of
the holder, at any time after the date of issuance, into fully
paid non-assessable shares of common stock as determined by the
then applicable conversion rate, which is generally
one-to-one. The
conversion rate is subject to adjustment from time to time for
certain subdivisions, dividends, combinations, consolidations,
dilutive issuances and certain other factors. As of
December 31, 2005, 61,230,251 shares of common stock
are reserved for the conversion of the preferred shares.
Automatic conversion occurs immediately upon the closing of a
firmly underwritten public offering pursuant to an effective
registration statement under the Securities Act of 1933 meeting
certain requirements set forth in the Company’s certificate
of incorporation, or with respect to
Series D-1
Preferred Stock, conversion occurs upon the written election of
the holders of a majority of the outstanding shares of the
Series D-1
Preferred Stock, voting as a single class, or with respect to
Series D Preferred Stock, conversion occurs upon written
election of the holders of 65% of the outstanding Series D
Preferred Stock, voting as a single class, or with respect to
shares of Series C Preferred Stock, conversion occurs upon
the written election of the holders of 75% of the outstanding
shares of Series C Preferred Stock, voting as a single
class, or with respect to shares of Series A Preferred
Stock and Series B Preferred Stock, conversion occurs upon
the written election of 75% of the outstanding shares of the
Series A and Series B Preferred Stock voting together
as a single class.
9.
Common Stock
Certain issued and outstanding shares of QuatRx’s common
stock are subject to vesting and the right of repurchase by
QuatRx at the option of QuatRx. Vesting is generally over four
years. Unvested shares are subject to repurchase at a price
equal to the original purchase price of the stock. As of
December 31, 2003,
Notes to Consolidated Financial
Statements — (Continued)
2004 and 2005 there were 1,969,333, 1,125,333 and 281,333
unvested shares, respectively, subject to repurchase at prices
ranging from $0.05 to $0.15 per share.
10.
Stock Option Plans and Employee Benefits
2000 Equity Incentive Plan
In December 2000, the Board of Directors approved QuatRx’s
2000 Equity Incentive Plan (“2000 Plan”), under which
QuatRx may grant options and restricted stock awards to
officers, employees, consultants and directors. Options granted
may be exercised for a period of not more than 10 years
from the date of grant or any shorter period as determined by
the Board of Directors. Options vest as determined by the Board
of Directors, generally over a four-year period.
Under the 2000 Plan, QuatRx granted 20,000 options to purchase
shares of common stock to a non-employee consultant during 2004
at an exercise price of $0.20 per share. These options vest
immediately based upon the occurrence of a qualifying
transaction. As of December 31, 2005, none of these options
are exercisable.
2005 Stock Incentive Plan
In April 2005, the Board of Directors approved QuatRx’s
2005 Stock Incentive Plan (“2005 Plan”). Under the
2005 Plan, QuatRx may grant options and restricted stock awards
to employees, directors and consultants of the Company. In 2005,
the QuatRx board of directors agreed that options for 1,625,000
shares of common stock would be granted to QuatRx management
upon the success of a phase II clinical trial and options
for 2,750,000 shares would be granted upon the success of a
phase III clinical trial, in each case, as determined by
the Company’s Board of Directors. No grants have been made
under this arrangement.
Options granted may be exercised for a period of not more than
10 years from the date of grant or any shorter period as
determined by the administrator of the plan. Options vest as
determined by the administrator of the plan, generally over a
four-year period. The option price of any incentive stock option
shall equal or exceed the fair value per share on the date of
grant as determined by the administrator of the plan, or 110% of
the fair value per share in the case of a 10% or greater
stockholder.
At December 31, 2005, QuatRx had reserved an aggregate of
8,175,259 shares of common stock for issuance under the
plans and 1,604,269 shares were available for grant.
QuatRx did not grant any options prior to 2003. The total
options outstanding and exercisable under the plans as of
December 31, 2004 and 2005 are as follows:
In 2003, QuatRx adopted a safe-harbor 401(k) employee savings
and retirement plan which is qualified under
Sections 401(a) and 401(k) of the Internal Revenue Code of
1986, as amended. Eligible employees may elect to defer current
compensation up to the statutorily prescribed annual limits and
have the amount of such
Notes to Consolidated Financial
Statements — (Continued)
reduction contributed to the 401(k) Plan. As a safe-harbor plan,
QuatRx contributes an amount equal to 3% of certain eligible
employee’s compensation annually as a nonelective
contribution to the Plan. Expense related to the plan totaled
$29,006, $12,000, $27,938 and $68,944 in 2003, 2004 and 2005,
and the period from inception (November 20, 2000) to
December 31, 2005, respectively.
QuatRx’s Finnish employees are covered by a defined
contribution pension plan as required by the TEL Employees
Pension Act. The pension plan payment levels are set annually by
the Finnish Ministry of Social Affairs and Health. In 2005,
QuatRx is required to contribute 17.3% of certain eligible
employees’ compensation to the plan. Since the acquisition
of Hormos in May 2005, QuatRx has contributed approximately
$154,252 to the plan through December 31, 2005.
11.
Income Taxes
Deferred income taxes reflect the net tax effects of temporary
differences between the carrying amounts of assets for financial
reporting and the amount reported for income tax purposes.
Significant components of QuatRx’s deferred tax assets are
shown below. A valuation allowance has been established, as
realization of such assets is uncertain due to the
Company’s history of generating net operating losses.
At December 31, 2004 and 2005, QuatRx had U.S. federal
tax net operating loss carryforwards of approximately
$18,527,000 and $30,517,000, respectively, which can be used to
offset future U.S. taxable income. The U.S. federal
tax loss carryforwards will begin to expire in 2021, unless
previously utilized. QuatRx had Finnish tax net operating loss
carryforwards of approximately $49,574,000 at December 31,2005, which can be used to offset future Finnish taxable income.
The Finnish tax loss carryforwards will begin to expire in 2008.
Utilization of the net operating loss carryforwards may be
subject to a substantial annual limitation due to ownership
change limitations provided by the Internal Revenue Code of
1986, as well as similar state and foreign provisions. These
ownership changes may limit the amount of net operating loss
carryforwards that can be utilized annually to offset future
taxable income and tax, respectively. Subsequent ownership
changes could further affect the limitation in future years.
These annual limitation provisions may result in the expiration
of certain net operating losses and credits before utilization.
Notes to Consolidated Financial
Statements — (Continued)
The Company’s effective tax rate differs from the
U.S. federal statutory rate of 34% due to the Company
providing a valuation allowance against deferred tax assets,
which primarily consists of net operating loss carryforwards.
The Company’s income tax provision (benefit) consisted of
the following:
Additional deferred tax assets totalling $12,344,000 and a
related full valuation allowance resulted due to the net
operating losses acquired in the Hormos transaction.
12.
Segment Information
In accordance with SFAS No. 131, Disclosures about
Segments of an Enterprise and Related Information, the
Company has determined that it is principally engaged in one
operating segment: the research and development of therapeutic
compounds primarily for treatment of endocrine, metabolic and
cardiovascular diseases. Management uses consolidated financial
information in determining how to allocate resources to its
company-wide research and product development efforts and assess
financial performance.
The Company operates in two geographic locations: the United
States and Finland. The following table summarizes selected
financial information of the Company’s operations by
geographic location:
In January 2006, the Company entered into an $18,000,000 debt
agreement with Hercules Technology Growth Capital, Inc., a third
party lending company, and borrowed $6,000,000 under the
agreement with $12,000,000 available for future draws through
the end of 2006. Each loan drawn under the agreement bears
interest at prime plus 3% with interest-only payments due during
the first 12 months of each loan. Principal is repaid over
36 months after the interest-only period, with a balloon
payment due at the end of the repayment period. Loans under the
agreement are collateralized by substantially all of the
Company’s assets other than intellectual property rights.
In addition, the debt agreement contains covenants restricting
the ability to incur further indebtedness, pay dividends or make
investments, subject to exceptions specified in the agreement.
In connection with the debt agreement, QuatRx issued a warrant
to the lender to purchase shares of QuatRx preferred stock. The
number of shares and exercise price in the warrant will be
determined by a formula based on the timing and price of the
next round of equity invested in the Company. The warrant is
exercisable for seven years from the date of issue, or three
years after an initial public offering of the Company’s
common stock.
In our opinion, the accompanying balance sheets and the related
income statements and cash flow statements present fairly, in
all material respects, the financial position of Hormos
Medical Oy at December 31, 2004 and December 31,2003, and the results of its operations and its cash flows for
the years then ended in conformity with accounting principles
generally accepted in Finland. These financial statements are
the responsibility of the Company’s management. Our
responsibility is to express an opinion on these financial
statements based on our audits. We conducted our audits of these
statements in accordance with auditing standards generally
accepted in the United States of America. 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, assessing the accounting principles used
and significant estimates made by management, and evaluating the
overall financial statement presentation. We believe that our
audits provide a reasonable basis for our opinion.
Accounting standards generally accepted in Finland vary in
certain significant respects from accounting principles
generally accepted in the United States of America. Information
relating to the nature and effect of such differences is
presented in Note 31 to the financial statements.
Accounting Policies and Notes to Financial Statements
1.
Background and Description of Business
Hormos Medical Oy is a pharmaceutical discovery and development
company established in 1997 in Turku, Finland. Its core
competence involves research in tissue-specific regulation
mechanisms of hormones and development of patented
pharmaceuticals, based on the core competence, for the
international market.
The Company has a license and research collaboration agreement
with the Belgian Solvay Pharmaceuticals. The agreement will
exploit Hormos Medical’s core competence in development of
a new medicine for the treatment of endometriosis. Net sales for
the financial year amounted to 2.03 million euros of which
1.94 million euros consist of research services delivered
to Solvay Pharmaceuticals.
During the reporting period the Company has continued its
development projects that all are involved in hormone dependent
treatment of diseases of the elderly. The company has research
and development activities in Turku and Oulu. In the end of the
financial period the number of personnel was 38, of whom in
Turku 30 employees and in Oulu 8 employees.
At the Annual General Meeting on March 15, 2004 it was
noted that the equity was less than half of the share capital.
The meeting decided to increase the share capital with not more
than 130.719 shares by issuing a convertible bond of
1 million euros. The loan was subscribed as a whole during
the financial year.
Prior to 2003, the Hormos Medical “Group”consisted of a parent company, Hormos Medical Oyj, and its
wholly owned subsidiary, Hormos Nutraceutical Oy. During
December 2003, Hormos Nutraceutical Oy was dissolved and merged
into Hormos Medical Oyj. As a result, the Company charged a
merger loss in 2003 to research and development expenses in the
amount of
€3,528,747,
relating to the accumulated losses of Hormos Nutraceutical Oy.
Hormos Medical Oyj changed its name to Hormos Medical Oy in 2005.
2.
Preparation of the Financial Statements
The Company’s financial statements have been prepared in
accordance with Finnish generally accepted accounting principles
(“Finnish GAAP”). The accounting methods have not
changed from previous year and thus the financial statements are
comparable. The Company’s financial statements are stated
in Euros
(“€”).
3.
Fixed Assets
Assets are recorded at historical cost less accumulated
depreciation. Grants received are recorded against the
acquisition cost of the related acquired assets.
Depreciation is calculated as follows:
•
Intangible assets (patents and in-licensing agreements) are
amortized on a straight-line method over 10 years.
•
Office equipment and furniture are depreciated using the 25%
residue value method.
•
The acquisition cost of machinery and equipment acquired for
research and development purposes is expensed as incurred.
•
Computer software is depreciated on a straight-line method over
4 years.
If the useful life for an asset is shorter than three years, the
acquisition costs are expensed as incurred.
4.
Foreign Currency Translation
Foreign currency denominated items are included only in trade
payables and all such foreign currency denominated payables have
been settled prior to the date of the signing of the financial
statements. As a result, all foreign currency denominated items
are valued by using the payment date rate.
Share capital at the beginning of the financial year
January 1,
206,031.33
206,031.33
Share capital at the end of the financial year
December 31,
206,031.33
206,031.33
Share premium reserve, beginning of the financial year
January 1,
7,589,243.37
7,589,243.37
Share premium reserve, end of the financial year
December 31,
7,589,243.37
7,589,243.37
Retained deficit
(16,952,267.11
)
(9,124,694.43
)
Loss for the financial year
(2,612,728.55
)
(7,827,572.68
)
Shareholders’ equity before capital loans
(11,769,720.96
)
(9,156,992.41
)
Capital loans
Sitra 1391
67,275.17
67,275.17
Tekes 729/97
287,584.54
287,584.54
Tekes 557/97
105,748.83
105,748.83
Tekes 129/99
504,563.78
504,563.78
Tekes 312/99
420,469.82
420,469.82
Tekes 313/99
420,469.82
420,469.82
Tekes 670/99
354,564.54
354,564.54
Tekes 677/00
420,469.82
420,469.82
Tekes 719/00
1,345,503.41
1,345,503.41
Tekes 720/00
1,194,134.28
1,194,134.28
Tekes 970/00
840,939.63
840,939.63
Tekes 225/01
1,295,047.03
1,295,047.03
Tekes 379/01
218,644.30
218,644.30
Tekes 539/01
456,382.00
456,382.00
Tekes 701/01
336,375.85
336,375.85
Tekes 291/02
92,382.00
43,798.00
Tekes 457/02
468,000.00
468,000.00
Tekes 835/02
227,010.00
128,747.00
Tekes 359/03
637,879.00
371,588.00
Tekes 439/04
768,823.00
—
Capital loans in total
10,462,266.82
9,280,305.82
Shareholders’ equity in total
(1,307,454.14
)
123,313.41
18.
Capital Loans
Booked as
Paid to Hormos
Capital
Lender
Medical €
Loan €
Loan Period
Sitra nro 1391
67,275.17
67,275.17
3/24/1997-8/31/2001
— Interest rate of the capital loan is
12 months’ euribor rate + 3%
Tekes, loans with capital loan term
12,016,598.82
10,462,266.82
6-8 years including 3-5 years without paybacks
In addition Tekes, the National Technology Agency has granted to
Hormos Medical capital loans worth 1,993,468.00 euros, which
have not been withdrawn by the Company as at December 31,2004.
The interest rate is one percent below the Bank of
Finland’s reference interest rate, however the minimum is
three percent.
•
The interest has been accounted in total as interest of a
subordinated capital loan and it has not been booked as
financial expense.
•
Tekes loans are not convertible into the company’s shares.
•
The terms of the subordinated capital loans are recognized
according to the chapter 5 in the Finnish Companies Act.
•
In addition the rules of Tekes are applied.
The capital loans can be repaid to the lenders only if the terms
in the Finnish Companies Act chapter 5 are fulfilled, i.e.
if the company has adequate equity capital after the repayment
of the loan.
Long-term liabilities consist of loans granted by Tekes, the
National Technology Agency. In addition, Tekes has granted to
Hormos Medical R&D loans amounting to 546,436.00 euros,
which had not been withdrawn by the Company as at
December 31, 2004.
The Company has rented from PharmaCity’s building a total
of
2,966 m2
office and laboratory facilities under a
10-year lease, which
ends in 2011. There is seven years left of the agreement. Of
these office and laboratory facilities, the Company has sublet
1,137 m2.
The rents due for the financial year 2005 of the
1,829 m2
are approximately
€390,000.
26.
Other Liabilities
The company has not booked the social security liability arising
from its share option plan.
27.
Income Taxes
Deferred tax assets from tax loss carry forwards as at
December 31, 2004 amounted to
€10,352,893.30.
The company has not recorded the deferred tax asset in its
financial statements.
The rights to 21,700 options have been returned to the Company
and expired due to the fact that the option right holders have
left the company before the subscription period has started.
The Company has deviated from the subscription right because the
options have been directed to the personnel. The option rights
accepted in the General Meeting on April 15, 1999 have been
given to the Company’s advisers in year 1999 as incentives
for the execution of the round. These options expire on
June 30, 2005.
The subscription prices have been defined on basis of the
previous share issue’s share price.
Other conditions attached to the subscription right: the company
has to be listed or all shareholders have been offered otherwise
a chance to discharge of 50 percent of the shares owned by
them, the employee has to be employed by the company
continuously until the beginning of the subscription period.
The terms and conditions for subscribing shares based on the
employee stock option plans did not fulfill and new shares
cannot be subscribed based on any of Hormos Medical’s
employee stock option plans.
29.
Convertible Bond
Total
Face
Subscription
Subscription
Number
Decision of the General Meeting
Value €
of the Share
Price €
of Shares
3/15/2004
22,222.23
10/15/2004- 3/15/2005
7.65
130,719.00
The nominal value for the convertible debt of
€1,000,000 is
included in short-term liabilities.
Loss for the financial year and adequacy of
shareholders’ equity
The Board proposes that the loss for the financial period
amounting to 2,612,728.55 euros shall be transferred to the
retained deficit account. There will be no dividends distributed.
The Extraordinary General Meeting approved the balance sheet
prepared under the Finnish Companies Act, which requires the
Board of Directors to follow shareholders’ equity
continuously. According to Chapter 13 of the Companies Act,
if the Board of Directors, when preparing the annual accounts
notices or if it otherwise has a reason to assume that the
shareholders’ equity of the Company is less than half of
its share capital, the Board of Directors must, as soon as
possible, prepare a balance sheet to ascertain the financial
situation of the company. If the shareholders’ equity of
the company, according to the balance sheet, is less than half
of the share capital, the Board of Directors must, without a
delay, submit the balance sheet to be audited by the auditors
and to convene the General Meeting of the Shareholders to decide
on actions required by the ratio of shareholders’ equity
and share capital.
In the Ordinary Shareholders’ Meeting held on
March 15, 2004, the balance sheet indicated that the level
of shareholder’s equity was less than half of the share
capital and, thus, the Board of Directors were given
12 months period to fix the ratio. Consequently, the Board
of Directors convened an Extraordinary Shareholders Meeting in
January 7, 2005 and presented an audited control balance
sheet demonstrating that on November 30, 2004 the
shareholders’ equity was more than half of the share
capital.
Hormos Medical merger with QuatRx Pharmaceuticals in May
2005
Hormos Medical announced the merger with QuatRx Pharmaceuticals,
a biopharmaceutical company based in Ann Arbor, Michigan, USA on
May 16, 2005.
In late 2004 Hormos Medical initiated negotiations on project
out-licensing with QuatRx Pharmaceuticals. The negotiations lead
to QuatRx’s offer to acquire all of Hormos Medical
Oy’s capital stock in the spring 2005. All shareholders of
Hormos Medical accepted the offer and the transaction was closed
on May 25, 2005.
The transaction had a positive effect on Hormos Medical as it
created access to the US capital markets and improved business
development and commercialization capabilities in the US market.
Supported by QuatRx Pharmaceuticals’ strong financial
standing the company has a possibility to advance the expensive
clinical development projects, ospemifene and fispemifene in
particular. Development of the earlier stage discovery projects
was also made possible through the secured financing position.
31.
Summary of Significant Differences Between Generally Accepted
Accounting Principles in Finland and Generally Accepted
Accounting Principles in the United States
The Company is in the development stage. The Company’s
financial statements have been prepared in accordance with
Finnish GAAP. The tables that follow are a reconciliation of the
significant differences relating to the profit and loss
statement and total shareholders’ equity for the last two
years as permitted by the U.S. Securities and Exchange
Commission. Cash flow statements according to U.S. GAAP are
included for the years ended December 31, 2004 and 2003.
Under Finnish GAAP, patent costs have been capitalized as a
long-term asset and
amortized. Under U.S. GAAP, patent costs have been expensed
in the period they were incurred.
(B)
Depreciation Expense
Under Finnish GAAP, research equipment has been fully
depreciated in the year of acquisition and other furniture and
office equipment has been depreciated using methods other than
straight-line. Under U.S. GAAP, depreciation expense has
been adjusted and recognized on the
straight-line basis
over the underlying asset’s depreciable lives consistent
with QuatRx.
(C)
Capital Leases
Under Finnish GAAP, classification of leases into finance or
operating leases is optional. The Company has treated all leases
as operating leases. Under U.S. GAAP, Statement of
Financial Accounting Standards No. 13, Accounting for
Leases, leases are classified as either operating or capital
leases. A lease meeting certain criteria must be treated as a
capital lease under U.S. GAAP. The lessee records a capital
lease as an asset and an obligation at an amount equal to the
lesser of the present value of the minimum lease payments at the
beginning of the lease term or the fair value of the leased
property. Under U.S. GAAP those leasing agreements which
qualify as capital leases have been adjusted in the
U.S. GAAP reconciliation.
(D)
Ospemifene Milestone Payment
Under Finnish GAAP a 200,000 Euro milestone payment due in
December 2004 was expensed in March 2005, when it was invoiced
to Hormos and payment was made. Under U.S. GAAP, the
milestone payment has been accrued as of December 31, 2004.
(E)
Long-Term Debt
Under Finnish GAAP, subordinated loans with Tekes and Sitra have
been classified as equity. Under U.S. GAAP, the loans have
been reclassified as long-term debt.
(F)
Interest Expense
Under Finnish GAAP, interest expense on subordinated loans is
not recorded until the Company has distributable retained
profits and has paid the interest. To date, no interest expense
has been recognized or paid on these subordinated loans. Under
U.S. GAAP, interest expense on the subordinated loans has
been accrued at each balance sheet date.
(G)
Grant Income
Under Finnish GAAP, grant income has been recognized and a grant
receivable recorded at the balance sheet date when a grant
application is expected to be filed shortly thereafter. Under
U.S. GAAP, grant income has been adjusted to recognize
grant income at the time grant proceeds were received.
(H)
Hormos Nutraceutical
Under Finnish GAAP, with the merger of Hormos Nutraceutical and
Hormos Medical in 2003, a cumulative
loss-to-date for Hormos
Nutraceutical as of December 2002 was recorded by Hormos Medical
as a current period research and development expense in 2003.
Under U.S. GAAP, the December 2002 cumulative
loss-to-date for Hormos
Nutraceutical has been reflected as a prior period adjustment in
Hormos Medical Oy’s 2003 financial statements.
Under U.S. GAAP, the amounts recorded as Net Sales by
Hormos, have been classified as Other Income by QuatRx. The
amounts represent contract research income.
(J)
Accounts Payable
Under Finnish GAAP, accounts payable denominated in foreign
currencies are valued at the exchange rate in effect at the time
of payment. Under U.S. GAAP, foreign currency denominated
payables are valued at the exchange rate in effect as of each
balance sheet date. As the differences were determined to be
insignificant, no adjustment was recorded.
Additional Disclosures under U.S. GAAP:
Comprehensive income
Under U.S. GAAP, comprehensive income includes net income
and “other” comprehensive income. “Other”
comprehensive income (OCI) includes charges or credits to
equity that are not the result of transactions with owners,
including examples such as adjustments to minimum pension
liabilities, unrealized gains and losses on available-for-sale
debt or equity securities, and gains or losses on certain
derivative instruments qualifying for hedge accounting. During
the periods presented, the Company has not had any transactions
that have resulted in OCI, and accordingly, net income of the
Company represents total comprehensive income of the Company.
UNAUDITED PRO FORMA CONDENSED COMBINED FINANCIAL
STATEMENTS
On May 25, 2005, the QuatRx Pharmaceuticals Company
(“QuatRx” or the “Company”) completed the
acquisition of Hormos Medical Oy (“Hormos”), a Finnish
development-stage pharmaceuticals company. Hormos is in the
development stage and is presumed not to be a business according
to the Emerging Issues Task Force (“EITF”)
98-3, Determining
Whether a Nonmonetary Transaction Involves Receipt of Productive
Assets or of a Business. The transaction was therefore
accounted for as a purchase of assets and assumption of
liabilities. In connection with the acquisition, the Company
acquired all of the outstanding capital stock of Hormos in
exchange for 857,145 shares of Series D and
3,408,025 shares of
Series D-1
Preferred Stock and 9,520,154 shares of common stock and
assumed current liabilities and notes payable totaling
$20,289,423. The Company also incurred $1,000,000 in
acquisition-related costs.
Adjustments were made to record the acquired net assets of
Hormos at fair value, including allocating a portion of the
total purchase price to in-process research and development.
Based on management’s review of the analysis of the
tangible and intangible assets and liabilities of Hormos, the
purchase price has been allocated as follows:
Total acquisition costs:
Issuance of Series D Preferred Stock
$
1,200,003
Issuance of Series D-1 Preferred Stock
4,771,235
Issuance of common stock
2,856,047
Acquisition-related costs
1,000,000
Assumed liabilities and notes payable
20,289,423
$
30,116,708
Allocated to assets and liabilities as follows:
Current assets
$
1,170,596
Property and equipment acquired
776,995
In-process research and development, expensed
25,800,000
Work force
480,000
Favorable loans
2,101,923
Note receivable
1,380,219
Accrued contingent consideration
(1,593,025
)
$
30,116,708
Contingent consideration associated with the acquisition
includes an additional 321,415 shares and
1,277,995 shares of Series D and
Series D-1
Preferred Stock, respectively, and 3,570,046 shares of
common stock, held in escrow and payable upon the occurrence of
certain future events.
One-third of the
contingent shares secure indemnification obligations of the
Hormos selling shareholders and will be released to the Company
in satisfaction of an indemnification claim or to the Hormos
shareholders one year after the closing date of the acquisition.
The remaining contingent shares will generally be released to
Hormos selling shareholders upon the first to occur of: the
closing of a qualified public offering of QuatRx’s common
stock or the dosing of the first patient in a second
phase III clinical trial of ospemifene. Additional purchase
consideration will be recorded as the contingent consideration
is released. The additional purchase consideration will be
allocated to the assets acquired based upon their relative fair
value and will result in additional expense for in-process
research and development, and accrued the contingent
consideration totaling $1,593,025 will be reclassified to equity.
The following sets forth pro forma condensed combined financial
statements (i) derived from the audited financial
statements of QuatRx for the year ended December 31, 2005
and (ii) derived from the unaudited financial statements of
Hormos for the period from January 1, 2005 to May 25,2005.
The unaudited pro forma condensed combined financial statements
and notes are presented to give effect to the acquisition of
Hormos by QuatRx and represent the combined company’s
unaudited pro forma statements of operations for the year ended
December 31, 2005. The statement of operations for the year
ended December 31, 2005 was derived by combining the
results for the year ended December 31, 2005 of QuatRx with
the results for the period from January 1, 2005 to
May 25, 2005 of Hormos.
The following unaudited pro forma condensed combined statements
of operations give effect to the acquisition transaction between
QuatRx and Hormos as if it occurred on January 1, 2005, the
first day of QuatRx’s fiscal year ended December 31,2005. The unaudited pro forma condensed combined financial
statements include adjustments directly attributable to the
acquisition transaction. The pro forma adjustments are described
in the accompanying notes. The pro forma adjustments are based
upon available information and assumptions that are factually
supportable including the completion of the acquisition
transaction. These unaudited pro forma condensed combined
financial statements are not necessarily indicative of the
results of operations that would have been achieved had the
transaction actually taken place at the date indicated and do
not purport to be indicative of future operating results.
Hormos’s historical condensed financial statements are
presented in Euros and were prepared in accordance with Finnish
GAAP, which differs in certain respects from U.S. GAAP.
QuatRx’s condensed financial statements were prepared in
accordance with U.S. GAAP and are presented in
U.S. dollars. As described in Note 1 to these
unaudited pro forma condensed combined financial statements,
Hormos’s historical condensed financial statements were
reconciled to U.S. GAAP and were translated from Euros to
U.S. dollars. As presented in Note 1, pro forma
adjustments have been made to the financial statements of Hormos
to conform to QuatRx’s presentation under U.S. GAAP.
The unaudited pro forma condensed combined financial statements
and related notes should be read in conjunction with the
historical consolidated financial statements and related notes
and other financial information pertaining to QuatRx and Hormos,
including “Management’s Discussion and Analysis of
Financial Condition and Results of Operations,” and
“Risk Factors” which appear elsewhere in this
prospectus.
Hormos’s financial statements were prepared in accordance
with Finnish GAAP, which differs in certain material respects
from U.S. GAAP. Hormos also classified certain costs
differently than QuatRx in their statement of operations. The
following schedule summarizes the necessary material adjustments
to conform the Hormos statement of operations for the period
from January 1, 2005 to May 25, 2005 to U.S. GAAP
and to reclassify certain amounts to QuatRx’s basis of
presentation.
Hormos amounts have been translated into U.S. dollars at a
rate of
€1.00 = US$1.2994,
the average daily exchange rate for the period from
January 1, 2005 to May 25, 2005
(b)
Revenue
Reclassification of Hormos contract research income to other
income (expense) to conform to QuatRx’s statement of
operations classification
Reclassification of Hormos contract research income to other
income (expense) to conform to QuatRx’s statement of
operations classification
€
1,279,699
U.S. GAAP adjustment for deferred revenue
(513,075
)
€
766,624
(g)
Other expense
U.S. GAAP adjustment for capital leases
€
(2,517
)
U.S. GAAP adjustment for interest expense on long-term debt
(182,088
)
Reclassification of other income from operations to other income
(expense) to conform to QuatRx’s statement of operations
classification
882
€
(183,723
)
2.
Pro Forma Adjustments
(A) Reflects an increase in depreciation and
amortization expense from the
step-up of
Hormos’s tangible and intangible assets to their estimated
fair values as follows:
(B) Reflects an increase in depreciation and
amortization expense from the
step-up of
Hormos’s tangible and intangible assets to their estimated
fair values as follows:
Increase in depreciation expense resulting from the step-up of
Hormos furniture and equipment to their estimated fair values
$
24,766
Increase in amortization expense resulting from the intangible
asset associated with the Hormos work force
15,870
$
40,636
(C) Reflects the elimination of the $25,800,000
purchased in-process research and development charge directly
resulting from the acquisition of Hormos.
(D) Reflects an increase in interest expense
resulting from the amortization of discount associated with the
Hormos favorable loans of $136,410 for December 31, 2005.
(E) The increase in weighted average common shares
outstanding for the basic and diluted earnings per share
calculations reflects the issuance of 9,520,154 shares of
QuatRx common stock issued in the acquisition.
Until ,
2006, all dealers that buy, sell or trade the common stock may
be required to deliver a prospectus, regardless of whether they
are participating in this offering. This is in addition to the
dealers’ obligation to deliver a prospectus when acting as
underwriters and with respect to their unsold allotments or
subscriptions.
The following table sets forth an itemization of the various
costs and expenses, all of which we will pay, in connection with
the issuance and distribution of the securities being
registered. All of the amounts shown are estimated except the
SEC Registration Fee, the Nasdaq National Market Listing Fee and
the NASD Filing Fee.
SEC Registration Fee
$
9,229
Nasdaq National Market Listing Fee
*
NASD Filing Fee
9,125
Printing and Engraving Fees
*
Legal Fees and Expenses
*
Accounting Fees and Expenses
*
NASD Legal Fees and Blue Sky Fees and Expenses
*
Transfer Agent and Registrar Fees
*
Miscellaneous
*
Total
$
*
*
To be filed by amendment.
Item 14.
Indemnification of Directors and Officers.
Our amended and restated certificate of incorporation and bylaws
provide that each person who was or is made a party or is
threatened to be made a party to or is otherwise involved
(including, without limitation, as a witness) in any action,
suit or proceeding, whether civil, criminal, administrative or
investigative, by reason of the fact that he or she is or was a
director or an officer of QuatRx or is or was serving at our
request as a director, officer, or trustee of another
corporation, or of a partnership, joint venture, trust or other
enterprise, including service with respect to an employee
benefit plan, whether the basis of such proceeding is alleged
action in an official capacity as a director, officer or trustee
or in any other capacity while serving as a director, officer or
trustee, shall be indemnified and held harmless by us to the
fullest extent authorized by the Delaware General Corporation
Law against all expense, liability and loss (including
attorneys’ fees, judgments, fines, ERISA excise taxes or
penalties and amounts paid in settlement) reasonably incurred or
suffered by such.
Section 145 of the Delaware General Corporation Law permits
a corporation to indemnify any director or officer of the
corporation against expenses (including attorneys’ fees),
judgments, fines and amounts paid in settlement actually and
reasonably incurred in connection with any action, suit or
proceeding brought by reason of the fact that such person is or
was a director or officer of the corporation, if such person
acted in good faith and in a manner that he reasonably believed
to be in, or not opposed to, the best interests of the
corporation, and, with respect to any criminal action or
proceeding, if he or she had no reasonable cause to believe his
or her conduct was unlawful. In a derivative action, (i.e., one
brought by or on behalf of the corporation), indemnification may
be provided only for expenses actually and reasonably incurred
by any director or officer in connection with the defense or
settlement of such an action or suit if such person acted in
good faith and in a manner that he or she reasonably believed to
be in, or not opposed to, the best interests of the corporation,
except that no indemnification shall be provided if such person
shall have been adjudged to be liable to the corporation, unless
and only to the extent that the court in which the action or
suit was brought shall determine that the defendant is fairly
and reasonably entitled to indemnity for such expenses despite
such adjudication of liability.
Pursuant to Section 102(b)(7) of the Delaware General
Corporation Law, Article Eighth of our amended and restated
certificate of incorporation eliminates the liability of a
director to us or our stockholders for monetary damages for such
a breach of fiduciary duty as a director, except for liabilities
arising:
•
from any breach of the director’s duty of loyalty to us or
our stockholders;
•
from acts or omissions not in good faith or which involve
intentional misconduct or a knowing violation of law;
•
under Section 174 of the Delaware General Corporation
Law; and
•
from any transaction from which the director derived an improper
personal benefit.
We carry insurance policies insuring our directors and officers
against certain liabilities that they may incur in their
capacity as directors and officers. In addition, we expect to
enter into indemnification agreements with each of our directors
and executive officers prior to completion of the offering.
Additionally, reference is made to the Purchase Agreement filed
as Exhibit 1.1 hereto, which provides for indemnification
by the underwriters of QuatRx, our directors and officers who
sign the registration statement and persons who control QuatRx,
under certain circumstances.
Item 15.
Recent Sales of Unregistered Securities.
In the three years preceding the filing of this registration
statement, we have sold the following securities that were not
registered under the Securities Act of 1933. No underwriters
were employed by us in connection with any of these transactions.
Issuances of Capital Stock
The sale and issuance of the securities set forth below were
deemed to be exempt from registration under the Securities Act
by virtue of Section 4(2) of Regulation D and
Regulation S promulgated thereunder.
1. On March 6, 2003, we issued
and sold 1,400,000 shares of our Series B Preferred
Stock at a price per share of $1.50 for an aggregate purchase
price of $2,100,000.
2. Between May 20, 2003 and
October 5, 2004, we issued and sold 25,596,491 shares
of our Series C Preferred Stock at a purchase price per
share of $1.14 for an aggregate purchase price of $29,179,999.74.
3. Between November 22, 2004
and October 31, 2005, we issued and sold
24,785,713.43 shares of our Series D Preferred Stock
at a purchase price per share of $1.40 for an aggregate purchase
price of $34,699,998.80.
4. On May 25, 2005, we issued
1,071,422 shares of our Series D Preferred Stock,
4,260,022 shares of our Series D-1 Preferred Stock and
11,900,185 shares of our common stock to the shareholders
of Hormos Medical Oy in exchange for shares and promissory notes
of Hormos representing 100% of all the outstanding capital stock
of Hormos and all securities or other instruments convertible
into or exercisable for capital stock of Hormos.
Certain Grants and Exercises of Stock Options
The sale and issuance of the securities described below were
deemed to be exempt from registration under the Securities Act
in reliance on Rule 701 promulgated under Section 3(b)
of the Securities Act, as transactions by an issuer not
involving a public offering or transactions pursuant to
compensatory benefit plans and contracts relating to
compensation as provided under Rule 701.
Exchange Agreement, dated May 20, 2005, by and among QuatRx
Pharmaceuticals Company, Hormos Medical Oy and the shareholders
of Hormos signatories thereto
2
.2**
Escrow Agreement, dated May 25, 2005, by and among QuatRx
Pharmaceuticals Company, Hormos Medical Oy, U.S. Bank
National Association and the shareholders of Hormos signatories
thereto
Form of Amended and Restated Certificate of Incorporation (to be
filed in connection with the closing of this offering and
effective upon the closing of this offering)
3
.6
Form of Amended and Restated Bylaws (to be effective upon the
closing of this offering)
4
.1**
Fourth Amended and Restated Investor Rights Agreement, entered
into as of November 22, 2004, by and among QuatRx
Pharmaceuticals Company. and certain investors named therein
4
.2**
Amendment to Fourth Amended and Restated Investor Rights
Agreement, entered into as of May 25, 2005, by and among
QuatRx Pharmaceuticals Company and certain investors named
therein
4
.3*
Specimen Common Stock Certificate
4
.4**
Warrant to Purchase Shares of the Series D Preferred Stock
of QuatRx Pharmaceuticals Company, dated as of January 26,2006, granted to Hercules Technology Growth Capital, Inc.
5
.1
Form of opinion of Heller Ehrman LLP
10
.1**
Amended and Restated 2005 Stock Incentive Plan
10
.2**
Form of Stock Option Agreement for Employee under Amended and
Restated 2005 Stock Incentive Plan
10
.3**
2000 Equity Incentive Plan
10
.4**
Form of Stock Option Agreement for Employee under 2000 Equity
Incentive Plan
10
.5**
Office Lease between Transwestern Great Lakes, L.P. and QuatRx
Pharmaceuticals Company, dated November 11, 2004
10
.6**
First Amendment to Lease, dated June 30, 2005, by and
between Transwestern Great Lakes REIT, L.P. and QuatRx
Pharmaceuticals Company
10
.7†**
Exclusive License Agreement, dated November 7, 2001, by and
between Deltanoid Pharmaceuticals, Inc. and QuatRx
Pharmaceuticals Company
10
.8†**
Amendment, dated November 8, 2004, to the Exclusive License
Agreement between Deltanoid Pharmaceuticals, Inc. and QuatRx
Pharmaceuticals Company dated November 7, 2001
Agreement, dated November 9, 2001, by and between Wisconsin
Alumni Research Foundation and QuatRx Pharmaceuticals Company
10
.10†**
Exclusive License Agreement dated February 14, 2005, by and
between EndoChem, Inc. and QuatRx Pharmaceuticals Company
10
.11†**
Letter, dated February 14, 2005, from The Regents of the
University of California to QuatRx Pharmaceuticals Company
10
.12†**
Exclusive License Agreement, dated May 19, 2003, by and
between ILEX Products, Inc. and QuatRx Pharmaceuticals Company
10
.13**
Amendment No. 1, dated September 30, 2004, to
Exclusive License Agreement, dated May 19, 2003, by and
between ILEX Products, Inc. and QuatRx Pharmaceuticals Company
10
.14†**
Patent License Agreement, dated March 25, 2004, by and
between Hormos Medical Oy and Orion Corporation
10
.15†**
Patent License Agreement, dated October 10, 2005, by and
between Hormos Medical Oy and Orion Corporation
10
.16†**
Restated Transfer Agreement, dated May 26, 2005, by and
between Hormos Medical Oy and Tess Diagnostics and
Pharmaceuticals Inc.
10
.17†**
Patent Assignment Agreement, dated June 4, 2004, by and
between Hormos Medical Oy and the University of Turku
10
.18†**
Agreement on Manufacturing, Sales and Distribution License for
HMRlignan, dated April 8, 2005, by and between Linnea S.A.
and Hormos Medical Oy
Loan and Security Agreement, dated January 26, 2006,
between QuatRx Pharmaceuticals Company and Hercules Technology
Growth Capital, Inc.
10
.21*
Loan Agreements between Tekes and Hormos Medical Oy
10
.22**
Lease Agreement, dated November 29, 2001, between BioTie
Therapies Oyj and Hormos Medical Oy (unofficial translation)
10
.23**
Lease Agreement, dated November 15, 2001, between Turun
Biolaakso Oy; and Hormos Medical Oy (unofficial translation)
10
.24*
Agreement on Development of the Synthesis of FC-1271a and
Manufacturing Option, dated May 1, 1999, by and between
Hormos Medical Oy, Tess Diagnostics and Pharmaceuticals, Inc.
and Orion Corporation Fermion
Application has been made to the Securities and Exchange
Commission to seek confidential treatment of certain provisions
of this exhibit under Rule 406 of the Securities Act of
1933. Omitted material for which confidential treatment has been
requested has been filed separately with the Securities and
Exchange Commission.
(b) Financial Statement Schedules.
Financial Statement schedules are omitted because the
information is included in our financial statements or notes to
those financial statements.
The undersigned registrant hereby undertakes to provide to the
underwriters at the closing specified in the Underwriting
Agreement, certificates in such denominations and registered in
such names as required by the underwriters to permit prompt
delivery to each purchaser.
Insofar as indemnification for liabilities arising under the
Securities Act may be permitted to directors, officers and
controlling persons of the registrant pursuant to the foregoing
provisions, or otherwise, the registrant has been advised that
in the opinion of the Securities and Exchange Commission such
indemnification is against public policy as expressed in the
Securities Act and is, therefore, unenforceable. In the event a
claim for indemnification against such liabilities (other than
the payment by the registrant of expenses incurred or paid by a
director, officer or controlling person of the registrant in the
successful defense of any action, suit or proceeding) is
asserted by such director, officer or controlling person in
connection with the securities being registered, the registrant
will, unless in the opinion of its counsel the matter has been
settled by controlling precedent, submit to a court of
appropriate jurisdiction the question whether such
indemnification by it is against public policy as expressed in
the Securities Act and will be governed by the final
adjudication of such issue.
The undersigned registrant hereby undertakes that:
(1) For purposes of determining any
liability under the Securities Act of 1933, the information
omitted from the form of prospectus filed as part of this
registration statement in reliance upon Rule 430A and
contained in a form of prospectus filed by the registrant
pursuant to Rule 424(b)(1) or (4) or 497(h) under the
Securities Act shall be deemed to be part of this registration
statement as of the time it was declared effective.
(2) For the purpose of determining
any liability under the Securities Act of 1933, each
post-effective amendment that contains a form of prospectus
shall be deemed to be a new registration statement relating to
the securities offered therein, and the offering of such
securities at that time shall be deemed to be the initial bona
fide offering thereof.
Pursuant to the requirements of the Securities Act of 1933, the
registrant has duly caused this Amendment No. 1 to the
Registration Statement to be signed on its behalf by the
undersigned, thereunto duly authorized in the City of New York,
State of New York, on March 14, 2006.
Pursuant to the requirements of the Securities Act of 1933, this
Amendment No. 1 to the Registration Statement has been
signed by the following persons in the capacities and on the
dates indicated.
Exchange Agreement, dated May 20, 2005, by and among QuatRx
Pharmaceuticals Company, Hormos Medical Oy and the shareholders
of Hormos signatories thereto
2
.2**
Escrow Agreement, dated May 25, 2005, by and among QuatRx
Pharmaceuticals Company, Hormos Medical Oy, U.S. Bank
National Association and the shareholders of Hormos signatories
thereto
Form of Amended and Restated Certificate of Incorporation (to be
filed in connection with the closing of this offering and
effective upon the closing of this offering)
3
.6
Form of Amended and Restated Bylaws (to be effective upon the
closing of this offering)
4
.1**
Fourth Amended and Restated Investor Rights Agreement, entered
into as of November 22, 2004, by and among QuatRx
Pharmaceuticals Company. and certain investors named therein
4
.2**
Amendment to Fourth Amended and Restated Investor Rights
Agreement, entered into as of May 25, 2005, by and among
QuatRx Pharmaceuticals Company and certain investors named
therein
4
.3*
Specimen Common Stock Certificate
4
.4**
Warrant to Purchase Shares of the Series D Preferred Stock
of QuatRx Pharmaceuticals Company, dated as of January 26,2006, granted to Hercules Technology Growth Capital, Inc.
5
.1
Form of opinion of Heller Ehrman LLP
10
.1**
Amended and Restated 2005 Stock Incentive Plan
10
.2**
Form of Stock Option Agreement for Employee under Amended and
Restated 2005 Stock Incentive Plan
10
.3**
2000 Equity Incentive Plan
10
.4**
Form of Stock Option Agreement for Employee under 2000 Equity
Incentive Plan
10
.5**
Office Lease between Transwestern Great Lakes, L.P. and QuatRx
Pharmaceuticals Company, dated November 11, 2004
10
.6**
First Amendment to Lease, dated June 30, 2005, by and
between Transwestern Great Lakes REIT, L.P. and QuatRx
Pharmaceuticals Company
10
.7†**
Exclusive License Agreement, dated November 7, 2001, by and
between Deltanoid Pharmaceuticals, Inc. and QuatRx
Pharmaceuticals Company
10
.8†**
Amendment, dated November 8, 2004, to the Exclusive License
Agreement between Deltanoid Pharmaceuticals, Inc. and QuatRx
Pharmaceuticals Company dated November 7, 2001
10
.9†**
Agreement, dated November 9, 2001, by and between Wisconsin
Alumni Research Foundation and QuatRx Pharmaceuticals Company
10
.10†**
Exclusive License Agreement dated February 14, 2005, by and
between EndoChem, Inc. and QuatRx Pharmaceuticals Company
10
.11†**
Letter, dated February 14, 2005, from The Regents of the
University of California to QuatRx Pharmaceuticals Company
10
.12†**
Exclusive License Agreement, dated May 19, 2003, by and
between ILEX Products, Inc. and QuatRx Pharmaceuticals Company
10
.13**
Amendment No. 1, dated September 30, 2004, to
Exclusive License Agreement, dated May 19, 2003, by and
between ILEX Products, Inc. and QuatRx Pharmaceuticals Company
10
.14†**
Patent License Agreement, dated March 25, 2004, by and
between Hormos Medical Oy and Orion Corporation
10
.15†**
Patent License Agreement, dated October 10, 2005, by and
between Hormos Medical Oy and Orion Corporation
10
.16†**
Restated Transfer Agreement, dated May 26, 2005, by and
between Hormos Medical Oy and Tess Diagnostics and
Pharmaceuticals Inc.
Loan and Security Agreement, dated January 26, 2006,
between QuatRx Pharmaceuticals Company and Hercules Technology
Growth Capital, Inc.
10
.21*
Loan Agreements between Tekes and Hormos Medical Oy
10
.22**
Lease Agreement, dated November 29, 2001, between BioTie
Therapies Oyj and Hormos Medical Oy (unofficial translation)
10
.23**
Lease Agreement, dated November 15, 2001, between Turun
Biolaakso Oyj and Hormos Medical Oy (unofficial translation)
10
.24*
Agreement on Development of the Synthesis of FC-1271a and
Manufacturing Option, dated May 1, 1999, by and between
Hormos Medical Oy, Tess Diagnostics and Pharmaceuticals, Inc.
and Orion Corporation Fermion
Indicates a management contract or compensatory plan.
†
Application has been made to the Securities and Exchange
Commission to seek confidential treatment of certain provisions
of this exhibit under Rule 406 of the Securities Act of
1933. Omitted material for which confidential treatment has been
requested has been filed separately with the Securities and
Exchange Commission.
Dates Referenced Herein and Documents Incorporated by Reference