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UNITED STATES
SECURITIES AND EXCHANGE COMMISSION
Washington, D.C. 20549
FORM 8-K
CURRENT REPORT
Pursuant to Section 13 or 15(d) of the
Securities Exchange Act of 1934
Date of Report (Date of earliest event reported): January 19, 2011
Ardea Biosciences, Inc.
(Exact name of registrant as specified in its charter)
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| Delaware
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1-33734
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94-3200380 |
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| (State or other jurisdiction
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(Commission
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(IRS Employer |
| of incorporation)
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File Number)
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Identification No.) |
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| 4939 Directors Place
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| San Diego, California
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92121 |
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(Zip Code) |
Registrant’s telephone number, including area code: (858) 652-6500
N/A
(Former name or former address, if changed since last report.)
Check the appropriate box below if the Form 8-K filing is intended to simultaneously satisfy the
filing obligation of the registrant under any of the following provisions:
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Written communications pursuant to Rule 425 under the Securities Act (17 CFR 230.425)
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Soliciting material pursuant to Rule 14a-12 under the Exchange Act (17 CFR 240.14a-12)
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Pre-commencement communications pursuant to Rule 14d-2(b) under the Exchange Act (17 CFR 240.14d-2(b))
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Pre-commencement communications pursuant to Rule 13e-4(c) under the Exchange Act (17 CFR 240.13e-4(c))
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TABLE OF CONTENTS
In this report, “Ardea,” “we,” “us” and “our” refer to Ardea Biosciences, Inc. and its
wholly-owned subsidiary, unless the context otherwise provides.
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| Item 2.02. |
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Results of Operations and Financial Condition. |
On January 19, 2011, we filed with the Securities and Exchange Commission, or SEC, a prospectus
supplement to our Registration Statement on Form S-3 (File No. 333-170105), which included the
following preliminary financial information as of December 31, 2010:
We
estimate that the total amount of our cash, cash equivalents and
short-term investments, available-for-sale as of December 31, 2010 was approximately $80.6 million.
This
amount is preliminary, has not been audited and is subject to change
upon completion of our ongoing audit. Moreover, this amount does not
reflect the $15 million milestone payment we received in January 2011
described in greater detail below. Additional information and
disclosures would be required for a more complete understanding of
our financial position and results of operations as of December 31, 2010.
We are filing the following information with the SEC for the purpose of updating certain aspects of
our publicly disclosed description of our business:
Overview
We are a biotechnology company focused on the development of small-molecule therapeutics for the
treatment of serious diseases. The current status of our development programs is as follows:
Product Portfolio
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| Product Candidate |
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Target Indication |
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Development Status |
RDEA594
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Gout
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Phase 2 completed |
Next-generation URAT 1 inhibitors
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Gout
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Preclinical development ongoing |
BAY 86-9766 (formerly known as RDEA119)
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Cancer
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Phase 2 ongoing |
Gout
Gout is a painful, debilitating and progressive disease. While gout is a treatable condition, there
are limited treatment options, and a number of adverse effects are associated with most current
therapies.
Gout is caused by abnormally elevated levels of uric acid in the blood stream. Drugs currently
used to treat the underlying cause of gout work by lowering blood or serum uric acid (“sUA”)
levels. Approximately 90 percent of gout patients are considered to have a defect in their ability
to excrete sufficient amounts of uric acid and are classified as “under-excreters” of uric acid,
which leads to excessive levels of uric acid in the blood stream. Our most advanced product
candidate, RDEA594, is an inhibitor of URAT1, a transporter in the kidney that regulates uric acid
excretion from the body. RDEA594 normalizes the amount of uric acid excreted by gout patients.
Since the majority of gout patients are “under-excreters”, normalizing uric acid excretion by
moderating URAT1 transporter activity with RDEA594 may provide the most physiologically appropriate
and effective means of reducing blood or sUA levels. In addition, because RDEA594 works by
increasing the excretion of uric acid rather than reducing the body’s production of uric acid, it
can be used in combination with sUA lowering agents that reduce the production of uric acid such as
allopurinol or febuxostat (Uloric®, Takeda Pharmaceutical Company Limited).
Allopurinol is the most commonly prescribed sUA lowering drug in the United States, currently
accounting for greater than 90 percent of U.S. unit sales of sUA lowering drugs. However, in
recent controlled clinical studies, only 30-40 percent of gout patients achieved an adequate
response to allopurinol as defined by the achievement of sUA levels of less than 6 mg/dL, a
commonly used medical target. We are developing RDEA594, both as monotherapy and to be used in
combination with drugs like allopurinol, in order to treat patients not adequately responding to
their current therapy.
To date, results from our RDEA594 Phase 2 development program have indicated RDEA594’s clinical
utility, as follows:
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In a Phase 2b study (Study 203) in 208 allopurinol refractory gout patients,
adding RDEA594 to allopurinol produced highly statistically significant reductions in
sUA of up to 30 percent with up to 89 percent of patients taking the
combination reaching the medically recommended target of reducing sUA to below 6 mg/dL at
the highest dose tested. The combination of RDEA594 and allopurinol was also well
tolerated, with no serious adverse events and only two discontinuations due to adverse
events on RDEA594. Patients admitted to the study had sUA levels greater than or equal
to 6 mg/dL despite being on a stable dose of allopurinol. In this 28-day, randomized,
double-blind, placebo-controlled study, each patient received once daily doses of 200 mg
of RDEA594, 400 mg of RDEA594, 600 mg of RDEA594 or placebo while remaining on the stable
dose of allopurinol such patient was receiving when he or she entered the study. Mean
reductions in sUA after 4 weeks on 200 mg, 400 mg and 600 mg of RDEA594 plus a standard
dose of allopurinol were 16 percent, 22 percent and 30 percent, respectively, compared to
an increase in sUA of 3 percent on placebo. Response rates on this study increased in a
dose-related manner and were highly clinically and statistically significant at all dose
levels when compared to allopurinol alone. Using a “last observation carried forward”
(LOCF) analysis, which was the method utilized for the U.S. approval of
Uloric®, the response rates for the 200 mg, 400 mg and 600 mg plus a standard
dose of allopurinol were 71 percent, 76 percent and 89 percent, respectively, compared to
29 percent on allopurinol alone. |
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In a Phase 1b clinical pharmacology study evaluating the use of RDEA594 in
combination with febuxostat (Study 111) in 21 gout patients with hyperuricemia (sUA
greater than or equal to 8 mg/dL), 100 percent of patients receiving the combination of
RDEA594 and febuxostat achieved sUA levels below the clinically important target level
of 6 mg/dL, compared to 67 percent and 56 percent for patients receiving 40 mg and 80
mg, respectively, of febuxostat alone. At the highest combination doses tested (600 mg
RDEA594 combined with 80 mg febuxostat), 100 percent of patients reached sUA levels
below 4 mg/dL, with 58 percent achieving levels below 3 mg/dL. No patient achieved these
reduced sUA levels on either dose of febuxostat alone. The combination of RDEA594 and
febuxostat was also well tolerated, with no serious adverse events or discontinuations
due to adverse events and no clinically relevant drug interactions observed between
RDEA594 and febuxostat. |
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In a 20-patient Phase 1b clinical pharmacology study evaluating the use of
RDEA594 in combination with 300 mg of allopurinol (Study 110) in gout patients with
hyperuricemia (sUA greater than or equal to 8mg/dL), 100 percent of patients at all
combination doses evaluated achieved sUA levels below the target of 6 mg/dL, compared to
20 percent of patients on allopurinol alone. Of patients receiving RDEA594 600 mg alone,
67 percent achieved sUA levels below 6 mg/dL, which was significantly higher than the
percent reaching target on allopurinol alone (p < 0.05). At the highest combination
doses tested (600 mg of RDEA594 combined with 300 mg of allopurinol), 90 percent of
patients reached sUA levels below 5 mg/dL, and 50 percent reached levels below 4 mg/dL.
The combination of RDEA594 and allopurinol was well tolerated, with no serious adverse
events or discontinuations that were considered possibly related to RDEA594 or the
combination. No clinically relevant drug interactions were observed between RDEA594 and
allopurinol in this study; however, plasma levels of oxypurinol, an active metabolite of
allopurinol, were decreased approximately 25-35 percent. |
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When administered as a single agent in a Phase 2b study (Study 202), RDEA594
was well tolerated and produced significant reductions in uric acid in the blood. In
this randomized, double-blind, placebo-controlled, dose-escalation study of 123 gout
patients with hyperuricemia (sUA levels greater than or equal to 8 mg/dL) the primary
endpoint was a significant increase in the proportion of patients who achieved a
response, defined as a reduction of uric acid in the blood to < 6 mg/dL after four
weeks of treatment, compared to placebo. The primary endpoint was achieved, uric acid
decreased and response rates increased in a dose-related manner and were highly
clinically and statistically significant at the two highest doses tested. At the
highest dose the response rate was 60 percent, compared to 0 percent for placebo (p <
0.0001). RDEA594 was also well tolerated in this study, with no serious adverse events
and only two discontinuations due to adverse events on RDEA594. |
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Results from multiple studies have indicated that the activity of RDEA594 is
not diminished in patients with mild renal impairment. A smaller dataset from Study 202
indicate that after 4 weeks of monotherapy with RDEA594, patients with moderate renal
impairment had similar reductions in sUA as compared to patients with no renal
impairment. |
We are also developing next-generation inhibitors of the URAT1 transporter for the treatment of
gout patients with hyperuricemia. Based on preclinical results, our next-generation inhibitors
demonstrate many of the same positive attributes as RDEA594, but with greater potency against the
URAT1 transporter. Preclinical development activities with respect to these next-generation product
candidates are ongoing.
Cancer
Mitogen-activated ERK kinase (“MEK”) is believed to play an important role in cancer cell
proliferation, apoptosis and metastasis. BAY 86-9766 (formerly known as RDEA119) is a potent and
selective inhibitor of MEK in development for the treatment of cancer. In vivo preclinical tests
have shown BAY 86-9766 to have potent anti-tumor activity. In addition, preclinical in vitro and
in vivo studies of BAY 86-9766 have demonstrated synergistic activity across multiple tumor types
when BAY 86-9766 is used in combination with other anti-cancer agents, including sorafenib
(Nexavar®, Bayer HealthCare AG (“Bayer”) and Onyx Pharmaceuticals, Inc.).
In April 2009, we entered into a global license agreement with Bayer to develop and commercialize
MEK inhibitors for the treatment of cancer. Under the license agreement, we are responsible for the
completion of the Phase 1 and Phase 1/2 studies. Thereafter, Bayer will be responsible for the
further development and commercialization of BAY 86-9766 and any of our other MEK inhibitors.
We have completed our Phase 1 study of BAY 86-9766 as a single agent in advanced cancer patients
with different tumor types and we have identified the maximum tolerated dose (“MTD”) of BAY 86-9766
in our Phase 1/2 study in combination with sorafenib. Dosing in the MTD expansion cohort of the
Phase 1/2 study is ongoing.
Phase 1 results to date in refractory patients with advanced solid tumors have demonstrated that
BAY 86-9766 is well tolerated with a number of patients achieving stable disease or partial
response to treatment. Based on the preclinical and Phase 1/2 results, Bayer recently initiated a
Phase 2 study of BAY 86-9766 in combination with sorafenib as first-line therapy for primary liver cancer.
Market Opportunity
We believe that there is a significant market opportunity for our products, should they be
successfully developed, approved and commercialized.
We believe that there is a significant need for new products for the treatment and prevention of
gout. There have been only two new products approved in the United States for the treatment of
gout in the last 40 years. According to the Decision Resources, an estimated 19.7 million adults
in the seven major markets (the United States, Japan, France, Germany, Italy, Spain and United
Kingdom) suffer from gout. The incidence and severity of gout is increasing in the United States.
According to the Annals of Rheumatic Diseases, there was a 288% increase in gout-related
hospitalizations from 1988-2005 and over $11.2 billion in gout-related hospital costs were incurred
in 2005 in the United States. Many chronic gout sufferers are unable to achieve target reductions
in uric acid with current treatments. Scientists have recently discovered defects in multiple
transporters in the kidney that play important roles in uric acid transport and are genetically
linked to a higher risk of gout. URAT1 has been identified as the most important transporter for
uric acid. We are developing products for the treatment of hyperuricemia and gout that inhibit
URAT1, thereby increasing the excretion of uric acid and lowering serum uric acid levels. In
addition, we believe there may be opportunities to develop uric acid-lowering agents to treat
diseases other than gout. Evidence suggests that the chronic elevation of uric acid associated
with gout, known as hyperuricemia, may also have systemic consequences, including an increased risk
for kidney dysfunction, elevated C-reactive protein, hypertension and possibly other cardiovascular risk factors.
We also believe that there is growing interest in the potential for targeted therapies, including
kinase inhibitors, for the treatment of both cancer and inflammatory disease. Sales of products
used in the treatment of cancer were $52.4 billion in 2009 according to IMS Health Incorporated,
fueled by strong acceptance of innovative and effective targeted therapies. In addition to treatment of cancer,
MEK appears to play a role in inflammatory diseases and we believe that BAY 86-9766 and our next
generation MEK inhibitors, if successfully developed, approved and commercialized, could
participate in these growing markets.
Bayer Relationship
Under the terms of our license agreement with Bayer, we granted to Bayer a worldwide, exclusive
license to develop and commercialize our MEK inhibitors for all indications. In June 2009, Bayer
paid us a non-refundable, upfront cash payment of $35 million in partial consideration for the
exclusive right to develop and commercialize our MEK inhibitors. In January 2011, we received a
$15 million milestone payment from Bayer triggered by the initiation of a Phase 2 study evaluating
BAY 86-9766 in combination with sorafenib.
Potential payments under the license agreement with Bayer could total up to $407 million, not
including royalties. This amount includes the upfront cash payment and the $15 million milestone
payment we received in January 2011, as well as additional cash payments upon achievement of
certain development, regulatory and sales-based milestones. We are also eligible to receive low
double-digit royalties on sales of products under the license agreement.
Valeant Relationship
In December 2006, we acquired intellectual property and other assets from Valeant Research &
Development, Inc. (“Valeant”) related to RDEA806 and our next generation non-nucleoside reverse
transcriptase inhibitor (“NNRTI”) program, as well as BAY 86-9766 and our next generation MEK inhibitor
program. In consideration for the assets purchased from Valeant and subject to the satisfaction of
certain conditions, Valeant received certain rights, including the right to receive from us
development-based milestone payments and sales-based royalty payments. There is one set of
potential milestones totaling up to $25 million for RDEA806 and the next generation NNRTI program,
and a separate set of potential milestones totaling up to $17 million for BAY 86-9766 and the next
generation MEK inhibitor program. The first milestone payment of $2 million in the NNRTI program
would be due after the first patient is dosed in the first Phase 2b study. The first milestone
payment of $1 million in the MEK inhibitor program was paid to
Valeant in January 2011 in connection with the initiation of a Phase 2 study relating to BAY 86-9766. The royalty
rates on all products under our agreement with Valeant are in the mid-single digits.
Forward-Looking Statements
Statements contained in this report regarding matters that are not historical facts are
“forward-looking statements” within the meaning of the Private Securities Litigation Reform Act of
1995. Because such statements are subject to risks and uncertainties, actual results may differ
materially from those expressed or implied by such forward-looking statements. Such statements
include, but are not limited to, statements regarding the safety and efficacy of our product
candidates; our expectations regarding the ability to utilize our
product candidates in combination with existing sUA lowering agents;
the progress, timing and results of clinical trials and research and development
efforts involving our product candidates; our plans to conduct future clinical trials or research and
development efforts; estimates of the potential markets for our product candidates; our operating
and growth strategies, industry and planned products; and our estimated
cash, cash equivalents and short-term investments, available for
sale. Risks that
contribute to the uncertain nature of the forward-looking statements include, among others, risks
related to the outcome of preclinical and clinical studies, risks related to regulatory approvals,
delays in commencement of preclinical and clinical studies, costs associated with our drug
discovery and development programs, risks related to the outcome of our business development
activities, including collaboration or license agreements, and risks
related to changes in estimated financial amounts based on the
completion of our ongoing audit. These and other risks and uncertainties
are described more fully under the headings “Risk Factors” in our most recently filed SEC
documents, including our Annual Report on Form 10-K and our Quarterly Reports on Form 10-Q. All
forward-looking statements contained in this report speak only as of the date on which they were
made. Ardea undertakes no obligation to update such statements to reflect events that occur or
circumstances that exist after the date on which they were made.
SIGNATURE
Pursuant to the requirements of the Securities Exchange Act of 1934, the Registrant has
duly caused this report to be signed on its behalf by the undersigned thereunto duly authorized.
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ARDEA BIOSCIENCES, INC.
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| Date: January 19, 2011 |
/s/ Christian Waage
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Christian Waage |
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General Counsel |
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