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Yale Cancer Center Sponsors Study of Phenoxodiol for Prostate Cancer
Researchers Seek to Build on Previous Study Indicating Investigational Drug Phenoxodiol Prolonged Time to Progression and PSA Doubling Time
| Quelle: Marshall Edwards, Inc.
NEW HAVEN, CT--(Marketwire - October 22, 2007) - Yale researchers have begun recruiting 60 men
for a clinical trial investigating an experimental new drug, oral
phenoxodiol, as a potential first line therapy for prostate cancer. The
study is funded by Yale Cancer Center.
The clinical trial will be conducted at two sites, Yale Cancer Center and
the West Haven (Conn.) Veterans Administration Hospital. Yale Cancer
Center, a National Cancer Institute designated comprehensive cancer center
for over 30 years, is one of only 39 Centers in the nation and the only
comprehensive center in Southern New England.
"Promising data on phenoxodiol in prostate cancer piqued our interest,"
said Wm. Kevin Kelly, D.O., principle investigator for the trial, Associate
Professor of Medicine and Associate Director of Clinical Investigations,
Yale Cancer Center. "This trial builds on the success of the previous
prostate cancer trial with phenoxodiol. We will compare results from two
types of prostate cancer patients -- those with androgen independent
disease and those with androgen dependent disease."
"If successful, development of phenoxodiol has the potential to provide a
significant advancement in the treatment of prostate cancer," said Dr.
Kelly.
About the Study
All patients in the trial will receive 400 mg of oral phenoxodiol every 8
hours daily for 28 consecutive days (1 cycle). Treatment outcome will be
evaluated after three cycles (12 weeks) of drug administration. Patients
with progression of disease will be taken off study. Responding and stable
disease patients will remain on study until disease progression or for a
maximum of 12 cycles (approximately 12 months).
The primary endpoint of the trial is to determine the proportion of
patients given phenoxodiol that have a 50 percent post-therapy prostate
specific antigen (PSA) decline at 12 weeks in patients with:
a) Androgen independent disease who are chemotherapy naïve (Group A); and
b) Rising PSA after radical prostatectomy or radiotherapy that are
androgen dependent (Group B)
The study will also evaluate safety of phenoxodiol in these patient
populations. PSA is a protein produced by the cells of the prostate gland.
PSA is present in small quantities in the serum of normal men, and is often
elevated in the presence of prostate cancer and in other prostate
disorders.
Selection Criteria
The study is open to prostate cancer patients of any race and ethnicity who
are at least 18 years of age. All patients have to show evidence of disease
progression and have adequate hematologic, renal and hepatic function.
Patients must not have had surgery in the 4 weeks prior to the trial.
A total of 60 eligible patients will be enrolled. The study calls for
enrolling 25 eligible subjects into Group A and 35 eligible subjects into
Group B.
A study coordinator will help patients interested in the trial to learn if
they are eligible, as other selection criteria apply. Interested patients
should contact Elin Rowen, RN, Yale Cancer Center, (203) 737-2445,
elin.rowen@yale.edu.
Earlier Study Indicates Phenoxodiol Delays Disease Progression
A Phase II clinical research study demonstrated a dose dependent anti-tumor
effect by phenoxodiol in men with hormone refractory prostate cancer. The
trial was designed to end after 24 weeks of treatment, but was extended to
90 weeks because of the unexpected prolongation of time to progression in
some patients. No phenoxodiol-associated toxicities were reported in the
study.
Researchers administered oral phenoxodiol to 26 patients at one of four
dose levels, two subtherapeutic levels (20 mg and 80 mg three times daily)
and two therapeutic levels (200 mg and 400 mg three times daily). Response
to therapy was determined on the basis of PSA response, PSA doubling time,
and time to progression.
While all 12 patients on the two lower dose levels of phenoxodiol showed
disease progression within 6 months, nine (9) of the 14 patients on the
higher doses of phenoxodiol remained progression-free on phenoxodiol after
6 months, indicating that disease progression occurred far more frequently
in the lower subtherapeutic dose treatment group. In terms of PSA levels,
the 12 patients in the two lower dose groups saw no improvement, while 3 of
the 14 patients in the higher dose groups experienced a PSA level reduction
of 50 percent or greater from baseline. The PSA doubling time increased
from a mean of 18 weeks to 43 weeks, not including the 3 of 14 patients who
remained on phenoxodiol beyond the term of the study.
This study was lead by Robert Davis, MD, Sir Charles Gairdner Hospital,
Perth, Australia, and was presented at the AACR-NCI-EORTC International
Conference on Molecular Targets and Cancer Therapeutics, Philadelphia,
November 17, 2005.
About Prostate Cancer
According to the National Cancer Institute, prostate cancer is the second
most common type of cancer among men in this country and the second leading
cause of cancer death among men in the U.S.(1) Only lung cancer is more
common and kills more men. Prostate cancer will be diagnosed in more than
230,000 men in 2006, and approximately 28,000 men will die of the
disease.(2) At least forty percent of all men diagnosed with prostate
cancer will at some point experience recurrent disease after definitive
local therapy with radiation or prostatectomy. Most commonly, recurrence
is manifested as a rising PSA and/or the development of metastatic
disease.(3)
Treatment options for early stage prostate cancer in androgen dependent
pre-metastatic disease are limited. Patient options typically include
"watchful waiting" or anti-androgen treatment, a form of chemical
castration that is particularly unattractive for men who at this stage of
disease are otherwise healthy.
About Phenoxodiol
Phenoxodiol is being developed by Marshall Edwards, Inc. as a therapy for
late-stage, chemoresistant ovarian cancer and for prostate and cervical
cancers. It is a novel-acting drug that inhibits key pro-survival
signaling pathways operating via sphingosine-1-phosphate and Akt.
Inhibition of these pathways leads to prevention of phosphorylation of key
anti-apoptotic proteins such as XIAP. Loss of activity of these proteins
induces cell death by apoptosis and restores the sensitivity of
chemoresistant tumor cells to other chemotherapy drugs. The putative
molecular target for phenoxodiol is a cancer-specific protein, accounting
for the highly selective nature of the drug.
This helps explain the findings that phenoxodiol has been shown not to
adversely affect normal cells in animal and laboratory testing.
Phenoxodiol has received Fast Track status from the FDA to facilitate
development as a therapy for recurrent ovarian and prostate cancers.
Phenoxodiol is an investigational drug and, as such, is not commercially
available. Under U.S. law, a new drug cannot be marketed until it has been
investigated in clinical trials and approved by FDA as being safe and
effective for the intended use.
Phase III Multinational Trial for Ovarian Cancer Patients Underway
Phenoxodiol in combination with carboplatin is currently being studied in a
multinational Phase III clinical trial called the OVATURE (OVArian TUmor
Response) Trial, following positive findings of previous trials conducted
in Australia and at Yale-New Haven Hospital. The OVATURE trial is taking
place at up to 60 clinical sites in the United States, Europe, and
Australia. Preliminary results from the trial are expected within 18
months. For more information on the trial, visit www.OVATUREtrial.com.
About Marshall Edwards, Inc.
Marshall Edwards, Inc. (NASDAQ : MSHL ) is majority owned by Novogen (NASDAQ : NVGN ), an Australian biotechnology company that is specializing in the
development of therapeutics based on a flavonoid technology platform.
Novogen, based in Sydney, Australia, is developing a range of therapeutics
across the fields of oncology, cardiovascular disease and inflammatory
diseases. More information on phenoxodiol and on the Novogen group of
companies can be found at http://www.marshalledwardsinc.com and
http://www.novogen.com.
Under U.S. law, a new drug cannot be marketed until it has been
investigated in clinical trials and approved by the FDA as being safe and
effective for the intended use. Statements included in this press release
that are not historical in nature are "forward-looking statements" within
the meaning of the "safe harbor" provisions of the Private Securities
Litigation Reform Act of 1995. You should be aware that our actual results
could differ materially from those contained in the forward-looking
statements, which are based on management's current expectations and are
subject to a number of risks and uncertainties, including, but not limited
to, our failure to successfully commercialize our product candidates; costs
and delays in the development and/or FDA approval, or the failure to obtain
such approval, of our product candidates; uncertainties in clinical trial
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of any revisions to these forward-looking statements.
(1) Ries LAG, Melbert D, Krapcho M, Mariotto A, Miller BA, Feuer EJ, Clegg
L, Horner MJ, Howlader N, Eisner MP, Reichman M, Edwards BK (eds). SEER
Cancer Statistics Review, 1975-2004, National Cancer Institute. Bethesda,
MD, http://seer.cancer.gov/csr/1975_2004/, based on November 2006 SEER data
submission, posted to the SEER web site, 2007.
(2) Jemal A, Siegel R, Ward E, et al: Cancer statistics, 2006. CA Cancer J
Clin 56:106-30, 2006.
(3) Moul JW, Ward JF: Management of the patient with a rising PSA alone.
Hematol Oncol Clin North Am 20:897-908, 2006.