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Topic Name: The New Era of Treating endometrial cancer patients
Category: Genetic Engineering
Research persons: Dr. Paul Goodfellow,Dr. Pamela Pollock
Location: 445 N. Fifth Street,Phoenix, AZ 85004, United States
Details
Researchers at the Translational Genomics Research Institute (TGen) today
announced a new approach to treating endometrial cancer patients that not only
stops the growth of tumors, but kills the cancer cells.
In a potentially major breakthrough, TGen scientists and collaborators at
Washington University School of Medicine in St. Louis discovered that
introducing a particular inhibitor drug can turn "off'' receptors responsible
for the growth of tumors in a significant number of patients with endometrial
cancer.
And, they found that the inhibitor drug proved effective even in cancer
tumors containing a commonly occurring mutant gene, PTEN, previously associated
with resistance to drug treatment.
TGen's findings appear today in a paper published as a priority report by
Cancer Research, a Philadelphia-based peer-reviewed journal dedicated to
original cancer research.
A clinical trial based on the TGen study will start within the next year.
Dr. Pamela Pollock, an associate investigator in TGen's Cancer and Cell
Biology Division and the paper's senior author, led a team that used the latest
genome-scanning technology to sequence 116 endometrioid endometrial tumor
samples. This work was done in association with Dr. Paul Goodfellow, an expert
in endometrial cancer and a professor in the departments of Surgery and of
Obstetrics and Gynecology at Washington University.
Pollock and colleagues in May 2007 announced that they had discovered
previously unrecognized alterations in the fibroblast growth factor receptor 2
(FGFR2) gene. The altered FGFR2 is present in the cancer cells of nearly 15
percent of women with
endometrioid endometrial tumors. These kinds of tumors represent 80 percent
of all endometrial cancers.
By introducing a commercially available inhibitor drug, PD173074, TGen
researchers showed that they could stop the growth of tumors, and even kill
cancer cells, in cases where the tumors contained the altered FGFR2 gene. The
altered gene causes the receptors to get stuck in the "on'' position and signal
the endometrial cells to grow out of control.
"These findings could accelerate the development of new treatments for
endometrial cancer because there are already drugs in clinical trials that
inhibit FGFR2 function,'' Pollock said.
Current treatment of endometrial cancer can involve surgical removal of the
uterus, radiation and chemotherapy. While many women are successfully treated
with these approaches, about 15 percent of those with endometrioid endometrial
cancer have persistent or recurring tumors that are resistant to current drug
therapies. Mutations in several genes previously have been identified in
endometrial tumors, but they have not been suitable drug targets – until now.
"This targeted approach holds great promise for patients with uterine cancer
(endometrioid endometrial) tumors that contain the FGFR2 mutation," said TGen
physician-in-chief, Dr. Daniel Von Hoff, "and offers yet another powerful
example of how genomic medicine is changing the way we look at and treat
cancer."
Goodfellow agreed, "The discovery that endometrial cancer cells die when
treated with an FGFR2 inhibitor - even when they carry other genetic
abnormalities common in uterine cancers - suggests anti-FGFR2 therapies have
great potential.''
The researchers' already established ties with the National Cancer Institute,
which will assist with the clinical trials, should speed the development of new
therapies, Goodfellow said. "Our collaborative group's strong ties with the
NCI's Gynecologic Oncology Group will allow us to rapidly take our findings from
the lab to patients.''
Endometrial cancer, which invades the inner wall of the uterus, is the most
common gynecological cancer in the United States. This year more than 40,000
women will be diagnosed and nearly 7,500 women will die of the disease,
according to the American Cancer Society (ACS).
Among women, only breast, lung and colon cancers strike with more frequency.
And while endometrial cancer is slow to develop, and often is not detected until
after age 60, nearly one in eight women who are diagnosed die within five years,
according to the ACS.
Pollock plans to start clinical trials with an FGFR inhibitor in endometrial
cancer patients within a year. The trials will be conducted in collaboration
with Dr. Matthew Powell, a gynecologic oncologist and assistant professor of
Obstetrics and Gynecology at Washington University School of Medicine.
Targeted drug therapy is a relatively new approach to cancer treatment that
is based on identifying the abnormalities in cancer cells that cause them to
grow uncontrollably. It involves treating tumors with drugs that specifically
inhibit the activity of these genetic abnormalities.
This approach of targeted therapy allows oncologists to match the therapy to
the specific genetic signature of each patient's tumor, a strategy that has been
effective in multiple cancer types, including breast cancer, lung cancer and
chronic myelogenous leukemia.
Researchers:
Dr. Paul
Goodfellow
Dr. Pamela
Pollock
About the Research center:
A comprehensive listing of TCRS clinical trials can be found at
www.tgen.org. Click on Research, Clinical
Research and then Clinical Trials.
The study was funded, in part, by a two-year, $100,000 ($50,000 per year)
grant from the Cary, N.C.-based, V Foundation for Cancer Research. The
foundation is named in remembrance of famed North Carolina State basketball
coach and award-winning broadcaster Jimmy Valvano, a cancer research advocate
who died of Metastatic Adenocarcinoma in 1993.
About TGen
The Translational Genomics Research Institute (TGen) is a non-profit
organization dedicated to conducting groundbreaking research with life changing
results. Research at TGen is focused on helping patients with diseases such as
cancer, neurological disorders and diabetes. TGen is on the cutting edge of
translational research where investigators are able to unravel the genetic
components of common and complex diseases. Working with collaborators in the
scientific and medical communities, TGen believes it can make a substantial
contribution to the efficiency and effectiveness of the translational process.
For more information, visit: www.tgen.org.
About Washington University School of Medicine
Washington University School of Medicine's 2,100 employed and volunteer
faculty physicians also are the medical staff of Barnes-Jewish and St. Louis
Children's hospitals. The School of Medicine is one of the leading medical
research, teaching and patient care institutions in the nation, currently ranked
third in the nation by U.S. News & World Report. Through its affiliations with
Barnes-Jewish and St. Louis Children's hospitals, the School of Medicine is
linked to BJC HealthCare. Visit:
medschool.wustl.edu.
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