March 3, 1999. Nearly 90 percent of prostate cancers  "the
typical, garden varieties," according to Johns Hopkins scientists
 are linked to a common genetic process that could be reversible. Previously
unsuspected, this process appears to be fundamental in cancer and is
found in other common forms of the disease, like breast cancer.
Unlike cancers due to mutations that make
structural changes in a gene, such as the colon cancers that run in
families, most prostate cancer may involve a process called "gene
switching," the researchers say. Switching occurs when certain
members of a family of genes are switched on while others in the family
shut down. "It's a process common during embryonic development,"
says molecular pathologist Shrihari S. Kadkol, M.D., Ph.D., one of the
researchers in a study March 1, 1999 Nature Medicine, "but
we believe this is the first time anyone's definitively linked gene
switching within a family of genes, with cancer."
"Most
important is that someday, it's likely we can reverse switching with
drugs," says Gary R. Pasternack, M.D., Ph.D., molecular pathologist,
who led the Hopkins research team. "This means one of the commonest
cancers in men has the potential of being corrected without using typical
gene therapy.".
The scientists used molecular probes to
highlight and compare the gene activity in cancer patients' normal prostate
tissue with that of their tumors. They found clear evidence that a gene
called pp32 was switched on in normal cells but generally switched off
in cancer cells. Earlier studies by the team showed pp32 acts as a suppressor
and keeps cells from turning malignant.
Yet close relatives of the gene, to the
researchers' surprise, act like pp32's genetic evil twins and encourage
tumor growth. The pp32r1 and pp32r2 genes are present and turned on
in perhaps 90 percent of the prostate cancers the team studied.
"We first thought pp32 had just mutated,"
says Kadkol, "but the types of differences between it and the variant
genes told us this wasn't the case." The researchers say switching
could be a fundamental process in cancer, and they've already linked
it with common forms of breast cancer. "In the breast cancer patients
we've examined," says Kadkol, "we saw this same pp32 switching
pattern."
"If we can understand how the switching
process works, what controls it," adds Pasternack, "we can
potentially reverse it. That's our next task." If their work goes
smoothly, he adds, they could screen and find drugs for this purpose
within two years. Then the candidate investigational drug would undergo
the usual FDA-sponsored tests in people.
"We also believe this work may have
a role in diagnosis or in predicting disease outcome," says Pasternack.
"Prostate specific antigen (PSA), the present common screen for
prostate cancer, doesn't always tell the complete story or, particularly
in older men, doesn't let us make a clear prognosis. This might help."
The prognostic studies are already underway as part of a congressionally-sponsored
project with the Army to speed select basic research into clinical applications.
The reported study was funded by a grant from the National Cancer Institute.
A patent is pending on the technology involved in the study. Other researchers
are Jonathan R. Brody, Jining Bai, Ph.D., and Jonathan Pevsner, Ph.D.
Input from science writer Marjorie Centofanti.
Related Web sites: http://pathology.jhu.edu/research_programs
(choose Molecular Pathology) or click here
March 3, 1999
PSA
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