BALTIMORE, Nov 03, 2009 (ASCRIBE NEWS via COMTEX) -- Men with lower cholesterol
are less likely than those with higher levels to develop high-grade prostate
cancer - an aggressive form of the disease with a poorer prognosis, according to
results of a Johns Hopkins collaborative study. In a prospective study of more
than 5,000 U.S. men, epidemiologists say they now have evidence that having
lower levels of heart-clogging fat may cut a man's risk of this form of cancer
by nearly 60 percent.
"For many reasons, we know that it's good to have a cholesterol level within the
normal range," says Elizabeth Platz, Sc.D., M.P.H., associate professor at the
Johns Hopkins Bloomberg School of Public Health and co-director of the cancer
prevention and control program at the Johns Hopkins Kimmel Cancer Center. "Now,
we have more evidence that among the benefits of low cholesterol may be a lower
risk for potentially deadly prostate cancers."
Normal range is defined as less than 200 mg/dL (milligrams per deciliter of
blood) of total cholesterol.
Platz and her colleagues found similar results in a study first published in
2008, and in 2006, she linked use of cholesterol-lowering statin drugs to lower
risk of advanced prostate cancer.
For the current study, Platz, members of the Southwest Oncology Group, and other
collaborators analyzed data from 5,586 men aged 55 and older enrolled in the
Prostate Cancer Prevention Trial from 1993 to 1996. Some 1,251 men were
diagnosed with prostate cancer during the study period.
Men with cholesterol levels lower than 200 mg/dL had a 59 percent lower risk of
developing high-grade prostate cancers, which tend to grow and spread rapidly.
High-grade cancers are identified by a pathological ranking called the Gleason
score. Scores at the highest end of the scale, between eight and 10, indicate
cancers considered the most worrisome to pathologists who examine samples of the
diseased prostate under the microscope.
In Platz's study, cholesterol levels had no significant effect on the entire
spectrum of prostate cancer incidence, only those that were high-grade, she
says.
Platz cautions that, while the group took into account factors that could bias
the results, such as smoking history, weight, family history of prostate cancer,
and dietary cholesterol, other things could have affected their results. One
example is whether men in the study were taking cholesterol-lowering drugs at
the time of the blood collections, a data point the researchers expect to
analyze soon.
Results of the current study are expected to be published online Nov. 3 in the
journal Cancer Epidemiology, Biomarkers & Prevention. Also in the journal is an
accompanying paper from the National Cancer Institute showing that lower
cholesterol in men conferred a 15 percent decrease in overall cancer cases.
"Cholesterol may affect cancer cells at a level where it influences key
signaling pathways controlling cell survival," says Platz. "Cancer cells use
these survival pathways to evade the normal cycle of cell life and death."
She says that targeting cholesterol metabolism may be one route to treating and
preventing the disease, but this remains to be tested.
Funding for the study was provided by the National Cancer Institute.
Authors of the study include Cathee Till, Phyllis J. Goodman, Marian L.
Neuhouser and Alan R. Kristal from the Fred Hutchinson Cancer Research Center;
Howard L. Parnes, William D. Figg, and Demetrius Albanes from the National
Cancer Institute; Eric A. Klein from the Cleveland Clinic; and Ian M. Thompson
Jr., from the University of Texas Health Sciences Center.
On the Web:
News release on statins and prostate cancer:
http://www.hopkinskimmelcancercenter.org/index.cfm/cID/1684/mpage/item.c
fm/itemID/461
Elizabeth Platz:
http://faculty.jhsph.edu/default.cfm?faculty_id=554&grouped=false&search
Text=&department_id=0&departmentName=Epidemiology
Cancer Epidemiology, Biomarkers & Prevention: http://cebp.aacrjournals.org
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NOTE TO EDITORS: The American Association for Cancer Research will host a press
briefing on this research on Nov. 3, 2009, at 11:30 a.m. ET. Reporters can call
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Access Code: 37083372 Topic: AACR