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Trichostatin A (TSA) may fight lupus and atherosclerosis
simultaneously
12/11/05 - 17/11/05, San Diego, USA
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Highlights of the American College of Rheumatology 70th Annual
Scientific Meeting - Nov. 12-17, San Diego, USA.
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WINSTON-SALEM, N.C.– People with lupus are prone to
premature accelerated atherosclerosis. Now scientists at Wake
Forest University School of Medicine think they have a way to
prevent or decrease this atherosclerosis and prevent heart
attacks.
"Premature accelerated atherosclerosis is one of the leading
causes of death and disability in lupus," said Nilamadhab Mishra,
M.D., a rheumatologist at Wake Forest University Baptist Medical
Center. Using a drug called Trichostatin A (TSA) "may prevent or
decrease premature atherosclerosis in lupus."
Mishra presented his findings today (Nov. 16) at the American
College of Rheumatology meeting in San Diego.
The findings represent a merger of two lines of Mishra's
animal research using TSA – one showing that the drug reduced
lupus symptoms, especially inflammation of the kidneys and
enlarged spleens, and the other showing that TSA was effective
against atherosclerosis.
Mishra was joined in the atherosclerosis research by several
leading scientists in the Medical School's long-standing
atherosclerosis research program.
Their research uses a mouse that was created to be prone to
atherosclerosis when fed a diet high in cholesterol and with 10
percent of calories from palm oil, one of the more dangerous
dietary vegetable fats since it is high in saturated fat.
Among the atherosclerosis researchers were John S. Parks,
Ph.D., professor of comparative medicine, and Richard St. Clair,
Ph.D., professor of pathology and head of the Section on
Comparative Medicine.

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For 12 weeks, the researchers fed a high-fat, high-cholesterol
diet to two groups of the atherosclerosis-prone mice. One group
got injections of TSA from the time they went on the diet, while
the other group got no TSA. The TSA-treated group had markedly
less atherosclerosis in key arteries, such as the aorta – the
body's main blood vessel – and what plaque there was contained
less cholesterol.
Scientists increasingly are viewing the depositing of
cholesterol in the walls of arteries as an inflammatory reaction
that attracts the disease-fighting macrophages, a type of white
blood cell, which then become incorporated with cholesterol
deposits to become plaque. The mice that had the TSA injections
had a reduction in the gathering of macrophages.
Mishra said that TSA may be beneficial because it prevents
certain genes from expressing proteins that are known to be
involved in both lupus and atherosclerosis.
Mishra had reported earlier that TSA showed promise in
treating lupus in a different, lupus-prone mouse model. The
research raises the hope, said Mishra, that "lupus and
atherosclerosis can be treated simultaneously."
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