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Drugs tested for Lou Gehrig's disease. (Biomedicine).


Two drugs better known for treating other diseases may also help people afflicted with amyotrophic lateral sclerosis amyotrophic lateral sclerosis (ALS) (ā'mīətrōf`ik, sklĭrō`sĭs) or motor neuron disease,  (ALS Als (äls), Ger. Alsen, island, 121 sq mi (313 sq km), Sønderjylland co., S Denmark, in the Lille Bælt, separated from the mainland by the narrow Alensund. ), the fatal neuromuscular illness also called Lou Gehrig's disease Lou Geh·rig's disease
n.
See amyotrophic lateral sclerosis.
.

One of the drugs is tamoxifen tamoxifen (təmŏk`sĭfĕn'), synthetic hormone used in the treatment of breast cancer. Introduced in 1978, tamoxifen is used to prevent recurrences of cancer in women who have already undergone surgery to remove their tumors. , which is often prescribed to women with breast cancer. Benjamin Brooks of the University of Wisconsin-Madison “University of Wisconsin” redirects here. For other uses, see University of Wisconsin (disambiguation).
A public, land-grant institution, UW-Madison offers a wide spectrum of liberal arts studies, professional programs, and student activities.
 and his colleagues became curious about the drug when they noticed that a patient with ALS, who was also receiving tamoxifen for breast cancer, maintained her muscle strength over a period of 4 years.

"Her course of ALS was much less severe than we had expected," says Brooks.

He then learned of a study showing that tamoxifen protects nerve cells from a chemical called glutamate glutamate /glu·ta·mate/ (gloo´tah-mat) a salt of glutamic acid; in biochemistry, the term is often used interchangeably with glutamic acid.

glu·ta·mate
n.
1. A salt of glutamic acid.
, which can over-stimulate the cells to the point of killing them. Since glutamate overstimulation of muscle-controlling nerve cells occurs in ALS, Brooks decided to test tamoxifen on mice. He and his colleagues infected the animals with a virus that causes ALS-like symptoms; the rodents typically would develop movement problems about 28 days after infection and then die about a week later.

Tamoxifen treatment delayed the onset of symptoms by 8 days and prolonged the animals' survival by 2 weeks, says Brooks. The investigators have just started a trial of the drug in ALS patients to see if it preserves their muscle strength.

The second potential ALS treatment is celecoxib, the arthritis drug marketed under the name Celebrex. This compound targets an enzyme called COX-2 that drives inflammation in the body. There's evidence that inflammation plays a role in the nerve cell death seen in ALS, so Jeffrey Rothstein of Johns Hopkins University Johns Hopkins University, mainly at Baltimore, Md. Johns Hopkins in 1867 had a group of his associates incorporated as the trustees of a university and a hospital, endowing each with $3.5 million. Daniel C.  in Baltimore and his colleagues tested celecoxib on mice genetically engineered to develop a form of the disease.

"Treatment with the COX-2 inhibitor increased survival by up to 4 weeks," says Rothstein. Riluzole, the only drug approved for ALS patients by the Food and Drug Administration, extends the lifespan of such mice by only 2 weeks, he notes.

Encouraged by the animal results, Rothstein and his colleagues have launched a trial of celecoxib in about 350 ALS patients. --J.T.
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Copyright 2001, Gale Group. All rights reserved. Gale Group is a Thomson Corporation Company.

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Title Annotation:tamoxifen, celecoxib
Publication:Science News
Article Type:Brief Article
Geographic Code:1USA
Date:Dec 8, 2001
Words:346
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