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Cleaning up glutamate slows deadly brain tumors.


A protein that removes excessive amount of the amino acid 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.
 from around nerve cells may protect a brain from tumors, according to two studies. Researchers could soon test whether drugs that increase production of this glutamate-sweeping protein stop otherwise-fatal cases of brain cancer.

Glutamate is essential to the healthy brain. It's one of the many compounds that nerve cells use to signal each other. Over the past few years, cancer researchers have discovered that many brain tumors, particularly ones called gliomas, secrete massive amounts of the amino acid. The tumors seem to wield glutamate as a machete of sorts, carving out room for growth by using the molecule to stimulate nerve cells until they die (SN: 9/1/01, p. 133).

The healthy brain uses the protein called excitatory ex·ci·ta·tive   or ex·ci·ta·to·ry
adj.
Causing or tending to cause excitation.

Adj. 1. excitatory - (of drugs e.g.
 amino acid transporter 2 (EAAT EAAT excitatory amino acid transporter
EAAT Escadrille Avions de l'Armee de Terre
2) to mop us excess glutamate outside nerve cells. In previous studies, researchers at George Washington University George Washington University, at Washington, D.C.; coeducational; chartered 1821 as Columbian College (one of the first nonsectarian colleges), opened 1822, became a university in 1873, renamed 1904.  in Washington, D.C., genetically engineered mice to overproduce o·ver·pro·duce  
tr.v. o·ver·pro·duced, o·ver·pro·duc·ing, o·ver·pro·duc·es
To produce in excess of need or demand.



o
 EAAT2. The scientists recently injected glioma glioma /gli·o·ma/ (gli-o´mah) a tumor composed of neuroglia in any of its states of development; sometimes extended to include all intrinsic neoplasms of the brain and spinal cord, as astrocytomas, ependymomas, etc.  cells into the brains of these mutant mice and found that the resulting tumors grew more slowly than they would have in the brains of typical mice.

Moreover, the mutant mice were slower to start experiencing seizures caused by their brain tumors and suffered less nerve cell death around the tumors than normal mice do, says Jamie L. Maguire, now at the University of California, Los Angeles UCLA comprises the College of Letters and Science (the primary undergraduate college), seven professional schools, and five professional Health Science schools. Since 2001, UCLA has enrolled over 33,000 total students, and that number is steadily rising. .

Kaleb H. Yohay of Johns Hopkins Medical Institutions in Baltimore recently surveyed the amount of EAAT2 in glioma samples from 60 patients. "There seems to be less of this major glutamate transporter in the higher-grade, more-invasive tumors," he says. Having less EAAT2 may prolong the time that glutamate from a glioma can kill nerve cells, he suggests.

As part of an effort to identify new treatments for a wide range of brain diseases, Yohay's colleague Jeffrey D. Rothstein recently screened more than 1,000 existing drugs, looking for ones that increase EAAT2 production. As it turned out, some common antibiotics do the trick. Given that there is no consistently effective treatment for gliomas, physicians will probably be eager to test such EAAT2 boosters on people with the tumors.--J.T.
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Title Annotation:Cancer
Publication:Science News
Date:Nov 29, 2003
Words:363
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