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Cancer drugs may thwart Huntington's. (Biomedicine).


Drugs developed to fight cancer could also be effective against Huntington's disease Huntington's disease, hereditary, acute disturbance of the central nervous system usually beginning in middle age and characterized by involuntary muscular movements and progressive intellectual deterioration; formerly called Huntington's chorea.  and several related neurodegenerative conditions, according to a new study of flies.

These brain illnesses are known as polygutamine disorders because in each, a mutated gene translates into proteins with an overabundance o·ver·a·bun·dance  
n.
A going or being beyond what is needed, desired, or appropriate; an excess: teenagers with an overabundance of energy.
 of the amino acid amino acid (əmē`nō), any one of a class of simple organic compounds containing carbon, hydrogen, oxygen, nitrogen, and in certain cases sulfur. These compounds are the building blocks of proteins.  glutamine glutamine (gl`təmēn), organic compound, one of the 20 amino acids commonly found in animal proteins.  (SN: 6/10/95, p. 360). Seeking to explain how different proteins cause these brain disorders, scientists have searched for molecules whose functions might be altered by glutamine-rich proteins.

This molecular hunt is turning up suspects. Earlier this year, for example, a group reported that Htt, the mutant protein encoded by the Huntington's disease gene, binds to a protein called CBP CBP

competitive protein binding.
 (SN: 4/28/01, p. 271).

CBP is an acetyltransferase, an enzyme that directly regulates DNA DNA: see nucleic acid.
DNA
 or deoxyribonucleic acid

One of two types of nucleic acid (the other is RNA); a complex organic compound found in all living cells and many viruses. It is the chemical substance of genes.
 and the genes it contains. Neuroscientist Leslie M. Thompson of the University of California The University of California has a combined student body of more than 191,000 students, over 1,340,000 living alumni, and a combined systemwide and campus endowment of just over $7.3 billion (8th largest in the United States). , Irvine and her colleagues have now found that Htt not only binds to CBP and other acetyltransferases, but also prevents these enzymes from doing their normal gene-orchestrating jobs.

Cancer researchers already have developed drugs that inhibit enzymes that undo the actions of acetyltransferases. Thompson's group theorized that such drugs, called HDAC inhibitors, also might counteract the gene disruptions caused by glutamineladen proteins. To test that idea, the researchers fed HDAC inhibitors to fruit flies genetically engineered to make Htt. In the Oct. 18 NATURE, the group reports that the treatment delays the brain-cell loss and death that normally strike the mutant insects.

Thomson's group and several other research teams already have started to test the drugs on mice genetically engineered to have a rodent version of Huntington's disease. "Depending on what these studies show, there may be human clinical trials," says Thompson. Citing other groups' published and unpublished work, she's optimistic that HDAC inhibitors also will become candidates for treating polyglutamine disorders other than Huntington's disease.

--J. T.
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Title Annotation:Huntington's disease and other neurodegenerative diseases may be affected by glutamine-rich proteins
Publication:Science News
Article Type:Brief Article
Date:Nov 24, 2001
Words:308
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