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. 2011 Dec 20;50(50):10764-70.
doi: 10.1021/bi201613d. Epub 2011 Nov 18.

Full-length human glutaminase in complex with an allosteric inhibitor

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Full-length human glutaminase in complex with an allosteric inhibitor

Byron DeLaBarre et al. Biochemistry. .

Abstract

Glutaminase (GLS1/2) catalyzes the conversion of L-glutamine to L-glutamate and ammonia. The level of a splice variant of GLS1 (GAC) is elevated in certain cancers, and GAC is specifically inhibited by bis-2-(5-phenylacetimido-1,2,4,thiadiazol-2-yl)ethyl sulfide (BPTES). We report here the first full-length crystal structure of GAC in the presence and absence of BPTES molecules. Two BPTES molecules bind at an interface region of the GAC tetramer in a manner that appears to lock the GAC tetramer into a nonproductive conformation. The importance of these loops with regard to overall enzymatic activity of the tetramer was revealed by a series of GAC point mutants designed to create a BPTES resistant GAC.

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