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Literature DB >> 16669643

Acquisition of a "Group A"-selective Src kinase inhibitor via a global targeting strategy.

Jung-Mi Hah¹, Vyas Sharma, Haishan Li, David S Lawrence.

Abstract

A "global" strategy for the acquisition of selective high affinity inhibitors for the Src kinase subfamily of tyrosine kinases is described. Members of the Src family exhibit a strong amino acid sequence homology. However, recent studies have revealed differences in the relative spatial relationships of the three distinct protein-binding domains present in these enzymes. We have constructed an inhibitor, using an amalgamation of combinatorial methods and directed design, which simultaneously associates with the active site and an ancillary protein-binding region (SH2 domain). The inhibitor exhibits high inhibitory potency and selectivity for the Group A versus Group B subset of Src kinases.

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Year: 2006 PMID： 16669643 PMCID： PMC2527056 DOI： 10.1021/ja060136i

Source DB: PubMed Journal: J Am Chem Soc ISSN： 0002-7863 Impact factor: 15.419

11 in total

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Authors: See-Hyoung Park; Jonghwa Won; Keun-Hyeung Lee
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Review 7. The chemical biology of protein phosphorylation.

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8. Light-mediated liberation of enzymatic activity: "small molecule" caged protein equivalents.

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9. Chemical Modification of Phage-Displayed Helix-Loop-Helix Peptides to Construct Kinase-Focused Libraries.

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10. SH2-catalytic domain linker heterogeneity influences allosteric coupling across the SFK family.

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