通过全局靶向策略获得一种“A组”选择性Src激酶抑制剂。
Acquisition of a "Group A"-selective Src kinase inhibitor via a global targeting strategy.
作者信息
Hah Jung-Mi, Sharma Vyas, Li Haishan, Lawrence David S
机构信息
Department of Biochemistry, The Albert Einstein College of Medicine of Yeshiva University, 1300 Morris Park Avenue, Bronx, New York 10461, USA.
出版信息
J Am Chem Soc. 2006 May 10;128(18):5996-7. doi: 10.1021/ja060136i.
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.
摘要
本文描述了一种用于获取酪氨酸激酶Src激酶亚家族选择性高亲和力抑制剂的“全局”策略。Src家族成员表现出很强的氨基酸序列同源性。然而,最近的研究揭示了这些酶中存在的三个不同蛋白质结合结构域的相对空间关系存在差异。我们利用组合方法和定向设计相结合构建了一种抑制剂,它能同时与活性位点和一个辅助蛋白质结合区域(SH2结构域)结合。该抑制剂对Src激酶的A组与B组亚型表现出高抑制效力和选择性。
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