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首页> 外文期刊>Proteins: Structure, Function, and Genetics >Classifying protein kinase structures guides use of ligand-selectivity profiles to predict inactive conformations: structure of lck/imatinib complex.
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Classifying protein kinase structures guides use of ligand-selectivity profiles to predict inactive conformations: structure of lck/imatinib complex.

机译:对蛋白激酶结构进行分类可指导配体选择性谱的使用,以预测非活性构象:lck /伊马替尼复合物的结构。

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摘要

We report a clustering of public human protein kinase structures based on the conformations of two structural elements, the activation segment and the C-helix, revealing three discrete clusters. One cluster includes kinases in catalytically active conformations. Each of the other clusters contains a distinct inactive conformation. Typically, kinases adopt at most one of the inactive conformations in available X-ray structures, implying that one of the conformations is preferred for many kinases. The classification is consistent with selectivity profiles of several well-characterized kinase inhibitors. We show further that inhibitor selectivity profiles guide kinase classification. For example, selective inhibition of lck among src-family kinases by imatinib (Gleevec) suggests that the relative stabilities of inactive conformations of lck are different from other src-family kinases. We report the X-ray structure of the lck/imatinib complex, confirming that the conformation adopted by lck is distinct from other structurally-characterized src-family kinases and instead resembles kinases abl1 and kit in complex with imatinib. Our classification creates new paths for designing small-molecule inhibitors.
机译:我们报告了基于两个结构元素,激活段和C螺旋的构象的公共人类蛋白激酶结构的聚类,揭示了三个离散的群集。一个簇包括具有催化活性构象的激酶。其他每个集群都包含一个独特的非活动构象。通常,激酶在可用的X射线结构中采用至多一种非活性构象,这意味着许多激酶优选一种构象。该分类与几种充分表征的激酶抑制剂的选择性概况一致。我们进一步表明抑制剂选择性概况指导激酶分类。例如,伊马替尼(Gleevec)对src家族激酶中lck的选择性抑制表明,lck失活构象的相对稳定性不同于其他src家族激酶。我们报告了lck /伊马替尼复合物的X射线结构,证实了lck采用的构象与其他结构表征的src家族激酶不同,而是类似于与伊马替尼复合的激酶abl1和试剂盒。我们的分类为设计小分子抑制剂创造了新途径。

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