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Feature-similarity protein classifier as a ligand engineering tool

机译:特征相似蛋白分类器作为配体工程工具

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hKinases have been often targeted in drug therapy aimed at blocking signaling pathways. However, the conservation of protein structure across homologs often leads to uncontrolled cross-reactivity. On the other hand, sticky packing defects in proteins are typically not conserved across homologs, making them ligand-anchoring sites potentially important to enhance selectivity. Thus, we introduce a hierarchical clustering of PDB-reported kinases according to packing differences. This kinome partitioning is highly correlated with proximity relations arising from the pharmacological profiling of kinases. A variable packing sensitivity is observed for individual drugs, with highly promiscuous ligands being the most insensitive to packing differences. Our classifier enables a strategy to design selective inhibitors. (c) 2006 Elsevier B.V. All rights reserved.
机译:h激酶在药物治疗中经常被靶向以阻断信号传导途径。然而,跨同源物的蛋白质结构的保守性经常导致不受控制的交叉反应性。另一方面,蛋白质中的粘性堆积缺陷通常在同源物中并不保守,这使它们成为配体固定位点,可能对提高选择性具有重要意义。因此,我们根据装箱差异引入了PDB报告的激酶的分级聚类。这种激酶组分配与激酶的药理学谱分析所产生的邻近关系高度相关。对于单个药物,观察到了不同的堆积敏感性,其中高度混杂的配体对堆积差异最不敏感。我们的分类器使设计选择性抑制剂的策略成为可能。 (c)2006 Elsevier B.V.保留所有权利。

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