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Predicting protein interaction sites: binding hot-spots in protein-protein and protein-ligand interfaces

机译:预测蛋白质相互作用位点:结合蛋白质-蛋白质和蛋白质-配体界面中的热点

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摘要

Motivation: Protein assemblies are currently poorly represented in structural databases and their structural elucidation is a key goal in biology. Here we analyse clefts in protein surfaces, likely to correspond to binding 'hot-spots', and rank them according to sequence conservation and simple measures of physical properties including hydrophobicity, desolvation, electrostatic and van der Waals potentials, to predict which are involved in binding in the native complex.
机译:动机:目前,蛋白质装配体在结构数据库中的表现不佳,其结构解析是生物学的主要目标。在这里,我们分析了可能与结合的“热点”相对应的蛋白质表面中的裂口,并根据序列保守性和物理性质(包括疏水性,去溶剂化性,静电和范德华势)的简单测量对它们进行了排序,以预测涉及哪些绑定在本机复合体中。

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