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Modeling regionalized volumetric differences in protein-ligand binding cavities

机译:模拟蛋白质-配体结合腔中的区域体积差异

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摘要

Identifying elements of protein structures that create differences in protein-ligand binding specificity is an essential method for explaining the molecular mechanisms underlying preferential binding. In some cases, influential mechanisms can be visually identified by experts in structural biology, but subtler mechanisms, whose significance may only be apparent from the analysis of many structures, are harder to find. To assist this process, we present a geometric algorithm and two statistical models for identifying significant structural differences in protein-ligand binding cavities. We demonstrate these methods in an analysis of sequentially nonredundant structural representatives of the canonical serine proteases and the enolase superfamily. Here, we observed that statistically significant structural variations identified experimentally established determinants of specificity. We also observed that an analysis of individual regions inside cavities can reveal areas where small differences in shape can correspond to differences in specificity.
机译:鉴定在蛋白质-配体结合特异性上产生差异的蛋白质结构元件是解释优先结合基础分子机制的基本方法。在某些情况下,结构生物学的专家可以从视觉上识别出影响机制,但是很难找到微妙的机制,其重要性只有从许多结构的分析中才能显现出来。为了协助这一过程,我们提出了一种几何算法和两个统计模型,用于识别蛋白质-配体结合腔中的显着结构差异。我们在规范的丝氨酸蛋白酶和烯醇酶超家族的顺序非冗余结构代表分析中证明了这些方法。在这里,我们观察到统计学上显着的结构变异确定了实验确定的特异性决定因素。我们还观察到,对腔体内各个区域的分析可以揭示出形状上的细微差异可以对应于特异性差异的区域。

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