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首页> 外文期刊>Journal of Bioinformatics and Computational Biology >An evolutionary conservation-based method for refining and reranking protein complex structures
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An evolutionary conservation-based method for refining and reranking protein complex structures

机译:一种基于进化保守性的精制和复杂蛋白质复合物结构的方法

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Detection of protein complexes and their structures is crucial for understanding their role in the basic biology of organisms. Computational docking methods can provide researchers with a good starting point for the analysis of protein complexes. However, these methods are often not accurate and their results need to be further refined to improve interface packing. In this paper, we introduce a refinement method that incorporates evolutionary information into a novel scoring function by employing Evolutionary Trace (ET)-based scores. Our method also takes Van der Waals interactions into account to avoid atomic clashes in refined structures. We tested our method on docked candidates of eight protein complexes and the results suggest that the proposed scoring function helps bias the search toward complexes with native interactions. We show a strong correlation between evolutionary-conserved residues and correct interface packing. Our refinement method is able to produce structures with better lRMSD (least RMSD) with respect to the known complexes and lower energies than initial docked structures. It also helps to filter out false-positive complexes generated by docking methods, by detecting little or no conserved residues on false interfaces. We believe this method is a step toward better ranking and prediction of protein complexes.
机译:蛋白质复合物及其结构的检测对于理解其在生物基本生物学中的作用至关重要。计算对接方法可以为研究人员提供分析蛋白质复合物的良好起点。但是,这些方法通常不准确,需要进一步完善其结果以改善界面填充。在本文中,我们介绍了一种细化方法,该方法通过使用基于进化跟踪(ET)的分数将进化信息整合到一种新颖的评分功能中。我们的方法还考虑了范德华相互作用,以避免精炼结构中发生原子碰撞。我们在八个蛋白质复合物的对接候选物上测试了我们的方法,结果表明,建议的评分功能有助于将搜索偏向具有天然相互作用的复合物。我们显示了进化保守残基和正确的界面堆积之间的强烈关联。与已知的配合物相比,我们的改进方法能够生产出具有更好的lRMSD(最低RMSD)的结构,并且能量要低于初始对接结构。通过检测错误接口上很少或没有保守残基,它还有助于滤除对接方法产生的错误阳性复合物。我们相信这种方法是朝着更好地对蛋白质复合物进行排名和预测的一步。

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