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GEM: A Gaussian evolutionary method for predicting protein side-chain conformations

机译:GEM:一种预测蛋白质侧链构象的高斯进化方法

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摘要

We have developed an evolutionary approach to predicting protein side-chain conformations. This approach, referred to as the Gaussian Evolutionary Method (GEM), combines both discrete and continuous global search mechanisms. The former helps speed up convergence by reducing the size of rotamer space, whereas the latter, integrating decreasing-based Gaussian mutations and self-adaptive Gaussian mutations, continuously adapts dihedrals to optimal conformations. We tested our approach on 38 proteins ranging in size from 46 to 325 residues and showed that the results were comparable to those using other methods. The average accuracies of our predictions were 80% for χ1, 66% for χ1 + 2, and 1.36 Å for the root mean square deviation of side-chain positions. We found that if our scoring function was perfect, the prediction accuracy was also essentially perfect. However, perfect prediction could not be achieved if only a discrete search mechanism was applied. These results suggest that GEM is robust and can be used to examine the factors limiting the accuracy of protein side-chain prediction methods. Furthermore, it can be used to systematically evaluate and thus improve scoring functions.
机译:我们已经开发了一种预测蛋白质侧链构象的进化方法。这种称为高斯进化方法(GEM)的方法结合了离散和连续的全局搜索机制。前者通过减小旋转异构体空间的大小来帮助加快收敛速度​​,而后者则结合了基于递减的高斯变异和自适应高斯变异,使二面体不断适应最佳构象。我们对38种蛋白质的方法进行了测试,这些蛋白质的大小从46到325个残基不等,结果表明该结果与使用其他方法的结果相当。我们预测的平均准确度对于χ1为80%,对于χ1+ 2为66%,对于侧链位置的均方根偏差为1.36Å。我们发现,如果我们的评分功能是完美的,则预测准确性也基本上是完美的。但是,如果仅应用离散搜索机制,则无法实现完美的预测。这些结果表明,GEM是可靠的,可用于检查限制蛋白质侧链预测方法准确性的因素。此外,它可以用于系统地评估,从而改善评分功能。

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