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On the Upper Bound of the Prediction Accuracy of Residue Contacts in Proteins with Correlated Mutations: The Case Study of the Similarity Matrices

机译:具有相关突变的蛋白质中残基接触的预测准确性的上限:相似矩阵的案例研究

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Correlated mutations in proteins are believed to occur in order to preserve the protein functional folding through evolution. Their values can be deduced from sequence and/or structural alignments and are indicative of residue contacts in the protein three-dimensional structure. A correlation among pairs of residues is routinely evaluated with the Pearson correlation coefficient and the MCLACHLAN similarity matrix. In this paper, we describe an optimization procedure that maximizes the correlation between the Pearson coefficient and the protein residue contacts with respect to different similarity matrices, including random. Our results indicate that there is a large number of equivalent matrices that perform similarly to MCLACHLAN. We also obtain that the upper limit to the accuracy achievable in the prediction of the protein residue contacts is independent of the optimized similarity matrix. This suggests that poor scoring may be due to the choice of the linear correlation function in evaluating correlated mutations.
机译:据信发生蛋白质中的相关突变是为了通过进化保留蛋白质功能性折叠。它们的值可以从序列和/或结构比对推导,并指示蛋白质三维结构中的残基接触。通常使用Pearson相关系数和MCLACHLAN相似度矩阵评估残基对之间的相关性。在本文中,我们描述了一种优化程序,该程序针对不同的相似性矩阵(包括随机性)最大化了Pearson系数和蛋白质残基接触之间的相关性。我们的结果表明,存在与MCLACHLAN相似的大量等效矩阵。我们还获得了蛋白质残基接触预测中可达到的准确度上限,与优化的相似度矩阵无关。这表明评分不佳可能是由于在评估相关突变时选择了线性相关函数。

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