Predicting ligand binding residues using multi-positional correlations and kernel canonical correlation analysis

Alvaro J. González, Li Liao, Cathy H. Wu
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引用次数: 5

Abstract

We present a new computational method for predicting ligand binding sites in protein sequences. The method uses kernelbased canonical correlation analysis and linear regression to identify binding sites in protein sequences as the residues that exhibit strong correlation between the residues' evolutionary characterization at the sites and the structure based functional classification of the proteins in the context of a functional family. We explore the effect of correlations among multiple positions in the sequences and show that their inclusion enhances the prediction accuracy significantly.
利用多位置相关和核典型相关分析预测配体结合残基
我们提出了一种新的预测蛋白质序列中配体结合位点的计算方法。该方法使用基于核的典型相关分析和线性回归来识别蛋白质序列中的结合位点作为残基,这些残基在这些位点上的进化特征与蛋白质在功能家族中的基于结构的功能分类之间表现出很强的相关性。我们探索了序列中多个位置之间的相关性的影响,并表明它们的包含显著提高了预测精度。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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