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Structure Based Functional Analysis of Bacteriophage f1 Gene V Protein

机译:噬菌体f1基因V蛋白的基于结构的功能分析

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摘要

A computational mutagenesis methodology utilizing a four-body, knowledge-based, statistical contact potential is applied toward globally quantifying relative structural changes (residual scores) in bacteriophage f1 gene V protein (GVP) due to single amino acid residue substitutions. We show that these residual scores correlate well with experimentally measured relative changes in protein function caused by the mutations. For each mutant, the approach also yields local measures of environmental perturbation occurring at every residue position (residual profile) in the protein. Implementation of the random forest algorithm, utilizing experimental GVP mutants whose feature vector components include environmental changes at the mutated position and at six nearest neighbors, correctly classifies mutants based on function with up to 72% accuracy while achieving 0.77 area under the receiver operating characteristic curve and a 0.42 correlation coefficient. An optimally trained random forest model is subsequently used to infer function for all remaining unexplored GVP mutants.
机译:利用四体,基于知识的统计接触电势的计算诱变方法应用于全局量化由于单个氨基酸残基取代而导致的噬菌体f1基因V蛋白(GVP)的相对结构变化(残值)。我们表明,这些残留分数与突变引起的蛋白功能的实验测量相对变化具有很好的相关性。对于每个突变体,该方法还产生了在蛋白质中每个残基位置(残基图)上发生的环境扰动的局部量度。利用实验性GVP突变体实现随机森林算法,该GVP突变体的特征向量成分包括突变位置和六个最近邻点的环境变化,可以根据功能正确分类突变体,准确度高达72%,同时在接收器工作特性曲线下达到0.77面积相关系数为0.42。随后,使用经过最佳训练的随机森林模型来推断所有其余未开发的GVP突变体的功能。

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