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Janus: Prediction and ranking of mutations required for functional interconversion of enzymes

机译:Janus:酶功能互变所需的突变的预测和排名

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摘要

Identification of residues responsible for functional specificity in enzymes is a challenging and important problem in protein chemistry. Active-site residues are generally easy to identify, but residues outside the active site are also important to catalysis and their identities and roles are more difficult to determine. We report a method based on analysis of multiple sequence alignments, embodied in our program Janus, for predicting mutations required to interconvert structurally related but functionally distinct enzymes. Conversion of aspartate aminotransferase into tyrosine aminotransferase is demonstrated and compared to previous efforts. Incorporation of 35 predicted mutations resulted in an enzyme with the desired substrate specificity but low catalytic activity. A single round of DNA back-shuffling with wild-type aspartate aminotransferase on this variant generated mutants with tyrosine aminotransferase activities better than those previously realized from rational design or directed evolution. Methods such as this, coupled with computational modeling, may prove invaluable in furthering our understanding of enzyme catalysis and engineering.
机译:鉴定负责酶功能特异性的残基是蛋白质化学中一个具有挑战性和重要的问题。活性位点的残基通常很容易识别,但活性位点以外的残基对催化也很重要,并且其身份和作用更难确定。我们报告了一种基于对多个序列比对的分析的方法,该方法体现在我们的程序Janus中,用于预测相互转化结构相关但功能不同的酶所需的突变。证实了天冬氨酸转氨酶向酪氨酸转氨酶的转化并与以前的努力进行了比较。掺入35个预测的突变产生具有所需底物特异性但催化活性低的酶。在此变体上用野生型天冬氨酸转氨酶进行的单轮DNA反洗改产生的酪氨酸转氨酶活性比先前从合理设计或定向进化中获得的突变体更好。诸如此类的方法,再加上计算模型,对于进一步加深我们对酶催化和工程学的理解可能是无价的。

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