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Using rigidity analysis to probe mutation-induced structural changes in proteins

机译:使用刚度分析来探究突变引起的蛋白质结构变化

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Predicting the effect of a single amino acid substitution on the stability of a protein structure is a fundamental task in macromolecular modeling. It has relevance to drug design and understanding of disease-causing protein variants. We present KINARI-Mutagen, a web server for performing in silico mutation experiments on protein structures from the Protein Data Bank. Our rigidity-theoretical approach permits fast evaluation of the effects of mutations that may not be easy to perform in vitro, because it is not always possible to express a protein with a specific amino acid substitution. We use KINARI-Mutagen to identify critical residues, and we show that our predictions correlate with destabilizing mutations to glycine. In two in-depth case studies we show that the mutated residues identified by KINARI-Mutagen as critical correlate with experimental data, and would not have been identified by other methods such as Solvent Accessible Surface Area measurements or residue ranking by contributions to stabilizing interactions. We also generate 48 mutants for 14 proteins, and compare our rigidity-based results against experimental mutation stability data. KINARI-Mutagen is available at http://kinari.cs.umass.edu.
机译:预测单个氨基酸取代对蛋白质结构稳定性的影响是大分子建模的基本任务。它与药物设计和对引起疾病的蛋白质变异的理解有关。我们介绍KINARI-Mutagen,这是一个网络服务器,用于对来自蛋白质数据库的蛋白质结构进行计算机突变实验。我们的刚性理论方法可以快速评估可能不易在体外进行的突变的影响,因为不一定总是可以表达具有特定氨基酸取代的蛋白质。我们使用KINARI-Mutagen识别关键残基,并且我们表明我们的预测与甘氨酸失稳突变相关。在两个深入的案例研究中,我们表明KINARI-Mutagen鉴定为突变残基与实验数据具有关键相关性,其他方法(例如溶剂可及表面积测量或通过对稳定化相互作用的贡献进行残基排序)则无法鉴定。我们还为14种蛋白质生成了48个突变体,并将基于刚度的结果与实验突变稳定性数据进行了比较。 KINARI-Mutagen可从http://kinari.cs.umass.edu获得。

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