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首页> 外文期刊>International Journal of Modern Physics, C. Physics and Computers >New method of evaluating relative thermal stabilities of proteins based on their amino acid sequences; Targetstar
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New method of evaluating relative thermal stabilities of proteins based on their amino acid sequences; Targetstar

机译:基于蛋白质氨基酸序列评估蛋白质相对热稳定性的新方法;目标之星

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摘要

Several computational methods have been developed to solve the problem of protein thermostabilization. One common drawback of them is that they must have the information of a backbone structure of a protein for the generation of a proper amino acid sequence. In this paper, we propose a new method called TargetStar by incorporating computational biology and statistical physics, in which an approximate partition function and a specific heat are used to calculate the folding transition temperature of a protein and then to predict the relative thermal stabilities for given proteins based only on their amino acid sequences. To evaluate the prediction accuracy of TargetStar, we calculated folding transition temperatures of 289 orthologous protein pairs using the proposed method, where each protein pair contains one hyperthermophilic protein and one mesophilic protein. According to our evaluation, hyperthermophilic and mesophilic proteins are distinguished from each other in terms of relative thermal stabilities with 77% prediction accuracy. Thus, TargetStar may serve as an efficient method to design an amino acid sequence of a target protein with the desired thermal stability prior to the expensive and time-consuming mutagenesis experiment.
机译:已经开发了几种计算方法来解决蛋白质热稳定化的问题。它们的一个普遍缺点是它们必须具有蛋白质的骨架结构的信息才能产生适当的氨基酸序列。在本文中,我们通过结合计算生物学和统计物理学提出了一种称为TargetStar的新方法,其中使用近似分配函数和比热来计算蛋白质的折叠转变温度,然后预测给定条件下的相对热稳定性。蛋白质仅基于其氨基酸序列。为了评估TargetStar的预测准确性,我们使用提出的方法计算了289个直系同源蛋白质对的折叠转变温度,其中每个蛋白质对都包含一个超嗜热蛋白和一个嗜温蛋白。根据我们的评估,嗜热蛋白和嗜温蛋白在相对热稳定性方面彼此区分,预测精度为77%。因此,在昂贵且费时的诱变实验之前,TargetStar可以用作设计具有所需热稳定性的靶蛋白氨基酸序列的有效方法。

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