Pep–Whisperer: Inhibitory peptide design

N. Hurwitz, D. Zaidman, H. Wolfson
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引用次数: 3

Abstract

Designing peptides for protein–protein interaction inhibition is of significant interest in computer‐aided drug design. Such inhibitory peptides could mimic and compete with the binding of the partner protein to the inhibition target. Experimental peptide design is a laborious, time consuming, and expensive multi‐step process. Therefore, in silico peptide design can be beneficial for achieving this task. We present a novel algorithm, Pep–Whisperer, which aims to design inhibitory peptides for protein–protein interaction. The desirable peptides would have a relatively high predicted binding affinity to the target protein in a given protein–protein complex. The algorithm outputs linear peptides which are based on an initial template. The template could either be a peptide which is retrieved from the interaction site, or a patch of nonconsecutive amino acids from the protein–protein interface which is completed to a linear peptide by short polyalanine linkers. In addition, the algorithm takes into consideration the conservation of the amino acids in the ligand‐protein binding site by using evolutionary information for choosing the preferred amino acids in each position of the designed peptide. Our algorithm was able to design peptides with high predicted binding affinity to the target protein. The method is fully automated and available as a web server at http://bioinfo3d.cs.tau.ac.il/PepWhisperer/.
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胡椒耳语者:抑制肽设计
设计蛋白质相互作用抑制肽是计算机辅助药物设计的重要内容。这种抑制肽可以模仿和竞争伴侣蛋白与抑制靶点的结合。实验肽设计是一个费力、耗时和昂贵的多步骤过程。因此,在硅肽设计可以有利于实现这一任务。我们提出了一种新的算法,Pep-Whisperer,旨在设计蛋白质-蛋白质相互作用的抑制肽。在给定的蛋白-蛋白复合物中,期望的肽对目标蛋白具有相对高的预测结合亲和力。该算法输出基于初始模板的线性肽。模板可以是从相互作用位点提取的肽,也可以是由短聚丙氨酸连接物完成的蛋白质-蛋白质界面上的不连续氨基酸片段。此外,该算法还考虑了配体-蛋白结合位点氨基酸的保守性,利用进化信息选择设计肽的每个位置的首选氨基酸。我们的算法能够设计出与目标蛋白具有高预测结合亲和力的肽。该方法是完全自动化的,可作为web服务器访问http://bioinfo3d.cs.tau.ac.il/PepWhisperer/。
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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