标题:
柔性多肽片段–蛋白质相互作用的全局对接方法Global Docking Method for Flexible Peptide Segment-Protein Interactions
作者:
来瑞颖, 万波, 黄强
关键字:
多肽–蛋白质相互作用, 多肽结合位点, 分子对接Protein-Peptide Interaction, Peptide-Binding Site, Molecular Docking
期刊名称:
《Hans Journal of Computational Biology》, Vol.4 No.2, 2014-06-24
摘要:
多肽–蛋白质的相互作用在生物细胞中发挥着各种各样重要的作用。通常情况下,它们之间的结合信息是未知的。所以,利用计算方法预测结合位点具有重要意义。而以Rosetta为代表的常用对接软件通常具有很强的初始位置依赖性。为克服这一局限性,本研究提出了一种全局对接的方法,以受体蛋白为球状系统的中心,将多肽平均地分布在球面26个位置上;同时定义了一个区分天然结合构象和非天然结合构象的筛选参数。用上述方法预测多肽–蛋白质的结合构象,结果显示该方法能成功预测蛋白质的结合位点,且多数多肽的预测构象的Cα-RMSD在5.5 Å以下。因此,研究结果表明,所发展的方法在蛋白质多肽结合位点预测方面有很好的应用价值。
Protein-peptide
binding plays various important roles in living cells. In many cases, the
peptide- binding sites of proteins are not known in prior. Then, computational
prediction of the peptide- binding sites is
desirable. Popular programs for protein-peptide docking usually depend strongly
on the initial positions of peptides, such as Rosetta. To overcome this
limitation, here we develop a global docking approach in which the peptide is
initially distributed evenly on 26 surface locations of a virtual sphere around
the protein, and define a selection parameter for discriminating native-like
binding site from non-native sites. We used this approach to predict the
native-like binding conformations of peptide-protein complexes, and in most
cases the peptide-binding sites were correctly predicted, with Cα-RMSDs
below 5.5 Å with respect to the crystal structures of peptides. The results of
this study suggested that our approach may be very useful for the
identification of peptide-binding sites of proteins.