蛋白质与进化保守界面信息的对接

I. Hashmi, Bahar Akbal-Delibas, Nurit Haspel, Amarda Shehu
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引用次数: 10

摘要

分子组装的结构建模是理解分子相互作用和生物功能的核心。我们提出了一种对接蛋白质分子和阐明蛋白质二聚体的天然样结构的方法。该方法基于几何哈希,保证了二聚体结构组合构象空间搜索的可行性。通过将寻找的刚体转换集中在具有进化保守氨基酸的表面区域周围,可以缩小搜索空间。最近对蛋白质组装的分析表明,许多功能界面在整个进化过程中都是显着保守的。我们在16种不同蛋白质二聚体的广泛列表上测试了我们的方法,并将发现的具有最低lRMSD的结构与已知的天然二聚体结构与其他小组报道的结构进行了比较。我们的研究结果表明,围绕进化保守的界面进行搜索可以降低lrmsd。
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Protein docking with information on evolutionary conserved interfaces
Structural modeling of molecular assemblies lies at the heart of understanding molecular interactions and biological function. We present a method for docking protein molecules and elucidating native-like structures of protein dimers. Our method is based on geometric hashing to ensure the feasibility of searching the combined conformational space of dimeric structures. The search space is narrowed by focusing the sought rigid-body transformations around surface areas with evolutionary-conserved amino-acids. Recent analysis of protein assemblies reveals that many functional interfaces are significantly conserved throughout evolution. We test our method on a broad list of sixteen diverse protein dimers and compare the structures found to have lowest lRMSD to the known native dimeric structures to those reported by other groups. Our results show that focusing the search around evolutionary-conserved interfaces results in lower lRMSDs.
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