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基于模板的蛋白质结构建模软件程序的系统和比较评估。

Systematic and Comparative Evaluation of Software Programs for Template-Based Modeling of Protein Structures.

机构信息

Metabolic and Biomolecular Engineering National Research Laboratory, Department of Chemical and Biomolecular Engineering (BK21 Plus Program), KAIST Institute for BioCentury, Korea Advanced Institute of Science and Technology (KAIST), Daejeon, 34141, Republic of Korea.

Systems Biology and Medicine Laboratory, Department of Chemical and Biomolecular Engineering (BK21 Plus Program), Korea Advanced Institute of Science and Technology (KAIST), Daejeon, 34141, Republic of Korea.

出版信息

Biotechnol J. 2020 Jun;15(6):e1900343. doi: 10.1002/biot.201900343. Epub 2020 Mar 18.

Abstract

Modeling protein structures is critical for understanding protein functions in various biological and biotechnological studies. Among representative protein structure modeling approaches, template-based modeling (TBM) is by far the most reliable and most widely used approach to model protein structures. However, it still remains as a challenge to select appropriate software programs for pairwise alignments and model building, two major steps of the TBM. In this paper, pairwise alignment methods for TBM are first compared with respect to the quality of structure models built using these methods. This comparative study is conducted using comprehensive datasets, which cover 6185 domain sequences from Structural Classification of Proteins extended for soluble proteins, and 259 Protein Data Bank entries (whole protein sequences) from Orientations of Proteins in Membranes database for membrane proteins. Overall, a profile-based method, especially PSI-BLAST, consistently shows high performance across the datasets and model evaluation metrics used. Next, use of two model building programs, MODELLER and SWISS-MODEL, does not seem to significantly affect the quality of protein structure models built except for the Hard group (a group of relatively less homologous proteins) of membrane proteins. The results presented in this study will be useful for more accurate implementation of TBM.

摘要

建模蛋白质结构对于理解各种生物和生物技术研究中的蛋白质功能至关重要。在代表性的蛋白质结构建模方法中,基于模板的建模(TBM)是迄今为止最可靠和最广泛使用的蛋白质结构建模方法。然而,选择合适的软件程序用于 TBM 的两个主要步骤,即成对比对和模型构建,仍然是一个挑战。在本文中,首先根据使用这些方法构建的结构模型的质量来比较 TBM 的成对比对方法。这项比较研究使用了综合数据集进行,这些数据集涵盖了来自可溶性蛋白质扩展结构分类的 6185 个结构域序列,以及来自膜蛋白Orientations of Proteins in Membranes 数据库的 259 个蛋白质数据库条目(整个蛋白质序列)。总体而言,基于轮廓的方法,特别是 PSI-BLAST,在使用的数据集和模型评估指标方面始终表现出良好的性能。接下来,除非是膜蛋白的 Hard 组(一组相对同源性较低的蛋白质),否则使用两个模型构建程序 MODELLER 和 SWISS-MODEL 似乎不会显著影响蛋白质结构模型的质量。本研究的结果将有助于更准确地实施 TBM。

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