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首页> 外文期刊>Computational and Structural Biotechnology Journal >Bioinformatic analysis of subfamily-specific regions in 3D-structures of homologs to study functional diversity and conformational plasticity in protein superfamilies
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Bioinformatic analysis of subfamily-specific regions in 3D-structures of homologs to study functional diversity and conformational plasticity in protein superfamilies

机译:同源物三种结构中亚家谱地区的生物信息分析,研究蛋白质超小心功能多样性和构象可塑性

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Local 3D-structural differences in homologous proteins contribute to functional diversity observed in a superfamily, but so far received little attention as bioinformatic analysis was usually carried out at the level of amino acid sequences. We have developed Zebra3D – the first-of-its-kind bioinformatic software for systematic analysis of 3D-alignments of protein families using machine learning. The new tool identifies subfamily-specific regions (SSRs) – patterns of local 3D-structure (i.e. single residues, loops, or secondary structure fragments) that are spatially equivalent within families/subfamilies, but are different among them, and thus can be associated with functional diversity and function-related conformational plasticity. Bioinformatic analysis of protein superfamilies by Zebra3D can be used to study 3D-determinants of catalytic activity and specific accommodation of ligands, help to prepare focused libraries for directed evolution or assist development of chimeric enzymes with novel properties by exchange of equivalent regions between homologs, and to characterize plasticity in binding sites. A companion Mustguseal web-server is available to automatically construct a 3D-alignment of functionally diverse proteins, thus reducing the minimal input required to operate Zebra3D to a single PDB code. The Zebra3D? ?Mustguseal combined approach provides the opportunity to systematically explore the value of SSRs in superfamilies and to use this information for protein design and drug discovery. The software is available open-access at https://biokinet.belozersky.msu.ru/Zebra3D .
机译:同源蛋白的局部3D结构差异有助于在超家族中观察到的功能多样性,但到目前为止,由于生物信息分析通常在氨基酸序列的水平下进行,因此迄今为止。我们开发了Zebra3d - 一种使用机器学习对蛋白质家庭的3D对齐系统分析的一类生物信息软件。新工具标识特定于基本的地区(SSR) - 本地3D结构的模式(即单个残基,循环或二级结构片段),其在家庭/亚属中,但在它们之间是不同的,因此可以关联具有功能分集和功能相关的构象可塑性。 Zebra3D的蛋白质超小心的生物信息分析可用于研究催化活性和特定配体的特定容纳的3D确定性,帮助编制聚焦文库,用于通过交换同源物之间的等效区域的新特性进行聚焦的演化或有助于开发嵌合酶在结合遗址中表征可塑性。可以使用伴随的Mustguseal Web-Server自动构建功能各种蛋白的3D对齐,从而减少了将Zebra3D运行到单个PDB代码所需的最小输入。 Zebra3d? ?Mustguseal联合方法提供了系统地探索Superfilies中SSR的价值,并使用这些信息进行蛋白质设计和药物发现。该软件可在https://biokinet.belozersky.msu.ru/zebra3d中获得开放式访问。

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