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All repeats are not equal: A module-based approach to guide repeat protein design

机译:所有重复均不相等:指导重复蛋白设计的基于模块的方法

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Repeat proteins composed of tandem arrays of a short structural motif often mediate protein-protein interactions. Past efforts to design repeat protein-based molecular recognition tools have focused on the creation of templates from the consensus of individual repeats, regardless of their natural context. Such an approach assumes that all repeats are essentially equivalent. In this study, we present the results of a "module-based" approach in which modules composed of tandem repeats are aligned to identify repeat-specific features. Using this approach to analyze tetratricopeptide repeat modules that contain three tandem repeats (3TPRs), we identify two classes of 3TPR modules with distinct structural signatures that are correlated with different sets of functional residues. Our analyses also reveal a high degree of correlation between positions across the entire ligand-binding surface, indicative of a coordinated, coevolving binding surface. Extension of our analyses to different repeat protein modules reveals more examples of repeat-specific features, especially in armadillo repeat modules. In summary, the module-based analyses that we present effectively capture key repeat-specific features that will be important to include in future repeat protein design templates.
机译:重复由较短结构基序的串联阵列组成的蛋白质通常介导蛋白质与蛋白质的相互作用。过去基于重复蛋白质的分子识别工具设计工作的重点是从单个重复的共识中创建模板,而不管其自然背景如何。这样的方法假定所有重复基本上都是相同的。在这项研究中,我们提出了一种“基于模块”方法的结果,在该方法中,由串联重复序列组成的模块被对齐以识别特定于重复序列的特征。使用此方法来分析包含三个串联重复序列(3TPR)的四肽重复序列模块,我们确定了两类3TPR模块,它们具有与不同功能残基集相关的不同结构特征。我们的分析还揭示了整个配体结合表面上各位置之间的高度相关性,这表明结合的表面会协同进化。将我们的分析扩展到不同的重复蛋白模块可以揭示更多重复特定功能的例子,尤其是在犰狳重复模块中。总之,我们介绍的基于模块的分析有效地捕获了关键的重复特定功能,这对于将来包含在重复蛋白质设计模板中将至关重要。

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