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突变扫描推断固有无序蛋白 CcdA 的结合能和结构。

Mutational scan inferred binding energetics and structure in intrinsically disordered protein CcdA.

机构信息

Molecular Biophysics Unit, Indian Institute of Science, Bangalore, India.

Institute for Stem Cell Science and Regenerative Medicine, Bangalore, India.

出版信息

Protein Sci. 2023 Mar;32(3):e4580. doi: 10.1002/pro.4580.

Abstract

Unlike globular proteins, mutational effects on the function of Intrinsically Disordered Proteins (IDPs) are not well-studied. Deep Mutational Scanning of a yeast surface displayed mutant library yields insights into sequence-function relationships in the CcdA IDP. The approach enables facile prediction of interface residues and local structural signatures of the bound conformation. In contrast to previous titration-based approaches which use a number of ligand concentrations, we show that use of a single rationally chosen ligand concentration can provide quantitative estimates of relative binding constants for large numbers of protein variants. This is because the extended interface of IDP ensures that energetic effects of point mutations are spread over a much smaller range than for globular proteins. Our data also provides insights into the much-debated role of helicity and disorder in partner binding of IDPs. Based on this exhaustive mutational sensitivity dataset, a rudimentary model was developed in an attempt to predict mutational effects on binding affinity of IDPs that form alpha-helical structures upon binding.

摘要

与球状蛋白不同,对无序蛋白(IDP)功能的突变效应研究得还不够充分。酵母表面展示突变文库的深度突变扫描为 CcdA IDP 的序列-功能关系提供了深入的了解。该方法能够方便地预测结合构象的界面残基和局部结构特征。与以前使用多种配体浓度的基于滴定的方法不同,我们表明,使用一个合理选择的配体浓度可以为大量蛋白质变体提供相对结合常数的定量估计。这是因为 IDP 的扩展界面确保了点突变的能量效应比球状蛋白分散在更小的范围内。我们的数据还深入探讨了 IDP 伴侣结合中螺旋性和无序性的作用这一备受争议的问题。基于这个详尽的突变敏感性数据集,我们开发了一个基本模型,试图预测在形成α-螺旋结构的 IDP 结合亲和力上的突变效应。

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