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二级结构的改变可以在蛋白质折叠和展开反应中弥散地发生,而不是模块地发生。

Secondary Structural Change Can Occur Diffusely and Not Modularly during Protein Folding and Unfolding Reactions.

机构信息

National Centre for Biological Sciences, Tata Institute of Fundamental Research , Bengaluru 560065, India.

出版信息

J Am Chem Soc. 2016 May 11;138(18):5866-78. doi: 10.1021/jacs.6b03356. Epub 2016 Apr 29.

DOI:10.1021/jacs.6b03356
PMID:27093885
Abstract

A major goal of protein folding studies is to understand the structural basis of the coupling between stabilizing interactions, which leads to cooperative conformational change. The goal is challenging because of the difficulty in simultaneously measuring global cooperativity by determining population distributions of the conformations present, and the structures of these conformations. Here, hydrogen exchange (HX) into the small protein monellin was carried out under conditions where structure-opening is rate limiting for most backbone amide sites. Detection by mass spectrometry allowed characterization of not only segment-specific structure-opening rates but also the cooperativity of unfolding of the different secondary structural segments of the protein. The segment-specific pattern of HX reveals that the backbone hydrogen-bonding network disassembles in a structurally diffuse, asynchronous manner. A comparison of the site-specific transient opening rates of secondary and tertiary structure in the protein provides a structural rationale for the observation that unfolding is hierarchical and describable by exponential kinetics, despite being diffuse. Since unfolding was studied in native conditions, the sequence of events during folding in the same conditions will be the reverse of the sequence of events observed during unfolding. Hence, the formation of secondary structural units during folding would also occur in a non-cooperative, diffuse, and asynchronous manner.

摘要

蛋白质折叠研究的一个主要目标是理解稳定相互作用之间的结构基础,这种相互作用导致协同构象变化。由于同时通过确定存在构象的种群分布和这些构象的结构来测量整体协同性的难度,因此这个目标具有挑战性。在这里,在大多数骨架酰胺位点的结构打开是限速步骤的条件下,对小蛋白莫内林进行了氢交换(HX)。通过质谱检测不仅可以表征片段特异性结构打开速率,还可以表征蛋白质不同二级结构片段的展开协同性。HX 的片段特异性模式表明,骨架氢键网络以结构弥散、异步的方式解体。蛋白质中二级和三级结构的位点特异性瞬时开口速率的比较为观察到的展开是分层的并且可以用指数动力学描述提供了结构基础,尽管是弥散的。由于在天然条件下研究了展开,因此在相同条件下折叠过程中的事件序列将与展开过程中观察到的事件序列相反。因此,在折叠过程中形成二级结构单元也将以非协同、弥散和异步的方式发生。

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