Structural dynamics of proteins explored via time-resolved x-ray liquidography

IF 6.1 Q2 CHEMISTRY, PHYSICAL
Yunbeom Lee, Hyosub Lee, H. Ihee
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引用次数: 2

Abstract

The structure of a protein is closely related to its biological function. In this regard, structural changes, as well as static structures, have been scrutinized as essential elements in understanding and controlling the function of a protein. In particular, the structural change in the solution phase needs to be elucidated to properly understand protein functions under physiological conditions. Time-resolved x-ray liquidography (TRXL), also known as time-resolved x-ray solution scattering, has attracted attention as a powerful experimental method for studying the structural dynamics of proteins in the solution phase. Initially, TRXL was used to study the structural dynamics of small molecules in the solution phase, and later, its application was extended to probe the structural changes in proteins. Via TRXL, structural changes ranging from large quaternary movements to subtle rearrangements of the tertiary structures have been successfully elucidated. In this review, we introduce various studies using TRXL to investigate the structural dynamics of proteins. These include early TRXL studies on model systems, those on photoreceptor proteins, and recent studies using stimuli beyond the direct photoexcitation of proteins.
通过时间分辨x射线液体学探索蛋白质的结构动力学
蛋白质的结构与其生物学功能密切相关。在这方面,结构变化以及静态结构已被视为理解和控制蛋白质功能的基本要素。特别是,需要阐明溶液相中的结构变化,以正确理解生理条件下的蛋白质功能。时间分辨x射线液相色谱(TRXL),也称为时间分辨x x射线溶液散射,作为研究溶液相中蛋白质结构动力学的一种强大的实验方法,引起了人们的关注。最初,TRXL用于研究溶液相中小分子的结构动力学,后来,它的应用扩展到探测蛋白质的结构变化。通过TRXL,从大的第四纪运动到第三系结构的细微重排,结构变化已经被成功阐明。在这篇综述中,我们介绍了使用TRXL研究蛋白质结构动力学的各种研究。其中包括早期TRXL对模型系统的研究,对感光蛋白的研究,以及最近使用蛋白质直接光激发之外的刺激的研究。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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