Blue and red in the protein world: Photoactive yellow protein and phytochromes as revealed by time-resolved crystallography

Marius Schmidt, Emina A. Stojković
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Abstract

Time-resolved crystallography (TRX) is a method designed to investigate functional motions of biological macromolecules on all time scales. Originally a synchrotron-based method, TRX is enabled by the development of TR Laue crystallography (TRLX). TR serial crystallography (TR-SX) is an extension of TRLX. As the foundations of TRLX were evolving from the late 1980s to the turn of the millennium, TR-SX has been inspired by the development of Free Electron Lasers for hard X-rays. Extremely intense, ultrashort x-ray pulses could probe micro and nanocrystals, but at the same time, they inflicted radiation damage that necessitated the replacement by a new crystal. Consequently, a large number of microcrystals are exposed to X-rays one by one in a serial fashion. With TR-SX methods, one of the largest obstacles of previous approaches, namely, the unsurmountable challenges associated with the investigation of non-cyclic (irreversible) reactions, can be overcome. This article describes successes and transformative contributions to the TRX field by Keith Moffat and his collaborators, highlighting two major projects on protein photoreceptors initiated in the Moffat lab at the turn of the millennium.
蛋白质世界中的蓝与红:时间分辨晶体学揭示的光活性黄蛋白和植物色素
时间分辨晶体学(TRX)是一种旨在研究所有时间尺度上生物大分子功能运动的方法。TRX 最初是一种基于同步加速器的方法,随着 TR Laue 晶体学(TRLX)的发展而得以实现。TR 序列晶体学(TR-SX)是 TRLX 的延伸。从 20 世纪 80 年代末到千年之交,TRLX 的基础不断发展,而 TR-SX 则受到了用于硬 X 射线的自由电子激光器发展的启发。极强的超短 X 射线脉冲可以探测微晶体和纳米晶体,但同时也会造成辐射损伤,必须更换新晶体。因此,需要将大量微晶逐个连续照射 X 射线。TR-SX 方法可以克服以往方法的最大障碍之一,即研究非循环(不可逆)反应所面临的难以克服的挑战。本文介绍了基思-莫法特及其合作者在 TRX 领域取得的成功和做出的变革性贡献,重点介绍了莫法特实验室在千年之交启动的两个关于蛋白质光感受器的重大项目。
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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