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蛋白质反应动力学的时间分辨结构研究:X射线方法的大杂烩。

Time-resolved structural studies of protein reaction dynamics: a smorgasbord of X-ray approaches.

作者信息

Westenhoff Sebastian, Nazarenko Elena, Malmerberg Erik, Davidsson Jan, Katona Gergely, Neutze Richard

机构信息

Department of Chemistry, Biochemistry and Biophysics, University of Gothenburg, Box 462, SE-40530 Gothenburg, Sweden.

出版信息

Acta Crystallogr A. 2010 Mar;66(Pt 2):207-19. doi: 10.1107/S0108767309054361. Epub 2010 Feb 18.

Abstract

Proteins undergo conformational changes during their biological function. As such, a high-resolution structure of a protein's resting conformation provides a starting point for elucidating its reaction mechanism, but provides no direct information concerning the protein's conformational dynamics. Several X-ray methods have been developed to elucidate those conformational changes that occur during a protein's reaction, including time-resolved Laue diffraction and intermediate trapping studies on three-dimensional protein crystals, and time-resolved wide-angle X-ray scattering and X-ray absorption studies on proteins in the solution phase. This review emphasizes the scope and limitations of these complementary experimental approaches when seeking to understand protein conformational dynamics. These methods are illustrated using a limited set of examples including myoglobin and haemoglobin in complex with carbon monoxide, the simple light-driven proton pump bacteriorhodopsin, and the superoxide scavenger superoxide reductase. In conclusion, likely future developments of these methods at synchrotron X-ray sources and the potential impact of emerging X-ray free-electron laser facilities are speculated upon.

摘要

蛋白质在其生物学功能过程中会发生构象变化。因此,蛋白质静止构象的高分辨率结构为阐明其反应机制提供了一个起点,但并未提供有关蛋白质构象动力学的直接信息。已经开发了几种X射线方法来阐明蛋白质反应过程中发生的那些构象变化,包括对三维蛋白质晶体的时间分辨劳厄衍射和中间捕获研究,以及对溶液相中蛋白质的时间分辨广角X射线散射和X射线吸收研究。本综述强调了这些互补实验方法在试图理解蛋白质构象动力学时的范围和局限性。使用一组有限的例子来说明这些方法,包括与一氧化碳结合的肌红蛋白和血红蛋白、简单的光驱动质子泵细菌视紫红质以及超氧化物清除剂超氧化物还原酶。总之,推测了这些方法在同步加速器X射线源的未来可能发展以及新兴的X射线自由电子激光设施的潜在影响。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7b48/2824530/f9b28fc0db5f/a-66-00207-fig1.jpg

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