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细菌视紫红质光循环中蛋白质构象变化的晶体学分析。

Crystallographic analysis of protein conformational changes in the bacteriorhodopsin photocycle.

作者信息

Subramaniam S, Henderson R

机构信息

Laboratory of Biochemistry, National Cancer Institute, Bethesda, MD 20892, USA.

出版信息

Biochim Biophys Acta. 2000 Aug 30;1460(1):157-65. doi: 10.1016/s0005-2728(00)00136-5.

Abstract

A variety of neutron, X-ray and electron diffraction experiments have established that the transmembrane regions of bacteriorhodopsin undergo significant light-induced changes in conformation during the course of the photocycle. A recent comprehensive electron crystallographic analysis of light-driven structural changes in wild-type bacteriorhodopsin and a number of mutants has established that a single, large protein conformational change occurs within 1 ms after illumination, roughly coincident with the time scale of formation of the M(2) intermediate in the photocycle of wild-type bacteriorhodopsin. Minor differences in structural changes that are observed in mutants that display long-lived M(2), N or O intermediates are best described as variations of one fundamental type of conformational change, rather than representing structural changes that are unique to the optical intermediate that is accumulated. These observations support a model for the photocycle of wild-type bacteriorhodopsin in which the structures of the initial state and the early intermediates (K, L and M(1)) are well approximated by one protein conformation in which the Schiff base has extracellular accessibility, while the structures of the later intermediates (M(2), N and O) are well approximated by the other protein conformation in which the Schiff base has cytoplasmic accessibility.

摘要

多种中子、X射线和电子衍射实验已证实,细菌视紫红质的跨膜区域在光循环过程中会经历显著的光诱导构象变化。最近对野生型细菌视紫红质和一些突变体的光驱动结构变化进行的全面电子晶体学分析表明,光照后1毫秒内会发生单一的、大的蛋白质构象变化,这大致与野生型细菌视紫红质光循环中M(2)中间体形成的时间尺度一致。在显示长寿命M(2)、N或O中间体的突变体中观察到的结构变化的微小差异,最好描述为一种基本构象变化类型的变体,而不是代表积累的光学中间体特有的结构变化。这些观察结果支持了野生型细菌视紫红质光循环的模型,其中初始状态和早期中间体(K、L和M(1))的结构可以很好地由一种蛋白质构象近似,在这种构象中席夫碱具有细胞外可及性,而后期中间体(M(2)、N和O)的结构可以很好地由另一种蛋白质构象近似,在这种构象中席夫碱具有细胞质可及性。

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