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生色团构象与光活性黄色蛋白三级结构变化的演变

Chromophore conformation and the evolution of tertiary structural changes in photoactive yellow protein.

作者信息

Anderson Spencer, Srajer Vukica, Pahl Reinhard, Rajagopal Sudarshan, Schotte Friedrich, Anfinrud Philip, Wulff Michael, Moffat Keith

机构信息

Department of Biochemistry and Molecular Biology, University of Chicago, Chicago, IL 60637, USA.

出版信息

Structure. 2004 Jun;12(6):1039-45. doi: 10.1016/j.str.2004.04.008.

Abstract

We use time-resolved crystallography to observe the structural progression of a bacterial blue light photoreceptor throughout its photocycle. Data were collected from 10 ns to 100 ms after photoactivation of the E46Q mutant of photoactive yellow protein. Refinement of transient chromophore conformations shows that the spectroscopically distinct intermediates are formed via progressive disruption of the hydrogen bond network to the chromophore. Although structural change occurs within a few nanoseconds on and around the chromophore, it takes milliseconds for a distinct pattern of tertiary structural change to fully progress through the entire molecule, thus generating the putative signaling state. Remarkably, the coupling between the chromophore conformation and the tertiary structure of this small protein is not tight: there are leads and lags between changes in the conformation of the chromophore and the protein tertiary structure.

摘要

我们利用时间分辨晶体学来观察一种细菌蓝光光感受器在其光循环过程中的结构变化。数据是在光激活光活性黄色蛋白的E46Q突变体后10纳秒至100毫秒内收集的。对瞬态发色团构象的优化表明,光谱上不同的中间体是通过与发色团的氢键网络的逐步破坏而形成的。尽管在发色团及其周围几纳秒内就发生了结构变化,但三级结构变化的独特模式要完全贯穿整个分子需要几毫秒,从而产生假定的信号状态。值得注意的是,这种小蛋白的发色团构象与三级结构之间的耦合并不紧密:发色团构象变化与蛋白质三级结构变化之间存在领先和滞后现象。

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