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近期对肌球蛋白的力作用和磷酸盐释放的相对时间的深入了解。

Recent insights into the relative timing of myosin's powerstroke and release of phosphate.

机构信息

Department of Kinesiology, Muscle Biophysics Lab, University of Massachusetts, Amherst, Massachusetts, USA.

出版信息

Cytoskeleton (Hoboken). 2021 Sep;78(9):448-458. doi: 10.1002/cm.21695. Epub 2022 Mar 21.

Abstract

Myosin is a motor enzyme that converts the chemical energy in ATP into mechanical work to drive a myriad of intracellular processes, from muscle contraction to vesicular transport. Key steps in the transduction of energy are the force-generating powerstroke, and the release of phosphate (P ) from the nucleotide-binding site. Both events occur rapidly after binding to actin, making it difficult to determine which event occurs first. Early efforts suggested that these events occur simultaneously; however, recent findings indicate that they are separate and distinct events that occur at different rates. High-resolution crystal structures of myosin captured in intermediate states of the ATPase cycle suggest that when P is in the active site it prevents the powerstroke from occurring, leading to the hypothesis that P -release precedes the powerstroke. However, advances in functional assays, enabling sub-millisecond temporal and nanometer spatial resolution, are challenging this hypothesis. For example, Föster Resonance Energy Transfer (FRET) based assays, as well as single molecule laser trap assays, suggest the opposite; that the powerstroke occurs prior to the release of P from myosin's active site. This review provides some historical context and then highlights recent reports that reveal exciting new insight into this fundamental mechanism of energy transduction by this prototypical motor enzyme.

摘要

肌球蛋白是一种运动酶,它将 ATP 中的化学能转化为机械功,驱动无数的细胞内过程,从肌肉收缩到囊泡运输。能量传递的关键步骤是产生力的动力冲程,以及核苷酸结合位点上磷酸盐(P )的释放。这两个事件都在与肌动蛋白结合后迅速发生,这使得很难确定哪个事件先发生。早期的研究表明这些事件同时发生;然而,最近的发现表明它们是独立和不同的事件,发生在不同的速率下。高分辨率的肌球蛋白晶体结构捕捉到了 ATP 酶循环中的中间状态,表明当 P 在活性位点时,它会阻止动力冲程的发生,从而导致 P 释放先于动力冲程的假设。然而,功能测定方面的进展,使亚毫秒级时间和纳米级空间分辨率成为可能,这对该假设提出了挑战。例如,基于Förster 共振能量转移(FRET)的测定以及单分子激光捕获测定表明相反的情况;即动力冲程先于 P 从肌球蛋白的活性位点释放。这篇综述提供了一些历史背景,然后重点介绍了最近的报告,这些报告揭示了这个原型运动酶的能量传递基本机制的令人兴奋的新见解。

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