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利用光镊研究肌球蛋白复合物在肌动蛋白丝束中的力学性质。

Probing Myosin Ensemble Mechanics in Actin Filament Bundles using Optical Tweezers.

机构信息

Department of Chemical Engineering, University of Mississippi.

Department of Biomedical Engineering, University of Mississippi.

出版信息

J Vis Exp. 2022 May 4(183). doi: 10.3791/63672.

Abstract

Myosins are motor proteins that hydrolyze ATP to step along actin filament (AF) tracks and are essential in cellular processes such as motility and muscle contraction. To understand their force-generating mechanisms, myosin II has been investigated both at the single-molecule (SM) level and as teams of motors in vitro using biophysical methods such as optical trapping. These studies showed that myosin force-generating behavior can differ greatly when moving from the single-molecule level in a three-bead arrangement to groups of motors working together on a rigid bead or coverslip surface in a gliding arrangement. However, these assay constructions do not permit evaluating the group dynamics of myosin within viscoelastic structural hierarchy as they would within a cell. We have developed a method using optical tweezers to investigate the mechanics of force generation by myosin ensembles interacting with multiple actin filaments. These actomyosin bundles facilitate investigation in a hierarchical and compliant environment that captures motor communication and ensemble force output. The customizable nature of the assay allows for altering experimental conditions to understand how modifications to the myosin ensemble, actin filament bundle, or the surrounding environment result in differing force outputs.

摘要

肌球蛋白是一种利用 ATP 水解沿肌动蛋白丝(AF)轨道运动的马达蛋白,在细胞运动和肌肉收缩等过程中是必不可少的。为了了解它们产生力的机制,肌球蛋白 II 已经在单分子(SM)水平和体外使用光学捕获等生物物理方法作为团队的马达进行了研究。这些研究表明,当从三珠排列的单分子水平移动到在滑动排列中一起在刚性珠或盖玻片表面上工作的马达组时,肌球蛋白产生力的行为会有很大的不同。然而,这些测定结构不允许评估细胞内粘弹性结构层次内肌球蛋白的群体动力学。我们已经开发了一种使用光学镊子的方法来研究与多个肌动蛋白丝相互作用的肌球蛋白集合体产生力的力学。这些肌动球蛋白束有利于在一个层次化和顺应的环境中进行研究,该环境可以捕获马达通讯和集合体力输出。该测定的可定制性质允许改变实验条件,以了解肌球蛋白集合体、肌动蛋白丝束或周围环境的修饰如何导致不同的力输出。

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