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细丝顺应性效应可以解释力产生过程中的张力过冲现象。

Filament compliance effects can explain tension overshoots during force development.

作者信息

Campbell Kenneth S

机构信息

Department of Physiology, University of Kentucky, Lexington, KY 40536-0298, USA.

出版信息

Biophys J. 2006 Dec 1;91(11):4102-9. doi: 10.1529/biophysj.106.087312. Epub 2006 Sep 1.

Abstract

Spatially explicit stochastic simulations of myosin S1 heads attaching to a single actin filament were used to investigate the process of force development in contracting muscle. Filament compliance effects were incorporated by adjusting the spacing between adjacent actin binding sites and adjacent myosin heads in response to cross-bridge attachment/detachment events. Appropriate model parameters were determined by multi-dimensional optimization and used to simulate force development records corresponding to different levels of Ca(2+) activation. Simulations in which the spacing between both adjacent actin binding sites and adjacent myosin S1 heads changed by approximately 0.06 nm after cross-bridge attachment/detachment events 1), exhibited tension overshoots with a Ca(2+) dependence similar to that measured experimentally and 2), mimicked the observed k(tr)-relative tension relationship without invoking a Ca(2+)-dependent increase in the rate of cross-bridge state transitions. Tension did not overshoot its steady-state value in control simulations modeling rigid thick and thin filaments with otherwise identical parameters. These results underline the importance of filament geometry and actin binding site availability in quantitative theories of muscle contraction.

摘要

利用肌球蛋白S1头部附着于单根肌动蛋白丝的空间明确随机模拟,来研究收缩肌肉中力的产生过程。通过响应横桥附着/脱离事件调整相邻肌动蛋白结合位点和相邻肌球蛋白头部之间的间距,纳入细丝顺应性效应。通过多维优化确定合适的模型参数,并用于模拟对应不同Ca(2+)激活水平的力产生记录。在横桥附着/脱离事件后,相邻肌动蛋白结合位点和相邻肌球蛋白S1头部之间的间距均改变约0.06 nm的模拟中,1)表现出与实验测量相似的Ca(2+)依赖性张力过冲,且2)模拟了观察到的k(tr)-相对张力关系,而无需引入Ca(2+)依赖性的横桥状态转变速率增加。在对刚性粗细肌丝进行建模且其他参数相同的对照模拟中,张力并未超过其稳态值。这些结果强调了细丝几何形状和肌动蛋白结合位点可用性在肌肉收缩定量理论中的重要性。

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