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Thick Filament Length and Isoform Composition Determine Self-Organized Contractile Units in Actomyosin Bundles

机译:粗丝的长度和同工型组成决定了放线菌素束中的自组织收缩单位

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摘要

Diverse myosin II isoforms regulate contractility of actomyosin bundles in disparate physiological processes by variations in both motor mechanochemistry and the extent to which motors are clustered into thick filaments. Although the role of mechanochemistry is well appreciated, the extent to which thick filament length regulates actomyosin contractility is unknown. Here, we study the contractility of minimal actomyosin bundles formed in vitro by mixtures of F-actin and thick filaments of nonmuscle, smooth, and skeletal muscle myosin isoforms with varied length. Diverse myosin II isoforms guide the self-organization of distinct contractile units within in vitro bundles with shortening rates similar to those of in vivo myofibrils and stress fibers. The tendency to form contractile units increases with the thick filament length, resulting in a bundle shortening rate proportional to the length of constituent myosin thick filament. We develop a model that describes our data, providing a framework in which to understand how diverse myosin II isoforms regulate the contractile behaviors of disordered actomyosin bundles found in muscle and nonmuscle cells. These experiments provide insight into physiological processes that use dynamic regulation of thick filament length, such as smooth muscle contraction.
机译:多样的肌球蛋白II亚型通过运动机械化学和运动成簇的细丝的程度的变化,在不同的生理过程中调节肌动球蛋白束的收缩性。尽管机械化学的作用已广为人知,但粗丝长度调节肌动球蛋白收缩性的程度尚不清楚。在这里,我们研究了由F-肌动蛋白和长度不等的非肌肉,平滑肌和骨骼肌肌球蛋白同工型的粗细丝的混合物在体外形成的最小肌动球蛋白束的收缩性。多样的肌球蛋白II亚型指导体外束中不同收缩单元的自组织,其缩短率类似于体内肌原纤维和应激纤维的缩短率。形成收缩单元的趋势随着细丝长度的增加而增加,从而导致束缩短率与组成肌球蛋白粗细丝的长度成比例。我们开发了一个描述我们的数据的模型,提供了一个框架,以了解不同的肌球蛋白II亚型如何调节在肌肉和非肌肉细胞中发现的无序肌动球蛋白束的收缩行为。这些实验提供了对利用粗纤维长度的动态调节(例如平滑肌收缩)的生理过程的见解。

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