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肌球蛋白 II 和 V 的马达功能由肌动蛋白 D 环的不同调节。

D-loop of actin differently regulates the motor function of myosins II and V.

机构信息

Department of Physics, Faculty of Science and Engineering, Waseda University, 3-4-1 Okubo, Shinjuku-ku,Tokyo, Japan.

出版信息

J Biol Chem. 2009 Dec 11;284(50):35251-8. doi: 10.1074/jbc.M109.013565. Epub 2009 Oct 18.

Abstract

To gain more information on the manner of actin-myosin interaction, we examined how the motile properties of myosins II and V are affected by the modifications of the DNase I binding loop (D-loop) of actin, performed in two different ways, namely, the proteolytic digestion with subtilisin and the M47A point mutation. In an in vitro motility assay, both modifications significantly decreased the gliding velocity on myosin II-heavy meromyosin due to a weaker generated force but increased it on myosin V. On the other hand, single molecules of myosin V "walked" with the same velocity on both the wild-type and modified actins; however, the run lengths decreased sharply, correlating with a lower affinity of myosin for actin due to the D-loop modifications. The difference between the single-molecule and the ensemble measurements with myosin V indicates that in an in vitro motility assay the non-coordinated multiple myosin V molecules impose internal friction on each other via binding to the same actin filament, which is reduced by the weaker binding to the modified actins. These results show that the D-loop strongly modulates the force generation by myosin II and the processivity of myosin V, presumably affecting actin-myosin interaction in the actomyosin-ADP.P(i) state of both myosins.

摘要

为了获得更多关于肌球蛋白与肌动蛋白相互作用方式的信息,我们研究了肌球蛋白 II 和 V 的运动特性是如何受到肌动蛋白的 DNase I 结合环(D-loop)修饰的影响,修饰是通过两种不同的方式进行的,即枯草杆菌蛋白酶的蛋白水解消化和 M47A 点突变。在体外运动分析中,由于产生的力较弱,这两种修饰都显著降低了肌球蛋白 II-重酶解肌球蛋白的滑行速度,但提高了肌球蛋白 V 的滑行速度。另一方面,在野生型和修饰的肌动蛋白上,单个肌球蛋白 V 分子以相同的速度“行走”;然而,运行长度急剧下降,与肌球蛋白与肌动蛋白的亲和力降低相关,这是由于 D-loop 修饰。肌球蛋白 V 的单分子和整体测量之间的差异表明,在体外运动分析中,未协调的多个肌球蛋白 V 分子通过结合到相同的肌动蛋白丝相互施加内部摩擦力,这种摩擦力通过与修饰的肌动蛋白较弱的结合而降低。这些结果表明,D-loop 强烈调节肌球蛋白 II 的力产生和肌球蛋白 V 的进程性,可能影响两种肌球蛋白的肌动球蛋白-ADP.P(i)状态下的肌球蛋白与肌动蛋白相互作用。

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