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杠杆臂旋转驱动负端定向驱动蛋白Ncd的运动。

A lever-arm rotation drives motility of the minus-end-directed kinesin Ncd.

作者信息

Endres Nicholas F, Yoshioka Craig, Milligan Ronald A, Vale Ronald D

机构信息

The Howard Hughes Medical Institute, and the Department of Cellular and Molecular Pharmacology, University of California San Francisco, 600 16th Street, San Francisco, California 94107, USA.

出版信息

Nature. 2006 Feb 16;439(7078):875-8. doi: 10.1038/nature04320. Epub 2005 Dec 28.

Abstract

Kinesins are microtubule-based motor proteins that power intracellular transport. Most kinesin motors, exemplified by Kinesin-1, move towards the microtubule plus end, and the structural changes that govern this directional preference have been described. By contrast, the nature and timing of the structural changes underlying the minus-end-directed motility of Kinesin-14 motors (such as Drosophila Ncd) are less well understood. Using cryo-electron microscopy, here we demonstrate that a coiled-coil mechanical element of microtubule-bound Ncd rotates approximately 70 degrees towards the minus end upon ATP binding. Extending or shortening this coiled coil increases or decreases velocity, respectively, without affecting ATPase activity. An unusual Ncd mutant that lacks directional preference shows unstable nucleotide-dependent conformations of its coiled coil, underscoring the role of this mechanical element in motility. These results show that the force-producing conformational change in Ncd occurs on ATP binding, as in other kinesins, but involves the swing of a lever-arm mechanical element similar to that described for myosins.

摘要

驱动蛋白是基于微管的驱动蛋白,为细胞内运输提供动力。大多数驱动蛋白,如驱动蛋白-1,朝着微管的正端移动,并且已经描述了控制这种方向偏好的结构变化。相比之下,驱动蛋白-14(如果蝇Ncd)向负端运动的结构变化的性质和时间则了解较少。在这里,我们使用冷冻电子显微镜证明,与微管结合的Ncd的卷曲螺旋机械元件在ATP结合时朝着负端旋转约70度。延长或缩短这个卷曲螺旋分别会增加或降低速度,而不影响ATP酶活性。一个缺乏方向偏好的异常Ncd突变体显示其卷曲螺旋的核苷酸依赖性构象不稳定,突出了这个机械元件在运动中的作用。这些结果表明,与其他驱动蛋白一样,Ncd中产生力的构象变化发生在ATP结合时,但涉及类似于肌球蛋白中描述的杠杆臂机械元件的摆动。

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