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PNAS Plus: Parsing the roles of neck-linker docking and tethered head diffusion in the stepping dynamics of kinesin

机译:PNAS Plus:解析颈部连接器对接和系留头扩散在驱动蛋白步进动力学中的作用

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摘要

Kinesin walks processively on microtubules (MTs) in an asymmetric hand-over-hand manner consuming one ATP molecule per 16-nm step. The individual contributions due to docking of the approximately 13-residue neck linker to the leading head (deemed to be the power stroke) and diffusion of the trailing head (TH) that contributes in propelling the motor by 16 nm have not been quantified. We use molecular simulations by creating a coarse-grained model of the MT–kinesin complex, which reproduces the measured stall force as well as the force required to dislodge the motor head from the MT, to show that nearly three-quarters of the step occurs by bidirectional stochastic motion of the TH. However, docking of the neck linker to the leading head constrains the extent of diffusion and minimizes the probability that kinesin takes side steps, implying that both the events are necessary in the motility of kinesin and for the maintenance of processivity. Surprisingly, we find that during a single step, the TH stochastically hops multiple times between the geometrically accessible neighboring sites on the MT before forming a stable interaction with the target binding site with correct orientation between the motor head and the α/β tubulin dimer.
机译:驱动蛋白以不对称的移交方式在微管(MTs)上进行性移动,每16 nm步消耗一个ATP分子。由于约13个残基的颈部连接器与前导头对接(被认为是动力冲程)以及后导头(TH)的扩散(有助于将电机推进16 nm),其个体贡献尚未得到量化。我们通过创建MT-驱动蛋白复合物的粗粒度模型来使用分子模拟,该模型可再现测得的失速力以及将电机头从MT上移出所需的力,以显示发生了近四分之三的步骤TH的双向随机运动。但是,将颈部连接器对接至前导头会限制扩散程度,并使驱动蛋白跨步的可能性降到最低,这意味着这两个事件对于驱动蛋白的运动性和维持持续性都是必要的。出乎意料的是,我们发现在单个步骤中,TH在MT上几何可及的相邻位点之间随机跳动多次,然后与目标结合位点形成稳定的相互作用,并在马达头和α/β微管蛋白二聚体之间正确定向。

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