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Cargo Transport by Two Coupled Myosin Va Motors on Actin Filaments and Bundles

机译:两个耦合的肌球蛋白VA电动机在肌动蛋白丝和束上的货物运输

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摘要

Myosin Va (myoVa) is a processive, actin-based molecular motor essential for intracellular cargo transport. When a cargo is transported by an ensemble of myoVa motors, each motor faces significant physical barriers and directional challenges created by the complex actin cytoskeleton, a network of actin filaments and actin bundles. The principles that govern the interaction of multiple motors attached to the same cargo are still poorly understood. To understand the mechanical interactions between multiple motors, we developed a simple in vitro model in which two individual myoVa motors labeled with different-colored Qdots are linked via a third Qdot that acts as a cargo. The velocity of this two-motor complex was reduced by 27% as compared to a single motor, whereas run length was increased by only 37%, much less than expected from multimotor transport models. Therefore, at low ATP, which allowed us to identify individual motor steps, we investigated the intermotor dynamics within the two-motor complex. The randomness of stepping leads to a buildup of tension in the linkage between motors—which in turn slows down the leading motor—and increases the frequency of backward steps and the detachment rate. We establish a direct relationship between the velocity reduction and the distribution of intermotor distances. The analysis of run lengths and dwell times for the two-motor complex, which has only one motor engaged with the actin track, reveals that half of the runs are terminated by almost simultaneous detachment of both motors. This finding challenges the assumptions of conventional multimotor models based on consecutive motor detachment. Similar, but even more drastic, results were observed with two-motor complexes on actin bundles, which showed a run length that was even shorter than that of a single motor.
机译:肌球蛋白Va(myoVa)是一种基于肌动蛋白的过程性分子运动,对于细胞内货物运输至关重要。当一组MyoVa电机运输货物时,每台电机都面临着严重的物理障碍和复杂的肌动蛋白细胞骨架,肌动蛋白丝和肌动蛋白束网络所造成的方向挑战。仍然很少了解控制连接到同一货物的多个电动机的相互作用的原理。为了了解多个电动机之间的机械相互作用,我们开发了一个简单的体外模型,其中两个带有不同颜色Qdot的独立MyoVa电动机通过充当货物的第三个Qdot进行链接。与单电机相比,该两电机复合体的速度降低了27%,而运行长度仅增加了37%,远低于多电机运输模型的预期。因此,在低ATP(允许我们识别单个运动步长)的情况下,我们研究了两运动复合体内的运动间动力学。步进的随机性会导致电动机之间的联动装置中的张力累积,进而使领先的电动机变慢,并增加后退频率和分离速度。我们在速度降低和电机间距离的分布之间建立了直接关系。对只有一个电机与肌动蛋白磁道接合的两个电机的复合体的行程长度和停留时间的分析显示,一半行程通过几乎同时拆卸两个电机而终止。这一发现挑战了基于连续电动机分离的传统多电动机模型的假设。在肌动蛋白束上使用两个电机的复合物观察到了相似但更为严峻的结果,其运行长度甚至比单个电机的运行长度还短。

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