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A Branched Kinetic Scheme Describes the Mechanochemical Coupling of Myosin Va Processivity in Response to Substrate

机译:分支动力学方案描述了肌球蛋白Va生产力对底物的响应的机械化学偶联。

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摘要

Myosin Va is a double-headed cargo-carrying molecular motor that moves processively along cellular actin filaments. Long processive runs are achieved through mechanical coordination between the two heads of myosin Va, which keeps their ATPase cycles out of phase, preventing both heads detaching from actin simultaneously. The biochemical kinetics underlying processivity are still uncertain. Here we attempt to define the biochemical pathways populated by myosin Va by examining the velocity, processive run-length, and individual steps of a Qdot-labeled myosin Va in various substrate conditions (i.e., changes in ATP, ADP, and Pi) under zero load in the single-molecule total internal reflection fluorescence microscopy assay. These data were used to globally constrain a branched kinetic scheme that was necessary to fit the dependences of velocity and run-length on substrate conditions. Based on this model, myosin Va can be biased along a given pathway by changes in substrate concentrations. This has uncovered states not normally sampled by the motor, and suggests that every transition involving substrate binding and release may be strain-dependent.
机译:Myosin Va是一种双头携带式分子电动机,可沿细胞肌动蛋白丝不断地移动。通过肌球蛋白Va的两个头部之间的机械协调可实现长过程运行,从而使它们的ATPase循环异相,从而防止两个头部同时从肌动蛋白分离。潜在生产力的生化动力学仍不确定。在这里,我们尝试通过在零以下各种底物条件下(即ATP,ADP和Pi的变化)检查Qdot标记的肌球蛋白Va的速度,连续运行长度和各个步骤来定义由肌球蛋白Va组成的生化途径。单分子全内反射荧光显微镜分析中的负载。这些数据用于全局约束分支动力学方案,该方案对于适应速度和行程长度对底物条件的依赖性是必需的。基于此模型,肌球蛋白Va可以通过底物浓度的变化沿给定的路径发生偏向。这揭示了马达通常不采样的状态,并暗示涉及底物结合和释放的每个转变可能是应变依赖性的。

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