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Direct measurements of the coordination of lever arm swing and the catalytic cycle in myosin V

机译:直接测量肌球蛋白V中杠杆臂摆动和催化循环的协调性

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摘要

Myosins use a conserved structural mechanism to convert the energy from ATP hydrolysis into a large swing of the force-generating lever arm. The precise timing of the lever arm movement with respect to the steps in the actomyosin ATPase cycle has not been determined. We have developed a FRET system in myosin V that uses three donor–acceptor pairs to examine the kinetics of lever arm swing during the recovery and power stroke phases of the ATPase cycle. During the recovery stroke the lever arm swing is tightly coupled to priming the active site for ATP hydrolysis. The lever arm swing during the power stroke occurs in two steps, a fast step that occurs before phosphate release and a slow step that occurs before ADP release. Time-resolved FRET demonstrates a 20-Å change in distance between the pre- and postpower stroke states and shows that the lever arm is more dynamic in the postpower stroke state. Our results suggest myosin binding to actin in the ADP.Pi complex triggers a rapid power stroke that gates the release of phosphate, whereas a second slower power stroke may be important for mediating strain sensitivity.
机译:肌球蛋白利用保守的结构机制将ATP水解产生的能量转换成力产生杠杆臂的大摆幅。尚未确定杠杆臂相对于肌动球蛋白ATPase循环步骤的精确运动时间。我们已经开发了一种在肌球蛋白V中的FRET系统,该系统使用三对供体-受体对来检查ATPase循环的恢复和功率冲程阶段杠杆臂摆动的动力学。在恢复冲程中,杠杆臂的摆动紧密地耦合在一起,以启动用于ATP水解的活性部位。动力冲程期间的杠杆臂摆动分为两个步骤,快速步骤发生在磷酸盐释放之前,慢速步骤发生在ADP释放之前。时间分辨的FRET证明了动力前和动力后冲程状态之间的距离变化了20Å,并且表明杠杆臂在动力后冲程状态下更具动力。我们的结果表明,肌球蛋白与ADP中的肌动蛋白结合.Pi复合物触发了快速中风,从而控制了磷酸盐的释放,而第二次较慢的中风对于介导应变敏感性可能很重要。

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