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Role of the lever arm in the processive stepping of myosin V

机译:杠杆臂在肌球蛋白V逐步进行中的作用

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Myosin V is a two-headed molecular motor that binds six light chains per heavy chain, which creates unusually long lever arms. This motor moves processively along its actin track in discrete 36-nm steps. Our model is that one head of the two-headed myosin V tightly binds to actin and swings its long lever arm through a large angle, providing a stroke. We created single-headed constructs with different-size lever arms and show that stroke size is proportional to lever arm length. In a two-headed molecule, the stroke provides the directional bias, after which the unbound head diffuses to find its binding site, 36 nm forward. Our two-headed construct with all six light chains per head reconstitutes the 36-nm processive step seen in tissue-purified myosin V. Two-headed myosin V molecules with only four light chains per head are still processive, but their step size is reduced to 24 nm. A further reduction in the length of the lever arms to one light chain per head results in a motor that is unable to walk processively. This motor produces single small ≈6-nm strokes, and ATPase and pyrene actin quench measurements show that only one of the heads of this dimer rapidly binds to actin for a given binding event. These data show that for myosin V with its normal proximal tail domain, both heads and a long lever arm are required for large, processive steps.
机译:Myosin V是一种双向分子马达,每条重链结合6条轻链,产生异常长的杠杆臂。该电机以不连续的36 nm步长沿其肌动蛋白轨迹进行性运动。我们的模型是,两头肌球蛋白V的一个头与肌动蛋白紧密结合,并将其长杠杆臂摆动大角度,以提供行程。我们创建了具有不同大小杠杆臂的单头构造,并显示了冲程大小与杠杆臂长度成比例。在双头分子中,笔划提供方向性偏差,此后未结合的头会扩散以找到其结合位点,即向前36 nm。我们的每头所有六个轻链的双头构建体重构了组织纯化的肌球蛋白V中所见的36 nm进行性步骤。每头仅具有四个轻链的双头肌球蛋白V分子仍是进行性的,但步长减小了至24纳米。杠杆臂的长度进一步减少到每头一个轻链,导致电动机无法进行有序地行走。该马达产生单个≈6nm的小冲程,并且ATPase和pyr肌动蛋白猝灭测量表明,对于给定的结合事件,该二聚体的只有一个头部能快速结合肌动蛋白。这些数据表明,对于具有正常近端尾部结构域的肌球蛋白V,需要较大的过程性步骤同时使用头部和长杠杆臂。

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