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平衡态肌肉横桥行为:肌球蛋白横桥与肌动蛋白的相互作用。

Equilibrium muscle crossbridge behavior: the interaction of myosin crossbridges with actin.

作者信息

Schoenberg M

机构信息

Laboratory of Physical Biology, National Institute of Arthritis and Musculoskeletal and Skin Diseases, National Institutes of Health, Bethesda, Maryland 20892.

出版信息

Adv Biophys. 1993;29:55-73. doi: 10.1016/0065-227x(93)90005-p.

Abstract

The interaction of myosin crossbridges with actin under equilibrium conditions is reviewed. Similarities and differences between the weakly- and strongly-binding interactions of myosin crossbridges with actin filaments are discussed. A precise, narrow definition of weakly-binding crossbridges is given. It is postulated that the fundamental difference between the weakly- and strongly-binding equilibrium interaction of crossbridges with actin is that the crossbridge heads are mobile after attachment in the first case but not in the second. It is argued that because the weakly-binding crossbridge heads are mobile after attachment, the heads appear to function independently of each other. The lack of head mobility in attached strongly-binding crossbridges makes the strongly-binding crossbridge heads appear to act cooperatively. This model of the strongly-binding crossbridge gives an explanation for two important and otherwise unexplained observations. It explains why the rate constant of force decay after a small stretch is a sigmoidal function of nucleotide analogue concentration, and why, in the presence of analogues or in rigor, the rate constant of force decay after a small stretch is often significantly slower than the rate constant for myosin subfragment-1 detachment from actin in solution. The model of the weakly-binding crossbridge accurately describes the behavior of the myosin-ATP crossbridge.

摘要

本文综述了在平衡条件下肌球蛋白横桥与肌动蛋白的相互作用。讨论了肌球蛋白横桥与肌动蛋白丝弱结合和强结合相互作用之间的异同。给出了弱结合横桥的精确、狭义定义。据推测,横桥与肌动蛋白弱结合和强结合平衡相互作用的根本区别在于,在第一种情况下,横桥头部在附着后是可移动的,而在第二种情况下则不是。有人认为,由于弱结合横桥头部在附着后是可移动的,因此这些头部似乎彼此独立发挥作用。附着的强结合横桥中头部缺乏移动性,使得强结合横桥头部似乎协同作用。这种强结合横桥模型对两个重要且无法用其他方式解释的观察结果给出了解释。它解释了为什么在小拉伸后力衰减的速率常数是核苷酸类似物浓度的S形函数,以及为什么在存在类似物或处于僵直状态时,小拉伸后力衰减的速率常数通常明显慢于溶液中肌球蛋白亚片段-1从肌动蛋白上脱离的速率常数。弱结合横桥模型准确地描述了肌球蛋白-ATP横桥的行为。

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