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首页> 外文期刊>Journal of Muscle Research and Cell Motility >Why choose myofibrils to study muscle myosin ATPase?
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Why choose myofibrils to study muscle myosin ATPase?

机译:为什么选择肌原纤维来研究肌肌球蛋白ATP酶?

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Our objective is to propose an overview of the usefulness of skeletal myofibril as an experimental system for studying mechanochemical coupling of skeletal muscles and myosin ATPase activity. The myofibril is a true functional mini-muscle that is able to contract in the presence of ATP. It also contains the machinery necessary for the calcium sensitivity of the contraction. In the absence of calcium, myofibrillar ATPase activity is basal, no shortening occurs and no active force is developed. In the presence of calcium, myofibrillar ATPase is activated and myofibrils either shorten with no external load (native myofibrils) or contract isometrically (cross-linked myofibrils). With this organised system, both chemical and mechanical studies can be carried out. For a decade, our laboratory has been using rabbit psoas myofibrils for exploring myosin ATPase activity. The first challenge was to successfully apply rapid kinetic approaches, such as rapid-flow-quench, to this organised system. Another challengewas to work with myofibrils in cryoenzymic conditions, i.e. in the presence of organic solvents and at sub-zero temperatures. In this overview, we highlight differences between the myosin ATPase in organised systems (myofibrils or fibres) and that of contractile proteins in solution (S1 or actoS1) that we observed using these approaches. We discuss the importance of these differences in terms of mechanochemical coupling. It is concluded that great care should be taken when extrapolating mechanochemical properties of the contractile proteins in solution to the whole muscle.
机译:我们的目标是概述骨骼肌原纤维作为研究骨骼肌机械化学偶联和肌球蛋白ATPase活性的实验系统的有用性。肌原纤维是一种真正的功能性微型肌肉,能够在ATP存在的情况下收缩。它还包含收缩钙敏感性所必需的机制。在没有钙的情况下,肌原纤维的ATP酶活性是基础的,不会发生缩短,也不会产生作用力。在钙的存在下,肌原纤维ATPase被激活,肌原纤维在无外部负荷的情况下缩短(天然肌原纤维)或等轴收缩(交联的肌原纤维)。有了这个有组织的系统,就可以进行化学和机械研究。十年来,我们的实验室一直在使用兔腰大肌肌原纤维来探索肌球蛋白ATPase的活性。第一个挑战是如何将快速动力学方法(例如快速流淬火)成功应用于此组织系统。另一个挑战是在低温酶促条件下,即在有机溶剂存在下和零下温度下,使用肌原纤维。在本概述中,我们重点介绍了使用这些方法观察到的有组织系统中的肌球蛋白ATPase(肌原纤维或纤维)与溶液中的收缩蛋白(S1或actoS1)之间的差异。我们讨论在机械化学耦合方面这些差异的重要性。结论是,将可收缩蛋白的机械化学特性外推到整个肌肉时应格外小心。

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