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脊椎动物横纹肌中的肌球蛋白轻链磷酸化:调节与功能

Myosin light chain phosphorylation in vertebrate striated muscle: regulation and function.

作者信息

Sweeney H L, Bowman B F, Stull J T

机构信息

Department of Physiology, University of Pennsylvania School of Medicine, Philadelphia 19104.

出版信息

Am J Physiol. 1993 May;264(5 Pt 1):C1085-95. doi: 10.1152/ajpcell.1993.264.5.C1085.

Abstract

The regulatory light chain of myosin (RLC) is phosphorylated in striated muscles by Ca2+/calmodulin-dependent myosin light chain kinase. Unique biochemical and cellular properties of this phosphorylation system in fast-twitch skeletal muscle maintain RLC in the phosphorylated form for a prolonged period after a brief tetanus or during low-frequency repetitive stimulation. This phosphorylation correlates with potentiation of the rate of development and maximal extent of isometric twitch tension. In skinned fibers, RLC phosphorylation increases force production at low levels of Ca2+ activation, via a leftward shift of the force-pCa relationship, and increases the rate of force development over a wide range of activation levels. In heart and slow-twitch skeletal muscle, the functional consequences of RLC phosphorylation are probably similar, and the primary physiological determinants are phosphorylation and dephosphorylation properties unique to each muscle. The mechanism for these physiological responses probably involves movement of the phosphorylated myosin cross bridges away from the thick-filament backbone. The movement of cross bridges may also contribute to the regulation of myosin interactions with actin in vertebrate smooth and invertebrate striated muscles.

摘要

肌球蛋白的调节轻链(RLC)在横纹肌中由Ca2+/钙调蛋白依赖性肌球蛋白轻链激酶磷酸化。快速收缩骨骼肌中这种磷酸化系统独特的生化和细胞特性,在短暂强直收缩后或低频重复刺激期间,能使RLC长时间保持磷酸化状态。这种磷酸化与等长收缩张力的发展速率增强以及最大程度增强相关。在去膜纤维中,RLC磷酸化通过力-pCa关系向左移动,在低水平Ca2+激活时增加力的产生,并在广泛的激活水平范围内增加力的发展速率。在心脏和慢收缩骨骼肌中,RLC磷酸化的功能后果可能相似,而主要的生理决定因素是每种肌肉特有的磷酸化和去磷酸化特性。这些生理反应的机制可能涉及磷酸化的肌球蛋白横桥从粗肌丝主干移开。横桥的移动也可能有助于调节脊椎动物平滑肌和无脊椎动物横纹肌中肌球蛋白与肌动蛋白的相互作用。

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