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心肌肌球蛋白结合蛋白C

Cardiac myosin binding protein C.

作者信息

Winegrad S

机构信息

Department of Physiology, School of Medicine, University of Pennsylvania, Philadelphia, PA 19104-6085, USA.

出版信息

Circ Res. 1999 May 28;84(10):1117-26. doi: 10.1161/01.res.84.10.1117.

Abstract

Myosin binding protein C (MyBP-C) is one of a group of myosin binding proteins that are present in the myofibrils of all striated muscle. The protein is found at 43-nm repeats along 7 to 9 transverse lines in a portion of the A band where crossbridges are found (C zone). MyBP-C contains myosin and titin binding sites at the C terminus of the molecule in all 3 of the isoforms (slow skeletal, fast skeletal, and cardiac). The cardiac isoform also includes a series of residues that contain 3 phosphorylatable sites and an additional immunoglobulin module at the N terminus that are not present in skeletal isoforms. The following 2 major functions of MyBP-C have been suggested: (1) a role in the formation of the sarcomeric myofibril as a result of binding to myosin and titin and (2) in the case of the cardiac isoform, regulation of contraction through phosphorylation. The first is supported by the demonstrated effect of MyBP-C on the packing of myosin in the thick filament, the coincidence of appearance of sarcomeres and MyBP-C during myofibrillogenesis, and the defective formation of sarcomeres when the titin and/or myosin binding sites of MyBP-C are missing. The second is supported by the specific phosphorylation sites in cardiac MyBP-C, the presence in the thick filament of an enzyme specific for MyBP-C phosphorylation, the alteration of thick filament structure by MyBP-C phosphorylation, and the accompaniment of MyBP-C phosphorylation with all major physiological mechanisms of modulation of inotropy in the heart.

摘要

肌球蛋白结合蛋白C(MyBP-C)是一组肌球蛋白结合蛋白之一,存在于所有横纹肌的肌原纤维中。在有横桥的A带的一部分(C区)中,沿着7至9条横向线以43纳米的重复间距发现该蛋白。在所有三种同工型(慢肌型、快肌型和心肌型)中,MyBP-C在分子的C末端都含有肌球蛋白和肌联蛋白结合位点。心肌同工型还包括一系列含有3个可磷酸化位点的残基,以及在N末端有一个额外的免疫球蛋白模块,而这些在骨骼肌同工型中不存在。MyBP-C有以下两个主要功能:(1)通过与肌球蛋白和肌联蛋白结合,在肌节肌原纤维的形成中发挥作用;(2)对于心肌同工型,通过磷酸化调节收缩。第一个功能得到了MyBP-C对粗肌丝中肌球蛋白组装的影响、肌节和MyBP-C在肌原纤维生成过程中出现的一致性,以及当MyBP-C的肌联蛋白和/或肌球蛋白结合位点缺失时肌节形成缺陷的支持。第二个功能得到了心肌MyBP-C中的特定磷酸化位点、粗肌丝中存在的一种对MyBP-C磷酸化具有特异性的酶、MyBP-C磷酸化对粗肌丝结构的改变,以及MyBP-C磷酸化与心脏收缩力调节的所有主要生理机制相伴出现的支持。

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