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免疫蛋白质组学方法研究骨骼肌和心肌的兴奋 - 收缩偶联:mitsugumins揭示的分子见解

Immuno-proteomic approach to excitation--contraction coupling in skeletal and cardiac muscle: molecular insights revealed by the mitsugumins.

作者信息

Weisleder Noah, Takeshima Hiroshi, Ma Jianjie

机构信息

Department of Physiology and Biophysics, UMDNJ-Robert Wood Johnson Medical School, NJ 08854, USA.

出版信息

Cell Calcium. 2008 Jan;43(1):1-8. doi: 10.1016/j.ceca.2007.10.006. Epub 2007 Dec 3.

Abstract

A comprehensive understanding of excitation-contraction (E-C) coupling in skeletal and cardiac muscle requires that all the major components of the Ca(2+) release machinery be resolved. We utilized a unique immuno-proteomic approach to generate a monoclonal antibody library that targets proteins localized to the skeletal muscle triad junction, which provides a structural context to allow efficient E-C coupling. Screening of this library has identified several mitsugumins (MG); proteins that can be localized to the triad junction in mammalian skeletal muscle. Many of these proteins, including MG29 and junctophilin, are important components in maintaining the structural integrity of the triad junction. Other triad proteins, such as calumin, play a more direct role in regulation of muscle Ca(2+) homeostasis. We have recently identified a family of trimeric intracellular cation-selective (TRIC) channels that allow for K(+) movement into the endoplasmic or sarcoplasmic reticulum to counter a portion of the transient negative charge produced by Ca(2+) release into the cytosol. Further study of TRIC channel function and other novel mitsugumins will increase our understanding of E-C coupling and Ca(2+) homoeostasis in muscle physiology and pathophysiology.

摘要

全面理解骨骼肌和心肌中的兴奋-收缩(E-C)偶联需要解析Ca(2+)释放机制的所有主要成分。我们采用了一种独特的免疫蛋白质组学方法来生成一个单克隆抗体文库,该文库靶向定位于骨骼肌三联体连接处的蛋白质,三联体连接处为高效的E-C偶联提供了结构背景。对该文库的筛选已鉴定出几种三谷蛋白(MG);这些蛋白质可定位于哺乳动物骨骼肌的三联体连接处。其中许多蛋白质,包括MG29和连接蛋白,是维持三联体连接处结构完整性的重要成分。其他三联体蛋白,如钙结合蛋白,在调节肌肉Ca(2+)稳态中发挥更直接的作用。我们最近鉴定出了一个三聚体细胞内阳离子选择性(TRIC)通道家族,该通道允许K(+)进入内质网或肌浆网,以抵消Ca(2+)释放到细胞质中产生的部分瞬时负电荷。对TRIC通道功能和其他新型三谷蛋白的进一步研究将增进我们对肌肉生理学和病理生理学中E-C偶联和Ca(2+)稳态的理解。

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