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m-钙蛋白酶在肌肉前体细胞激活过程中对细胞周期的影响。

m-Calpain implication in cell cycle during muscle precursor cell activation.

作者信息

Raynaud F, Carnac G, Marcilhac A, Benyamin Y

机构信息

UMR 5539-CNRS, Laboratoire de Motilité Cellulaire, EPHE, cc107, University of Montpellier 2 place Eugène Bataillon, 34090 France.

出版信息

Exp Cell Res. 2004 Aug 1;298(1):48-57. doi: 10.1016/j.yexcr.2004.03.053.

Abstract

Milli-calpain, a member of the ubiquitous cysteine protease family, is known to control late events of cell-cell fusion in skeletal muscle tissue through its involvement in cell membrane and cytoskeleton component reorganization. In this report, we describe the characterization of m-calpain compartmentalization and activation during the initial steps of muscle precursor cell recruitment and differentiation. By immunofluorescence analysis, we show that m-calpain is present throughout the cell cycle in the nucleus of proliferating myoblast C2 cells. However, when myoblasts enter a quiescent/G0 stage, m-calpain staining is detected only in the cytoplasm. Moreover, comparison of healthy and injured muscle shows distinct m-calpain localization in satellite stem cells. Indeed, m-calpain is not found in quiescent satellite cells, but following muscle injury, when satellite cells start to proliferate, m-calpain appears in the nucleus. To determine the implication of m-calpain during the cell cycle progression, quiescent myoblasts were forced to re-enter the cell cycle in the presence or not of the specific calpain inhibitor MDL 28170. We demonstrate that this calpain inhibitor blocks the cell cycle, prevents accumulation of MyoD in the G1 phase and enhances Myf5 expression. These data support an important new role for m-calpain in the control of muscle precursor cell activation and thus suggest its possible implication during the initial events of muscle regeneration.

摘要

微钙蛋白酶是普遍存在的半胱氨酸蛋白酶家族的一员,已知它通过参与细胞膜和细胞骨架成分的重组来控制骨骼肌组织中细胞间融合的后期事件。在本报告中,我们描述了在肌肉前体细胞募集和分化的初始阶段微钙蛋白酶的区室化和激活特征。通过免疫荧光分析,我们发现微钙蛋白酶在增殖的成肌细胞C2细胞核的整个细胞周期中均有存在。然而,当成肌细胞进入静止/G0期时,仅在细胞质中检测到微钙蛋白酶染色。此外,对健康肌肉和损伤肌肉的比较显示,卫星干细胞中微钙蛋白酶的定位不同。实际上,在静止的卫星细胞中未发现微钙蛋白酶,但在肌肉损伤后,当卫星细胞开始增殖时,微钙蛋白酶出现在细胞核中。为了确定微钙蛋白酶在细胞周期进程中的作用,在存在或不存在特异性钙蛋白酶抑制剂MDL 28170的情况下,迫使静止的成肌细胞重新进入细胞周期。我们证明这种钙蛋白酶抑制剂会阻断细胞周期,阻止MyoD在G1期积累,并增强Myf5表达。这些数据支持了微钙蛋白酶在控制肌肉前体细胞激活方面的一个重要新作用,因此表明它可能在肌肉再生的初始事件中发挥作用。

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