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首页> 外文期刊>The Journal of Physiology >Phosphocreatine as an energy source for actin cytoskeletal rearrangements during myoblast fusion.
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Phosphocreatine as an energy source for actin cytoskeletal rearrangements during myoblast fusion.

机译:磷酸肌酸是成肌细胞融合过程中肌动蛋白细胞骨架重排的能源。

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摘要

Myoblast fusion is essential for muscle development, postnatal growth and muscle repair after injury. Recent studies have demonstrated roles for actin polymerization during myoblast fusion. Dynamic cytoskeletal assemblies directing cell-cell contact, membrane coalescence and ultimately fusion require substantial cellular energy demands. Various energy generating systems exist in cells but the partitioning of energy sources during myoblast fusion is unknown. Here, we demonstrate a novel role for phosphocreatine (PCr) as a spatiotemporal energy buffer during primary mouse myoblast fusion with nascent myotubes. Creatine treatment enhanced cell fusion in a creatine kinase (CK)-dependent manner suggesting that ATP-consuming reactions are replenished through the PCr/CK system. Furthermore, selective inhibition of actin polymerization prevented myonuclear addition following creatine treatment. As myotube formation is dependent on cytoskeletal reorganization, our findings suggest that PCr hydrolysis is coupledto actin dynamics during myoblast fusion. We conclude that myoblast fusion is a high-energy process, and can be enhanced by PCr buffering of energy demands during actin cytoskeletal rearrangements in myoblast fusion. These findings implicate roles for PCr as a high-energy phosphate buffer in the fusion of multiple cell types including sperm/oocyte, trophoblasts and macrophages. Furthermore, our results suggest the observed beneficial effects of oral creatine supplementation in humans may result in part from enhanced myoblast fusion.
机译:成肌细胞融合对于损伤后的肌肉发育,产后生长和肌肉修复至关重要。最近的研究表明肌动蛋白融合过程中肌动蛋白的聚合作用。指导细胞与细胞接触,膜聚结以及最终融合的动态细胞骨架组装需要大量的细胞能量需求。细胞中存在各种能量产生系统,但是成肌细胞融合过程中能量的分配是未知的。在这里,我们展示了磷酸肌酸(PCr)作为初生小鼠成肌细胞与新生肌管融合时空时空缓冲的新型作用。肌酸治疗以肌酸激酶(CK)依赖的方式增强了细胞融合,表明通过PCr / CK系统补充了ATP消耗反应。此外,肌动蛋白聚合的选择性抑制阻止了肌酸处理后肌核的添加。由于肌管的形成取决于细胞骨架的重组,因此我们的发现表明,成肌细胞融合过程中PCr水解与肌动蛋白动力学相关。我们得出结论,成肌细胞融合是一个高能量的过程,可以通过肌动蛋白融合中肌动蛋白细胞骨架重排过程中能量需求的PCr缓冲来增强。这些发现暗示了PCr作为高能磷酸盐缓冲液在多种细胞类型(包括精子/卵母细胞,滋养细胞和巨噬细胞)融合中的作用。此外,我们的结果表明,观察到的口服肌酸对人体的有益作用可能部分源于成肌细胞融合的增强。

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