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Multiple signaling pathways regulate contractile activity‐mediated PGC‐1α gene expression and activity in skeletal muscle cells

机译:多种信号通路调节骨骼肌细胞中收缩活性介导的PGC-1α基因表达和活性

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摘要

PGC‐1α is an important transcriptional coactivator that plays a key role in mediating mitochondrial biogenesis. Within seconds of the onset of contractile activity, a number of rapid cellular events occur that form part of the initial signaling processes involved in PGC‐1α gene regulation, such as elevations in cytoplasmic calcium, AMPK and p38 activation, and elevated ROS production. We observed that basal levels of PGC‐1α promoter activity were more sensitive to resting Ca2+ levels, compared to ROS, p38 or, AMPK signaling. Moreover, enhanced PGC‐1α transcription and post‐translational activity on DNA were a result of the activation of multiple signal transduction pathways during contractile activity of myotubes. AMPK, ROS, and Ca2+ appear to be necessary for the regulation of contractile activity‐induced PGC‐1α gene expression, governed partly through p38 MAPK and CaMKII activity. Whether these signaling pathways are arranged as a linear sequence of events, or as largely independent pathways during contractile activity, remains to be determined.
机译:PGC-1α是重要的转录共激活因子,在介导线粒体生物发生中起关键作用。在收缩活动开始的几秒钟内,发生了许多快速的细胞事件,这些事件构成了参与PGC-1α基因调控的初始信号传导过程的一部分,例如细胞质钙,AMPK和p38活化的升高以及ROS生成的增加。我们观察到,与ROS,p38或AMPK信号传导相比,基础水平的PGC-1α启动子活性对静止的Ca 2 + 水平更为敏感。此外,增强的PGC-1α转录和对DNA的翻译后活性是肌管收缩活动过程中多个信号转导通路激活的结果。 AMPK,ROS和Ca 2 + 似乎是调节收缩活性诱导的PGC-1α基因表达所必需的,部分通过p38 MAPK和CaMKII活性来控制。这些信号传导途径是以事件的线性顺序排列,还是在收缩活动中以很大程度上独立的途径排列,尚待确定。

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