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Prostaglandin F2α stimulates growth of skeletal muscle cells via an NFATC2-dependent pathway

机译:前列腺素F2α通过NFATC2依赖性途径刺激骨骼肌细胞的生长

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摘要

Skeletal muscle growth requires multiple steps to form large multinucleated muscle cells. Molecules that stimulate muscle growth may be therapeutic for muscle loss associated with aging, injury, or disease. However, few factors are known to increase muscle cell size. We demonstrate that prostaglandin F2α (PGF2α) as well as two analogues augment muscle cell size in vitro. This increased myotube size is not due to PGF2α-enhancing cell fusion that initially forms myotubes, but rather to PGF2α recruiting the fusion of cells with preexisting multinucleated cells. This growth is mediated through the PGF2α receptor (FP receptor). As the FP receptor can increase levels of intracellular calcium, the involvement of the calcium-regulated transcription factor nuclear factor of activated T cells (NFAT) in mediating PGF2α-enhanced cell growth was examined. We show that NFAT is activated by PGF2α, and the isoform NFATC2 is required for PGF2α-induced muscle cell growth and nuclear accretion, demonstrating the first intersection between prostaglandin receptor activation and NFAT signaling. Given this novel role for PGF2α in skeletal muscle cell growth, these studies raise caution that extended use of drugs that inhibit PG production, such as nonsteroidal antiinflammatory drugs, may be deleterious for muscle growth.
机译:骨骼肌生长需要多个步骤才能形成大的多核肌肉细胞。刺激肌肉生长的分子可以治疗与衰老,受伤或疾病相关的肌肉丢失。但是,很少有因素会增加肌肉细胞的大小。我们证明前列腺素F2α(PGF2α)以及两个类似物在体外可增加肌肉细胞大小。这种增加的肌管大小不是由于最初形成肌管的PGF2α增强细胞融合,而是由于PGF2α募集了细胞与预先存在的多核细胞的融合。这种生长是通过PGF2α受体(FP受体)介导的。由于FP受体可以增加细胞内钙的水平,因此研究了活化T细胞的钙调节转录因子核因子(NFAT)在介导PGF2α增强的细胞生长中的参与。我们显示NFAT被PGF2α激活,而亚型NFATC2是PGF2α诱导的肌肉细胞生长和核增生所必需的,这表明前列腺素受体激活和NFAT信号之间的第一个交集。鉴于PGF2α在骨骼肌细胞生长中具有这种新颖的作用,这些研究引起了人们的警惕,即长期使用抑制PG产生的药物(例如非甾体类抗炎药)可能对肌肉生长有害。

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