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NDRG2 a novel regulator of myoblast proliferation is regulated by anabolic and catabolic factors

机译:NDRG2是成肌细胞增殖的新型调节剂受合成代谢和分解代谢因子调节

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摘要

Skeletal muscle tissue undergoes adaptive changes in response to stress and the genes that control these processes are incompletely characterised. NDRG2 (N-myc downstream-regulated gene 2), a stress- and growth-related gene, was investigated in skeletal muscle growth and adaption. While NDRG2 expression levels were found to be up-regulated in both differentiated human and mouse myotubes compared with undifferentiated myoblasts, the suppression of NDRG2 in C2C12 myoblasts resulted in slowed myoblast proliferation. The increased expression levels of the cell cycle inhibitors, p21 Waf1/Cip1 and p27 Kip1, and of various muscle differentiation markers in NDRG2-deficient myoblasts indicate that a lack of NDRG2 promoted cell cycle exiting and the onset of myogenesis. Furthermore, the analysis of NDRG2 regulation in C2C12 myotubes treated with catabolic and anabolic agents and in skeletal muscle from human subjects following resistance exercise training revealed NDRG2 gene expression to be down-regulated during hypertrophic conditions, and conversely, up-regulated during muscle atrophy. Together, these data demonstrate that NDRG2 expression is highly responsive to different stress conditions in skeletal muscle and suggest that the level of NDRG2 expression may be critical to myoblast growth and differentiation.
机译:骨骼肌组织响应压力而发生适应性变化,控制这些过程的基因的特征不完整。 NDRG2(N-myc下游调控基因2)是与骨骼肌生长和适应有关的与压力和生长相关的基因。尽管与未分化的成肌细胞相比,在分化的人和小鼠肌管中NDRG2表达水平均被上调,但C2C12成肌细胞中NDRG2的抑制导致成肌细胞增殖减慢。在缺乏NDRG2的成肌细胞中,细胞周期抑制剂p21 Waf1 / Cip1和p27 Kip1以及各种肌肉分化标记物的表达水平增加,表明缺乏NDRG2促进了细胞周期的退出和成肌的开始。此外,在抵抗运动训练后,对使用分解代谢和合成代谢药物处理过的C2C12肌管以及人类受试者的骨骼肌中NDRG2调控的分析显示,NDRG2基因表达在肥大条件下被下调,反之在肌肉萎缩过程中被上调。在一起,这些数据表明NDRG2表达对骨骼肌中的不同应激条件具有高度响应,并表明NDRG2表达水平可能对成肌细胞的生长和分化至关重要。

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