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Emerging role for regulated in development and DNA damage 1 (REDD1) in the regulation of skeletal muscle metabolism

机译:在骨骼肌代谢调节中对发育和DNA损伤1(REDD1)调控的新兴作用

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摘要

Since its discovery, the protein regulated in development and DNA damage 1 (REDD1) has been implicated in the cellular response to various stressors. Most notably, its role as a repressor of signaling through the central metabolic regulator, the mechanistic target of rapamycin in complex 1 (mTORC1) has gained considerable attention. Not surprisingly, changes in REDD1 mRNA and protein have been observed in skeletal muscle under various physiological conditions (e.g., nutrient consumption and resistance exercise) and pathological conditions (e.g., sepsis, alcoholism, diabetes, obesity) suggesting a role for REDD1 in regulating mTORC1-dependent skeletal muscle protein metabolism. Our understanding of the causative role of REDD1 in skeletal muscle metabolism is increasing mostly due to the availability of genetically modified mice in which the REDD1 gene is disrupted. Results from such studies provide support for an important role for REDD1 in the regulation of mTORC1 as well as reveal unexplored functions of this protein in relation to other aspects of skeletal muscle metabolism. The goal of this work is to provide a comprehensive review of the role of REDD1 (and its paralog REDD2) in skeletal muscle during both physiological and pathological conditions.
机译:自发现以来,在发育和DNA损伤1(REDD1)中受调节的蛋白质已参与细胞对各种应激源的反应。最显着的是,它作为通过中央代谢调节剂(复合物1中雷帕霉素的机械靶标)(mTORC1)的信号传导阻遏物的作用受到了广泛关注。毫不奇怪,在各种生理状况(例如营养消耗和抵抗运动)和病理状况(例如败血症,酒精中毒,糖尿病,肥胖)下,骨骼肌中REDD1 mRNA和蛋白质的变化均得到观察,表明REDD1在调节mTORC1中的作用依赖性骨骼肌蛋白代谢。我们对REDD1在骨骼肌代谢中的致病作用的了解日益增加,这主要是由于REDD1基因被破坏的转基因小鼠的可用性。这些研究的结果为REDD1在调节mTORC1中发挥重要作用提供了支持,并揭示了该蛋白与骨骼肌代谢其他方面相关的未开发功能。这项工作的目的是全面回顾REDD1(及其旁系REDD2)在生理和病理状况下在骨骼肌中的作用。

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