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骨骼肌中的心磷脂合成具有节律性,并可通过年龄和饮食进行调节。

Cardiolipin Synthesis in Skeletal Muscle Is Rhythmic and Modifiable by Age and Diet.

机构信息

Department of Biochemistry and Molecular Biology, The University of Texas Health Science Center at Houston, 6431 Fannin St., Houston, TX 77030, USA.

出版信息

Oxid Med Cell Longev. 2020 Jun 14;2020:5304768. doi: 10.1155/2020/5304768. eCollection 2020.

Abstract

Circadian clocks regulate metabolic processes in a tissue-specific manner, which deteriorates during aging. Skeletal muscle is the largest metabolic organ in our body, and our previous studies highlight a key role of circadian regulation of skeletal muscle mitochondria in healthy aging. However, a possible circadian regulation of cardiolipin (CL), the signature lipid class in the mitochondrial inner membrane, remains largely unclear. Here, we show that CL levels oscillate during the diurnal cycle in C2C12 myotubes. Disruption of the genes, encoding the ROR nuclear receptors in the secondary loop of the circadian oscillator, in C2C12 cells was found to dampen core circadian gene expression. Importantly, several genes involved in CL synthesis, including and , displayed rhythmic expression which was disrupted or diminished in Ror-deficient C2C12 cells. studies using skeletal muscle tissues collected from young and aged mice showed diverse effects of the clock and aging on the oscillatory expression of CL genes, and CL levels in skeletal muscle were enhanced in aged mice relative to young mice. Finally, consistent with a regulatory role of RORs, Nobiletin, a natural agonist of RORs, was found to partially restore transcripts levels of CL synthesis genes in aged muscle under a dietary challenge condition. Together, these observations highlight a rhythmic CL synthesis in skeletal muscle that is dependent on RORs and modifiable by age and diet.

摘要

生物钟以组织特异性的方式调节代谢过程,而这种调节在衰老过程中会恶化。骨骼肌是我们体内最大的代谢器官,我们之前的研究强调了生物钟对骨骼肌线粒体的调节在健康衰老中的关键作用。然而,生物钟对心磷脂(CL)的调节作用(CL 是线粒体内膜的标志性脂质)在很大程度上仍不清楚。在这里,我们发现在 C2C12 肌管中,CL 水平在昼夜节律中波动。在 C2C12 细胞中,破坏生物钟振荡器二级环中编码 ROR 核受体的 基因,会抑制核心生物钟基因的表达。重要的是,几个参与 CL 合成的基因,包括 和 ,表现出节律性表达,而在 Ror 缺陷型 C2C12 细胞中,这种表达被打乱或减弱。使用从小鼠中收集的年轻和衰老的骨骼肌组织进行的 研究表明,时钟和衰老对 CL 基因的振荡表达有不同的影响,并且与年轻小鼠相比,衰老小鼠的骨骼肌中 CL 水平增强。最后,与 RORs 的调节作用一致,一种天然的 RORs 激动剂诺贝汀被发现可以在饮食挑战条件下部分恢复衰老肌肉中 CL 合成基因的转录水平。综上所述,这些观察结果强调了骨骼肌中存在节律性的 CL 合成,这种合成依赖于 RORs,并可被年龄和饮食所调节。

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