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脂肪细胞 Rnf20 缺失通过溶血磷脂酰胆碱 16:0 增加骨骼肌中的快肌纤维。

Adipocyte Rnf20 ablation increases the fast-twitch fibers of skeletal muscle via lysophosphatidylcholine 16:0.

机构信息

State Key Laboratory of Animal Biotech Breeding, Institute of Animal Science, Chinese Academy of Agricultural Sciences, Beijing, 100193, China.

College of Animal Science and Technology, China Agricultural University, Beijing, 100193, China.

出版信息

Cell Mol Life Sci. 2023 Aug 9;80(9):243. doi: 10.1007/s00018-023-04896-4.

Abstract

Both adipose tissue and skeletal muscle are highly dynamic tissues and interact at the metabolic and hormonal levels in response to internal and external stress, and they coordinate in maintaining whole-body metabolic homeostasis. In our previous study, we revealed that adipocyte-specific Rnf20 knockout mice (ASKO mice) exhibited lower fat mass but higher lean mass, providing a good model for investigating the adipose-muscle crosstalk and exploring the effect of the adipocyte Rnf20 gene on the physiology and metabolism of skeletal muscle. Here, we confirmed that ASKO mice exhibited the significantly increased body weight and gastrocnemius muscle weight. Fiber-type switching in the soleus muscle of ASKO mice was observed, as evidenced by the increased number of fast-twitch fibers and decreased number of slow-twitch fibers. Serum metabolites with significant alteration in abundance were identified by metabolomic analysis and the elevated lysophosphatidylcholine 16:0 [LysoPC (16:0)] was observed in ASKO mice. In addition, lipidome analysis of gonadal white adipose tissue revealed a significant increase in LysoPCs and LysoPC (16:0) in ASKO mice. Furthermore, knockdown of Rnf20 gene in 3T3-L1 cells significantly increased the secretion of LysoPC, suggesting that LysoPC might be a critical metabolite in the adipose-muscle crosstalk of ASKO mice. Furthermore, in vitro study demonstrated that LysoPC (16:0) could induce the expression of fast-twitch muscle fibers related genes in differentiated C2C12 cells, indicating its potential role in adipose-muscle crosstalk. Taken together, these findings not only expand our understanding of the biological functions of Rnf20 gene in systemic lipid metabolism, but also provide insight into adipose tissue dysfunction-induced physiological alterations in skeletal muscle.

摘要

脂肪组织和骨骼肌都是高度动态的组织,它们在代谢和激素水平上相互作用,以响应内部和外部压力,并且它们在维持全身代谢稳态方面协调一致。在我们之前的研究中,我们揭示了脂肪细胞特异性 Rnf20 敲除小鼠(ASKO 小鼠)表现出较低的脂肪量但较高的瘦肉量,为研究脂肪-肌肉串扰和探索脂肪细胞 Rnf20 基因对骨骼肌生理学和代谢的影响提供了良好的模型。在这里,我们证实 ASKO 小鼠表现出显著增加的体重和比目鱼肌重量。ASKO 小鼠的比目鱼肌纤维类型发生转换,表现为快肌纤维数量增加和慢肌纤维数量减少。通过代谢组学分析鉴定出丰度有显著改变的血清代谢物,并观察到 ASKO 小鼠中溶血磷脂酰胆碱 16:0 [LysoPC(16:0)] 的升高。此外,性腺白色脂肪组织的脂质组学分析显示 ASKO 小鼠中的 LysoPC 和 LysoPC(16:0)显著增加。此外,3T3-L1 细胞中 Rnf20 基因的敲低显著增加了 LysoPC 的分泌,表明 LysoPC 可能是 ASKO 小鼠脂肪-肌肉串扰的关键代谢物。此外,体外研究表明 LysoPC(16:0)可诱导分化的 C2C12 细胞中快肌纤维相关基因的表达,表明其在脂肪-肌肉串扰中的潜在作用。总之,这些发现不仅扩展了我们对 Rnf20 基因在全身脂质代谢中的生物学功能的理解,还深入了解了脂肪组织功能障碍引起的骨骼肌生理变化。

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