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首页> 外文期刊>Molecular Metabolism >Beige fat is dispensable for the metabolic benefits associated with myostatin deletion
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Beige fat is dispensable for the metabolic benefits associated with myostatin deletion

机译:米色脂肪可分配与肌球蛋白删除相关的代谢益处

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Objective Increasing muscle mass and activating beige fat both have great potential for ameliorating obesity and its comorbidities. Myostatin null mice have increased skeletal muscle mass and are protected from obesity and its sequelae. Deletion of myostatin has also been suggested to result in the activation of beige adipocytes, thermogenic fat cells with anti-obesity and anti-diabetes properties. It is not known whether beige fat activation contributes to the protection from obesity in myostatin null mice. Methods To investigate the role of beige fat activation in the metabolic benefits associated with myostatin deletion, we crossed myostatin null mice to adipocyte-specific PRDM16 knockout mice. We analyzed this new mouse model using molecular profiling, whole mount three-dimensional tissue imaging, tissue respiration, and glucose and insulin tolerance tests in models of diet-induced obesity. Results Here, we report that PRDM16 is required for the activation of beige fat in the absence of myostatin. However, we show in both male and female mice that beige fat activation is dispensable for the protection from obesity, glucose intolerance, insulin resistance, and hepatic steatosis mediated by myostatin deletion. Conclusion These findings demonstrate that increasing muscle mass can compensate for the inactivation of beige fat and raise the possibility of targeting muscle mass as a therapeutic approach to offset the deleterious effects of adipose tissue dysfunction in obesity and metabolic syndrome.
机译:目的增加肌肉质量和激活米色脂肪都具有改善肥胖及其合并症的巨大潜力。肌肉抑制素核小鼠具有增加的骨骼肌肿块,受到肥胖和后遗症的保护。还提出了肌肉素的缺失,导致米色脂肪细胞的激活,具有抗肥胖和抗糖尿病性能的热脂肪细胞。不知道米色脂肪活化是否有助于免受肥胖的肥胖症患者肌肤小鼠的保护。研究探讨米色脂肪活化在与肌肌热素缺失相关的代谢益处中的作用的方法,我们将肌肉抑制素Null小鼠交叉给脂肪细胞特异性PRDM16敲除小鼠。我们使用分子分析,全部安装三维组织成像,组织呼吸和葡萄糖和胰岛素耐受试验在饮食诱导的肥胖模型中分析了这种新的小鼠模型。结果在此,我们报告称PRDM16是在没有肌球素的情况下激活米色脂肪所必需的。然而,我们展示了肌肉和女性的小鼠,即米色脂肪活化可分配免受肥胖,葡萄糖不耐受,胰岛素抵抗和由Myostatin缺失介导的肝脏脂肪变性的保护。结论这些研究结果表明,肌肉质量增加可以补偿米色脂肪的失活,并提高靶向肌肉质量作为治疗方法的可能性,以抵消肥胖组织功能障碍在肥胖症和代谢综合征中的有害影响。

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