Institute for Research in Biomedicine (IRB Barcelona), The Barcelona Institute of Science and Technology, 08028 Barcelona, Spain.
Centro de Investigación Biomédica en Red de Diabetes y Enfermedades Metabólicas Asociadas (CIBERDEM), 28029 Madrid, Spain.
Int J Mol Sci. 2023 Jan 29;24(3):2574. doi: 10.3390/ijms24032574.
Many lines of evidence demonstrate a correlation between liver glycogen content and food intake. We previously demonstrated that mice overexpressing protein targeting to glycogen (PTG) specifically in the liver-which have increased glycogen content in this organ-are protected from high-fat diet (HFD)-induced obesity by reduced food intake. However, the use of PTG to increase liver glycogen implies certain limitations. PTG stimulates glycogen synthesis but also inhibits the enzyme responsible for glycogen degradation. Furthermore, as PTG is a regulatory subunit of protein phosphatase 1 (PP1), which regulates many cellular functions, its overexpression could have side effects beyond the regulation of glycogen metabolism. Therefore, it is necessary to determine whether the direct activation of glycogen synthesis, without affecting its degradation or other cellular functions, has the same effects. To this end, we generated mice overexpressing a non-inactivatable form of glycogen synthase (GS) specifically in the liver (9A-MGS mice). Control and 9a-MGS mice were fed a standard diet (SD) or HFD for 16 weeks. Glucose tolerance and feeding behavior were analyzed. 9A-MGS mice showed an increase in hepatic glycogen in fed and fasting conditions. When fed an HFD, these animals preserved their hepatic energy state, had a reduced food intake, and presented a lower body weight and fat mass than control animals, without changes in energy expenditure. Furthermore, 9A-MGS animals showed improved glucose tolerance when fed an SD or HFD. Moreover, liver triacylglycerol levels that were increased after HFD feeding were lower in these mice. These results confirm that increased liver glycogen stores contribute to decreased appetite and improve glucose tolerance in mice fed an HFD. On the basis of our findings, strategies to preserve hepatic glycogen stores emerge as potential treatments for obesity and hyperglycemia.
大量证据表明肝糖原含量与食物摄入之间存在相关性。我们之前的研究表明,在肝脏中特异性过表达蛋白靶向糖原(PTG)的小鼠——其器官内糖原含量增加——通过减少食物摄入,从而免受高脂肪饮食(HFD)诱导的肥胖。然而,使用 PTG 来增加肝糖原存在一定的局限性。PTG 刺激糖原合成,但也抑制负责糖原降解的酶。此外,由于 PTG 是蛋白磷酸酶 1(PP1)的调节亚基,它调节许多细胞功能,其过表达可能会产生除调节糖原代谢之外的副作用。因此,有必要确定是否直接激活糖原合成而不影响其降解或其他细胞功能会产生相同的效果。为此,我们生成了特异性在肝脏中过表达不可失活形式的糖原合酶(GS)的小鼠(9A-MGS 小鼠)。对照和 9A-MGS 小鼠分别喂食标准饮食(SD)或 HFD 16 周。分析葡萄糖耐量和摄食行为。9A-MGS 小鼠在进食和禁食条件下肝糖原含量增加。当喂食 HFD 时,这些动物保持其肝能量状态,减少食物摄入,体重和脂肪质量低于对照动物,而能量消耗没有变化。此外,9A-MGS 动物在喂食 SD 或 HFD 时表现出改善的葡萄糖耐量。此外,喂食 HFD 后肝三酰甘油水平升高的情况在这些小鼠中较低。这些结果证实,增加肝糖原储存有助于减少喂食 HFD 的小鼠的食欲并改善其葡萄糖耐量。基于我们的发现,保留肝糖原储存的策略可能成为肥胖和高血糖的潜在治疗方法。
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