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首页> 外文期刊>Molecular Metabolism >microRNA-205-5p is a modulator of insulin sensitivity that inhibits FOXO function
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microRNA-205-5p is a modulator of insulin sensitivity that inhibits FOXO function

机译:microRNA-205-5p是胰岛素敏感性调节剂,可抑制FOXO功能

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摘要

Objectives Hepatic insulin resistance is a hallmark of type 2 diabetes and obesity. Insulin receptor signaling through AKT and FOXO has important metabolic effects that have traditionally been ascribed to regulation of gene expression. However, whether all the metabolic effects of FOXO arise from its regulation of protein-encoding mRNAs is unknown. Methods To address this question, we obtained expression profiles of FOXO-regulated murine hepatic microRNAs (miRNAs) during fasting and refeeding using mice lacking Foxo1, 3a, and 4 in liver (L-Foxo1,3a, 4). Results Out of 439 miRNA analyzed, 175 were differentially expressed in Foxo knockouts. Their functions were associated with insulin, Wnt, Mapk signaling, and aging. Among them, we report a striking increase of miR-205-5p expression in L-Foxo1,3a,4 knockouts, as well as in obese mice. We show that miR-205-5p gain-of-function increases AKT phosphorylation and decreases SHIP2 in primary hepatocytes, resulting in FOXO inhibition. This results in decreased hepatocyte glucose production. Consistent with these observations, miR-205-5p gain-of-function in mice lowered glucose levels and improved pyruvate tolerance. Conclusions These findings reveal a homeostatic miRNA loop regulating insulin signaling, with potential implications for in?vivo glucose metabolism.
机译:目的肝胰岛素抵抗是2型糖尿病和肥胖症的标志。通过AKT和FOXO传递的胰岛素受体信号具有重要的代谢作用,传统上将其归因于基因表达的调节。但是,尚不清楚FOXO的所有代谢作用是否都来自其对蛋白质编码mRNA的调节。方法为了解决这个问题,我们使用了在肝脏中缺乏Foxo1、3a和4的小鼠(L-Foxo1、3a,4),在禁食和重新喂养期间获得了FOXO调节的小鼠肝微小RNA(miRNA)的表达谱。结果在分析的439个miRNA中,有175个在Foxo基因敲除物中差异表达。它们的功能与胰岛素,Wnt,Mapk信号传导和衰老有关。其中,我们报告了在L-Foxo1,3a,4基因敲除以及肥胖小鼠中miR-205-5p表达的惊人增加。我们显示,miR-205-5p功能获得性增加了AKT磷酸化并降低了原代肝细胞中的SHIP2,从而抑制了FOXO。这导致肝细胞葡萄糖产生减少。与这些观察结果一致,miR-205-5p在小鼠中的功能获得降低了葡萄糖水平并提高了丙酮酸耐受性。结论这些发现揭示了调节胰岛素信号的稳态miRNA环,对体内葡萄糖代谢具有潜在的影响。

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