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首页> 外文期刊>EMBO Molecular Medicine >MicroRNA‐146b promotes adipogenesis by suppressing the SIRT1‐FOXO1 cascade
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MicroRNA‐146b promotes adipogenesis by suppressing the SIRT1‐FOXO1 cascade

机译:MicroRNA‐146b通过抑制SIRT1-FOXO1级联反应促进脂肪生成

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AbstractSirtuin 1 (SIRT1) plays a critical role in the maintenance of metabolic homeostasis and promotes fat mobilization in white adipose tissue. However, regulation of SIRT1 during adipogenesis, particularly through microRNAs, remains unclear. We observed that miR-146b expression was markedly increased during adipogenesis in 3T3-L1 cells. Differentiation of 3T3-L1 was induced by overexpression of miR-146b. Conversely, inhibition of miR-146b decreased adipocyte differentiation. Bioinformatics-based studies suggested that SIRT1 is a target of miR-146b. Further analysis confirmed that SIRT1 was negatively regulated by miR-146b. We also observed that miR-146b bound directly to the 3′-untranslated region of SIRT1 and inhibited adipogenesis through SIRT1 downregulation. The miR-146b/SIRT1 axis mediates adipogenesis through increased acetylation of forkhead box O1 (FOXO1). Expression of miR-146b was increased and SIRT1 mRNA subsequently decreased in the adipose tissues of diet-induced and genetically obese mice. Furthermore, in vivo knockdown of miR-146b by a locked nucleic acid miR-146b antagomir significantly reduced body weight and fat volume in accordance with upregulation of SIRT1 and subsequent acetylation of FOXO1. Therefore, the miR-146b/SIRT1 pathway could be a potential target for obesity prevention and treatment.
机译:摘要Sirtuin 1(SIRT1)在维持代谢稳态中起着关键作用,并促进白色脂肪组织中的脂肪动员。但是,尚不清楚在脂肪形成过程中SIRT1的调控,特别是通过微小RNA的调控。我们观察到,在3T3-L1细胞的脂肪形成过程中,miR-146b表达显着增加。 miR-146b的过表达诱导了3T3-L1的分化。相反,抑制miR-146b会降低脂肪细胞的分化。基于生物信息学的研究表明,SIRT1是miR-146b的靶标。进一步分析证实,SIRT1被miR-146b负调控。我们还观察到miR-146b直接与SIRT1的3'-非翻译区结合,并通过SIRT1下调抑制脂肪生成。 miR-146b / SIRT1轴通过叉头盒O1(FOXO1)的乙酰化增加来介导脂肪形成。在饮食诱导和遗传性肥胖小鼠的脂肪组织中,miR-146b的表达增加,SIRT1 mRNA随后减少。此外,根据SIRT1的上调和随后FOXO1的乙酰化作用,通过锁定的核酸miR-146b antagomir对miR-146b的体内敲除显着降低了体重和脂肪量。因此,miR-146b / SIRT1途径可能是肥胖症预防和治疗的潜在目标。

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