| Literature DB >> 25471065 |
Wei Liu1, Hongchao Cao1, Cheng Ye1, Cunjie Chang2, Minghua Lu3, Yanyan Jing1, Duo Zhang1, Xuan Yao1, Zhengjun Duan1, Hongfeng Xia1, Yu-Cheng Wang4, Jingjing Jiang5, Mo-Fang Liu3, Jun Yan2, Hao Ying1.
Abstract
Understanding the regulation of insulin signalling in tissues provides insights into carbohydrate and lipid metabolism in physiology and disease. Here we show that hepatic miR-378/378* expression changes in response to fasting and refeeding in mice. Mice overexpressing hepatic miR-378/378* exhibit pure hepatic insulin resistance. miR-378 inhibits hepatic insulin signalling through targeting p110α, a subunit of PI3K and hence a critical component of insulin signalling. Knockdown of hepatic p110α mimics the effect of miR-378, while restoration of p110α expression abolishes the action of miR-378 on insulin signalling as well as its systemic effects on glucose and lipid homeostasis. miR-378/378* knockout mice display hypoglycemia and increased hepatic triglyceride level with enhanced insulin sensitivity. Inhibition of hepatic p110α in miR-378/378* knockout mice corrects the abnormal glucose tolerance. Finally, we show that overexpression of hepatic miR-378/378* ameliorates hepatic steatosis in ob/ob mice without exacerbating hyperglycemia. Our findings establish fasting-responsive miR-378 as a critical regulator of hepatic insulin signalling.Entities:
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Year: 2014 PMID: 25471065 DOI: 10.1038/ncomms6684
Source DB: PubMed Journal: Nat Commun ISSN: 2041-1723 Impact factor: 14.919