| Literature DB >> 33520119 |
Jing Li1, Yujing Zhang1, Yangyang Ye1, Dameng Li1, Yuchen Liu1, Eunyoung Lee2,3, Mingliang Zhang4, Xin Dai5, Xiang Zhang1, Shibei Wang1, Junfeng Zhang1, Weiping Jia4, Ke Zen1, Antonio Vidal-Puig1,3,6,7, Xiaohong Jiang1, Chen-Yu Zhang1.
Abstract
Secreted microRNAs (miRNAs) are novel endocrine factors that play essential pathological and physiological roles. Here, we report that pancreatic β cell-released exosomal miR-29 family members (miR-29s) regulate hepatic insulin sensitivity and control glucose homeostasis. Cultured pancreatic islets were shown to secrete miR-29s in response to high levels of free fatty acids (FFAs) in vitro. In vivo, high levels of FFAs, promoted by either high-fat diet (HFD) feeding (physiopathological) or fasting (physiological), increased the secretion of miR-29s into plasma. Intravenous administration of exosomal miR-29s attenuated insulin sensitivity. The overexpression of miR-29s in the β cells of transgenic (TG) mice promoted the secretion of miR-29s and inhibited the insulin-mediated suppression of glucose output in the liver. We used selective overexpression of traceable heterogenous mutant miR-29s in β cells to confirm that islet-derived exosomal miR-29s target insulin signalling in the liver and blunt hepatic insulin sensitivity. Moreover, in vivo disruption of miR-29s expression in β cells reversed HFD-induced insulin resistance. In vitro experiments demonstrated that isolated exosomes enriched in miR-29s inhibited insulin signalling in the liver and increased hepatic glucose production. These results unveil a novel β cell-derived secretory signal-exosomal miR-29s-and provide insight into the roles of miR-29s in manipulating glucose homeostasis.Entities:
Keywords: exosomal miRNAs; glucose homeostasis; pancreatic β cell‐released miRNAs
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Year: 2021 PMID: 33520119 PMCID: PMC7820156 DOI: 10.1002/jev2.12055
Source DB: PubMed Journal: J Extracell Vesicles ISSN: 2001-3078