Obesity-induced overexpression of miR-802 impairs insulin transcription and secretion.
Fangfang ZhangDongshen MaWanli ZhaoDanwei WangTingsheng LiuYuhong LiuYue YangYue LiuJinming MuBingbing LiYanfeng ZhangYi PanChangying GuoHong DuLing LiXianghui FuZheng-Yu CaoLiang JinPublished in: Nature communications (2020)
B cell dysfunction due to obesity can be associated with alterations in the levels of micro-RNAs (miRNAs). However, the role of miRNAs in these processes remains elusive. Here, we show that miR-802 is increased in the pancreatic islets of obese mouse models and demonstrate that inducible transgenic overexpression of miR-802 in mice causes impaired insulin transcription and secretion. We identify Foxo1 as a transcription factor of miR-802 promoting its transcription, and NeuroD1 and Fzd5 as targets of miR-802-dependent silencing. Repression of NeuroD1 in β cell and primary islets impairs insulin transcription and reduction of Fzd5 in β cell, which, in turn, impairs Ca2+ signaling, thereby repressing calcium influx and decreasing insulin secretion. We functionally create a novel network between obesity and β cell dysfunction via miR-802 regulation. Elucidation of the impact of obesity on microRNA expression can broaden our understanding of pathophysiological development of diabetes.
Keyphrases
- cell proliferation
- type diabetes
- transcription factor
- long non coding rna
- long noncoding rna
- weight loss
- metabolic syndrome
- high fat diet induced
- insulin resistance
- poor prognosis
- single cell
- glycemic control
- weight gain
- cell therapy
- adipose tissue
- bariatric surgery
- signaling pathway
- single molecule
- sensitive detection
- fluorescent probe
- stress induced
- living cells