Steatotic hepatocyte‐derived extracellular vesicles promote β‐cell apoptosis and diabetes via microRNA‐126a‐3p.

Extracellular vesicles (EVs) have emerged as a unique mediator of interorgan communications, playing important roles in the pathophysiologic process of various diseases, including diabetes and other metabolic diseases. Here, we reported that the EVs released by steatotic hepatocytes exerted a detrimental effect on pancreatic β cells, leading to β‐cell apoptosis and dysfunction. The effect was profoundly attributable to an up‐regulation of miR‐126a‐3p in the steatotic hepatocyte‐derived EVs. Accordingly, overexpression of miR‐126a‐3p promoted, whereas inhibition of miR‐126a‐3p prevented β‐cell apoptosis, through a mechanism related to its target gene, insulin receptor substrate‐2. Moreover, inhibition of miR‐126a‐3p by its specific antagomir was able to partially reverse the loss of β‐cell mass and ameliorate hyperglycaemia in diabetic mice. Thus, the findings reveal a novel pathogenic role of steatotic hepatocyte‐derived EVs, which mechanistically links nonalcoholic fatty liver disease to the development of diabetes. [ABSTRACT FROM AUTHOR]