The mechanism of long non‐coding RNA MEG3 for hepatic ischemia‐reperfusion: Mediated by miR‐34a/Nrf2 signaling pathway

To investigate the function of MEG3 in hepatic ischemia‐reperfusion (HIR) progress, involving its association with the level of miR‐34a during hypoxia‐induced hypoxia re‐oxygenation (H/R) in vitro. HIR mice model in vivo was established. MEG3, miR‐34a expression, along with Nrf2 mRNA and protein level were detected in tissues and cells. Serum biochemical parameters (ALT and AST) were assessed in vivo. A potential binding region between MEG3 and miR34a was confirmed by luciferase assays. Hepatic cells HL7702 were subjected to hypoxia treatment in vitro for functional studies, including TUNEL‐positive cells detection and ROS analysis. MEG3, Nrf2 expression was significantly down‐regulated in infarction lesion from HIR mice, as opposed to increased miR‐34a production, while similar results were also observed in H/R HL7702 cells, while the above effects were reversed by MEG3 over‐expression. By using bioinformatics study and RNA pull down combined with luciferase assays, we demonstrated that MEG3 functioned as a competing endogenous RNA (ceRNA) for miR‐34a, and there was reciprocal repression between MEG3 and miR‐34a in an Argonaute 2‐dependent manner. Functional studies demonstrated that MEG3 showed positive regulation on TUNEL‐positive cells and ROS level. Further in vivo study confirmed that MEG3 over‐expression could improve hepatic function of HIR mice, and markedly decreased the expression of serum ALT and AST. MEG3 protected hepatocytes from HIR injury through down‐regulating miR‐34a expression, which could add our understanding of the molecular mechanisms in HIR injury.