Insulin-induced gene 2 protects against hepatic ischemia-reperfusion injury via metabolic remodeling

J Transl Med. 2023 Oct 19;21(1):739. doi: 10.1186/s12967-023-04564-y.

Abstract

Background: Hepatic ischemia-reperfusion (IR) injury is the primary reason for complications following hepatectomy and liver transplantation (LT). Insulin-induced gene 2 (Insig2) is one of several proteins that anchor the reticulum in the cytoplasm and is essential for metabolism and inflammatory responses. However, its function in IR injury remains ambiguous.

Methods: Insig2 global knock-out (KO) mice and mice with adeno-associated-virus8 (AAV8)-delivered Insig2 hepatocyte-specific overexpression were subjected to a 70% hepatic IR model. Liver injury was assessed by monitoring hepatic histology, inflammatory responses, and apoptosis. Hypoxia/reoxygenation stimulation (H/R) of primary hepatocytes and hypoxia model induced by cobalt chloride (CoCl2) were used for in vitro experiments. Multi-omics analysis of transcriptomics, proteomics, and metabolomics was used to investigate the molecular mechanisms underlying Insig2.

Results: Hepatic Insig2 expression was significantly reduced in clinical samples undergoing LT and the mouse IR model. Our findings showed that Insig2 depletion significantly aggravated IR-induced hepatic inflammation, cell death and injury, whereas Insig2 overexpression caused the opposite phenotypes. The results of in vitro H/R experiments were consistent with those in vivo. Mechanistically, multi-omics analysis revealed that Insig2 is associated with increased antioxidant pentose phosphate pathway (PPP) activity. The inhibition of glucose-6-phosphate-dehydrogenase (G6PD), a rate-limiting enzyme of PPP, rescued the protective effect of Insig2 overexpression, exacerbating liver injury. Finally, our findings indicated that mouse IR injury could be attenuated by developing a nanoparticle delivery system that enables liver-targeted delivery of substrate of PPP (glucose 6-phosphate).

Conclusions: Insig2 has a protective function in liver IR by upregulating the PPP activity and remodeling glucose metabolism. The supplementary glucose 6-phosphate (G6P) salt may serve as a viable therapeutic target for alleviating hepatic IR.

Keywords: Glycolysis; Hepatic ischemia–reperfusion injury; Insulin-induced gene 2; Pentose phosphate pathway.

Publication types

  • Research Support, Non-U.S. Gov't

MeSH terms

  • Animals
  • Antioxidants / metabolism
  • Apoptosis / genetics
  • Glucose / metabolism
  • Hepatectomy / adverse effects
  • Hepatocytes* / metabolism
  • Hepatocytes* / pathology
  • Hypoxia / complications
  • Hypoxia / genetics
  • Hypoxia / metabolism
  • Insulins* / metabolism
  • Liver / blood supply
  • Liver / injuries
  • Liver / metabolism
  • Liver / pathology
  • Liver Diseases* / genetics
  • Liver Diseases* / metabolism
  • Liver Diseases* / pathology
  • Liver Diseases* / surgery
  • Liver Transplantation / adverse effects
  • Mice
  • Phosphates / metabolism
  • Phosphates / pharmacology
  • Reperfusion Injury* / genetics
  • Reperfusion Injury* / metabolism
  • Reperfusion Injury* / pathology
  • Reperfusion Injury* / prevention & control

Substances

  • Antioxidants
  • Glucose
  • Insig2 protein, mouse
  • Insulins
  • Phosphates