International Journal of Molecular Sciences (Aug 2022)

Involvement of Ferroptosis in Diabetes-Induced Liver Pathology

  • Ana Stancic,
  • Ksenija Velickovic,
  • Milica Markelic,
  • Ilijana Grigorov,
  • Tamara Saksida,
  • Nevena Savic,
  • Milica Vucetic,
  • Vesna Martinovic,
  • Andjelija Ivanovic,
  • Vesna Otasevic

DOI
https://doi.org/10.3390/ijms23169309
Journal volume & issue
Vol. 23, no. 16
p. 9309

Abstract

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Cell death plays an important role in diabetes-induced liver dysfunction. Ferroptosis is a newly defined regulated cell death caused by iron-dependent lipid peroxidation. Our previous studies have shown that high glucose and streptozotocin (STZ) cause β-cell death through ferroptosis and that ferrostatin-1 (Fer-1), an inhibitor of ferroptosis, improves β-cell viability, islet morphology, and function. This study was aimed to examine in vivo the involvement of ferroptosis in diabetes-related pathological changes in the liver. For this purpose, male C57BL/6 mice, in which diabetes was induced with STZ (40 mg/kg/5 consecutive days), were treated with Fer-1 (1 mg/kg, from day 1–21 day). It was found that in diabetic mice Fer-1 improved serum levels of ALT and triglycerides and decreased liver fibrosis, hepatocytes size, and binucleation. This improvement was due to the Fer-1-induced attenuation of ferroptotic events in the liver of diabetic mice, such as accumulation of pro-oxidative parameters (iron, lipofuscin, 4-HNE), decrease in expression level/activity of antioxidative defense-related molecules (GPX4, Nrf2, xCT, GSH, GCL, HO-1, SOD), and HMGB1 translocation from nucleus into cytosol. We concluded that ferroptosis contributes to diabetes-related pathological changes in the liver and that the targeting of ferroptosis represents a promising approach in the management of diabetes-induced liver injury.

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