Mitochondrial iron overload mediated by cooperative transfer of plasma membrane ATP5B and TFR2 to mitochondria triggers hepatic insulin resistance under PFOS exposure

Mitochondrial iron overload mediated by cooperative transfer of plasma membrane ATP5B and TFR2 to mitochondria triggers hepatic insulin resistance under PFOS exposure

In general populations, insulin resistance (IR) is related to perfluorooctane sulfonate (PFOS), a persistent organic pollutant. However, the underlying mechanism remains unclear. In this study, PFOS induced mitochondrial iron accumulation in the liver of mice and human hepatocytes L-O2. In the PFOS-...

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Veröffentlicht in:Ecotoxicology and environmental safety 2023-03, Vol.253, p.114662-114662, Article 114662
Hauptverfasser: Wang, Jianyu, Wang, Jinling, Qiu, Tianming, Wu, Jialu, Sun, Xiance, Jiang, Liping, Liu, Xiaofang, Yang, Guang, Cao, Jun, Yao, Xiaofeng
Format: Artikel
Sprache:eng
Schlagworte:
Adenosine Triphosphate - metabolism
Cell Membrane - metabolism
Ectopic ATP synthase
Humans
Insulin Resistance
Iron - metabolism
Iron Overload
Liver - metabolism
Mitochondria - metabolism
Mitochondrial iron
Perfluorooctane sulphonate
Receptors, Transferrin - genetics
Receptors, Transferrin - metabolism
Transferrin receptor 2
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Zusammenfassung:In general populations, insulin resistance (IR) is related to perfluorooctane sulfonate (PFOS), a persistent organic pollutant. However, the underlying mechanism remains unclear. In this study, PFOS induced mitochondrial iron accumulation in the liver of mice and human hepatocytes L-O2. In the PFOS-treated L-O2 cells, mitochondrial iron overload preceded the occurrence of IR, and pharmacological inhibition of mitochondrial iron relieved PFOS-caused IR. Both transferrin receptor 2 (TFR2) and ATP synthase β subunit (ATP5B) were redistributed from the plasma membrane to mitochondria with PFOS treatment. Inhibiting the translocation of TFR2 to mitochondria reversed PFOS-induced mitochondrial iron overload and IR. In the PFOS-treated cells, ATP5B interacted with TFR2. Stabilizing ATP5B on the plasma membrane or knockdown of ATP5B disturbed the translocation of TFR2. PFOS inhibited the activity of plasma-membrane ATP synthase (ectopic ATP synthase, e-ATPS), and activating e-ATPS prevented the translocation of ATP5B and TFR2. Consistently, PFOS induced ATP5B/TFR2 interaction and redistribution of ATP5B and TFR2 to mitochondria in the liver of mice. Thus, our results indicated that mitochondrial iron overload induced by collaborative translocation of ATP5B and TFR2 was an up-stream and initiating event for PFOS-related hepatic IR, providing novel understandings of the biological function of e-ATPS, the regulatory mechanism for mitochondrial iron and the mechanism underlying PFOS toxicity. [Display omitted] •PFOS induces mitochondrial iron overload in vivo and in vitro.•Mitochondrial iron overload triggers hepatic IR upon PFOS exposure.•An increase in mitochondrial TFR2 mediates PFOS-induced mitochondrial iron overload.•ATP5B transfers TFR2 from the plasma membrane to mitochondria after PFOS treatment.•PFOS inhibits e-ATPS, which leads to the translocation of ATP5B and TFR2.
ISSN:0147-6513
1090-2414
DOI:10.1016/j.ecoenv.2023.114662