Hexavalent chromium [Cr(VI)] has aroused the main interest of environmental health researchers due to its high toxicity. Liver is the main target organ of Cr(VI), and the purpose of this study was to explore whether mitophagy contributes to Cr(VI)-induced hepatotoxicity and to demonstrate the potential mechanisms. Cr(VI) exposure induced mitochondrial loss, energy metabolism disorders and cell apoptosis, which were associated with the occurrence of excessive mitophagy characterized by the increased number of green fluorescent protein-microtubule-associated protein light chain 3 (GFP-LC3) puncta and lysosomal colocalization with mitochondria. In addition, the suppression of mitophagy by autophagy-related 5 (ATG5) siRNA can effectively inhibit Cr(VI)-induced mitochondrial loss and cytotoxicity. In summary, we reached the conclusion that Cr(VI)-induced overactive mitophagy contributes to mitochondrial loss and cytotoxicity in L02 hepatocytes, which will further reveal the possible mechanisms of Cr(VI)-induced hepatotoxicity, and provide a new experimental basis for the study of the health hazard effects of chromium.
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July 2020
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Cover Image
Cover Image
3D reconstruction of septin filaments, which orientation is colour coded, bound to liposomes (purple) and obtained by cryo-electron tomography. The polymerization of Shs1 capped protomers is enhanced in the presence of biomimetic membranes. For more information, see the article by Taveneau and colleagues in this issue (pp. 2697–2714). The image was provided by Aurélie Bertin.
Research Article|
July 24 2020
Cr(VI)-induced overactive mitophagy contributes to mitochondrial loss and cytotoxicity in L02 hepatocytes
Biochem J (2020) 477 (14): 2607–2619.
Article history
Received:
March 29 2020
Revision Received:
June 22 2020
Accepted:
June 26 2020
Accepted Manuscript online:
June 29 2020
