DJ‐1 plays an obligatory role in the cardioprotection of delayed hypoxic preconditioning against hypoxia/reoxygenation‐induced oxidative stress through maintaining mitochondrial complex I activity

DJ‐1 was recently reported to mediate the cardioprotection of delayed hypoxic preconditioning (DHP) by suppressing hypoxia/reoxygenation (H/R)‐induced oxidative stress, but its mechanism against H/R‐induced oxidative stress during DHP is not fully elucidated. Here, using the well‐established cellula...

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Bibliographic Details
Published in:Cell biochemistry and function 2018-04, Vol.36 (3), p.147-154
Main Authors: Ding, Hao, Xu, Xing‐Wang, Wang, Huan, Xiao, Lin, Zhao, Le, Duan, Guang‐Ling, Li, Xiao‐Ran, Ma, Zhao‐Xia, Chen, He‐Ping
Format: Article
Language:English
Subjects:
delayed hypoxic preconditioning
DJ‐1
Electron transport chain
Glutathione
Hypoxia
hypoxia/reoxygenation
L-Lactate dehydrogenase
Lactate dehydrogenase
Lactic acid
Malondialdehyde
Mitochondria
mitochondrial complex I
NADH-ubiquinone oxidoreductase
Oxidation
Oxidative stress
Pharmacology
Preconditioning
Reactive oxygen species
Ribonucleic acid
RNA
Rotenone
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Summary:DJ‐1 was recently reported to mediate the cardioprotection of delayed hypoxic preconditioning (DHP) by suppressing hypoxia/reoxygenation (H/R)‐induced oxidative stress, but its mechanism against H/R‐induced oxidative stress during DHP is not fully elucidated. Here, using the well‐established cellular model of DHP, we again found that DHP significantly improved cell viability and reduced lactate dehydrogenase release with concurrently up‐regulated DJ‐1 protein expression in H9c2 cells subjected to H/R. Importantly, DHP efficiently improved mitochondrial complex I activity following H/R and attenuated H/R‐induced mitochondrial reactive oxygen species (ROS) generation and subsequent oxidative stress, as demonstrated by a much smaller decrease in reduced glutathione/oxidized glutathione ratio and a much smaller increase in intracellular ROS and malondialdehyde contents than that observed for the H/R group. However, the aforementioned effects of DHP were antagonized by DJ‐1 knockdown with short hairpin RNA but mimicked by DJ‐1 overexpression. Intriguingly, pharmacological inhibition of mitochondria complex I with Rotenone attenuated all the protective effects caused by DHP and DJ‐1 overexpression, including maintenance of mitochondria complex I and suppression of mitochondrial ROS generation and subsequent oxidative stress. Taken together, this work revealed that preserving mitochondrial complex I activity and subsequently inhibiting mitochondrial ROS generation could be a novel mechanism by which DJ‐1 mediates the cardioprotection of DHP against H/R‐induced oxidative stress damage.
ISSN:0263-6484
1099-0844
DOI:10.1002/cbf.3326