DUSP1 alleviates cardiac ischemia/reperfusion injury by suppressing the Mff-required mitochondrial fission and Bnip3-related mitophagy via the JNK pathways

Qinhua Jin; Ruibing Li; Nan Hu; Ting Xin; Pingjun Zhu; Shunying Hu; Sai Ma; Hong Zhu; Jun Ren; Hao Zhou

doi:10.1016/j.redox.2017.11.004

DUSP1 alleviates cardiac ischemia/reperfusion injury by suppressing the Mff-required mitochondrial fission and Bnip3-related mitophagy via the JNK pathways

Redox Biol. 2018 Apr:14:576-587. doi: 10.1016/j.redox.2017.11.004. Epub 2017 Nov 6.

Authors

Qinhua Jin¹, Ruibing Li², Nan Hu³, Ting Xin⁴, Pingjun Zhu¹, Shunying Hu¹, Sai Ma³, Hong Zhu³, Jun Ren³, Hao Zhou⁵

Affiliations

¹ Chinese PLA General Hospital, Medical School of Chinese PLA, Beijing 100853, China.
² Chinese PLA General Hospital, Medical School of Chinese PLA, Beijing 100853, China; Department of Human Genetics, Emory University, Atlanta, GA, 30322, USA.
³ Center for Cardiovascular Research and Alternative Medicine, Wyoming University, Laramie, WY 82071, USA.
⁴ Chinese PLA General Hospital, Medical School of Chinese PLA, Beijing 100853, China; Department of Cardiology, Tianjin First Central Hospital, Tianjin 300192, China.
⁵ Chinese PLA General Hospital, Medical School of Chinese PLA, Beijing 100853, China; Center for Cardiovascular Research and Alternative Medicine, Wyoming University, Laramie, WY 82071, USA. Electronic address: zhouhao301@outlook.com.

Abstract

Mitochondrial fission and selective mitochondrial autophagy (mitophagy) form an essential axis of mitochondrial quality control that plays a critical role in the development of cardiac ischemia-reperfusion (IR) injury. However, the precise upstream molecular mechanism of fission/mitophagy remains unclear. Dual-specificity protein phosphatase1 (DUSP1) regulates cardiac metabolism, but its physiological contribution in the reperfused heart, particularly its influence on mitochondrial homeostasis, is unknown. Here, we demonstrated that cardiac DUSP1 was downregulated following acute cardiac IR injury. In vivo, compared to wild-type mice, DUSP1 transgenic mice (DUSP1^TG mice) demonstrated a smaller infarcted area and the improved myocardial function. In vitro, the IR-induced DUSP1 deficiency promoted the activation of JNK which upregulated the expression of the mitochondrial fission factor (Mff). A higher expression level of Mff was associated with elevated mitochondrial fission and mitochondrial apoptosis. Additionally, the loss of DUSP1 also amplified the Bnip3 phosphorylated activation via JNK, leading to the activation of mitophagy. Increased mitophagy overtly consumed mitochondrial mass resulting into the mitochondrial metabolism disorder. However, the reintroduction of DUSP1 blunted Mff/Bnip3 activation and therefore alleviated the fatal mitochondrial fission/mitophagy by inactivating the JNK pathway, providing a survival advantage to myocardial tissue following IR stress. The results of our study suggest that DUSP1 and its downstream JNK pathway are therapeutic targets for conferring protection against IR injury by repressing Mff-mediated mitochondrial fission and Bnip3-required mitophagy.

Keywords: Bnip3; Cardiac IR injury; DUSP1; JNK; Mff; Mitochondrial fission; Mitophagy.

MeSH terms

Animals
Dual Specificity Phosphatase 1 / metabolism*
MAP Kinase Signaling System*
Membrane Proteins / metabolism*
Mice, Transgenic
Mitochondria, Heart / metabolism
Mitochondria, Heart / pathology
Mitochondrial Dynamics*
Mitochondrial Proteins / metabolism*
Mitophagy*
Myocardial Reperfusion Injury / metabolism*
Myocardial Reperfusion Injury / pathology
Myocardium / metabolism
Myocardium / pathology

Substances

BNip3 protein, mouse
Membrane Proteins
Mitochondrial Proteins
mitochondrial fission factor, mouse
Dual Specificity Phosphatase 1
Dusp1 protein, mouse