PHB2 ameliorates Doxorubicin-induced cardiomyopathy through interaction with NDUFV2 and restoration of mitochondrial complex I function

Mingjie Yang; Miyesaier Abudureyimu; Xiang Wang; Yuan Zhou; Yingmei Zhang; Jun Ren

doi:10.1016/j.redox.2023.102812

PHB2 ameliorates Doxorubicin-induced cardiomyopathy through interaction with NDUFV2 and restoration of mitochondrial complex I function

Redox Biol. 2023 Sep:65:102812. doi: 10.1016/j.redox.2023.102812. Epub 2023 Jul 12.

Authors

Mingjie Yang¹, Miyesaier Abudureyimu², Xiang Wang¹, Yuan Zhou³, Yingmei Zhang⁴, Jun Ren⁵

Affiliations

¹ Department of Cardiology, Zhongshan Hospital, Fudan University, Shanghai Institute of Cardiovascular Diseases, Shanghai, 200032, China; National Clinical Research Center for Interventional Medicine, Shanghai, 200032, China.
² Cardiovascular Department, Shanghai Xuhui Central Hospital, Fudan University, Shanghai, 200031, China.
³ Department of Biomedical Informatics, School of Basic Medical Sciences, Peking University, Beijing, 100191, China.
⁴ Department of Cardiology, Zhongshan Hospital, Fudan University, Shanghai Institute of Cardiovascular Diseases, Shanghai, 200032, China; National Clinical Research Center for Interventional Medicine, Shanghai, 200032, China. Electronic address: zhang.yingmei@zs-hospital.sh.cn.
⁵ Department of Cardiology, Zhongshan Hospital, Fudan University, Shanghai Institute of Cardiovascular Diseases, Shanghai, 200032, China; National Clinical Research Center for Interventional Medicine, Shanghai, 200032, China. Electronic address: ren.jun@zs-hospital.sh.cn.

Abstract

Background: Doxorubicin (DOX) is among the most widely employed antitumor agents, although its clinical applications have been largely hindered by severe cardiotoxicity. Earlier studies described an essential role of mitochondrial injury in the pathogenesis of DOX cardiomyopathy. PHB2 (Prohibitin 2) is perceived as an essential regulator for mitochondrial dynamics and oxidative phosphorylation (OXPHOS) although its involvement in DOX cardiomyopathy remains elusive.

Methods: To decipher the possible role of PHB2 in DOX cardiomyopathy, tamoxifen-induced cardiac-specific PHB2 conditional knockout mice were generated and subjected to DOX challenge. Cardiac function and mitochondrial profiles were examined. Screening of downstream mediators of PHB2 was performed using proteomic profiling and bioinformatic analysis, and was further verified using co-immunoprecipitation and pulldown assays.

Results: Our data revealed significantly downregulated PHB2 expression in DOX-challenged mouse hearts. PHB2^CKO mice were more susceptible to DOX cardiotoxicity compared with PHB2^flox/flox mice, as evidenced by more pronounced cardiac atrophy, interstitial fibrosis and decrease in left ventricular ejection fraction and fractional shortening. Mechanistically, PHB2 deficiency resulted in the impairment of mitochondrial bioenergetics and oxidative phosphorylation in DOX cardiotoxicity. Proteomic profiling and interactome analyses revealed that PHB2 interacted with NDUFV2 (NADH-ubiquinone oxidoreductase core subunit V2), a key subunit of mitochondrial respiratory Complex I to mediate regulatory property of PHB2 on mitochondrial metabolism. PHB2 governed the expression of NDUFV2 by promoting its stabilization, while PHB2 deficiency significantly downregulated NDUFV2 in DOX-challenged hearts. Cardiac overexpression of PHB2 alleviated mitochondrial defects in DOX cardiomyopathy both in vivo and in vitro.

Conclusions: Our study defined a novel role for PHB2 in mitochondrial dynamics and energetic metabolism through interacting with NDUFV2 in DOX-challenged hearts. Forced overexpression of PHB2 may be considered a promising therapeutic approach for patients with DOX cardiomyopathy.

Keywords: Doxorubicin cardiotoxicity; Mitochondrial complex I; NDUFV2; PHB2.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
Apoptosis
Cardiomyopathies* / chemically induced
Cardiomyopathies* / genetics
Cardiotoxicity*
Doxorubicin / adverse effects
Electron Transport Complex I / genetics
Electron Transport Complex I / metabolism
Mice
Oxidative Stress
Proteomics
Stroke Volume
Ventricular Function, Left

Substances

Electron Transport Complex I
Doxorubicin