Jmjd4 Facilitates Pkm2 Degradation in Cardiomyocytes and Is Protective Against Dilated Cardiomyopathy

Yansong Tang; Mengying Feng; Yang Su; Teng Ma; Hongjie Zhang; Hongchun Wu; Xiaoyu Wang; Shuyue Shi; Ying Zhang; Yawei Xu; Shijun Hu; Ke Wei; Dachun Xu

doi:10.1161/CIRCULATIONAHA.123.064121

Jmjd4 Facilitates Pkm2 Degradation in Cardiomyocytes and Is Protective Against Dilated Cardiomyopathy

Circulation. 2023 May 30;147(22):1684-1704. doi: 10.1161/CIRCULATIONAHA.123.064121. Epub 2023 Apr 17.

Authors

Yansong Tang^#¹, Mengying Feng^#², Yang Su¹, Teng Ma¹, Hongjie Zhang², Hongchun Wu³, Xiaoyu Wang⁴, Shuyue Shi^{2

3}, Ying Zhang², Yawei Xu¹, Shijun Hu³, Ke Wei², Dachun Xu¹

Affiliations

¹ Department of Cardiology, Shanghai Tenth People's Hospital, Tongji University School of Medicine, China (Y.T., Y.S., T.M., Y.X., D.X.).
² Institute for Regenerative Medicine, Shanghai East Hospital, Shanghai Institute of Stem Cell Research and Clinical Translation, Shanghai Key Laboratory of Signaling and Disease Research, Frontier Science Center for Stem Cell Research, School of Life Sciences and Technology, Tongji University, China (M.F., H.Z., S.S., Y.Z., K.W.).
³ Department of Cardiovascular Surgery of the First Affiliated Hospital & Institute for Cardiovascular Science, Collaborative Innovation Center of Hematology, State Key Laboratory of Radiation Medicine and Protection, Medical College, Soochow University, Suzhou, China (H.W., S.H.).
⁴ Research Center for Translational Medicine, Shanghai East Hospital, Tongji University School of Medicine, China (X.W.).

^# Contributed equally.

PMID: 37066795
DOI: 10.1161/CIRCULATIONAHA.123.064121

Abstract

Background: A large portion of idiopathic and familial dilated cardiomyopathy (DCM) cases have no obvious causal genetic variant. Although altered response to metabolic stress has been implicated, the molecular mechanisms underlying the pathogenesis of DCM remain elusive. The JMJD family proteins, initially identified as histone deacetylases, have been shown to be involved in many cardiovascular diseases. Despite their increasingly diverse functions, whether JMJD family members play a role in DCM remains unclear.

Methods: We examined Jmjd4 expression in patients with DCM, and conditionally deleted and overexpressed Jmjd4 in cardiomyocytes in vivo to investigate its role in DCM. RNA sequencing, metabolites profiling, and mass spectrometry were used to dissect the molecular mechanism of Jmjd4-regulating cardiac metabolism and hypertrophy.

Results: We found that expression of Jmjd4 is significantly decreased in hearts of patients with DCM. Induced cardiomyocyte-specific deletion of Jmjd4 led to spontaneous DCM with severely impaired mitochondrial respiration. Pkm2, the less active pyruvate kinase compared with Pkm1, which is normally absent in healthy adult cardiomyocytes but elevated in cardiomyopathy, was found to be drastically accumulated in hearts with Jmjd4 deleted. Jmjd4 was found mechanistically to interact with Hsp70 to mediate degradation of Pkm2 through chaperone-mediated autophagy, which is dependent on hydroxylation of K66 of Pkm2 by Jmjd4. By enhancing the enzymatic activity of the abundant but less active Pkm2, TEPP-46, a Pkm2 agonist, showed a significant therapeutic effect on DCM induced by Jmjd4 deficiency, and heart failure induced by pressure overload, as well.

Conclusions: Our results identified a novel role of Jmjd4 in maintaining metabolic homeostasis in adult cardiomyocytes by degrading Pkm2 and suggest that Jmjd4 and Pkm2 may be therapeutically targeted to treat DCM, and other cardiac diseases with metabolic dysfunction, as well.

Keywords: HSP70 heat-shock proteins; JMJD4 protein, mouse; Pkm2 protein; cardiomyopathy, dilated; chaperone-mediated autophagy; hydroxylation; mouse.

Publication types

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

MeSH terms

Cardiomyopathy, Dilated* / pathology
Heart Failure* / pathology
Humans
Myocytes, Cardiac / metabolism