Asparagine Synthetase Marks a Distinct Dependency Threshold for Cardiomyocyte Dedifferentiation

Yike Zhu; Matthew Ackers-Johnson; Muthu K Shanmugam; Leroy Sivappiragasam Pakkiri; Chester Lee Drum; Yanpu Chen; Johnny Kim; Wyatt G Paltzer; Ahmed I Mahmoud; Wilson Lek Wen Tan; Mick Chang Jie Lee; Jianming Jiang; Danh Anh Tuan Luu; Shi Ling Ng; Peter Yi Qing Li; Anhui Wang; Rong Qi; Gabriel Jing Xiang Ong; Timothy Ng Yu; Jody J Haigh; Zenia Tiang; A Mark Richards; Roger Foo

doi:10.1161/CIRCULATIONAHA.123.063965

Asparagine Synthetase Marks a Distinct Dependency Threshold for Cardiomyocyte Dedifferentiation

Circulation. 2024 Apr 8. doi: 10.1161/CIRCULATIONAHA.123.063965. Online ahead of print.

Authors

Yike Zhu^{1

2}, Matthew Ackers-Johnson^{1

2}, Muthu K Shanmugam^{1

2}, Leroy Sivappiragasam Pakkiri^{1

2}, Chester Lee Drum^{1

2}, Yanpu Chen³, Johnny Kim^{3

4}, Wyatt G Paltzer⁵, Ahmed I Mahmoud⁵, Wilson Lek Wen Tan^{1

2}, Mick Chang Jie Lee^{1

2}, Jianming Jiang^{1

2}, Danh Anh Tuan Luu^{1

2}, Shi Ling Ng^{1

2}, Peter Yi Qing Li^{1

2}, Anhui Wang^{6

7}, Rong Qi^{6

7}, Gabriel Jing Xiang Ong^{1

2}, Timothy Ng Yu^{1

2}, Jody J Haigh^{8

9}, Zenia Tiang^{1

2}, A Mark Richards^{1

2

10}, Roger Foo^{1

2

11}

Affiliations

¹ Cardiovascular Research Institute, Yong Loo Lin School of Medicine, National University of Singapore, National University Health Systems, Singapore. (Y.Z., M.A.-J., M.K.S., L.S.P., C.L.D., W.L.W.T., M.C.J.L., J.J., L.D.A.T., S.L.N., P.Y.Q.L. G.J.X.O., T.N.Y., Z.T., A.M.R., R.F.).
² Cardiovascular Metabolic Disease Translational Research Programme, National University Health Systems, Singapore. (Y.Z., M.A.-J., M.K.S., L.S.P., C.L.D., W.L.W.T., M.C.J.L., J.J., L.D.A.T., S.L.N., P.Y.Q.L. G.J.X.O., T.N.Y., Z.T., A.M.R., R.F.).
³ Max Planck Institute for Heart and Lung Research, Bad Nauheim, Germany (C.Y., J.K.).
⁴ German Centre for Cardiovascular Research (DZHK), Partner site Rhein/Main, Bad Nauheim, Peking University, China. (J.K.).
⁵ Department of Cell and Regenerative Biology, School of Medicine and Public Health, University of Wisconsin-Madison, Peking University, China. (W.G.P., A.I.M.).
⁶ Department of Pharmacology, School of Basic Medical Sciences, Peking University Health Science Centre, Peking University, China. (W.A., Q.R.).
⁷ State Key Laboratory of Vascular Homeostasis and Remodelling, Peking University, China. (W.A., Q.R.).
⁸ CancerCare Manitoba Research Institute, Department of Pharmacology and Therapeutics, Rady Faculty of Health Sciences, University of Manitoba, Winnipeg, Canada (J.J.H.).
⁹ VIB, Flanders Institute for Biotechnology, Ghent University, Ghent, Belgium (J.J.H.).
¹⁰ Christchurch Heart Institute, University of Otago, New Zealand (A.M.R.).
¹¹ Institute of Molecular and Cell Biology, A*STAR, Singapore (R.F.).

PMID: 38586957
DOI: 10.1161/CIRCULATIONAHA.123.063965

Abstract

Background: Adult mammalian cardiomyocytes have limited proliferative capacity, but in specifically induced contexts they traverse through cell-cycle reentry, offering the potential for heart regeneration. Endogenous cardiomyocyte proliferation is preceded by cardiomyocyte dedifferentiation (CMDD), wherein adult cardiomyocytes revert to a less matured state that is distinct from the classical myocardial fetal stress gene response associated with heart failure. However, very little is known about CMDD as a defined cardiomyocyte cell state in transition.

Methods: Here, we leveraged 2 models of in vitro cultured adult mouse cardiomyocytes and in vivo adeno-associated virus serotype 9 cardiomyocyte-targeted delivery of reprogramming factors (Oct4, Sox2, Klf4, and Myc) in adult mice to study CMDD. We profiled their transcriptomes using RNA sequencing, in combination with multiple published data sets, with the aim of identifying a common denominator for tracking CMDD.

Results: RNA sequencing and integrated analysis identified Asparagine Synthetase (Asns) as a unique molecular marker gene well correlated with CMDD, required for increased asparagine and also for distinct fluxes in other amino acids. Although Asns overexpression in Oct4, Sox2, Klf4, and Myc cardiomyocytes augmented hallmarks of CMDD, Asns deficiency led to defective regeneration in the neonatal mouse myocardial infarction model, increased cell death of cultured adult cardiomyocytes, and reduced cell cycle in Oct4, Sox2, Klf4, and Myc cardiomyocytes, at least in part through disrupting the mammalian target of rapamycin complex 1 pathway.

Conclusions: We discovered a novel gene Asns as both a molecular marker and an essential mediator, marking a distinct threshold that appears in common for at least 4 models of CMDD, and revealing an Asns/mammalian target of rapamycin complex 1 axis dependency for dedifferentiating cardiomyocytes. Further study will be needed to extrapolate and assess its relevance to other cell state transitions as well as in heart regeneration.

Keywords: cell dedifferentiation; cell self-renewal; myocytes, cardiac; regeneration.

Grants and funding

T32 HL007936/HL/NHLBI NIH HHS/United States