Systematic transcriptomic and phenotypic characterization of human and murine cardiac myocyte cell lines and primary cardiomyocytes reveals serious limitations and low resemblances to adult cardiac phenotype

Zsófia Onódi; Tamás Visnovitz; Bernadett Kiss; Szabolcs Hambalkó; Anna Koncz; Bence Ágg; Barnabás Váradi; Viktória É. Tóth; Regina N. Nagy; Tamás G. Gergely; Dorottya Gergő; András Makkos; Csilla Pelyhe; Nóra Varga; Dóra Reé; Ágota Apáti; Przemysław Leszek; Tamás Kovács; Nándor Nagy; Péter Ferdinandy; Edit I. Buzás; Anikó Görbe; Zoltán Giricz; Zoltán V. Varga

doi:10.1016/j.yjmcc.2021.12.007

Systematic transcriptomic and phenotypic characterization of human and murine cardiac myocyte cell lines and primary cardiomyocytes reveals serious limitations and low resemblances to adult cardiac phenotype

Zsófia Onódi(Semmelweis University), Tamás Visnovitz(Semmelweis University), Bernadett Kiss(Semmelweis University), Szabolcs Hambalkó(Semmelweis University), Anna Koncz(Semmelweis University), Bence Ágg(Semmelweis University), Barnabás Váradi(Semmelweis University), Viktória É. Tóth(Semmelweis University), Regina N. Nagy(Semmelweis University), Tamás G. Gergely(Semmelweis University), Dorottya Gergő(Semmelweis University), András Makkos(Semmelweis University), Csilla Pelyhe(Semmelweis University), Nóra Varga(Institute of Molecular Life Sciences), Dóra Reé(Institute of Molecular Life Sciences), Ágota Apáti(Institute of Molecular Life Sciences), Przemysław Leszek(Institute of Cardiology), Tamás Kovács(Semmelweis University), Nándor Nagy(Semmelweis University), Péter Ferdinandy(Semmelweis University), Edit I. Buzás(Semmelweis University), Anikó Görbe(Semmelweis University), Zoltán Giricz(Semmelweis University), Zoltán V. Varga(Semmelweis University)

Journal of Molecular and Cellular Cardiology

December 24, 2021

10.1016/j.yjmcc.2021.12.007

Cited by 105Open Access

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Abstract

BACKGROUND: Cardiac cell lines and primary cells are widely used in cardiovascular research. Despite increasing number of publications using these models, comparative characterization of these cell lines has not been performed, therefore, their limitations are undetermined. We aimed to compare cardiac cell lines to primary cardiomyocytes and to mature cardiac tissues in a systematic manner. METHODS AND RESULTS: Cardiac cell lines (H9C2, AC16, HL-1) were differentiated with widely used protocols. Left ventricular tissue, neonatal primary cardiomyocytes, and human induced pluripotent stem cell-derived cardiomyocytes served as reference tissue or cells. RNA expression of cardiac markers (e.g. Tnnt2, Ryr2) was markedly lower in cell lines compared to references. Differentiation induced increase in cardiac- and decrease in embryonic markers however, the overall transcriptomic profile and annotation to relevant biological processes showed consistently less pronounced cardiac phenotype in all cell lines in comparison to the corresponding references. Immunocytochemistry confirmed low expressions of structural protein sarcomeric alpha-actinin, troponin I and caveolin-3 in cell lines. Susceptibility of cell lines to sI/R injury in terms of viability as well as mitochondrial polarization differed from the primary cells irrespective of their degree of differentiation. CONCLUSION: Expression patterns of cardiomyocyte markers and whole transcriptomic profile, as well as response to sI/R, and to hypertrophic stimuli indicate low-to-moderate similarity of cell lines to primary cells/cardiac tissues regardless their differentiation. Low resemblance of cell lines to mature adult cardiac tissue limits their potential use. Low translational value should be taken into account while choosing a particular cell line to model cardiomyocytes.

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