Generation of mature compact ventricular cardiomyocytes from human pluripotent stem cells

Shunsuke Funakoshi(University Health Network), Ian Fernandes(University Health Network), Olya Mastikhina(University Health Network), Dan Wilkinson, Thinh Ngoc Tran(University of Toronto), Wahiba Dhahri(University Health Network), Amine Mazine(University Health Network), Donghe Yang(University Health Network), Benjamin Burnett, Jeehoon Lee, Stephanie Protze(University Health Network), Gary D. Bader(University of Toronto), Sara S. Nunes(University Health Network), Michael A. Laflamme(University Health Network), Gordon Keller(University of Toronto)
Nature Communications
May 26, 2021
Cited by 163Open Access
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Abstract

Compact cardiomyocytes that make up the ventricular wall of the adult heart represent an important therapeutic target population for modeling and treating cardiovascular diseases. Here, we established a differentiation strategy that promotes the specification, proliferation and maturation of compact ventricular cardiomyocytes from human pluripotent stem cells (hPSCs). The cardiomyocytes generated under these conditions display the ability to use fatty acids as an energy source, a high mitochondrial mass, well-defined sarcomere structures and enhanced contraction force. These ventricular cells undergo metabolic changes indicative of those associated with heart failure when challenged in vitro with pathological stimuli and were found to generate grafts consisting of more mature cells than those derived from immature cardiomyocytes following transplantation into infarcted rat hearts. hPSC-derived atrial cardiomyocytes also responded to the maturation cues identified in this study, indicating that the approach is broadly applicable to different subtypes of the heart. Collectively, these findings highlight the power of recapitulating key aspects of embryonic and postnatal development for generating therapeutically relevant cell types from hPSCs.


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