Human embryonic-stem-cell-derived cardiomyocytes regenerate non-human primate hearts

人类胚胎干细胞衍生的心肌细胞再生非人类灵长类动物的心脏

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作者:James J H Chong, Xiulan Yang, Creighton W Don, Elina Minami, Yen-Wen Liu, Jill J Weyers, William M Mahoney, Benjamin Van Biber, Savannah M Cook, Nathan J Palpant, Jay A Gantz, James A Fugate, Veronica Muskheli, G Michael Gough, Keith W Vogel, Cliff A Astley, Charlotte E Hotchkiss, Audrey Baldessari,

Abstract

Pluripotent stem cells provide a potential solution to current epidemic rates of heart failure by providing human cardiomyocytes to support heart regeneration. Studies of human embryonic-stem-cell-derived cardiomyocytes (hESC-CMs) in small-animal models have shown favourable effects of this treatment. However, it remains unknown whether clinical-scale hESC-CM transplantation is feasible, safe or can provide sufficient myocardial regeneration. Here we show that hESC-CMs can be produced at a clinical scale (more than one billion cells per batch) and cryopreserved with good viability. Using a non-human primate model of myocardial ischaemia followed by reperfusion, we show that cryopreservation and intra-myocardial delivery of one billion hESC-CMs generates extensive remuscularization of the infarcted heart. The hESC-CMs showed progressive but incomplete maturation over a 3-month period. Grafts were perfused by host vasculature, and electromechanical junctions between graft and host myocytes were present within 2 weeks of engraftment. Importantly, grafts showed regular calcium transients that were synchronized to the host electrocardiogram, indicating electromechanical coupling. In contrast to small-animal models, non-fatal ventricular arrhythmias were observed in hESC-CM-engrafted primates. Thus, hESC-CMs can remuscularize substantial amounts of the infarcted monkey heart. Comparable remuscularization of a human heart should be possible, but potential arrhythmic complications need to be overcome.

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