Combined Treatment of Human Induced Pluripotent Stem Cell–Derived Cardiomyocytes and Endothelial Cells Regenerate the Infarcted Heart in Mice and Non-Human Primates

诱导多能干细胞 医学 移植 心功能曲线 血管生成 体内 细胞疗法 干细胞 细胞 心脏病学 心肌梗塞 内皮干细胞 内科学 癌症研究 细胞生物学 体外 心力衰竭 生物 胚胎干细胞 基因 生物技术 生物化学 遗传学
作者
Yu‐Che Cheng,Marvin L. Hsieh,Chen‐Ju Lin,Cindy M. Chang,Ching-Ying Huang,Riley Puntney,Amy Moy,Chien-Yu Ting,Darien Zhing-Herr Chan,Martin W. Nicholson,Po‐Ju Lin,Hung-Chih Chen,Gina C. Kim,Jianhua Zhang,Jennifer Coonen,Puja Basu,Heather A. Simmons,Yen-Wen Liu,Timothy A. Hacker,Timothy J. Kamp,Patrick C.H. Hsieh
出处
期刊:Circulation [Lippincott Williams & Wilkins]
卷期号:148 (18): 1395-1409 被引量:15
标识
DOI:10.1161/circulationaha.122.061736
摘要

BACKGROUND: Remuscularization of the mammalian heart can be achieved after cell transplantation of human induced pluripotent stem cell (hiPSC)–derived cardiomyocytes (CMs). However, several hurdles remain before implementation into clinical practice. Poor survival of the implanted cells is related to insufficient vascularization, and the potential for fatal arrhythmogenesis is associated with the fetal cell–like nature of immature CMs. METHODS: We generated 3 lines of hiPSC-derived endothelial cells (ECs) and hiPSC-CMs from 3 independent donors and tested hiPSC–CM sarcomeric length, gap junction protein, and calcium-handling ability in coculture with ECs. Next, we examined the therapeutic effect of the cotransplantation of hiPSC-ECs and hiPSC-CMs in nonobese diabetic-severe combined immunodeficiency (NOD-SCID) mice undergoing myocardial infarction (n≥4). Cardiac function was assessed by echocardiography, whereas arrhythmic events were recorded using 3-lead ECGs. We further used healthy non-human primates (n=4) with cell injection to study the cell engraftment, maturation, and integration of transplanted hiPSC-CMs, alone or along with hiPSC-ECs, by histological analysis. Last, we tested the cell therapy in ischemic reperfusion injury in non-human primates (n=4, 3, and 4 for EC+CM, CM, and control, respectively). Cardiac function was evaluated by echocardiography and cardiac MRI, whereas arrhythmic events were monitored by telemetric ECG recorders. Cell engraftment, angiogenesis, and host–graft integration of human grafts were also investigated. RESULTS: We demonstrated that human iPSC-ECs promote the maturity and function of hiPSC-CMs in vitro and in vivo. When cocultured with ECs, CMs showed more mature phenotypes in cellular structure and function. In the mouse model, cotransplantation augmented the EC-accompanied vascularization in the grafts, promoted the maturity of CMs at the infarct area, and improved cardiac function after myocardial infarction. Furthermore, in non-human primates, transplantation of ECs and CMs significantly enhanced graft size and vasculature and improved cardiac function after ischemic reperfusion. CONCLUSIONS: These results demonstrate the synergistic effect of combining iPSC-derived ECs and CMs for therapy in the postmyocardial infarction heart, enabling a promising strategy toward clinical translation.
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