Regeneration of Nonhuman Primate Hearts With Human Induced Pluripotent Stem Cell–Derived Cardiac Spheroids-Reference-Cited by-同舟云学术

Regeneration of Nonhuman Primate Hearts With Human Induced Pluripotent Stem Cell–Derived Cardiac Spheroids

Published:2024-08-20 Issue:8 Volume:150 Page:611-621
ISSN:0009-7322
Container-title:Circulation
language:en
Short-container-title:Circulation

Author:

Kobayashi Hideki¹^ORCID,Tohyama Shugo²^ORCID,Ichimura Hajime³⁴,Ohashi Noburo³,Chino Shuji³,Soma Yusuke²,Tani Hidenori²,Tanaka Yuki³⁴,Yang Xiao⁴,Shiba Naoko⁴^ORCID,Kadota Shin⁴⁵^ORCID,Haga Kotaro²^ORCID,Moriwaki Taijun²^ORCID,Morita-Umei Yuika²⁶,Umei Tomohiko C.²,Sekine Otoya²,Kishino Yoshikazu²^ORCID,Kanazawa Hideaki²^ORCID,Kawagishi Hiroyuki⁷⁵^ORCID,Yamada Mitsuhiko⁷^ORCID,Narita Kazumasa⁸⁹,Naito Takafumi⁸⁹^ORCID,Seto Tatsuichiro³²,Kuwahara Koichiro¹⁵^ORCID,Shiba Yuji⁴⁵^ORCID,Fukuda Keiichi²^ORCID

Affiliation:

1. Department of Cardiovascular Medicine (H. Kobayashi, K.K.), Shinshu University, Matsumoto, Japan.

2. Department of Cardiology, Keio University School of Medicine, Tokyo, Japan (S.T., Y. Soma, H.T., K.H., T.M., Y.M.-U., T.C.U., O.S., Y.K., H. Kanazawa, K.F.).

3. Division of Cardiovascular Surgery, Department of Surgery (H.I., N.O., S.C., Y.T., T.S.), Shinshu University, Matsumoto, Japan.

4. School of Medicine, Department of Regenerative Science and Medicine (H.I., Y.T., X.Y., N.S., S.K., Y. Shiba), Shinshu University, Matsumoto, Japan.

5. Institute for Biomedical Sciences (S.K., H. Kawagishi, K.K., Y. Shiba), Shinshu University, Matsumoto, Japan.

6. Kanagawa Institute of Industrial Science and Technology, Japan (Y.M.-U.).

7. Department of Molecular Pharmacology (H. Kawagishi, M.Y.), Shinshu University, Matsumoto, Japan.

8. Department of Clinical Pharmacology and Therapeutics, Graduate School of Medicine (K.N., T.N.), Shinshu University, Matsumoto, Japan.

9. Department of Pharmacy, Shinshu University Hospital, Matsumoto, Japan (K.N., T.N.).

Abstract

BACKGROUND: The clinical application of human induced pluripotent stem cell–derived cardiomyocytes (CMs) for cardiac repair commenced with the epicardial delivery of engineered cardiac tissue; however, the feasibility of the direct delivery of human induced pluripotent stem cell–derived CMs into the cardiac muscle layer, which has reportedly induced electrical integration, is unclear because of concerns about poor engraftment of CMs and posttransplant arrhythmias. Thus, in this study, we prepared purified human induced pluripotent stem cell–derived cardiac spheroids (hiPSC-CSs) and investigated whether their direct injection could regenerate infarcted nonhuman primate hearts. METHODS: We performed 2 separate experiments to explore the appropriate number of human induced pluripotent stem cell–derived CMs. In the first experiment, 10 cynomolgus monkeys were subjected to myocardial infarction 2 weeks before transplantation and were designated as recipients of hiPSC-CSs containing 2×10 7 CMs or the vehicle. The animals were euthanized 12 weeks after transplantation for histological analysis, and cardiac function and arrhythmia were monitored during the observational period. In the second study, we repeated the equivalent transplantation study using more CMs (6×10 7 CMs). RESULTS: Recipients of hiPSC-CSs containing 2×10 7 CMs showed limited CM grafts and transient increases in fractional shortening compared with those of the vehicle (fractional shortening at 4 weeks after transplantation [mean ± SD]: 26.2±2.1%; 19.3±1.8%; P <0.05), with a low incidence of posttransplant arrhythmia. Transplantation of increased dose of CMs resulted in significantly greater engraftment and long-term contractile benefits (fractional shortening at 12 weeks after transplantation: 22.5±1.0%; 16.6±1.1%; P <0.01, left ventricular ejection fraction at 12 weeks after transplantation: 49.0±1.4%; 36.3±2.9%; P <0.01). The incidence of posttransplant arrhythmia slightly increased in recipients of hiPSC-CSs containing 6×10 7 CMs. CONCLUSIONS: We demonstrated that direct injection of hiPSC-CSs restores the contractile functions of injured primate hearts with an acceptable risk of posttransplant arrhythmia. Although the mechanism for the functional benefits is not fully elucidated, these findings provide a strong rationale for conducting clinical trials using the equivalent CM products.

Publisher

Ovid Technologies (Wolters Kluwer Health)

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