Enhancing induced pluripotent stem cell toward differentiation into functional cardiomyocytes

增强诱导多能干细胞向功能性心肌细胞分化的能力

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作者:Chien,Chian-Shiu,Wang,Chien-Ying,Leu,Hsin-Bang,Chien,Yueh,Yang,Yi-Ping,Wang,Chia-Lin,Tai,Hsiao-Yun,Ko,Yu-Ling,Tsai,Fu-Ting,Chou,Shih-Jie,Yu,Wen-Chung,Yang,Meng-Yin
期刊:影响因子:
时间:2020起止号:2020 Jul;83(7):657-660
doi:10.1097/JCMA.0000000000000301研究方向: 细胞生物学发育与干细胞
细胞类型: 干细胞

Abstract

BACKGROUND: Heart diseases, especially myocardial ischemia, remain one of the leading causes of mortality worldwide and usually result in irreparable cardiomyocyte damage and severe heart failure. Recent advances in induced pluripotent stem cell (iPSC) technologies for applied regenerative medicine and stem cell research, especially for iPSC-derived cardiomyocytes have increased the hope for heart repair. However, the driver molecules of myocardial differentiation and the functional reconstruction capacity of iPSC-derived cardiomyocytes are still questionable. METHODS: Herein, we established a rapid differentiated platform that is involved in cardiomyogenic differentiation and maturation from iPSCs in vitro. Functional analysis is performed in miR-181a-transfected iPSC-derived cardiomyocyte (iPSC-cardio/miR-181a) under a time-lapse microscope. In addition, we calculated the beating area and frequency of iPSC-cardio/miR-181a cells in the presence of HCN4 shRNA or miR-181a SPONGE. RESULTS: miR-181a enhanced the beating area and maintained the beating frequency of iPSC-derived cardiomyocytes by enhancing HCN4 expression. CONCLUSION: miR-181a would play a key role on maintaining proper beating function in iPSC-derived cardiomyocytes.

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