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Insulin‐Like Growth Factor Binding Protein 4 Enhances Cardiomyocytes Induction in Murine‐Induced Pluripotent Stem Cells

诱导多能干细胞 胚状体 细胞生物学 基因敲除 胚胎干细胞 化学 细胞分化 生物 细胞凋亡 生物化学 基因
作者
Yuanyuan Xue,Yuan Yan,Hui Gong,Bo Fang,Yin Zhou,Zhiwen Ding,Peipei Yin,Guoping Zhang,Yong Ye,Chunjie Yang,Junbo Ge,Yunzeng Zou
出处
期刊:Journal of Cellular Biochemistry [Wiley]
日期:2014-07-15 卷期号:115 (9): 1495-1504 被引量:26
链接
nih.govdoi.org
标识
DOI:10.1002/jcb.24804
摘要
Insulin-like growth factor binding protein 4 (IGFBP4) has been reported to play critical role in cardiomyocytes differentiation of embryonic stem cells (ESCs). But whether it promotes cardiomyocytes induction of iPSCs is unclear. In the present study, we aim to explore the role of IGFBP4 in the cardiogenesis of mouse iPSCs. We observed that IGFBP4 treatment at late stage during differentiation process of mouse iPSCs greatly enhanced the beating frequency of embryoid bodies (EBs). The expressions of Nkx2.5 (cardiac-specific transcription factor), α-MHC, α-actinin, and Troponin I (cardiac-specific protein) were significantly enhanced by IGFBP4 treatment. Immunostaining analysis showed that α-MHC, TNNT2 and connexin 43, typical cardiac markers, were obviously expressed in isolated cardiomyocytes from iPSCs with or without IGFBP4 treatment. Further study revealed that IGFBP4 had little effect on the apoptosis of EBs, but it significantly promoted the proliferation of cardiomyocytes from iPSCs characterized by higher ratio EdU positive cells in differentiated cardiomyocytes. We next observed that IGFBP4 inhibited β-catenin expression in cytosol of EBs at late stage during differentiation of iPSCs. Knockdown of β-catenin using a siRNA technique promoted the proliferation of differentiated cardiomyocytes and enhanced cardiomyocytes induction of iPSCs, suggesting that the effect of IGFBP4 on cardiomyocytes differentiation of iPSCs has relationship with β-catenin signaling pathway. In conclusion, IGFBP4 promotes cardiogenesis of iPSCs by enhancing the proliferation of differentiated cardiomyocytes through inhibiting β-catenin signaling.
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