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INO80 Is Required for the Cell Cycle Control, Survival, and Differentiation of Mouse ESCs by Transcriptional Regulation

细胞生物学 细胞周期 生物 胚胎干细胞 体细胞 染色质 基因表达调控 转录因子 表观遗传学 转录调控 细胞命运测定 遗传学 细胞 基因
作者
Seonho Yoo,Eun Joo Lee,Nguyen Xuan Thang,Hyeonwoo La,Hyeonji Lee,Chanhyeok Park,Dong‐Wook Han,Sang Jun Uhm,Hyuk Song,Jeong Tae,Youngsok Choi,Kwonho Hong
出处
期刊:International Journal of Molecular Sciences [MDPI AG]
卷期号:23 (23): 15402-15402 被引量:7
标识
DOI:10.3390/ijms232315402
摘要

Precise regulation of the cell cycle of embryonic stem cells (ESCs) is critical for their self-maintenance and differentiation. The cell cycle of ESCs differs from that of somatic cells and is different depending on the cell culture conditions. However, the cell cycle regulation in ESCs via epigenetic mechanisms remains unclear. Here, we showed that the ATP-dependent chromatin remodeler Ino80 regulates the cell cycle genes in ESCs under primed conditions. Ino80 loss led to a significantly extended length of the G1-phase in ESCs grown under primed culture conditions. Ino80 directly bound to the transcription start site and regulated the expression of cell cycle-related genes. Furthermore, Ino80 loss induced cell apoptosis. However, the regulatory mechanism of Ino80 in differentiating ESC cycle slightly differed; an extended S-phase was detected in differentiating inducible Ino80 knockout ESCs. RNA-seq analysis of differentiating ESCs revealed that the expression of genes associated with organ development cell cycle is persistently altered in Ino80 knockout cells, suggesting that cell cycle regulation by Ino80 is not limited to undifferentiated ESCs. Therefore, our study establishes the function of Ino80 in ESC cycle via transcriptional regulation, at least partly. Moreover, this Ino80 function may be universal to other cell types.

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