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Whole-genome bisulfite sequencing of two distinct interconvertible DNA methylomes of mouse embryonic stem cells

机译:全基因组亚硫酸氢盐测序的小鼠胚胎干细胞的两个不同的可互换DNA甲基化组

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The use of two kinase inhibitors (2i) enables derivation of mouse embryonic stem cells (ESCs) in the pluripotent ground state. Using whole-genome bisulfite sequencing (WGBS), we show that male 2i ESCs are globally hypomethylated compared to conventional ESCs maintained in serum. In serum, female ESCs are hypomethyated similarly to male ESCs in 2i, and DNA methylation is further reduced in 2i. Regions with elevated DNA methylation in 2i strongly correlate with the presence of H3K9me3 on endogenous retroviruses (ERVs) and imprinted loci. The methylome of male ESCs in serum parallels postimplantation blastocyst cells, while 2i stalls ESCs in a hypomethylated, ICM-like state. WGBS analysis during adaptation of 2i ESCs to serum suggests that deposition of DNA methylation is largely random, while loss of DNA methylation during reversion to 2i occurs passively, initiating at TET1 binding sites. Together, our analysis provides insight into DNA methylation dynamics in cultured ESCs paralleling early developmental processes.
机译:使用两种激酶抑制剂(2i)可以衍生多能性基态的小鼠胚胎干细胞(ESC)。使用全基因组亚硫酸氢盐测序(WGBS),我们显示,与血清中维持的常规ESC相比,雄性2i ESC总体上甲基化程度较低。在血清中,女性ESC在2i中与男性ESC类似地被甲基化,并且在2i中DNA甲基化进一步降低。 2i中DNA甲基化水平升高的区域与内源性逆转录病毒(ERV)和印迹基因座上H3K9me3的存在密切相关。血清中雄性ESC的甲基化与植入后的胚泡细胞相似,而2i使ESC处于低甲基化,ICM样状态。在2i ESC对血清的适应过程中的WGBS分析表明,DNA甲基化的沉积在很大程度上是随机的,而在恢复为2i的过程中DNA甲基化的损失是被动发生的,始于TET1结合位点。总之,我们的分析提供了对与早期发育过程平行的培养的ESC中DNA甲基化动力学的了解。

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