论文标题

增强剂之间的协作引起的DNA甲基化异质性

DNA methylation heterogeneity induced by collaborations between enhancers

论文作者

Ye, Yusong, Yang, Zhuoqin, Lei, Jinzhi

论文摘要

在哺乳动物的胚胎发育过程中,DNA甲基化的重编程在擦除亲本表观遗传记忆和建立幼稚的多元细胞中起着重要作用。调节甲基化和脱甲基化过程的多种酶共同塑造基因组尺度DNA甲基化的模式和GUID的细胞分化过程。最近从单细胞全基因组亚硫酸盐测序(SCBS-seq)提供的甲基化信息的可用性为研究单个细胞中整个基因组中的DNA甲基化动力学提供了一个机会,这揭示了胚胎干细胞中增强剂的异质甲基化分布(ESC)。在这项研究中,我们开发了一种增强子甲基化遗传的计算模型,以研究在脱离多能力期间基因组尺度DNA甲基化重编程的动力学。该模型使我们能够在胚胎发育过程中跟踪单细胞水平的基因组规模DNA甲基化重编程,并重现SCBS-Seq报道的DNA甲基化异质性。模型模拟表明,DNA甲基化异质性是沿着开发过程驱动的固有特性,并且相邻增强子之间的协作是异质甲基化所必需的。我们的研究表明,Rulands等人提出的基因组规模振荡的机制。 (2018)在从多能力中退出期间,DNA甲基化可能无需。

During mammalian embryo development, reprogramming of DNA methylation plays important roles in the erasure of parental epigenetic memory and the establishment of naïve pluripogent cells. Multiple enzymes that regulate the processes of methylation and demethylation work together to shape the pattern of genome-scale DNA methylation and guid the process of cell differentiation. Recent availability of methylome information from single-cell whole genome bisulfite sequencing (scBS-seq) provides an opportunity to study DNA methylation dynamics in the whole genome in individual cells, which reveal the heterogeneous methylation distributions of enhancers in embryo stem cells (ESCs). In this study, we developed a computational model of enhancer methylation inheritance to study the dynamics of genome-scale DNA methylation reprogramming during exit from pluripotency. The model enables us to track genome-scale DNA methylation reprogramming at single-cell level during the embryo development process, and reproduce the DNA methylation heterogeneity reported by scBS-seq. Model simulations show that DNA methylation heterogeneity is an intrinsic property driven by cell division along the development process, and the collaboration between neighboring enhancers is required for heterogeneous methylation. Our study suggest that the mechanism of genome-scale oscillation proposed by Rulands et al. (2018) might not necessary to the DNA methylation during exit from pluripotency.

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