Department of Genome Regulation, Max Planck Institute for Molecular Genetics, Berlin, Germany.
Department of Stem Cell and Regenerative Biology, Harvard University, Cambridge, MA, USA.
Nat Struct Mol Biol. 2018 Apr;25(4):327-332. doi: 10.1038/s41594-018-0046-4. Epub 2018 Mar 12.
Cytosine methylation is widespread among organisms and essential for mammalian development. In line with early postulations of an epigenetic role in gene regulation, symmetric CpG methylation can be mitotically propagated over many generations with extraordinarily high fidelity. Here, we combine BrdU labeling and immunoprecipitation with genome-wide bisulfite sequencing to explore the inheritance of cytosine methylation onto newly replicated DNA in human cells. Globally, we observe a pronounced lag between the copying of genetic and epigenetic information in embryonic stem cells that is reconsolidated within hours to accomplish faithful mitotic transmission. Populations of arrested cells show a global reduction of lag-induced intermediate CpG methylation when compared to proliferating cells, whereas sites of transcription factor engagement appear cell-cycle invariant. Alternatively, the cancer cell line HCT116 preserves global epigenetic heterogeneity independently of cell-cycle arrest. Taken together, our data suggest that heterogeneous methylation largely reflects asynchronous proliferation, but is intrinsic to actively engaged cis-regulatory elements and cancer.
胞嘧啶甲基化在生物界中广泛存在,对哺乳动物的发育至关重要。与早期提出的在基因调控中具有表观遗传作用的观点一致,对称的 CpG 甲基化可以在许多代中以极高的保真度进行有丝分裂传播。在这里,我们结合 BrdU 标记和免疫沉淀与全基因组亚硫酸氢盐测序,探索在人类细胞中新复制的 DNA 上胞嘧啶甲基化的遗传。总体而言,我们观察到胚胎干细胞中遗传和表观遗传信息复制之间存在明显的滞后,这种滞后在数小时内重新整合,以完成忠实的有丝分裂传递。与增殖细胞相比,停滞细胞群体中滞后诱导的中间 CpG 甲基化总体减少,而转录因子结合位点似乎在细胞周期中不变。相反,癌细胞系 HCT116 独立于细胞周期停滞而保持全局表观遗传异质性。总之,我们的数据表明,异质甲基化主要反映了细胞的增殖不同步,但它是活跃的顺式调控元件和癌症所固有的。
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