Epigenetics Programme, The Babraham Institute, Cambridge CB22 3AT, UK.
Curr Opin Cell Biol. 2013 Jun;25(3):281-8. doi: 10.1016/j.ceb.2013.02.013. Epub 2013 Mar 17.
DNA methylation is a carrier of important regulatory information that undergoes global reprogramming in the mammalian germ line, including pre-implantation embryos and primordial germ cells (PGCs). A flurry of recent studies have employed technical advances to generate global profiles of methylation and hydroxymethylation in these cells, unravelling the dynamics of methylation erasure at single locus resolution. Active demethylation in the zygote, involving extensive oxidation, is followed by passive loss over early cell divisions. Certain gamete-contributed methylation marks appear to have evolved non-canonical mechanisms for targeted maintenance of methylation in the face of these processes. These protected sequences include the imprinting control regions (ICRs) required for parental imprinting but also a surprising number of other regions. Such targeted maintenance mechanisms may also operate at certain sequences during early PGC migration when global passive demethylation occurs. In later gonadal PGCs, imprints must be reset and this may be achieved through the targeting of active mechanisms including oxidation. Thus, emerging evidence paints a complex picture whereby active and passive demethylation pathways operate synergistically and in parallel to ensure robust erasure in the early embryo and PGCs.
DNA 甲基化是一种重要的调控信息载体,在哺乳动物生殖系中经历了全面的重编程,包括着床前胚胎和原始生殖细胞(PGCs)。最近的大量研究利用技术进步,在这些细胞中生成了甲基化和羟甲基化的全局图谱,揭示了单基因座分辨率下甲基化消除的动力学。在合子中,涉及广泛氧化的主动去甲基化,随后在早期细胞分裂中被动丢失。某些配子贡献的甲基化标记似乎已经进化出针对这些过程的靶向甲基化维持的非经典机制。这些受保护的序列包括印迹控制区(ICR),其对于亲本印迹是必需的,但也包括许多其他区域。在早期 PGC 迁移期间发生全局被动去甲基化时,这种靶向维持机制可能也会在某些序列上起作用。在后来的性腺 PGC 中,印记必须被重置,这可能通过靶向包括氧化在内的主动机制来实现。因此,新出现的证据描绘了一幅复杂的图景,其中主动和被动去甲基化途径协同和并行运作,以确保早期胚胎和 PGC 中强大的消除。
