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小鼠早期胚胎中DNA甲基化的动态重编程。

Dynamic reprogramming of DNA methylation in the early mouse embryo.

作者信息

Santos Fátima, Hendrich Brian, Reik Wolf, Dean Wendy

机构信息

Laboratory of Developmental Genetics and Imprinting, The Babraham Institute, Cambridge, CB2 4AT, United Kingdom.

出版信息

Dev Biol. 2002 Jan 1;241(1):172-82. doi: 10.1006/dbio.2001.0501.

DOI:10.1006/dbio.2001.0501
PMID:11784103
Abstract

Dynamic epigenetic modification of the genome occurs during early development of the mouse. Active demethylation of the paternal genome occurs in the zygote, followed by passive demethylation during cleavage stages, and de novo methylation, which is thought to happen after implantation. We have investigated these processes by using indirect immunofluorescence with an antibody to 5-methyl cytosine. In contrast to previous work, we show that demethylation of the male pronucleus is completed within 4 h of fertilisation. This activity is intricately linked with and not separable from pronucleus formation. In conditions permissive for polyspermy, up to five male pronuclei underwent demethylation in the same oocyte. Paternal demethylation in fertilised oocytes deficient for MBD2, the only candidate demethylase, occurred normally. Passive loss of methylation occurred in a stepwise fashion up to the morulae stage without any evidence of spatial compartmentalisation. De novo methylation was observed specifically in the inner cell mass (ICM) but not in the trophectoderm of the blastocyst and hence may have an important role in early lineage specification. This is the first complete and detailed analysis of the epigenetic reprogramming cycle during preimplantation development. The three phases of methylation reprogramming may have roles in imprinting, the control of gene expression, and the establishment of nuclear totipotency.

摘要

基因组的动态表观遗传修饰发生在小鼠早期发育过程中。父本基因组的主动去甲基化发生在合子中,随后在卵裂阶段发生被动去甲基化,而从头甲基化被认为发生在着床后。我们通过使用针对5-甲基胞嘧啶的抗体进行间接免疫荧光来研究这些过程。与之前的工作相反,我们发现雄原核的去甲基化在受精后4小时内完成。这种活性与原核形成紧密相连且不可分割。在允许多精受精的条件下,同一个卵母细胞中多达五个雄原核会发生去甲基化。在缺乏唯一候选去甲基酶MBD2的受精卵母细胞中,父本去甲基化正常发生。甲基化的被动丢失以逐步的方式发生,直至桑椹胚阶段,且没有任何空间分隔的证据。在囊胚的内细胞团(ICM)中特异性地观察到了从头甲基化,而在滋养外胚层中未观察到,因此其可能在早期谱系特化中发挥重要作用。这是对植入前发育过程中表观遗传重编程循环的首次完整而详细的分析。甲基化重编程的三个阶段可能在印记、基因表达控制和核全能性的建立中发挥作用。

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