DNA methylation reprogramming of functional elements during mammalian embryonic development

被引:0
作者
Congru Li
Yong Fan
Guoqiang Li
Xiaocui Xu
Jialei Duan
Rong Li
Xiangjin Kang
Xin Ma
Xuepeng Chen
Yuwen Ke
Jie Yan
Ying Lian
Ping Liu
Yue Zhao
Hongcui Zhao
Yaoyong Chen
Yang Yu
Jiang Liu
机构
[1] Center of Reproductive Medicine,Ministry of Education Key Laboratory of Assisted Reproduction, and Beijing Key Laboratory of Reproductive Endocrinology and Assisted Reproductive Technology
[2] Peking University Third Hospital,CAS Key Laboratory of Genome Sciences and Information, Collaborative Innovation Center of Genetics and Development
[3] Beijing Institute of Genomics,Key Laboratory for Major Obstetric Diseases of Guangdong Province
[4] CAS,undefined
[5] University of Chinese Academy of Sciences,undefined
[6] Third Affiliated Hospital of Guangzhou Medical University,undefined
来源
Cell Discovery | / 4卷
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摘要
DNA methylation plays important roles during development. However, the DNA methylation reprogramming of functional elements has not been fully investigated during mammalian embryonic development. Herein, using our modified MethylC-Seq library generation method and published post-bisulphite adapter-tagging (PBAT) method, we generated genome-wide DNA methylomes of human gametes and early embryos at single-base resolution and compared them with mouse methylomes. We showed that the dynamics of DNA methylation in functional elements are conserved between humans and mice during early embryogenesis, except for satellite repeats. We further found that oocyte-specific hypomethylated promoters usually exhibit low CpG densities. Genes with oocyte-specific hypomethylated promoters generally show oocyte-specific hypomethylated genic and intergenic regions, and these hypomethylated regions contribute to the hypomethylation pattern of mammalian oocytes. Furthermore, hypomethylated genic regions with low CG densities correlate with gene silencing in oocytes, whereas hypomethylated genic regions with high CG densities correspond to high gene expression. We further show that methylation reprogramming of enhancers during early embryogenesis is highly associated with the development of almost all human organs. Our data support the hypothesis that DNA methylation plays important roles during mammalian development.
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