Genome wide abnormal DNA methylome of human blastocyst in assisted reproductive technology

重编程 生物 甲基化 DNA甲基化 表观遗传学 基因组印记 非整倍体 遗传学 胚胎干细胞 胚胎 胚泡 基因 胚胎发生 男科 DNA 医学 基因表达 染色体
作者
Guoqiang Li,Yang Yu,Yong Fan,Congru 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,Xiaofang Sun,Jianqiao Liu,Jie Qiao
出处
期刊:Journal of Genetics and Genomics [Elsevier BV]
卷期号:44 (10): 475-481 被引量:36
标识
DOI:10.1016/j.jgg.2017.09.001
摘要

Proper reprogramming of parental DNA methylomes is essential for mammalian embryonic development. However, it is unknown whether abnormal methylome reprogramming occurs and is associated with the failure of embryonic development. Here we analyzed the DNA methylomes of 57 blastocysts and 29 trophectoderm samples with different morphological grades during assisted reproductive technology (ART) practices. Our data reveal that the global methylation levels of high-quality blastocysts are similar (0.30 ± 0.02, mean ± SD), while the methylation levels of low-quality blastocysts are divergent and away from those of high-quality blastocysts. The proportion of blastocysts with a methylation level falling within the range of 0.30 ± 0.02 in different grades correlates with the live birth rate for that grade. Moreover, abnormal methylated regions are associated with the failure of embryonic development. Furthermore, we can use the methylation data of cells biopsied from trophectoderm to predict the blastocyst methylation level as well as to detect the aneuploidy of the blastocysts. Our data indicate that global abnormal methylome reprogramming often occurs in human embryos, and suggest that DNA methylome is a potential biomarker in blastocyst selection in ART.
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