Single-cell multiomics sequencing reveals the functional regulatory landscape of early embryos

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作者
Yang Wang
Peng Yuan
Zhiqiang Yan
Ming Yang
Ying Huo
Yanli Nie
Xiaohui Zhu
Jie Qiao
Liying Yan
机构
[1] Peking University Third Hospital,Beijing Advanced Innovation Center for Genomics, Center for Reproductive Medicine, Department of Obstetrics and Gynecology
[2] Key Laboratory of Assisted Reproduction,Peking
[3] Ministry of Education,Tsinghua Center for Life Sciences
[4] Beijing Key Laboratory of Reproductive Endocrinology and Assisted Reproductive Technology,undefined
[5] Peking University,undefined
[6] National Clinical Research Center for Obstetrics and Gynecology,undefined
[7] Research Units of Comprehensive Diagnosis and Treatment of Oocyte Maturation Arrest,undefined
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Extensive epigenetic reprogramming occurs during preimplantation embryo development. However, it remains largely unclear how the drastic epigenetic reprogramming contributes to transcriptional regulatory network during this period. Here, we develop a single-cell multiomics sequencing technology (scNOMeRe-seq) that enables profiling of genome-wide chromatin accessibility, DNA methylation and RNA expression in the same individual cell. We apply this method to depict a single-cell multiomics map of mouse preimplantation development. We find that genome-wide DNA methylation remodeling facilitates the reconstruction of genetic lineages in early embryos. Further, we construct a zygotic genome activation (ZGA)-associated regulatory network and reveal coordination among multiple epigenetic layers, transcription factors and repeat elements that instruct proper ZGA. Cell fates associated cis-regulatory elements are activated stepwise in post-ZGA stages. Trophectoderm (TE)-specific transcription factors play dual roles in promoting the TE program while repressing the inner cell mass (ICM) program during the ICM/TE separation.
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