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. 2024 Jun;26(6):962-974.
doi: 10.1038/s41556-024-01422-x. Epub 2024 Jun 5.

Mapping putative enhancers in mouse oocytes and early embryos reveals TCF3/12 as key folliculogenesis regulators

Bofeng Liu #  1   2 Yuanlin He #  3   4 Xiaotong Wu #  2   5 Zili Lin #  1   2 Jing Ma #  1   2 Yuexin Qiu  3 Yunlong Xiang  1   2 Feng Kong  1   2 Fangnong Lai  1   2 Mrinmoy Pal  6 Peizhe Wang  7 Jia Ming  7 Bingjie Zhang  1   2 Qiujun Wang  1   2 Jingyi Wu  1   2 Weikun Xia  1   2 Weimin Shen  2   5 Jie Na  7 Maria-Elena Torres-Padilla  6 Jing Li  8   9 Wei Xie  10   11
Affiliations

Mapping putative enhancers in mouse oocytes and early embryos reveals TCF3/12 as key folliculogenesis regulators

Bofeng Liu et al. Nat Cell Biol. 2024 Jun.

Abstract

Dynamic epigenomic reprogramming occurs during mammalian oocyte maturation and early development. However, the underlying transcription circuitry remains poorly characterized. By mapping cis-regulatory elements using H3K27ac, we identified putative enhancers in mouse oocytes and early embryos distinct from those in adult tissues, enabling global transitions of regulatory landscapes around fertilization and implantation. Gene deserts harbour prevalent putative enhancers in fully grown oocytes linked to oocyte-specific genes and repeat activation. Embryo-specific enhancers are primed before zygotic genome activation and are restricted by oocyte-inherited H3K27me3. Putative enhancers in oocytes often manifest H3K4me3, bidirectional transcription, Pol II binding and can drive transcription in STARR-seq and a reporter assay. Finally, motif analysis of these elements identified crucial regulators of oogenesis, TCF3 and TCF12, the deficiency of which impairs activation of key oocyte genes and folliculogenesis. These data reveal distinctive regulatory landscapes and their interacting transcription factors that underpin the development of mammalian oocytes and early embryos.

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