Remodelling bivalent chromatin is essential for mouse peri-implantation embryogenesis

Yanhe Li; Jincan He; Yingdong Liu; Yi Hui; Shanyao Liu; Yalin Zhang; Yan Xiong; Tingting Xu; Ziwen Xu; Zhuoao Zhang; Yan Zhang; Guang Yang; Jia Zhao; Dandan Bai; Xinyi Lei; Xiaochen Kou; Yanhong Zhao; Jing Du; Zheng Guo; Jiqing Yin; Xiaoqing Zhang; Congling Xu; Yawei Gao; Miaoxin Chen; Hong Wang; Cizhong Jiang; Shaorong Gao; Wenqiang Liu

doi:10.1038/s41556-025-01776-w

Remodelling bivalent chromatin is essential for mouse peri-implantation embryogenesis

Yanhe Li
, Jincan He
, Yingdong Liu
, Yi Hui
, Shanyao Liu
, Yalin Zhang
, Yan Xiong
, Tingting Xu
, Ziwen Xu
, Zhuoao Zhang
, Yan Zhang
, Guang Yang
, Jia Zhao
, Dandan Bai
, Xinyi Lei
, Xiaochen Kou
, Yanhong Zhao
, Jing Du
, Zheng Guo
, Jiqing Yin

Xiaoqing Zhang, Congling Xu, Yawei Gao, Miaoxin Chen, Hong Wang, Cizhong Jiang^*, Shaorong Gao^*, Wenqiang Liu^*

^*Corresponding author for this work

School of Biological Science and Medical Engineering

Research output: Contribution to journal › Article › peer-review

1 Scopus citations

Abstract

Bivalency regulates developmental genes during lineage commitment. However, mechanisms governing bivalent domain establishment, maintenance and resolution in early embryogenesis remain unclear. Here we comprehensively trace bivalent chromatin remodelling throughout mouse peri-implantation development, revealing bifurcated establishment modes that partition epiblast and primitive endoderm regulatory programmes. We identify transiently maintained bivalent domains (TB domains) enriched in the epiblast, where gradual resolution fine-tunes pluripotency progression. Through targeted screening in embryos, we uncover 22 TB domain regulators, including the essential factor ZBTB17. Genetic ablation or degradation of ZBTB17 causes peri-implantation arrest. Mechanistically, ZBTB17 collaborates with KDM6A/B to resolve bivalency by removing H3K27me3 and priming the activation of key pluripotency genes. Remarkably, TB domain dynamics are evolutionarily shared in human pluripotent transitions, with ZBTB17 involvement despite species differences. Our work establishes a framework for bivalent chromatin regulation in early mammalian development and elucidates how its resolution precisely controls lineage commitment.

Original language	English
Pages (from-to)	1797-1811
Number of pages	15
Journal	Nature Cell Biology
Volume	27
Issue number	10
DOIs	https://doi.org/10.1038/s41556-025-01776-w
State	Published - Oct 2025

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@article{01a7be09d6844eaa93cb3f7b6cd2cd28,

title = "Remodelling bivalent chromatin is essential for mouse peri-implantation embryogenesis",

abstract = "Bivalency regulates developmental genes during lineage commitment. However, mechanisms governing bivalent domain establishment, maintenance and resolution in early embryogenesis remain unclear. Here we comprehensively trace bivalent chromatin remodelling throughout mouse peri-implantation development, revealing bifurcated establishment modes that partition epiblast and primitive endoderm regulatory programmes. We identify transiently maintained bivalent domains (TB domains) enriched in the epiblast, where gradual resolution fine-tunes pluripotency progression. Through targeted screening in embryos, we uncover 22 TB domain regulators, including the essential factor ZBTB17. Genetic ablation or degradation of ZBTB17 causes peri-implantation arrest. Mechanistically, ZBTB17 collaborates with KDM6A/B to resolve bivalency by removing H3K27me3 and priming the activation of key pluripotency genes. Remarkably, TB domain dynamics are evolutionarily shared in human pluripotent transitions, with ZBTB17 involvement despite species differences. Our work establishes a framework for bivalent chromatin regulation in early mammalian development and elucidates how its resolution precisely controls lineage commitment.",

author = "Yanhe Li and Jincan He and Yingdong Liu and Yi Hui and Shanyao Liu and Yalin Zhang and Yan Xiong and Tingting Xu and Ziwen Xu and Zhuoao Zhang and Yan Zhang and Guang Yang and Jia Zhao and Dandan Bai and Xinyi Lei and Xiaochen Kou and Yanhong Zhao and Jing Du and Zheng Guo and Jiqing Yin and Xiaoqing Zhang and Congling Xu and Yawei Gao and Miaoxin Chen and Hong Wang and Cizhong Jiang and Shaorong Gao and Wenqiang Liu",

note = "Publisher Copyright: {\textcopyright} The Author(s), under exclusive licence to Springer Nature Limited 2025.",

year = "2025",

month = oct,

doi = "10.1038/s41556-025-01776-w",

language = "英语",

volume = "27",

pages = "1797--1811",

journal = "Nature Cell Biology",

issn = "1465-7392",

publisher = "Nature Research",

number = "10",

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Li, Y, He, J, Liu, Y, Hui, Y, Liu, S, Zhang, Y, Xiong, Y, Xu, T, Xu, Z, Zhang, Z, Zhang, Y, Yang, G, Zhao, J, Bai, D, Lei, X, Kou, X, Zhao, Y, Du, J, Guo, Z, Yin, J, Zhang, X, Xu, C, Gao, Y, Chen, M, Wang, H, Jiang, C, Gao, S & Liu, W 2025, 'Remodelling bivalent chromatin is essential for mouse peri-implantation embryogenesis', Nature Cell Biology, vol. 27, no. 10, pp. 1797-1811. https://doi.org/10.1038/s41556-025-01776-w

TY - JOUR

T1 - Remodelling bivalent chromatin is essential for mouse peri-implantation embryogenesis

AU - Li, Yanhe

AU - He, Jincan

AU - Liu, Yingdong

AU - Hui, Yi

AU - Liu, Shanyao

AU - Zhang, Yalin

AU - Xiong, Yan

AU - Xu, Tingting

AU - Xu, Ziwen

AU - Zhang, Zhuoao

AU - Zhang, Yan

AU - Yang, Guang

AU - Zhao, Jia

AU - Bai, Dandan

AU - Lei, Xinyi

AU - Kou, Xiaochen

AU - Zhao, Yanhong

AU - Du, Jing

AU - Guo, Zheng

AU - Yin, Jiqing

AU - Zhang, Xiaoqing

AU - Xu, Congling

AU - Gao, Yawei

AU - Chen, Miaoxin

AU - Wang, Hong

AU - Jiang, Cizhong

AU - Gao, Shaorong

AU - Liu, Wenqiang

PY - 2025/10

Y1 - 2025/10

N2 - Bivalency regulates developmental genes during lineage commitment. However, mechanisms governing bivalent domain establishment, maintenance and resolution in early embryogenesis remain unclear. Here we comprehensively trace bivalent chromatin remodelling throughout mouse peri-implantation development, revealing bifurcated establishment modes that partition epiblast and primitive endoderm regulatory programmes. We identify transiently maintained bivalent domains (TB domains) enriched in the epiblast, where gradual resolution fine-tunes pluripotency progression. Through targeted screening in embryos, we uncover 22 TB domain regulators, including the essential factor ZBTB17. Genetic ablation or degradation of ZBTB17 causes peri-implantation arrest. Mechanistically, ZBTB17 collaborates with KDM6A/B to resolve bivalency by removing H3K27me3 and priming the activation of key pluripotency genes. Remarkably, TB domain dynamics are evolutionarily shared in human pluripotent transitions, with ZBTB17 involvement despite species differences. Our work establishes a framework for bivalent chromatin regulation in early mammalian development and elucidates how its resolution precisely controls lineage commitment.

AB - Bivalency regulates developmental genes during lineage commitment. However, mechanisms governing bivalent domain establishment, maintenance and resolution in early embryogenesis remain unclear. Here we comprehensively trace bivalent chromatin remodelling throughout mouse peri-implantation development, revealing bifurcated establishment modes that partition epiblast and primitive endoderm regulatory programmes. We identify transiently maintained bivalent domains (TB domains) enriched in the epiblast, where gradual resolution fine-tunes pluripotency progression. Through targeted screening in embryos, we uncover 22 TB domain regulators, including the essential factor ZBTB17. Genetic ablation or degradation of ZBTB17 causes peri-implantation arrest. Mechanistically, ZBTB17 collaborates with KDM6A/B to resolve bivalency by removing H3K27me3 and priming the activation of key pluripotency genes. Remarkably, TB domain dynamics are evolutionarily shared in human pluripotent transitions, with ZBTB17 involvement despite species differences. Our work establishes a framework for bivalent chromatin regulation in early mammalian development and elucidates how its resolution precisely controls lineage commitment.

UR - https://www.scopus.com/pages/publications/105017719118

U2 - 10.1038/s41556-025-01776-w

DO - 10.1038/s41556-025-01776-w

M3 - 文章

C2 - 41034520

AN - SCOPUS:105017719118

SN - 1465-7392

VL - 27

SP - 1797

EP - 1811

JO - Nature Cell Biology

JF - Nature Cell Biology

IS - 10

ER -

Remodelling bivalent chromatin is essential for mouse peri-implantation embryogenesis

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