Nucleosome organization of mouse embryos during pre-implantation development

Sexual reproduction begins with sperm–oocyte fusion to form a zygote, where chromatin undergoes dramatic reorganization to establish totipotency. Although nucleosomes- the basic units of eukaryotic chromatin and key epigenetic regulators- are extensively remodeled during early embryogenesis, their d...

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Published inScientific reports Vol. 15; no. 1; pp. 21894 - 17
Main Authors Zeng, Jitao, Tu, Xiaojuan, Qu, Siming, Chen, Xichan, Wang, Ying, Liu, Xiaona, Kang, Enchuan, Tian, Yi, Xiang, Qianming, Lai, Binbin, Gao, Weiwu, Ni, Bing, He, Wei
Format Journal Article
LanguageEnglish
Published London Nature Publishing Group UK 01.07.2025
Nature Portfolio
Subjects
631/136
631/136/2086
631/208
631/208/177
Animals
Blastocyst - metabolism
Chromatin - metabolism
Chromatin Assembly and Disassembly
Chromatin organization
Embryo, Mammalian - metabolism
Embryonic Development - genetics
Embryos
Female
Gene Expression Regulation, Developmental
H3K4me3
Histones - metabolism
Humanities and Social Sciences
Male
Mice
multidisciplinary
Nucleosome position
Nucleosomes - genetics
Nucleosomes - metabolism
Science
Science (multidisciplinary)
scMNase-seq
Transcription Initiation Site
Chromatin organization
Nucleosome position
Embryos
H3K4me3
scMNase-seq
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Summary:Sexual reproduction begins with sperm–oocyte fusion to form a zygote, where chromatin undergoes dramatic reorganization to establish totipotency. Although nucleosomes- the basic units of eukaryotic chromatin and key epigenetic regulators- are extensively remodeled during early embryogenesis, their dynamic repositioning mechanisms and biological implications remain unclear. Here, we employed single-cell MNase sequencing (scMNase-seq) to map genome-wide nucleosome positioning and chromatin accessibility in individual mammalian embryos. We found that nucleosome positioning mirrored somatic cell patterns until the 4-cell stage, with nucleosome depletion and phasing at CTCF sites not fully established until morula formation. By integrating H3K4me3 localization and transcriptomic data, we revealed that nucleosome sparsity at transcription start sites (TSS) and flanking regions correlated with expression levels of genes critical for preimplantation development. Notably, these nucleosome-depleted regions likely serve as regulatory hubs influencing histone modification dynamics. Our study systematically delineates nucleosome reorganization principles during mammalian embryogenesis and provides a high-resolution resource for understanding chromatin remodeling in early development.
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ISSN:2045-2322
2045-2322
DOI:10.1038/s41598-025-05642-5