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Divergent wiring of repressive and active chromatin interactions between mouse embryonic and trophoblast lineages

机译:小鼠胚胎和滋养细胞谱系之间的染色质相互作用和压抑相互作用的不同接线

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摘要

The establishment of the embryonic and trophoblast lineages is a developmental decision underpinned by dramatic differences in the epigenetic landscape of the two compartments. However, it remains unknown how epigenetic information and transcription factor networks map to the 3D arrangement of the genome, which in turn may mediate transcriptional divergence between the two cell lineages. Here, we perform promoter capture Hi-C experiments in mouse trophoblast (TSC) and embryonic (ESC) stem cells to understand how chromatin conformation relates to cell-specific transcriptional programmes. We find that key TSC genes that are kept repressed in ESCs exhibit interactions between H3K27me3-marked regions in ESCs that depend on Polycomb repressive complex 1. Interactions that are prominent in TSCs are enriched for enhancer–gene contacts involving key TSC transcription factors, as well as TET1, which helps to maintain the expression of TSC-relevant genes. Our work shows that the first developmental cell fate decision results in distinct chromatin conformation patterns establishing lineage-specific contexts involving both repressive and active interactions.
机译:胚胎和滋养细胞谱系的建立是一个发展决定,其依据是两个区隔的表观遗传学景观存在显着差异。然而,尚不清楚表观遗传信息和转录因子网络如何映射到基因组的3D排列,而3D排列又可以介导两个细胞谱系之间的转录分歧。在这里,我们在小鼠滋养细胞(TSC)和胚胎(ESC)干细胞中进行启动子捕获Hi-C实验,以了解染色质构象如何与细胞特异性转录程序相关。我们发现,保持在ESC中的关键TSC基因在依赖于Polycomb阻遏复合物1的ESC中显示出H3K27me3标记区域之间的相互作用。在TSC中突出的相互作用也丰富了涉及关键TSC转录因子的增强子-基因接触。 TET1,有助于维持TSC相关基因的表达。我们的工作表明,第一个发育细胞的命运决定会导致不同的染色质构象模式,从而建立涉及抑制性和主动性相互作用的特定于谱系的环境。

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