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R环塑造染色质结构以促进分化过程中的平衡谱系分配。

R-loops shape chromatin architecture to promote balanced lineage allocation during differentiation.

作者信息

Chao Chun-Hao, Fazzio Thomas G

机构信息

Department of Molecular, Cell, and Cancer Biology, University of Massachusetts Medical School, Worcester, MA 01605, USA.

Lead Contact.

出版信息

bioRxiv. 2025 Jun 25:2025.06.23.661125. doi: 10.1101/2025.06.23.661125.

Abstract

R-loops-RNA:DNA hybrids that often form co-transcriptionally-are emerging as key regulators of genome function, yet their roles in shaping chromatin architecture and developmental potential remain incompletely defined. Here, we use inducible expression in mouse embryonic stem cells (mESCs) to achieve acute, global R-loop depletion and systematically interrogate their impact on chromatin structure and lineage specification. We find that R-loop loss has minimal effect on steady-state gene expression or self-renewal. Instead, it leads to a striking reduction in H2A.Z occupancy at both active and bivalent promoters, accompanied by increased nucleosome density-revealing a previously unrecognized role for R-loops in maintaining promoter architecture. During gastruloid differentiation, R-loop-depleted mESCs exhibit a pronounced bias toward ectodermal fates, along with dysregulation of lineage-specific transcription factors and impaired cell-cell signaling. Consistent with these alterations, R-loop-depleted cells show widespread perturbations in gene regulatory networks across several early cell types. These findings uncover a critical role for R-loops in shaping the H2A.Z chromatin landscape and preserving balanced lineage trajectories during early development, offering new insights into the epigenomic regulation of stem cell fate.

摘要

R环——通常在转录过程中形成的RNA:DNA杂交体——正逐渐成为基因组功能的关键调节因子,但其在塑造染色质结构和发育潜能方面的作用仍未完全明确。在此,我们利用小鼠胚胎干细胞(mESCs)中的诱导表达来实现急性、全基因组的R环缺失,并系统地探究其对染色质结构和谱系特化的影响。我们发现,R环缺失对稳态基因表达或自我更新影响极小。相反,它导致活性启动子和双价启动子处H2A.Z占据显著减少,同时核小体密度增加——揭示了R环在维持启动子结构方面此前未被认识的作用。在原肠胚样分化过程中,R环缺失的mESCs表现出对外胚层命运的明显偏向,同时谱系特异性转录因子失调且细胞间信号传导受损。与这些改变一致,R环缺失的细胞在几种早期细胞类型的基因调控网络中表现出广泛的扰动。这些发现揭示了R环在早期发育过程中塑造H2A.Z染色质格局和维持平衡的谱系轨迹方面的关键作用,为干细胞命运的表观基因组调控提供了新的见解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/07a1/12262388/b8e5cf104f9b/nihpp-2025.06.23.661125v1-f0001.jpg

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