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三维基因组结构协调乳腺上皮细胞谱系特化的关键调节因子。

Three-dimensional genome architecture coordinates key regulators of lineage specification in mammary epithelial cells.

作者信息

Milevskiy Michael J G, Coughlan Hannah D, Kane Serena R, Johanson Timothy M, Kordafshari Somayeh, Chan Wing Fuk, Tsai Minhsuang, Surgenor Elliot, Wilcox Stephen, Allan Rhys S, Chen Yunshun, Lindeman Geoffrey J, Smyth Gordon K, Visvader Jane E

机构信息

ACRF Cancer Biology and Stem Cells Division, The Walter and Eliza Hall Institute of Medical Research, Parkville, VIC 3052, Australia.

Department of Medical Biology, The University of Melbourne, Parkville, VIC 3010, Australia.

出版信息

Cell Genom. 2023 Oct 16;3(11):100424. doi: 10.1016/j.xgen.2023.100424. eCollection 2023 Nov 8.

Abstract

Although lineage-specific genes have been identified in the mammary gland, little is known about the contribution of the 3D genome organization to gene regulation in the epithelium. Here, we describe the chromatin landscape of the three major epithelial subsets through integration of long- and short-range chromatin interactions, accessibility, histone modifications, and gene expression. While basal genes display exquisite lineage specificity via distal enhancers, luminal-specific genes show widespread promoter priming in basal cells. Cell specificity in luminal progenitors is largely mediated through extensive chromatin interactions with super-enhancers in gene-body regions in addition to interactions with polycomb silencer elements. Moreover, lineage-specific transcription factors appear to be controlled through cell-specific chromatin interactivity. Finally, chromatin accessibility rather than interactivity emerged as a defining feature of the activation of quiescent basal stem cells. This work provides a comprehensive resource for understanding the role of higher-order chromatin interactions in cell-fate specification and differentiation in the adult mouse mammary gland.

摘要

尽管已经在乳腺中鉴定出了谱系特异性基因,但对于三维基因组组织在上皮细胞基因调控中的作用却知之甚少。在这里,我们通过整合长程和短程染色质相互作用、可及性、组蛋白修饰和基因表达,描述了三种主要上皮亚群的染色质景观。虽然基底细胞基因通过远端增强子表现出精细的谱系特异性,但管腔特异性基因在基底细胞中显示出广泛的启动子起始。管腔祖细胞中的细胞特异性在很大程度上是通过与基因体区域中的超级增强子进行广泛的染色质相互作用以及与多梳抑制元件的相互作用来介导的。此外,谱系特异性转录因子似乎是通过细胞特异性染色质相互作用来控制的。最后,染色质可及性而非相互作用成为静止基底干细胞激活的决定性特征。这项工作为理解高阶染色质相互作用在成年小鼠乳腺细胞命运决定和分化中的作用提供了一个全面的资源。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8824/10667557/63bc8bc1beab/fx1.jpg

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