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p63 and Brg1 control developmentally regulated higher-order chromatin remodelling at the epidermal differentiation complex locus in epidermal progenitor cells

机译:p63和Brg1在表皮祖细胞的表皮分化复合物基因座上控制发育调节的高级染色质重塑

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摘要

Chromatin structural states and their remodelling, including higherorder chromatin folding and three-dimensional (3D) genome organisation, play an important role in the control of gene expression. The role of 3D genome organisation in the control and execution of lineage-specific transcription programmes during the development and differentiation of multipotent stem cells into specialised cell types remains poorly understood. Here, we show that substantial remodelling of the higher-order chromatin structure of the epidermal differentiation complex (EDC), a keratinocyte lineage-specific gene locus on mouse chromosome 3, occurs during epidermal morphogenesis. During epidermal development, the locus relocates away from the nuclear periphery towards the nuclear interior into a compartment enriched in SC35-positive nuclear speckles. Relocation of the EDC locus occurs prior to the full activation of EDC genes involved in controlling terminal keratinocyte differentiation and is a lineage-specific, developmentally regulated event controlled by transcription factor p63, a master regulator of epidermal development. We also show that, in epidermal progenitor cells, p63 directly regulates the expression of the ATP-dependent chromatin remodeller Brg1, which binds to distinct domains within the EDC and is required for relocation of the EDC towards the nuclear interior. Furthermore, Brg1 also regulates gene expression within the EDC locus during epidermal morphogenesis. Thus, p63 and its direct target Brg1 play an essential role in remodelling the higher-order chromatin structure of the EDC and in the specific positioning of this locus within the landscape of the 3D nuclear space, as required for the efficient expression of EDC genes in epidermal progenitor cells during skin development.
机译:染色质的结构状态及其重塑,包括高阶染色质折叠和三维(3D)基因组组织,在控制基因表达中起着重要作用。 3D基因组组织在多能干细胞发育和分化为特定细胞类型的过程中在控制和执行谱系特异性转录程序中的作用仍然知之甚少。在这里,我们显示表皮分化复合物(EDC),小鼠染色体3上的角质形成细胞谱系特异性基因位点的高阶染色质结构的实质重塑。在表皮发育过程中,基因座从核外围移向核内部,进入一个富含SC35阳性核斑点的隔室。 EDC基因座的重新定位发生在参与控制末端角质形成细胞分化的EDC基因完全活化之前,并且是由表皮发育的主要调控因子转录因子p63所控制的特定于谱系的发育调控事件。我们还显示,在表皮祖细胞中,p63直接调节ATP依赖的染色质重塑剂Brg1的表达,该蛋白与EDC内的不同域结合,并且是EDC向核内部重新定位所必需的。此外,Brg1还调节表皮形态发生过程中EDC基因座内的基因表达。因此,p63及其直接靶标Brg1在重塑EDC的高级染色质结构以及此基因座在3D核空间景观中的特定位置方面起着至关重要的作用,这是EDC基因在大肠杆菌中高效表达所必需的。皮肤发育过程中的表皮祖细胞。

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