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Spatial Genome Re-organization between Fetal and Adult Hematopoietic Stem Cells

机译:胎儿和成人造血干细胞之间的空间基因组重组。

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Fetal hematopoietic stem cells (HSCs) undergo a developmental switch to become adult HSCs with distinct functional properties. To better understand the molecular mechanisms underlying the developmental switch, we have conducted deep sequencing of the 3D genome, epigenome, and transcriptome of fetal and adult HSCs in mouse. We find that chromosomal compartments and topologically associating domains (TADs) are largely conserved between fetal and adult HSCs. However, there is a global trend of increased compartmentalization and TAD boundary strength in adult HSCs. In contrast, intra-TAD chromatin interactions are much more dynamic and widespread, involving over a thousand gene promoters and distal enhancers. These developmental-stage-specific enhancer-promoter interactions are mediated by different sets of transcription factors, such as TCF3 and MAFB in fetal HSCs, versus NR4A1 and GATA3 in adult HSCs. Loss-of-function studies of TCF3 confirm the role of TCF3 in mediating condition-specific enhancer-promoter interactions and gene regulation in fetal HSCs.
机译:胎儿造血干细胞(HSC)经历了发展的转变,成为具有独特功能特性的成年HSC。为了更好地理解发育转换的分子机制,我们对小鼠的胎儿和成年HSC的3D基因组,表观基因组和转录组进行了深度测序。我们发现,在染色体和成人HSC之间,染色体区室和拓扑相关域(TADs)基本上是保守的。然而,在成年HSC中,存在全球性的趋势,即其分隔和TAD边界强度增加。相比之下,TAD内染色质相互作用更为动态和广泛,涉及上千种基因启动子和远端增强子。这些发育阶段特异性增强子-启动子相互作用是由不同组的转录因子介导的,例如胎儿HSC中的TCF3和MAFB,而成人HSC中的NR4A1和GATA3。 TCF3的功能丧失研究证实了TCF3在介导胎儿HSC中的条件特异性增强子-启动子相互作用和基因调控中的作用。

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