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Global changes in nuclear positioning of genes and intra- and inter-domain genomic interactions that orchestrate B cell fate

机译:在基因和分子内和域间基因组的互动核定位全球变化编排B细胞命运

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摘要

The genome is folded into domains located in either transcriptionally inert or permissive compartments. Here we used genome-wide strategies to characterize domains during B cell development. Structured Interaction Matrix Analysis revealed that CTCF occupancy was primarily associated with intra-domain interactions, whereas p300, E2A and PU.1 bound sites were associated with intra- and inter-domain interactions that are developmentally regulated. We identified a spectrum of genes that switched nuclear location during early B cell development. In progenitors the transcriptionally inactive Ebf1 locus was sequestered at the nuclear lamina, thereby preserving multipotency. Upon development into the pro-B cell stage Ebf1 and other genes switched compartments to establish de novo intra- and inter-domain interactions that are associated with a B lineage specific transcription signature.
机译:基因组被折叠成位于转录惰性或允许区室的结构域。在这里,我们使用了全基因组策略来表征B细胞发育过程中的结构域。结构化相互作用矩阵分析显示,CTCF占用主要与域内相互作用相关,而p300,E2A和PU.1结合位点与受发育调控的域内和域间相互作用相关。我们鉴定了在早期B细胞发育过程中切换核位置的一系列基因。在祖细胞中,转录无活性的Ebf1基因座被隔离在核层中,从而保持了多能性。在发展为亲B细胞阶段后,Ebf1和其他基因切换隔室,以建立与B谱系特异性转录标记相关的从头域内和域间相互作用。

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