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Molecular maps of the reorganization of genome-nuclear lamina interactions during differentiation.

机译:分化过程中基因组与核层板相互作用的重组分子图。

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The three-dimensional organization of chromosomes within the nucleus and its dynamics during differentiation are largely unknown. To visualize this process in molecular detail, we generated high-resolution maps of genome-nuclear lamina interactions during subsequent differentiation of mouse embryonic stem cells via lineage-committed neural precursor cells into terminally differentiated astrocytes. This reveals that a basal chromosome architecture present in embryonic stem cells is cumulatively altered at hundreds of sites during lineage commitment and subsequent terminal differentiation. This remodeling involves both individual transcription units and multigene regions and affects many genes that determine cellular identity. Often, genes that move away from the lamina are concomitantly activated; many others, however, remain inactive yet become unlocked for activation in a next differentiation step. These results suggest that lamina-genome interactions are widely involved in the control of gene expression programs during lineage commitment and terminal differentiation.
机译:核内染色体的三维组织及其在分化过程中的动力学是未知的。为了在分子细节上可视化此过程,我们在小鼠胚胎干细胞通过谱系组成的神经前体细胞分化为最终分化的星形胶质细胞的后续分化过程中,生成了基因组与核层间相互作用的高分辨率图。这揭示了胚胎干细胞中存在的基础染色体结构在谱系定型和随后的终末分化期间在数百个位点处累积改变。这种重塑涉及单个转录单位和多基因区域,并影响许多决定细胞身份的基因。通常,从叶片移开的基因会同时被激活。但是,许多其他设备仍处于非活动状态,但在下一步的区分步骤中被解锁以进行激活。这些结果表明,在沿袭定型和终末分化期间,层板基因组相互作用广泛参与基因表达程序的控制。

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