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Cbx2 stably associates with mitotic chromosomes via a PRC2- or PRC1-independent mechanism and is needed for recruiting PRC1 complex to mitotic chromosomes

机译:Cbx2通过不依赖PRC2或PRC1的机制与有丝分裂染色体稳定缔合,是将PRC1复合物募集到有丝分裂染色体所必需的

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摘要

Polycomb group (PcG) proteins are epigenetic transcriptional factors that repress key developmental regulators and maintain cellular identity through mitosis via a poorly understood mechanism. Using quantitative live-cell imaging in mouse ES cells and tumor cells, we demonstrate that, although Polycomb repressive complex (PRC) 1 proteins (Cbx-family proteins, Ring1b, Mel18, and Phc1) exhibit variable capacities of association with mitotic chromosomes, Cbx2 overwhelmingly binds to mitotic chromosomes. The recruitment of Cbx2 to mitotic chromosomes is independent of PRC1 or PRC2, and Cbx2 is needed to recruit PRC1 complex to mitotic chromosomes. Quantitative fluorescence recovery after photobleaching analysis indicates that PRC1 proteins rapidly exchange at interphasic chromatin. On entry into mitosis, Cbx2, Ring1b, Mel18, and Phc1 proteins become immobilized at mitotic chromosomes, whereas other Cbx-family proteins dynamically bind to mitotic chromosomes. Depletion of PRC1 or PRC2 protein has no effect on the immobilization of Cbx2 on mitotic chromosomes. We find that the N-terminus of Cbx2 is needed for its recruitment to mitotic chromosomes, whereas the C-terminus is required for its immobilization. Thus these results provide fundamental insights into the molecular mechanisms of epigenetic inheritance.
机译:polycomb group(PcG)蛋白是表观遗传的转录因子,可抑制关键的发育调节因子,并通过人们了解的机制通过有丝分裂维持细胞身份。使用小鼠ES细胞和肿瘤细胞中的定量活细胞成像,我们证明,尽管Polycomb Repressed Complex(PRC)1蛋白(Cbx家族蛋白,Ring1b,Mel18和Phc1)表现出与有丝分裂染色体Cbx2关联的可变能力绝大多数与有丝分裂染色体结合。 Cbx2募集到有丝分裂染色体独立于PRC1或PRC2,并且需要Cbx2才能将PRC1复杂募集到有丝分裂染色体。光漂白分析后定量荧光恢复表明,PRC1蛋白在相间染色质快速交换。进入有丝分裂后,Cbx2,Ring1b,Mel18和Phc1蛋白固定在有丝分裂染色体上,而其他Cbx家族蛋白则动态结合到有丝分裂染色体上。 PRC1或PRC2蛋白的消耗对Cbx2在有丝分裂染色体上的固定没有影响。我们发现Cbx2的N末端是其募集到有丝分裂染色体所必需的,而C末端是其固定化所必需的。因此,这些结果为表观遗传遗传的分子机制提供了基本的见识。

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