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CENP-B controls centromere formation depending on the chromatin context

机译:CENP-B根据染色质环境控制着丝粒的形成

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The centromere is a chromatin region that serves as the spindle attachment point and directs accurate inheritance of eukaryotic chromosomes during cell divisions. However, the mechanism by which the centromere assembles and stabilizes at a specific genomic region is not clear. The de novo formation of a human/mammalian artificial chromosome (HAC/MAC) with a functional centromere assembly requires the presence of alpha-satellite DNA containing binding motifs for the centromeric CENP-B protein. We demonstrate here that de novo centromere assembly on HAC/MAC is dependent on CENP-B. In contrast, centromere formation is suppressed in cells expressing CENP-B when alpha-satellite DNA was integrated into a chromosomal site. Remarkably, on those integration sites CENP-B enhances histone H3-K9 trimethylation and DNA methylation, thereby stimulating heterochromatin formation. Thus, we propose that CENP-B plays a dual role in centromere formation, ensuring de novo formation on DNA lacking a functional centromere but preventing the formation of excess centromeres on chromosomes.
机译:着丝粒是一个染色质区域,它充当纺锤体附着点,并在细胞分裂过程中指导真核染色体的准确遗传。但是,着丝粒在特定基因组区域组装并稳定的机制尚不清楚。从头形成具有功能着丝粒装配的人/哺乳动物人工染色体(HAC / MAC)要求存在含有着丝粒CENP-B蛋白结合基序的α-卫星DNA。我们在这里证明,HAC / MAC上的从头着丝粒组装依赖于CENP-B。相反,当α-卫星DNA整合入染色体位点时,表达CENP-B的细胞的着丝粒形成受到抑制。值得注意的是,在那些整合位点,CENP-B增强了组蛋白H3-K9三甲基化和DNA甲基化,从而刺激了异染色质的形成。因此,我们建议CENP-B在着丝粒形成中起双重作用,确保在缺乏功能着丝粒的DNA上从头形成,但防止染色体上多余着丝粒的形成。

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