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首页> 外文期刊>The Journal of biological chemistry >Acidic Nucleoplasmic DNA-binding Protein (And-1) Controls Chromosome Congression by Regulating the Assembly of Centromere Protein A (CENP-A) at Centromeres
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Acidic Nucleoplasmic DNA-binding Protein (And-1) Controls Chromosome Congression by Regulating the Assembly of Centromere Protein A (CENP-A) at Centromeres

机译:酸性骨髓DNA结合蛋白(和-1)通过在Centromeres中调节Centromere蛋白A(CENP-A)的组装来控制染色体乳腺

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The centromere is an epigenetically designated chromatin domain that is essential for the accurate segregation of chromosomes during mitosis. The incorporation of centromere protein A (CENP-A) into chromatin is fundamental in defining the centromeric loci. Newly synthesized CENP-A is loaded at centromeres in early G1 phase by the CENP-A-specific histone chaperone Holliday junction recognition protein (HJURP) coupled with other chromatin assembly factors. However, it is unknown whether there are additional HJURP-interacting factor(s) involving in this process. Here we identify acidic nucleoplasmic DNA-binding protein 1 (And-1) as a new factor that is required for the assembly of CENP-A nucleosomes. And-1 interacts with both CENP-A and HJURP in a prenucleosomal complex, and the association of And-1 with CENP-A is increased during the cell cycle transition from mitosis to G1 phase. And-1 down-regulation significantly compromises chromosome congression and the deposition of HJURP-CENP-A complexes at centromeres. Consistently, overexpression of And-1 enhances the assembly of CENP-A at centromeres. We conclude that And-1 is an important factor that functions together with HJURP to facilitate the cell cycle-specific recruitment of CENP-A to centromeres.
机译:Centromere是一种表观指定的染色质结构域,对于在有丝分裂期间染色体的准确分离是必不可少的。将Centromere蛋白A(CENP-A)的掺入染色质是定义焦化基因座的基础。新合成的CENP-A通过CENP-A特异性组蛋白霍尔达结识别蛋白(HJURP)与其他染色质组装因子一起加载以升高的G1相。然而,尚不清楚是否存在涉及该过程的额外的Hjurp相互作用因子。在这里,我们将酸性核状DNA结合蛋白1(和-1)鉴定为组装CENP-A核肉所需的新因素。 AND-1在预核糖瓜复合物中与CENP-A和HJURP相互作用,并且在细胞周期转换到从丝分裂到G1相时,CENP-A的关联和-1的关联增加。和1个下调显着损害染色体会非和沉淀铬蛋白 - 在Centromeres的复合物的沉积。始终如一地,过表达和1增强CENP-A在CENTORES的组装。我们得出结论,和-1是与Hjurp一起致力于促进CENP-A的细胞循环募集的重要因素。

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