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首页> 外文期刊>Nature Communications >Mechanism of centromere recruitment of the CENP-A chaperone HJURP and its implications for centromere licensing
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Mechanism of centromere recruitment of the CENP-A chaperone HJURP and its implications for centromere licensing

机译:CENTMERE招募CENP-A伴侣HJURP的机制及其对CENTROMERE许可的影响

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Nucleosomes containing the histone H3 variant CENP-A are the epigenetic mark of centromeres, the kinetochore assembly sites required for chromosome segregation. HJURP is the CENP-A chaperone, which associates with Mis18α, Mis18β, and M18BP1 to target centromeres and deposit new CENP-A. How these proteins interact to promote CENP-A deposition remains poorly understood. Here we show that two repeats in human HJURP proposed to be functionally distinct are in fact interchangeable and bind concomitantly to the 4:2:2 Mis18α:Mis18β:M18BP1 complex without dissociating it. HJURP binds CENP-A:H4 dimers, and therefore assembly of CENP-A:H4 tetramers must be performed by two Mis18αβ:M18BP1:HJURP complexes, or by the same complex in consecutive rounds. The Mis18α N-terminal tails blockade two identical HJURP-repeat binding sites near the Mis18αβ C-terminal helices. These were identified by photo-cross-linking experiments and mutated to separate Mis18 from HJURP centromere recruitment. Our results identify molecular underpinnings of eukaryotic chromosome inheritance and shed light on how centromeres license CENP-A deposition.
机译:含有组蛋白H3变体CENP-A的核体是焦体的表观遗传标记,染色体偏析所需的KINETOCHORE组装位点。 Hjurp是CENP-A伴侣,其与MIS18α,MIS18β和M18BP1相关联,以靶心圆环并存放新的CENP-A。这些蛋白质如何相互作用,促进CENP-A沉积仍然明确。在这里,我们表明,人类Hjurp中的两次重复建议在功能上独立实际上是可互换的,并结合到4:2:2mis18α:MIS18β:M18BP1复合物而不分解它。 Hjurp结合CENP-A:H4二聚体,因此CENP-A的组装:H4四聚体必须由两种MIS18αβ:M18BP1:Hjurp络合物或在连续回合中的相同复合物进行。 MIS18αn末端尾部阻止MIS18αβC终端螺旋附近的两个相同的Hjurp-Repeating站点。这些通过光交联实验鉴定并突变以与Hjurp Centromere招聘中的单独MIS18进行突变。我们的结果鉴定了真核染色体遗传和棚光的分子底层,以CENROMERES许可CENP-A沉积。

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