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Assembly in G1 phase and long-term stability are unique intrinsic features of CENP-A nucleosomes

机译:G1期组装和长期稳定性是CENP-A核小体的独特内在特征

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Centromeres are the site of kinetochore formation during mitosis. Centromere protein A (CENP-A), the centromere-specific histone H3 variant, is essential for the epigenetic maintenance of centromere position. Previously we showed that newly synthesized CENP-A is targeted to centromeres exclusively during early G1 phase and is subsequently maintained across mitotic divisions. Using SNAP-based fluorescent pulse labeling, we now demonstrate that cell cycle–restricted chromatin assembly at centromeres is unique to CENP-A nucleosomes and does not involve assembly of other H3 variants. Strikingly, stable retention is restricted to the CENP-A/H4 core of the nucleosome, which we find to outlast general chromatin across several cell divisions. We further show that cell cycle timing of CENP-A assembly is independent of centromeric DNA sequences and instead is mediated by the CENP-A targeting domain. Unexpectedly, this domain also induces stable transmission of centromeric nucleosomes, independent of the CENP-A deposition factor HJURP. This demonstrates that intrinsic properties of the CENP-A protein direct its cell cycle–restricted assembly and induces quantitative mitotic transmission of the CENP-A/H4 nucleosome core, ensuring long-term stability and epigenetic maintenance of centromere position.
机译:着丝粒是有丝分裂期间动粒形成的部位。着丝粒蛋白A(CENP-A)是着丝粒特异的组蛋白H3变体,对着丝粒位置的表观遗传保持至关重要。以前,我们表明,新合成的CENP-A仅在G1早期就靶向着丝粒,随后在有丝分裂中得以维持。现在,使用基于SNAP的荧光脉冲标记,我们证明了着丝粒上受细胞周期限制的染色质组装是CENP-A核小体所独有的,并且不涉及其他H3变体的组装。令人惊讶的是,稳定的保留仅限于核小体的CENP-A / H4核心,我们发现其在几个细胞分裂中都比一般的染色质持久。我们进一步表明,CENP-A程序集的细胞周期时机独立于着丝粒DNA序列,而是由CENP-A靶向域介导。出乎意料的是,该结构域还诱导着着丝粒核小体的稳定传递,而与CENP-A沉积因子HJURP无关。这表明CENP-A蛋白的内在特性指导其细胞周期受限的组装,并诱导CENP-A / H4核小体核的定量有丝分裂传递,从而确保了长期稳定和着丝粒位置的表观遗传维持。

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