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首页> 外文期刊>Journal of cell biology >Centromere-localized Aurora B kinase is required for the fidelity of chromosome segregation
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Centromere-localized Aurora B kinase is required for the fidelity of chromosome segregation

机译:Centromere局部化的Aurora B激酶是染色体隔离的保真所必需的

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Aurora B kinase plays an essential role in chromosome bi-orientation, which is a prerequisite for equal segregation of chromosomes during mitosis. However, it remains largely unclear whether centromere-localized Aurora B is required for faithful chromosome segregation. Here we show that histone H3 Thr-3 phosphorylation (H3pT3) and H2A Thr-120 phosphorylation (H2ApT120) can independently recruit Aurora B. Disrupting H3pT3-mediated localization of Aurora B at the inner centromere impedes the decline in H2ApT120 during metaphase and causes H2ApT120-dependent accumulation of Aurora B at the kinetochore-proximal centromere. Consequently, silencing of the spindle assembly checkpoint (SAC) is delayed, whereas the fidelity of chromosome segregation is negligibly affected. Further eliminating an H2ApT120-dependent pool of Aurora B restores proper timing for SAC silencing but increases chromosome missegregation. Our data indicate that H2ApT120-mediated localization of Aurora B compensates for the loss of an H3pT3-dependent pool of Aurora B to correct improper kinetochore–microtubule attachments. This study provides important insights into how centromeric Aurora B regulates SAC and kinetochore attachment to microtubules to ensure error-free chromosome segregation.
机译:Aurora B激酶在染色体双向中起重要作用,这是在有丝分裂期间相等染色体偏析的先决条件。然而,它仍然很大程度上尚不清楚忠实染色体隔离所需的甲状腺局部化的极光B是否需要。在这里,我们表明组蛋白H3 Thr-3磷酸化(H3PT3)和H2A Thr-120磷酸化(H2APT120)可以独立地募集Aurora B.破坏内厘罗米雷姆在中期期间的H2APT120的下降的H3PT3介导的定位并导致H2APT120 - 在Kinetochore-Proximromere的Aurora B依存积累。因此,延迟了主轴组件检查点(SAC)的沉默,而染色体隔离的保真度是可忽视的影响。进一步消除了Aurora B的H2APT120依赖性池恢复囊沉默的适当时刻,但增加了染色体错误误导。我们的数据表明,AURORA B的H2APT120介导的定位补偿了Aurora B的H3PT3依赖性池的损失,以纠正不正确的Kinetochore-Microtubule附件。本研究提供了浓溴铁罗拉B如何调节对微管的囊和Kinetochore附着的重要见解,以确保无差错的染色体隔离。

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