首页> 外文期刊>Genes and Development: a Journal Devoted to the Molecular Analysis of Gene Expression in Eukaryotes, Prokaryotes, and Viruses >A mitotic topoisomerase II checkpoint in budding yeast is required for genome stability but acts independently of Pds1/securin.
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A mitotic topoisomerase II checkpoint in budding yeast is required for genome stability but acts independently of Pds1/securin.

机译:发芽酵母中的有丝分裂拓扑异构酶II检查点是基因组稳定所必需的,但其作用独立于Pds1 / securin。

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摘要

Topoisomerase II (Topo II) performs topological modifications on double-stranded DNA molecules that are essential for chromosome condensation, resolution, and segregation. In mammals, G2 and metaphase cell cycle delays induced by Topo II poisons have been proposed to be the result of checkpoint activation in response to the catenation state of DNA. However, the apparent lack of such controls in model organisms has excluded genetic proof that Topo II checkpoints exist and are separable from the conventional DNA damage checkpoint controls. But here, we define a Topo II-dependent G2/M checkpoint in a genetically amenable eukaryote, budding yeast, and demonstrate that this checkpoint enhances cell survival. Conversely, a lack of the checkpoint results in aneuploidy. Neither DNA damage-responsive pathways nor Pds1/securin are needed for this checkpoint. Unusually, spindle assembly checkpoint components are required for the Topo II checkpoint, but checkpoint activation is not the result of failed chromosome biorientation or a lack of spindle tension. Thus, compromised Topo II function activates a yeast checkpoint system that operates by a novel mechanism.
机译:拓扑异构酶II(Topo II)对双链DNA分子进行拓扑修饰,这对于染色体浓缩,分离和分离必不可少。在哺乳动物中,Topo II毒物诱导的G2和中期细胞周期延迟被认为是响应DNA的连接状态而激活检查点的结果。但是,在模型生物中明显缺乏这种控制,已经排除了遗传证据证明Topo II检查点存在,并且可以与常规的DNA损伤检查点控制区分开。但是在这里,我们在遗传上可接受的真核生物,发芽酵母中定义了一个依赖Topo II的G2 / M检查点,并证明了该检查点可以提高细胞存活率。相反,缺少检查点会导致非整倍性。此检查点既不需要DNA损伤反应途径,也不需要Pds1 / securin。通常,Topo II检查点需要主轴组件检查点组件,但检查点激活不是染色体生物定向失败或缺少主轴张力的结果。因此,受损的Topo II功能会激活通过新机制运行的酵母检查点系统。

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