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Relief of the Dma1-mediated checkpoint requires Dma1 autoubiquitination and dynamic localization

机译:缓解Dma1介导的检查点需要Dma1自体泛素化和动态定位

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摘要

Chromosome segregation and cell division are coupled to prevent aneuploidy and cell death. In the fission yeast Schizosaccharomyces pombe, the septation initiation network (SIN) promotes cytokinesis, but upon mitotic checkpoint activation, the SIN is actively inhibited to prevent cytokinesis from occurring before chromosomes have safely segregated. SIN inhibition during the mitotic checkpoint is mediated by the E3 ubiquitin ligase Dma1. Dma1 binds to the CK1-phosphorylated SIN scaffold protein Sid4 at the spindle pole body (SPB), and ubiquitinates it. Sid4 ubiquitination antagonizes the SPB localization of the Pololike kinase Plo1, the major SIN activator, so that SIN signaling is delayed. How this checkpoint is silenced once spindle defects are resolved has not been clear. Here we establish that Dma1 transiently leaves SPBs during anaphase B due to extensive autoubiquitination. The SIN is required for Dma1 to return to SPBs later in anaphase. Blocking Dma1 removal from SPBs by permanently tethering it to Sid4 prevents SIN activation and cytokinesis. Therefore, controlling Dma1’s SPB dynamics in anaphase is an essential step in S. pombe cell division and the silencing of the Dma1-dependent mitotic checkpoint.
机译:染色体分离和细胞分裂相结合以防止非整倍性和细胞死亡。在裂殖酵母裂殖酵母中,分隔启动网络(SIN)促进胞质分裂,但在有丝分裂检查点激活后,SIN被积极抑制,以防止胞质分裂在染色体安全分离之前发生。有丝分裂检查点期间的SIN抑制是由E3泛素连接酶Dma1介导的。 Dma1在纺锤极体(SPB)上与CK1磷酸化的SIN支架蛋白Sid4结合,并使其泛素化。 Sid4泛素化拮抗主要SIN激活剂Pololike激酶Plo1的SPB定位,因此SIN信号传导被延迟。解决主轴缺陷后如何使此检查点静音,目前尚不清楚。在这里,我们建立Dma1由于广泛的自体泛素化而在后期B短暂离开SPB。 Dma1在后期后期返回SPB时需要SIN。通过将Dma1永久地绑定到Sid4来阻止从SPB中移除Dma1,可防止SIN激活和胞质分裂。因此,后期控制Dma1的SPB动力学是粟酒裂殖酵母细胞分裂和Dma1依赖性有丝分裂检查点沉默的重要步骤。

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