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Slx5p‐Slx8p Promotes Accurate Chromosome Segregation by Mediating the Degradation of Synaptonemal Complex Components during Meiosis

机译:SLX5P-SLX8P通过在减数分裂期间介导Synaponemal复合体组分的降解来促进精确的染色体隔离

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Meiosis increases genetic diversity, yet the genome complement needs to be stable to ensure offspring viability. Both small ubiquitin‐like modifier (SUMO) and ubiquitin have been reported to participate in meiotic regulation, yet functions of the SUMO‐ubiquitination crosstalk in meiosis remain unclear. Here, it is reported that a SUMO‐targeted ubiquitin ligase, Slx8p, promotes accurate chromosome segregation during meiosis, since the deletion of SLX8 leads to increased aneuploidy due to a defect in synaptonemal complex (SC) component degradation. Both the RING domain and SUMO interacting motifs of Slx8p are essential for meiotic progression and maintaining spore viability, and the expression of tetraubiquitin fused with SUMO partially rescues meiotic defects in the SLX8‐deletion strain. Furthermore, Slx5p‐Slx8p can directly add ubiquitin to SUMOylated Zip1p and Ecm11p, and forced degradation of Ecm11p partially rescues the sporulation defects of the SLX8 deletion strain. These findings provide a mechanism for SC disassembly and reveal that the crosstalk between SUMOylation and ubiquitination facilitates accurate chromosome segregation by promoting SC component degradation during meiosis.
机译:减数分裂增加了遗传多样性,但基因组补充需要稳定,以确保后代存活率。据报道,遍布泛素样改性剂(SUMO)和泛素均据报道参与减数分裂调节,但在白鱼中的Sumo-ubiquitation串扰的功能仍然尚不清楚。这里,据报道,由于Sysemal复合物(SC)组分降解的缺陷导致SLX8导致SLX8的缺失导致SLX8的缺失,SLX8P,SLX8P,SLX8P,SLX8P,促进了SLX8P的SLX8P,促进了减数分裂中的精确染色体隔离。 SLX8P的环形结构域和SUMO相互作用基序均为减数分裂性和维持孢子活力至关重要,并且与SUMO融合的四沸蛋白的表达部分抵押SLX8缺失菌株中的减少生物缺陷。此外,SLX5P-SLX8P可以直接将泛素添加到SumoyLated Zip1P和ECM11P中,并且ECM11P的强制劣化部分地抵押SLX8缺失菌株的孢子缺陷。这些发现提供了SC拆卸的机制,并揭示了Suboylation和泛素化之间的串扰通过在减数分裂期间促进SC组分降解来促进精确的染色体隔离。

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