小泛素样修饰物(SUMO)修饰调控酿酒酵母减数分裂中突触复合体和多复合体的组装。
SUMO modifications control assembly of synaptonemal complex and polycomplex in meiosis of Saccharomyces cerevisiae.
作者信息
Cheng Chung-Hsu, Lo Yu-Hui, Liang Shu-Shan, Ti Shih-Chieh, Lin Feng-Ming, Yeh Chia-Hui, Huang Han-Yi, Wang Ting-Fang
机构信息
Institute of Biochemical Science, National Taiwan University, Taipei.
出版信息
Genes Dev. 2006 Aug 1;20(15):2067-81. doi: 10.1101/gad.1430406. Epub 2006 Jul 17.
Abstract
The synaptonemal complex (SC) is a proteinaceous complex that apparently mediates synapsis between homologous chromosomes during meiotic prophase. In Saccharomyces cerevisiae, the Zip1 protein is the integral component of the SC. In the absence of a DNA double-strand break or the SC initiation protein Zip3, Zip1 proteins aggregate to form a polycomplex (PC). In addition, Zip1 is also responsible for DSB-independent nonhomologous centromere coupling at early meiotic prophase. We report here that Zip3 is a SUMO (small ubiquitin-related modifier) E3 ligase and that Zip1 is a binding protein for SUMO-conjugated products. Our results also suggest that at early meiotic prophase, Zip1 interacts with Zip3-independent Smt3 conjugates (e.g., Top2) to promote nonhomologous centromere coupling. At and after mid-prophase, the Zip1 protein begins to associate with Zip3-dependent Smt3 conjugates (e.g., Red1) along meiotic chromosomes in the wild-type cell to form SCs and with Smt3 polymeric chains in the zip3 mutant to form PCs.
摘要
联会复合体(SC)是一种蛋白质复合体,在减数分裂前期显然介导同源染色体之间的联会。在酿酒酵母中,Zip1蛋白是SC的主要组成部分。在没有DNA双链断裂或SC起始蛋白Zip3的情况下,Zip1蛋白聚集形成多复合体(PC)。此外,Zip1还负责减数分裂前期早期不依赖双链断裂的非同源着丝粒配对。我们在此报告,Zip3是一种小泛素相关修饰物(SUMO)E3连接酶,而Zip1是SUMO共轭产物的结合蛋白。我们的结果还表明,在减数分裂前期早期,Zip1与不依赖Zip3的Smt3共轭物(如Top2)相互作用,以促进非同源着丝粒配对。在前期中期及之后,Zip1蛋白开始在野生型细胞中沿着减数分裂染色体与依赖Zip3的Smt3共轭物(如Red1)结合形成SCs,并在zip3突变体中与Smt3聚合链结合形成PCs。
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