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错配修复系统减少减数分裂中的同源重组,并刺激依赖重组的染色体丢失。

The mismatch repair system reduces meiotic homeologous recombination and stimulates recombination-dependent chromosome loss.

作者信息

Chambers S R, Hunter N, Louis E J, Borts R H

机构信息

Yeast Genetics, Institute of Molecular Medicine, John Radcliffe Hospital, Oxford, United Kingdom.

出版信息

Mol Cell Biol. 1996 Nov;16(11):6110-20. doi: 10.1128/MCB.16.11.6110.

Abstract

Efficient genetic recombination requires near-perfect homology between participating molecules. Sequence divergence reduces the frequency of recombination, a process that is dependent on the activity of the mismatch repair system. The effects of chromosomal divergence in diploids of Saccharomyces cerevisiae in which one copy of chromosome III is derived from a closely related species, Saccharomyces paradoxus, have been examined. Meiotic recombination between the diverged chromosomes is decreased by 25-fold. Spore viability is reduced with an observable increase in the number of tetrads with only two or three viable spores. Asci with only two viable spores are disomic for chromosome III, consistent with meiosis I nondisjunction of the homeologs. Asci with three viable spores are highly enriched for recombinants relative to tetrads with four viable spores. In 96% of the class with three viable spores, only one spore possesses a recombinant chromosome III, suggesting that the recombination process itself contributes to meiotic death. This phenomenon is dependent on the activities of the mismatch repair genes PMS1 and MSH2. A model of mismatch-stimulated chromosome loss is proposed to account for this observation. As expected, crossing over is increased in pms1 and msh2 mutants. Furthermore, genetic exchange in pms1 msh2 double mutants is affected to a greater extent than in either mutant alone, suggesting that the two proteins act independently to inhibit homeologous recombination. All mismatch repair-deficient strains exhibited reductions in the rate of chromosome III nondisjunction.

摘要

高效的基因重组需要参与重组的分子之间具有近乎完美的同源性。序列差异会降低重组频率,这一过程依赖于错配修复系统的活性。研究了酿酒酵母二倍体中染色体差异的影响,其中第三条染色体的一个拷贝来自密切相关的物种——奇异酿酒酵母。差异染色体之间的减数分裂重组减少了25倍。孢子活力降低,四分体中只有两个或三个活孢子的数量明显增加。只有两个活孢子的子囊对于第三条染色体是二体的,这与同源染色体在减数分裂I中的不分离一致。与有四个活孢子的四分体相比,有三个活孢子的子囊高度富集重组体。在96%有三个活孢子的类别中,只有一个孢子拥有重组的第三条染色体,这表明重组过程本身导致了减数分裂死亡。这种现象依赖于错配修复基因PMS1和MSH2的活性。提出了一个错配刺激染色体丢失的模型来解释这一观察结果。正如预期的那样,pms1和msh2突变体中的交叉增加。此外,pms1 msh2双突变体中的基因交换比单独的任何一个突变体受到的影响更大,这表明这两种蛋白质独立发挥作用以抑制同源重组。所有错配修复缺陷菌株的第三条染色体不分离率均降低。

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