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Mating-type switching by homology-directed recombinational repair: a matter of choice

机译:通过同源性指导的重组修复进行交配类型切换:选择问题

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摘要

In eukaryotes, all DNA transactions happen in the context of chromatin that often takes part in regulatory mechanisms. In particular, chromatin structure can regulate exchanges of DNA occurring through homologous recombination. Few systems have provided as detailed a view on this phenomenon as mating-type switching in yeast. Mating-type switching entails the choice of a template for the gene conversions of the expressed mating-type locus. In the fission yeast Schizosaccharomyces pombe, correct template choice requires two competing small recombination enhancers, SRE2 and SRE3, that function in the context of heterochromatin. These two enhancers act with the Swi2/Swi5 recombination accessory complex to initiate strand exchange in a cell-type-specific manner, from SRE2 in M cells and SRE3 in P cells. New research indicates that the Set1C complex, responsible for H3K4 methylation, and the Brl2 ubiquitin ligase, that catalyzes H2BK119 ubiquitylation, participate in the cell-type-specific selection of SRE2 or SRE3. Here, we review these findings, compare donor preference in S. pombe to the distantly related budding yeast Saccharomyces cerevisiae, and contrast the positive effects of heterochromatin on the donor selection process with other situations, where heterochromatin represses recombination.
机译:在真核生物中,所有DNA交易都是在染色质的背景下发生的,而染色质通常参与调节机制。特别地,染色质结构可以调节通过同源重组发生的DNA交换。很少有系统提供关于这种现象的详细视图,例如酵母中的交配类型转换。交配型转换需要选择用于表达的交配型基因座的基因转化的模板。在裂殖酵母粟酒裂殖酵母中,正确的模板选择需要两个竞争的小型重组增强子SRE2和SRE3,它们在异染色质的背景下起作用。这两个增强子与Swi2 / Swi5重组辅助复合体一起发挥作用,以细胞类型特异性的方式启动链交换,从M细胞中的SRE2和P细胞中的SRE3。新研究表明,负责H3K4甲基化的Set1C复合体和催化H2BK119泛素化的Brl2泛素连接酶参与了SRE2或SRE3的细胞类型特异性选择。在这里,我们回顾这些发现,将粟酒裂殖酵母中的供体偏好与远缘萌芽的酿酒酵母进行比较,并比较异染色质对供体选择过程的积极影响以及其他情况,其中异染色质会抑制重组。

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