Welz-Voegele Caroline, Jinks-Robertson Sue
Department of Molecular Genetics and Microbiology, Duke University Medical Center, Durham, North Carolina 27710, USA.
Genetics. 2008 Jul;179(3):1251-62. doi: 10.1534/genetics.108.090233. Epub 2008 Jun 18.
Homologous recombination between dispersed repeated sequences is important in shaping eukaryotic genome structure, and such ectopic interactions are affected by repeat size and sequence identity. A transformation-based, gap-repair assay was used to examine the effect of 2% sequence divergence on the efficiency of mitotic double-strand break repair templated by chromosomal sequences in yeast. Because the repaired plasmid could either remain autonomous or integrate into the genome, the effect of sequence divergence on the crossover-noncrossover (CO-NCO) outcome was also examined. Finally, proteins important for regulating the CO-NCO outcome and for enforcing identity requirements during recombination were examined by transforming appropriate mutant strains. Results demonstrate that the basic CO-NCO outcome is regulated by the Rad1-Rad10 endonuclease and the Sgs1 and Srs2 helicases, that sequence divergence impedes CO to a much greater extent than NCO events, that an intact mismatch repair system is required for the discriminating identical and nonidentical repair templates, and that the Sgs1 and Srs2 helicases play additional, antirecombination roles when the interacting sequences are not identical.
分散重复序列之间的同源重组在塑造真核生物基因组结构方面很重要,而且这种异位相互作用会受到重复序列大小和序列同一性的影响。一种基于转化的缺口修复试验被用于检测2%的序列差异对酵母中染色体序列介导的有丝分裂双链断裂修复效率的影响。由于修复后的质粒既可以保持自主状态,也可以整合到基因组中,因此还检测了序列差异对交换-非交换(CO-NCO)结果的影响。最后,通过转化合适的突变菌株,研究了对调控CO-NCO结果以及在重组过程中强化同一性要求至关重要的蛋白质。结果表明,基本的CO-NCO结果受Rad1-Rad10核酸内切酶以及Sgs1和Srs2解旋酶的调控,序列差异对交换的阻碍程度远大于对非交换事件的阻碍,区分相同和不同的修复模板需要完整的错配修复系统,并且当相互作用的序列不同时,Sgs1和Srs2解旋酶还发挥额外的抗重组作用。