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首页> 外文期刊>Genetics: A Periodical Record of Investigations Bearing on Heredity and Variation >Genetic control of intrachromosomal recombination in Saccharomyces cerevisiae. I. Isolation and genetic characterization of hyper-recombination mutations.
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Genetic control of intrachromosomal recombination in Saccharomyces cerevisiae. I. Isolation and genetic characterization of hyper-recombination mutations.

机译:酿酒酵母中染色体内重组的遗传控制。 I.超重组突变的分离和遗传表征。

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Eight complementation groups have been defined for recessive mutations conferring an increased mitotic intrachromosomal recombination phenotype (hpr genes) in Saccharomyces cerevisiae. Some of the mutations preferentially increase intrachromosomal gene conversion (hpr4, hpr5 and hpr8) between repeated sequences, some increase loss of a marker between duplicated genes (hpr1 and hpr6), and some increase both types of events (hpr2, hpr3 and hpr7). New alleles of the CDC2 and CDC17 genes were recovered among these mutants. The mutants were also characterized for sensitivity to DNA damaging agents and for mutator activity. Among the more interesting mutants are hpr5, which shows a biased gene conversion in a leu2-112::URA3::leu2-k duplication; and hpr1, which has a much weaker effect on interchromosomal mitotic recombination than on intrachromosomal mitotic recombination. These analyses suggest that gene conversion and reciprocal exchange can be separated mutationally. Further studies are required to show whether different recombination pathways or different outcomes of the same recombination pathway are controlled by the genes identified in this study.
机译:八个互补组已被定义为隐性突变,赋予啤酒酵母中有丝分裂染色体内重组表型(hpr基因)增加。一些突变优先增加重复序列之间的染色体内基因转化(hpr4,hpr5和hpr8),一些突变增加重复基因之间的标记丢失(hpr1和hpr6),而某些突变则增加两种事件(hpr2,hpr3和hpr7)。在这些突变体中恢复了CDC2和CDC17基因的新等位基因。还对突变体表征了对DNA损伤剂的敏感性和突变体的活性。在更有趣的突变体中是hpr5,它在leu2-112 :: URA3 :: leu2-k复制中显示有偏向的基因转化; hpr1对染色体间有丝分裂重组的影响要比对染色体内有丝分裂重组的弱得多。这些分析表明,基因转化和相互交换可以突变分离。需要进行进一步的研究,以显示不同的重组途径或同一重组途径的不同结果是否受本研究中鉴定的基因控制。

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