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Interaction of excision repair gene products and mitotic recombination functions in yeast
Authors:Beth A. Montelone  Bee Choo Liang-Chong
Affiliation:(1) Division of Biology, Kansas State University, 66506 Manhattan, KS, USA;(2) Department of Physics, Kansas State University, 66506 Manhattan, KS, USA
Abstract:
We have tested the ability of mutants of three additional genes in the excision repair pathway of Saccharomyces cerevisiae to suppress the hyper-recombination and rad52 double-mutant lethality phenotypes of the rad3-102 (formerly rem1-2) mutation. Such suppression has previously been been observed with mutant alleles of RAD1 and RAD4. We had hypothesized that the rad3-102 mutation created elevated levels of DNA lesions which could be processed by the products of the RAD1 and RAD4 genes into recombinogenic double-strand breaks requiring the RAD52 product for repair. In this report, we show that the RAD2, RAD7, and RAD10 genes are also necessary for this processing. We discuss our observations of varying levels of mitotic crossingover in Rem-rad double-mutant strains.
Keywords:Mitotic recombination  RAD3 gene  Nucleotide excision repair  Yeast
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