期刊
DNA REPAIR
卷 7, 期 11, 页码 1846-1854出版社
ELSEVIER
DOI: 10.1016/j.dnarep.2008.07.011
关键词
Dog-1 mutator; Fanconi anemia; FANCJ; Genome instability; Chromosome instability (CIN); Chromosomal rearrangement; Lethal analysis
资金
- Natural Science and Engineering Research Council (NSERC)
The Caenorhabditis elegans ortholog of the Fanconi anemia pathway component J (FANCJ) is DOG-1, which is essential for genome stability. Previous studies have shown that disruption of the dog-1 gene generates small deletions of poly-C/poly-G tracts detectable by PCR and results in a mutator phenotype. In this paper, we describe the isolation and characterization of lethal mutations resulting from the loss of dog-1 function. The mutant strains were analyzed using a combination of techniques including genetic mapping, SNP mapping, and oaCGH (oligo array Comparative Genome Hybridization). Using the eT1 balancer system to recover lethal mutants, we isolated, in addition to small deletions, large chromosomal rear-rangements, including duplications, translocations and deficiencies. The forward mutation frequency was 10-fold higher than the spontaneous frequency for eT1, and equivalent to that observed for low doses of standard mutagens. From a screen for suppressors of mdf-1/MAD1 lethality, we previously had isolated such-4(h2168), shown here to be a large tandem duplication. Thus, the range of mutational events caused by lack of DOG-1/FANCJ is much broader than previously described. (C) 2008 Elsevier B.V. All rights reserved.
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