UvrA and UvrB Suppress Illegitimate Recombination: Synergistic Action with RecQ Helicase

Illegitimate recombination is a major cause of genetic instability in prokaryotes as well as in eukaryotes. This recombination usually occurs at a low frequency, but it is greatly enhanced by UV irradiation or other environmental stresses. DNA damages produced by these environmental stresses are tho...

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Bibliographic Details
Published in:Proceedings of the National Academy of Sciences - PNAS 2000-05, Vol.97 (11), p.5989-5994
Main Authors: Hanada, Katsuhiro, Iwasaki, Mihoko, Ihashi, Sonoe, Ikeda, Hideo
Format: Article
Language:English
Subjects:
Adenosine Triphosphatases - physiology
Annealing
Bacteria
Bacterial Proteins - physiology
Bacteriophage lambda - genetics
Bacteriophages
Biological Sciences
DNA
DNA Damage
DNA Helicases - physiology
DNA Repair
DNA, Bacterial - genetics
DNA, Bacterial - metabolism
DNA, Bacterial - radiation effects
DNA-Binding Proteins - physiology
Endodeoxyribonucleases
Escherichia coli - genetics
Escherichia coli - radiation effects
Escherichia coli Proteins
Genetic mutation
Genetics
Irradiation
Lesions
Mutation
Overproduction
Phenotypes
Plasmids
Proteins
Recombination, Genetic - physiology
RecQ helicase
RecQ Helicases
Ultraviolet Rays
uvrA gene
UvrA protein
uvrB gene
UvrB protein
uvrC gene
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Summary:Illegitimate recombination is a major cause of genetic instability in prokaryotes as well as in eukaryotes. This recombination usually occurs at a low frequency, but it is greatly enhanced by UV irradiation or other environmental stresses. DNA damages produced by these environmental stresses are thought to induce DNA double-strand breaks, leading to illegitimate recombination. In this paper we show that UV-induced illegitimate recombination is enhanced by mutations of nucleotide excision repair genes, uvrA or uvrB, and partially by uvrC mutation, but not by uvrD mutation. Unexpectedly, the recombination was enhanced by the uvrA uvrB double mutation even without UV irradiation, but the uvrB uvrC double mutation has not shown this effect, suggesting that illegitimate recombination is mostly suppressed by UvrA and UvrB. Moreover, illegitimate recombination was synergistically enhanced by the recQ uvrA double mutation. In addition, overproduction of the UvrA protein suppressed the hyperrecombination phenotype of the recQ or uvrB mutant, but it did not affect the UV-sensitive phenotype of the uvrB mutant. We concluded that the UvrAB complex suppresses illegitimate recombination in a pathway shared with RecQ helicase. In addition, UvrA protein alone can suppress illegitimate recombination in the pathway, in which RecQ helicase and UvrAB complex work. Possible functions of the proteins involved in these pathways are also discussed.
ISSN:0027-8424
1091-6490
DOI:10.1073/pnas.100101297