Affiliation:
1. Department of Microbiology, University of Illinois at Urbana-Champaign, Urbana, Illinois
Abstract
ABSTRACT
Endonuclease V, encoded by the
nfi
gene, initiates removal of the base analogs hypoxanthine and xanthine from DNA, acting to prevent mutagenesis from purine base deamination within the DNA. On the other hand, the RdgB nucleotide hydrolase in
Escherichia coli
is proposed to prevent hypoxanthine and xanthine incorporation into DNA by intercepting the noncanonical DNA precursors dITP and dXTP. Because many base analogs are mutagenic when incorporated into DNA, it is intuitive to think of RdgB as acting to prevent similar mutagenesis from deaminated purines in the DNA precursor pools. To test this idea, we used a set of Claire Cupples' strains to detect changes in spontaneous mutagenesis spectra, as well as in nitrous acid-induced mutagenesis spectra, in wild-type cells and in
rdgB
single,
nfi
single, and
rdgB nfi
double mutants. We found neither a significant increase in spontaneous mutagenesis in
rdgB
and
nfi
single mutants or the double mutant nor any changes in nitrous acid-induced mutagenesis for
rdgB
mutant strains. We conclude that incorporation of deaminated purines into DNA is nonmutagenic.
Publisher
American Society for Microbiology
Subject
Molecular Biology,Microbiology
Cited by
28 articles.
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