Comparison of the spectra of genetic damage in N4-hydroxycytidine-induced ad-3 mutations between nucleotide excision repair-proficient and -deficient heterokaryons of Neurospora crassa

Abstract A comparison has been made of the mutagenic effects of N 4 -hydroxycytidine (HC) in the adenine-3 ( ad-3 ) region of two-component heterokaryons of Neurospora crassa : nucleotide excision repair-proficient ( uvs-2 + / uvs-2 + ) heterokaryon 12 (H-12) and nucleotide excision repair-deficient ( uvs-2 / uvs-2 ) heterokaryon 59 (H-59). HC was found to produce mutations predominantly, if not exclusively, by AT to GC base-pair transitions in Escherichia coli strain K12 by Janion and Glickman (1980, Mutation Res., 72, 43–47) and Sledziewska-Gojska et al. (1992, Mutagenesis, 7, 41–46). The ad-3 forward-mutation, specific-locus assay system permits the recovery of ad-3A and/or ad-3B mutants resulting from gene/point mutation, multiple-locus mutation, and multilocus deletion mutation. Uvs-2 , which is homokaryotic in H-59, results in a recovery of HC-induced ad-3 forward mutations at a frequency in H-59 that is comparable to that found in H-12. Genetic analysis of ad-3 mutants recovered from experiments with HC treatment demonstrates that predominantly gene/point mutations were found in both strains: 99.3% (540/544) in H-12, and 97.4% (531/545) in H-59. Genetic analysis of allelic complementation among the ad-3B R mutations demonstrated that HC induced the highest percentage of complementing mutants ever found with base analogs both in H-12 (99.7% [328/329]) and H-59 (91.2% [290/318]). As a result of these findings, the majority of HC-induced ad-3 mutations are postulated to have resulted from missense mutations. Thus, we conclude that the results in Neurospora are consistent with the observations in E. coli strain K-12, where HC induces predominantly AT to GC base-pair transitions.