@article{mbs:/content/journal/jmm/10.1099/jmm.0.45701-0, author = "Gerrits, Monique M and van der Wouden, Egbert-Jan and Bax, Dorine A and van Zwet, Anton A and van Vliet, Arnoud HM and de Jong, Albertine and Kusters, Johannes G and Thijs, Jaap C and Kuipers, Ernst J", title = "Role of the rdxA and frxA genes in oxygen-dependent metronidazole resistance of Helicobacter pylori", journal= "Journal of Medical Microbiology", year = "2004", volume = "53", number = "11", pages = "1123-1128", doi = "https://doi.org/10.1099/jmm.0.45701-0", url = "https://www.microbiologyresearch.org/content/journal/jmm/10.1099/jmm.0.45701-0", publisher = "Microbiology Society", issn = "1473-5644", type = "Journal Article", abstract = "Almost 50 % of all Helicobacter pylori isolates are resistant to metronidazole, which reduces the efficacy of metronidazole-containing regimens, but does not make them completely ineffective. This discrepancy between in vitro metronidazole resistance and treatment outcome may partially be explained by changes in oxygen pressure in the gastric environment, as metronidazole-resistant (MtzR) H. pylori isolates become metronidazole-susceptible (MtzS) under low oxygen conditions in vitro. In H. pylori the rdxA and frxA genes encode reductases which are required for the activation of metronidazole, and inactivation of these genes results in metronidazole resistance. Here the role of inactivating mutations in these genes on the reversibility of metronidazole resistance under low oxygen conditions is established. Clinical H. pylori isolates containing mutations resulting in a truncated RdxA and/or FrxA protein were selected and incubated under anaerobic conditions, and the effect of these conditions on the MICs of metronidazole, amoxycillin, clarithromycin and tetracycline, and cell viability were determined. While anaerobiosis had no effect on amoxycillin, clarithromycin and tetracycline resistance, all isolates lost their metronidazole resistance when cultured under anaerobic conditions. This loss of metronidazole resistance also occurred in the presence of the protein synthesis inhibitor chloramphenicol. Thus, factor(s) that activate metronidazole under low oxygen tension are not specifically induced by low oxygen conditions, but are already present under microaerophilic conditions. As there were no significant differences in cell viability between the clinical isolates, it is likely that neither the rdxA nor the frxA gene participates in the reversibility of metronidazole resistance.", }