| Literature DB >> 35037621 |
Anamaria Babosan1, David Skurnik2, Anaëlle Muggeo3, Gerald B Pier4, Zeynep Baharoglu5, Thomas Jové6, Marie-Cécile Ploy6, Sophie Griveau7, Fethi Bedioui7, Sébastien Vergnolle8, Sophie Moussalih1, Christophe de Champs3, Didier Mazel5, Thomas Guillard3.
Abstract
The plasmid-mediated quinolone resistance (PMQR) genes have been shown to promote high-level bacterial resistance to fluoroquinolone antibiotics, potentially leading to clinical treatment failures. In Escherichia coli, sub-minimum inhibitory concentrations (sub-MICs) of the widely used fluoroquinolones are known to induce the SOS response. Interestingly, the expression of several PMQR qnr genes is controlled by the SOS master regulator, LexA. During the characterization of a small qnrD-plasmid carried in E. coli, we observed that the aminoglycosides become able to induce the SOS response in this species, thus leading to the elevated transcription of qnrD. Our findings show that the induction of the SOS response is due to nitric oxide (NO) accumulation in the presence of sub-MIC of aminoglycosides. We demonstrated that the NO accumulation is driven by two plasmid genes, ORF3 and ORF4, whose products act at two levels. ORF3 encodes a putative flavin adenine dinucleotide (FAD)-binding oxidoreductase which helps NO synthesis, while ORF4 codes for a putative fumarate and nitrate reductase (FNR)-type transcription factor, related to an O2-responsive regulator of hmp expression, able to repress the Hmp-mediated NO detoxification pathway of E. coli. Thus, this discovery, that other major classes of antibiotics may induce the SOS response could have worthwhile implications for antibiotic stewardship efforts in preventing the emergence of resistance.Entities:
Keywords: E. coli; Escherichia coli; SOS; aminoglycosides; infectious disease; microbiology; qnr; stress
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Year: 2022 PMID: 35037621 PMCID: PMC8789287 DOI: 10.7554/eLife.69511
Source DB: PubMed Journal: Elife ISSN: 2050-084X Impact factor: 8.140