Paula Díaz-de-Alba scite author profile

Bactericidal activity of quinolones has been related to a combination of DNA fragmentation, reactive oxygen species (ROS) production and programmed cell death (PCD) systems. The underlying molecular systems responsible for reducing bactericidal effect during antimicrobial therapy in low-level quinolone resistance (LLQR) phenotypes need to be clarified. To do this and also define possible new antimicrobial targets, the transcriptome profile of isogenic Escherichia coli harboring quinolone resistance mechanisms in the presence of a clinical relevant concentration of ciprofloxacin was evaluated. A marked differential response to ciprofloxacin of either up- or downregulation was observed in LLQR strains. Multiple genes implicated in ROS modulation (related to the TCA cycle, aerobic respiration and detoxification systems) were upregulated (sdhC up to 63.5-fold) in mutants with LLQR. SOS system components were downregulated (recA up to 30.7-fold). yihE, a protective kinase coding for PCD, was also upregulated (up to 5.2-fold). SdhC inhibition sensitized LLQR phenotypes (up to ΔLog = 2.3 after 24 h). At clinically relevant concentrations of ciprofloxacin, gene expression patterns in critical systems to bacterial survival and mutant development were significantly modified in LLQR phenotypes. Chemical inhibition of SdhC (succinate dehydrogenase) validated modulation of ROS as an interesting target for bacterial sensitization.

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Characterization of Plasmid-Mediated Quinolone Resistance Determinants in High-Level Quinolone-ResistantEnterobacteriaceaeIsolates from the Community: First Report ofqnrDGene in Algeria

Yanat

Machuca

Díaz-de-Alba

et al. 2017

Microbial Drug Resistance

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Assessment of a phenotypic algorithm to detect plasmid-mediated quinolone resistance in Enterobacteriaceae

Rodríguez-Martínez

López-Cerero

Díaz-de-Alba

et al. 2015

J. Antimicrob. Chemother.

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