Shared and Unique Evolutionary Trajectories to Ciprofloxacin Resistance in Gram-Negative Bacterial Pathogens
Author(s) -
Jaime E. Zlamal,
Semen A. Leyn,
Mallika Iyer,
Marinela L. Elane,
Nicholas A. Wong,
James W. Wamsley,
Maarten Vercruysse,
Fernando García-Alcalde,
Andrei L. Osterman
Publication year - 2021
Publication title -
mbio
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 3.562
H-Index - 121
eISSN - 2161-2129
pISSN - 2150-7511
DOI - 10.1128/mbio.00987-21
Subject(s) - antibiotic resistance , biology , microbial genetics , resistance (ecology) , computational biology , genome , antibiotics , whole genome sequencing , evolutionary dynamics , genetics , microbiology and biotechnology , gene , medicine , population , ecology , environmental health
Resistance to the broad-spectrum antibiotic ciprofloxacin is detected at high rates for a wide range of bacterial pathogens. To investigate the dynamics of ciprofloxacin resistance development, we applied a comparative resistomics workflow for three clinically relevant species of Gram-negative bacteria: Escherichia coli , Acinetobacter baumannii , and Pseudomonas aeruginosa . We combined experimental evolution in a morbidostat with deep sequencing of evolving bacterial populations in time series to reveal both shared and unique aspects of evolutionary trajectories. Representative clone characterization by sequencing and MIC measurements enabled direct assessment of the impact of mutations on the extent of acquired drug resistance. In all three species, we observed a two-stage evolution: (i) early ciprofloxacin resistance reaching 4- to 16-fold the MIC for the wild type, commonly as a result of single mutations in DNA gyrase target genes ( gyrA or gyrB ), and (ii) additional genetic alterations affecting the transcriptional control of the drug efflux machinery or secondary target genes (DNA topoisomerase parC or parE ).
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