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Impact of plasmid-borne oqxAB on the development of fluoroquinolone resistance and bacterial fitness in Escherichia coli.

Authors :
Jing Wang
Ze-Wen Guo
Chan-Ping Zhi
Tong Yang
Jing-Jing Zhao
Xiao-Jie Chen
Li Zeng
Lu-Chao Lv
Zhen-Ling Zeng
Jian-Hua Liu
Wang, Jing
Guo, Ze-Wen
Zhi, Chan-Ping
Yang, Tong
Zhao, Jing-Jing
Chen, Xiao-Jie
Zeng, Li
Lv, Lu-Chao
Zeng, Zhen-Ling
Liu, Jian-Hua
Source :
Journal of Antimicrobial Chemotherapy (JAC). May2017, Vol. 72 Issue 5, p1293-1302. 10p.
Publication Year :
2017

Abstract

<bold>Objectives: </bold>To investigate the impact of plasmid-borne oqxAB genes on the development of fluoroquinolone resistance, mutations and bacterial fitness in Escherichia coli .<bold>Methods: </bold>MICs and mutation prevention concentrations were compared among E. coli strain TOP10 and two corresponding transformants harbouring the OqxAB-encoding plasmids. Mutants were selected by serial passages with the 0.5-fold MIC of ciprofloxacin, and were randomly selected to determine mutations. Bacterial fitness was evaluated by competition assays in vitro and in vivo .<bold>Results: </bold>The oqxAB -carrying plasmids contributed to a 4-8-fold increase in the ciprofloxacin MIC and increased the ciprofloxacin mutation prevention concentration by 8-16-fold. The MIC of ciprofloxacin for the two transformants increased faster than that of E. coli TOP10 by serial passaging. Novel mutations in gyrB (A468P or F458V) were first observed. Mutations in gyrA were distributed at codons 87 and 83 in the two transformants, whereas mutation A119E in gyrA dominated in the TOP10 mutants. Although the two oqxAB -bearing plasmids caused a decrease in fitness in vitro , their fitness increased when combined with more than one chromosomal mutation, and clear biological benefits were observed in vivo . The mutations in gyrB were associated with a fitness cost, which could be compensated for by additional mutations. The novel mutation gyrA ΔS83 significantly reduced biological fitness both in vitro and in vivo , and was thus quickly replaced by more beneficial mutations in the population.<bold>Conclusions: </bold>The possession of plasmid-borne oqxAB may facilitate the evolution of fluoroquinolone resistance, and the fitness cost of OqxAB-encoding plasmids could be compensated by additional chromosomal mutations. [ABSTRACT FROM AUTHOR]

Details

Language :
English
ISSN :
03057453
Volume :
72
Issue :
5
Database :
Academic Search Index
Journal :
Journal of Antimicrobial Chemotherapy (JAC)
Publication Type :
Academic Journal
Accession number :
122690327
Full Text :
https://doi.org/10.1093/jac/dkw576