In Vitro Microevolution and Co-Selection Assessment of Florfenicol Impact on Escherichia coli Resistance Development

Ádám Kerek; Bence Török; Levente Laczkó; Gábor Kardos; Krisztián Bányai; Zoltán Somogyi; Eszter Kaszab; Krisztina Bali; Ákos Jerzsele

doi:10.3390/antibiotics12121728

In Vitro Microevolution and Co-Selection Assessment of Florfenicol Impact on Escherichia coli Resistance Development

Antibiotics (Basel). 2023 Dec 14;12(12):1728. doi: 10.3390/antibiotics12121728.

Authors

Ádám Kerek^{1

2}, Bence Török¹, Levente Laczkó³, Gábor Kardos^{2

3}, Krisztián Bányai^{1

2

4}, Zoltán Somogyi^{1

2}, Eszter Kaszab^{2

4}, Krisztina Bali⁴, Ákos Jerzsele^{1

2}

Affiliations

¹ Department of Pharmacology and Toxicology, University of Veterinary Medicine Budapest, 1078 Budapest, Hungary.
² National Laboratory of Infectious Animal Diseases, Antimicrobial Resistance, Veterinary Public Health and Food Chain Safety, University of Veterinary Medicine Budapest, 1078 Budapest, Hungary.
³ Institute of Metagenomics, University of Debrecen, 4032 Debrecen, Hungary.
⁴ Veterinary Medical Research Institute, 1143 Budapest, Hungary.

Abstract

The issue of antimicrobial resistance is becoming an increasingly serious challenge in both human and veterinary medicine. Prudent antimicrobial use in veterinary medicine is warranted and supported by international guidelines, with the Antimicrobial Advice Ad Hoc Expert Group (AMEG) placing particular emphasis on the critically important group B antimicrobials. These antimicrobials are commonly employed, especially in the poultry and swine industry. The impact of florfenicol, a veterinary antibiotic, was studied on the resistance development of Escherichia coli. The aim of the study was to investigate the effect of the use of florfenicol on the development of phenotypic and genomic resistances, not only to the drug itself but also to other drugs. The minimum inhibitory concentrations (MICs) of the antibiotics were investigated at 1×, 10×, 100× and 1000× concentrations using the adapted Microbial Evolution and Growth Arena (MEGA-plate) method. The results demonstrate that florfenicol can select for resistance to fluoroquinolone antibiotics (167× MIC value increase) and cephalosporins (67× MIC value increase). A total of 44 antimicrobial resistance genes were identified, the majority of which were consistent across the samples. Chromosomal point mutations, including alterations in resistance-associated and regulatory genes (acrB, acrR, emrR and robA), are thought to trigger multiple drug efflux pump activations, leading to phenotypically increased resistance. The study underscores the impact of florfenicol and its role in the development of antimicrobial resistance, particularly concerning fluoroquinolone antibiotics and cephalosporins. This study is the first to report florfenicol's dose-dependent enhancement of other antibiotics' MICs, linked to mutations in SOS-box genes (mdtABC-tolC, emrAB-tolC and acrAB-tolC) and increased multidrug efflux pump genes. Mutations in the regulatory genes acrR, emrR and rpbA support the possibility of increased gene expression. The results are crucial for understanding antimicrobial resistance and its development, highlighting the promising potential of in vitro evolutionary and coselection studies for future research.

Keywords: Escherichia coli; MEGA-plate; NGS; co-selection; florfenicol; microevolution.

Abstract

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