Development of amoxicillin resistance in Escherichia coli after exposure to remnants of a non-related phagemid-containing E. coli: an exploratory study.

Joep J J M Stohr Marjolein F Q Kluytmans-van den Bergh Carlo J M M Verhulst John W A Rossen Jan A J W Kluytmans

Antimicrob Resist Infect Control

Department of Infection Control, Amphia Hospital, Breda, the Netherlands.

Published: March 2020

- The study aimed to investigate how exposure to remnants of a specific E. coli strain, previously treated with a propanol-based hand rub, influences antimicrobial resistance in E. coli isolates.
- A total of 200 experiments were conducted, revealing that 11% of E. coli isolates exposed to remnants of the treated strain developed amoxicillin resistance, while less than 2% showed resistance when exposed to a control strain or the hand rub alone.
- The observed resistance was attributed to mutations affecting the regulation of the AmpC beta-lactamase gene, which is linked to increased production of the enzyme that contributes to resistance against antibiotics.

Objective: To determine the effect of exposure to remnants of a phagemid-containing E. coli, killed by treatment with a propanol-based hand rub, on antimicrobial resistance in E. coli isolates.

Methods: An in vitro model was developed in which a clinical E. coli isolate (EUR1) was exposed to remnants of an E. coli K-12 strain containing a phagemid (pBS-E12) strain treated with Sterillium®. A series of 200 experiments was performed using this in vitro model. As a control, a series of 400 experiments was performed where the EUR1 was exposed either to the remnants of an E. coli K-12 strain (not containing a phagemid) (E12) treated with Sterillium® (n = 200) or to dried Sterillium® only (n = 200). The number of experiments that showed growth of an amoxicillin-resistant EUR1 isolate was evaluated in all three groups. An additional 48 experiments were performed in which a different clinical E. coli isolate (EUR2) was exposed to remnants of the pBS-E12 treated with Sterillium®. Whole-genome sequencing and phenotypic testing for AmpC beta-lactamase production was performed to investigate the mechanism behind this resistance development.

Results: In 22 (11.0%) of 200 experiments in which the EUR1 isolate was exposed to remnants of a pBS-E12 an amoxicillin-resistant mutant isolate was obtained, as opposed to only 2 (1.0%) of 200 experiments involving the exposure of the EUR1 to Sterillium® only (risk difference: 10.0%; 95% CI 5.4-14.6%)) and 1 (0.5%) of 200 experiments involving the exposure of the EUR1 isolate to the remnants of the phagemid-free E12 (risk difference: 10.5%; 95% CI 6.1-14.9%). In 1 (2.1%) of the 48 experiments in which the EUR2 isolate was exposed to remnants of a pBS-E12 an amoxicillin-resistant mutant isolate was obtained. The development of resistance in all experiments was due to mutations in the promoter/attenuator region of the chromosomal AmpC beta-lactamase (cAmpC) gene leading to cAmpC hyperproduction.

Conclusion: Exposure of an E. coli isolate to another phagemid-containing E. coli that was treated with propanol-based hand rub increased the development of amoxicillin resistance. Although phagemids are cloning vectors that are not present in clinical isolates, this finding may have implications for hand disinfection practices in healthcare facilities.

Download full-text PDF	Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC7077161	PMC
http://dx.doi.org/10.1186/s13756-020-00708-7	DOI Listing

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