Interplay Between Membrane Permeability and Enzymatic Barrier Leads to Antibiotic-Dependent Resistance in Klebsiella Pneumoniae

Interplay Between Membrane Permeability and Enzymatic Barrier Leads to Antibiotic-Dependent Resistance in Klebsiella Pneumoniae

The interplay between membrane permeability alterations and the enzymatic barrier contributes to multidrug resistance. We assessed the specific effect of the efflux levels of the main efflux pumps (AcrAB and OqxAB), alone and associated with the loss of the main porins (OmpK35 and OMPK36), on the ac...

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Published in:Frontiers in microbiology Vol. 9; p. 1422
Main Authors: Nicolas-Chanoine, Marie-Helene, Mayer, Noémie, Guyot, Kathleen, Dumont, Estelle, Pagès, Jean-Marie
Format: Journal Article
Language:English
Published: Switzerland Frontiers Media 29-06-2018
Frontiers Media S.A
Subjects:
Bacteriology
beta-lactamases
ceftolozane+tazobactam
efflux pump
Klebsiella pneumoniae
Life Sciences
Microbiology
Microbiology and Parasitology
porins
resistance mechanism interplay
ceftolozane+tazobactam
resistance mechanism interplay
efflux pump
beta-lactamases
ceftazidime+avibactam
porins
Klebsiella pneumoniae
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Summary:The interplay between membrane permeability alterations and the enzymatic barrier contributes to multidrug resistance. We assessed the specific effect of the efflux levels of the main efflux pumps (AcrAB and OqxAB), alone and associated with the loss of the main porins (OmpK35 and OMPK36), on the activity of various antibiotics by constructing a set of isogenic strains, including strains with plasmid-mediated β-lactamases (DHA-1, CTX-M-15, and OXA-48). The two pumps contributed to intrinsic chloramphenicol resistance and AcrAB to that of nalidixic acid and cefoxitin, whereas they had no impact on the activity of the other 11 antibiotics tested. We confirmed the expulsion of these three antibiotics by the two overproduced pumps and that of tigecycline by overproduced AcrAB, and showed that overproduced AcrAB also expelled ertapenem, piperacillin, ceftolozane, and ceftazidime. The sole loss of porins did not significantly affect the activity of the tested antibiotics, except ertapenem. The effect of efflux increases and porin loss on β-lactam activity was the highest in plasmid-mediated β-lactamase-producing strains. Thus, DHA-1-producing strains became non-susceptible (NS) to (i) ertapenem when there was an increase in efflux or porin loss, (ii) imipenem and ceftazidime+avibactam when the two mechanisms were associated, and (iii) temocillin when AcrAB was overproduced. The CTX-M-15-producing strains became NS to (i) ertapenem when there was no porin, (ii) ceftolozane+tazobactam when there was either overproduced OqxAB or porin loss, and (iii) temocillin when AcrAB was overproduced. OXA-48-producing strains known to be NS to temocillin were also NS to ceftolozane and they became NS to imipenem when the two pumps were overproduced or there was porin loss. Overall, this study shows that the balance between influx and efflux differentially modulates the activity of the tested antibiotics, an important point for evaluating the activity of future antibiotics or new combinations.
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Reviewed by: Jessica M. A. Blair, University of Birmingham, United Kingdom; Hiroshi Nikaido, University of California, Berkeley, United States
Present Address: Kathleen Guyot, Laboratoire de Biologie, Centre Hospitalier Victor Provo, Roubaix, France
Edited by: Helen Zgurskaya, University of Oklahoma, United States
This article was submitted to Antimicrobials, Resistance and Chemotherapy, a section of the journal Frontiers in Microbiology
ISSN:1664-302X
1664-302X
DOI:10.3389/fmicb.2018.01422