| Literature DB >> 33572723 |
Bence Balázs1,2, Zoltán Tóth1,2, Fruzsina Nagy1,2, Renátó Kovács1, Hajnalka Tóth1,2, József Bálint Nagy1,2, Ákos Tóth3, Krisztina Szarka1, László Majoros1, Gábor Kardos1.
Abstract
The dominant carbapenem resistant Acinetobacter baumannii harboring blaOXA-23-like carbapenemase was replaced by blaOXA-40-like carriers in a Hungarian tertiary-care center with high meropenem but relatively low imipenem use. We hypothesized that alterations in antibiotic consumption may have contributed to this switch. Our workgroup previous study examined the relation between resistance spiral and the antibiotic consumption, and the results suggest that the antibiotic usage provoked the increasing resistance in case of A. baumannii. We aimed at measuring the activity of imipenem and meropenem to compare the selection pressure exerted by the different carbapenems in time-kill assays. Strain replacement was confirmed by whole genome sequencing, core-genome multilocus sequence typing (cgMLST), and resistome analysis. Based on results of the time-kill assays, we found a significant difference between two different sequence-types (STs) in case of meropenem, but not in case of imipenem susceptibility. The newly emerged ST636 and ST492 had increased resistance level against meropenem compared to the previously dominant ST2 and ST49. On the other hand, the imipenem and colistin resistance profiles were similar. These results suggest, that the uniform meropenem usage may have contributed to A. baumannii strain replacement in our setting.Entities:
Keywords: blaOXA-23-like-carbapenemase; blaOXA-40-like carbapenemase; carbapenem resistant Acinetobacter baumannii; changepoint analysis; clonal dynamics; multidrug resistance; strain replacement
Year: 2021 PMID: 33572723 PMCID: PMC7911629 DOI: 10.3390/antibiotics10020127
Source DB: PubMed Journal: Antibiotics (Basel) ISSN: 2079-6382