Affiliation:
1. Center for Anti-Infective Research and Development, Hartford Hospital, Hartford, Connecticut
2. Department of Medicine, Division of Infectious Diseases, Hartford Hospital, Hartford, Connecticut
Abstract
ABSTRACT
We have previously demonstrated that a high-dose, prolonged-infusion meropenem regimen (2 g every 8 h [q8h]; 3-hour infusion) can achieve 40% free drug concentration above the MIC against
Pseudomonas aeruginosa
with MICs of ≤16 μg/ml. The objective of this experiment was to compare the efficacy of this high-dose, prolonged-infusion regimen against carbapenemase-producing
Klebsiella pneumoniae
isolates with the efficacy against
P. aeruginosa
isolates having similar meropenem MICs. An
in vitro
pharmacodynamic model was used to simulate human serum concentrations. Eleven genotypically confirmed
K. pneumoniae
carbapenemase (KPC)-producing isolates and six clinical
P. aeruginosa
isolates were tested for 24 h, and time-kill curves were constructed. High-performance liquid chromatography (HPLC) was used to verify meropenem concentrations in each experiment. Meropenem achieved a rapid ≥3 log CFU reduction against all KPC isolates within 6 h, followed by regrowth in all but two isolates. The targeted %
f
T>MIC (percent time that free drug concentrations remain above the MIC) exposure was achieved against both of these KPC isolates (100%
f
T>MIC versus MIC = 2 μg/ml, 75%
f
T>MIC versus MIC = 8 μg/ml). Against KPC isolates with MICs of 8 and 16 μg/ml that did regrow, actual meropenem exposures were significantly lower than targeted due to rapid
in vitro
hydrolysis, whereby targeted %
f
T>MIC was reduced with each subsequent dosing. In contrast, a ≥3 log CFU reduction was maintained over 24 h for all
Pseudomonas
isolates with meropenem MICs of 8 and 16 μg/ml. Although KPC and
P. aeruginosa
isolates may share similar meropenem MICs, the differing resistance mechanisms produce discordant responses to a high-dose, prolonged infusion of meropenem. Thus, predicting the efficacy of an antimicrobial regimen based on MIC may not be a valid assumption for KPC-producing organisms.
Publisher
American Society for Microbiology
Subject
Infectious Diseases,Pharmacology (medical),Pharmacology
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