Dose optimization of piperacillin/tazobactam, cefepime, and ceftazidime for carbapenem-resistant Pseudomonas aeruginosa isolates in Türkiye

Ecem Buyukyanbolu; Christian M Gill; Leyla Genc; Mehmet Karakus; Fusun Comert; Baris Otlu; Elif Aktas; David P Nicolau

doi:10.1007/s10096-024-04990-w

Dose optimization of piperacillin/tazobactam, cefepime, and ceftazidime for carbapenem-resistant Pseudomonas aeruginosa isolates in Türkiye

Eur J Clin Microbiol Infect Dis. 2024 Nov 15. doi: 10.1007/s10096-024-04990-w. Online ahead of print.

Authors

Ecem Buyukyanbolu^{1

2}, Christian M Gill³, Leyla Genc⁴, Mehmet Karakus⁵, Fusun Comert⁶, Baris Otlu⁷, Elif Aktas⁴, David P Nicolau³

Affiliations

¹ Department of Medical Microbiology, University of Health Sciences Hamidiye Etfal Training and Research Hospital, Istanbul, Turkey. [email protected].
² Center for Anti-Infective Research & Development, Hartford Hospital, 80 Seymour Street, Hartford, CT, 06102, USA. [email protected].
³ Center for Anti-Infective Research & Development, Hartford Hospital, 80 Seymour Street, Hartford, CT, 06102, USA.
⁴ Department of Medical Microbiology, University of Health Sciences Hamidiye Etfal Training and Research Hospital, Istanbul, Turkey.
⁵ Department of Medical Microbiology, University of Health Sciences, Istanbul, Turkey.
⁶ Faculty of Medicine, Department of Medical Microbiology, Bulent Ecevit University, Zonguldak, Turkey.
⁷ Faculty of Medicine, Department of Medical Microbiology, Inonu University, Malatya, Turkey.

PMID: 39546100
DOI: 10.1007/s10096-024-04990-w

Abstract

Introduction: Although CRPA may test susceptible to other β-lactams such as ceftazidime (CAZ), cefepime (FEP), and piperacillin/tazobactam (TZP), reduced potency has been observed. We assessed the adequacy of EUCAST Susceptible (S) or Susceptible Increased Exposure (SIE)/(I) doses for CAZ, FEP, and TZP against CRPA clinical isolates.

Methods: CRPA isolates were collected from patients at three Turkish hospitals. CAZ, FEP, and TZP MICs were determined using broth microdilution. Monte Carlo simulations were performed to determine the probability of target attainment (PTA) for a free time above the MIC (fT > MIC) targets for various doses of each agent against isolates defined as susceptible. fT > MIC targets were 70% for CAZ or FEP and 50% for TZP. Cumulative fraction of response (CFR) was calculated. Optimal PTA and CFR was 90% target achievement.

Results: The percentages of isolates SIE/I to CAZ, FEP, and TZP were 49,8%, 47%, and 31,8% respectively. Reduced potency was noted with 54,1% of CAZ-S isolates having MICs of 4 or 8 mg/L. Of the FEP and TZP-S isolates, MICs at the breakpoint (8 and 16 mg/L, respectively) were the mode with 45,2 and 53,9% of isolates for each, respectively. At an MIC of 8 mg/L for CAZ, the EUCAST standard dose was insufficient (CFR of 85%). 3 h infusions of EUCAST SIE doses were required for 90% PTA at MIC of 8 mg/L and an optimized CFR of 100%. For FEP, the SIE dose of 2 g q8h 0.5 h infusion of was effective (CFR 96%), utilization of an extended 3 h infusion further optimized the PTA at 8 mg/L (CFR 99%). For TZP, the standard dose of 4.5 q6h administered as a 0.5 h infusion was inadequate (CFR 86%). A standard TZP dose with an extended infusion (4.5 g q8h over 4 h) and the SIE dose 4.5 g q6h 3 h infusion resulted in CFRs > 95%.

Conclusion: These data support the EUCAST SIE breakpoints for FEP and TZP. To optimize PTA at the SIE breakpoint for CAZ, prolonged infusion is required.

Keywords: P. aeruginosa; Carbapenem resistance; Cephalosporin; Dose optimization; PK/PD.