Population pharmacokinetics and pharmacodynamic target attainment analysis of cefazolin using total and unbound serum concentration in patients with prostatectomy or nephrectomy

Author:

Komatsu Toshiaki1ORCID,Kawai Yuka2,Takayama Yoko3,Akamada Yuto1,Kusume Eri1,Ikeda Masaomi4,Tsumura Hideyasu4,Ishii Daisuke4,Iwamura Masatsugu4,Okamoto Hirotsugu5,Hanaki Hideaki6,Otori Katsuya2

Affiliation:

1. Department of Pharmacy, Kitasato University Hospital, Kanagawa, Japan

2. Pharmacy Practice and Science I, Research and Education Center for Clinical Pharmacy, Kitasato University School of Pharmacy, Kanagawa, Japan

3. Department of Infection Control and Infectious Diseases, Research and Development Center for New Medical Frontiers, Kitasato University School of Medicine, Kanagawa, Japan

4. Department of Urology, Kitasato University of Medicine, Kanagawa, Japan

5. Department of Anesthesiology, Kitasato University School of Medicine, Kanagawa, Japan

6. Infection Control Research Center, Kitasato Institute for Life Sciences, Kitasato University, Tokyo, Japan

Abstract

ABSTRACT The aim of this study was to analyze the population pharmacokinetics of total and unbound concentrations of prophylactic cefazolin (CFZ) in patients with prostatectomy or nephrectomy. We also aimed to calculate a pharmacodynamics target unbound concentration that exceeded the minimum inhibitory concentration (MIC), to design an effective dosing regimen. Briefly, 614 total concentration and 610 unbound concentration samples from 152 individuals were evaluated, using a nonlinear mixed-effects model. The obtained pharmacodynamics index target value reflected the probability of maintaining CFZ unbound trough concentrations exceeding MIC 90 , 0.5 mg/L, and MIC 50 , and 1.0 mg/L, to account for methicillin-susceptible Staphylococcus aureus (MSSA) or Escherichia coli . Population pharmacokinetics were estimated using a two-compartment model with nonlinear protein binding. Unbound systemic clearance (CL) was significantly associated with creatinine clearance, while the maximum protein-binding constant was significantly associated with albumin levels. The probability of achieving an unbound concentration exceeding the MIC 50 for E. coli or MIC 90 for MSSA in a patient with normal renal function following a 1 g CFZ infusion over 15 min was above 90% at 3 h after the initial dose. Our findings indicated that population pharmacokinetic parameters are useful for determining unbound CFZ pharmacokinetics and evaluating intraoperative CFZ redosing intervals.

Funder

Morinomiyako Medical Reserch Fundation

JPSS KAKENHI

Publisher

American Society for Microbiology

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