A Nonparametric Pharmacokinetic Approach to Determine the Optimal Dosing Regimen for 30-Minute and 3-Hour Meropenem Infusions in Critically Ill Patients

Sumith K Mathew; Binu S Mathew; Michael N Neely; Girish S Naik; Ratna Prabha; Gijoe G Jacob; Subramani K; Denise H Fleming

doi:10.1097/FTD.0000000000000323

A Nonparametric Pharmacokinetic Approach to Determine the Optimal Dosing Regimen for 30-Minute and 3-Hour Meropenem Infusions in Critically Ill Patients

Ther Drug Monit. 2016 Oct;38(5):593-9. doi: 10.1097/FTD.0000000000000323.

Authors

Sumith K Mathew¹, Binu S Mathew, Michael N Neely, Girish S Naik, Ratna Prabha, Gijoe G Jacob, Subramani K, Denise H Fleming

Affiliation

¹ *Clinical Pharmacology Unit, Department of Pharmacology and Clinical Pharmacology, Christian Medical College, Vellore, India; †Laboratory of Applied Pharmacokinetics and Bioinformatics (LAPKB), Children's Hospital of Los Angeles, Keck School of Medicine, University of Southern California, Los Angeles, California; ‡Biocon Research Limited, Bangalore, India; and §Surgical Intensive Care Unit, Division of Critical Care, Christian Medical College, Vellore, India.

PMID: 27454665
DOI: 10.1097/FTD.0000000000000323

Abstract

Background: Pharmacokinetics of meropenem differ widely in the critically ill population. It is imperative to maintain meropenem concentrations above the inhibitory concentrations for most of the interdose interval. A population pharmacokinetic/pharmacodynamic model was developed to determine the probability of target attainment for 3-hour and 30-minute infusion regimens in this population.

Methods: This study was performed in an intensive care setting among adult patients who were initiated on meropenem at a dose of 1000 mg. Multiple blood specimens were collected at predetermined time points during the interdose period, and meropenem concentrations were measured using high performance liquid chromatography. Using Pmetrics, a pharmacokinetic/pharmacodynamic model was developed and validated. Monte Carlo simulation was performed, and probability of target attainment (100% T > minimum inhibitory concentration (MIC), with a probability >0.9) for doubling MICs was determined for different regimens of meropenem.

Results: A 2-compartment multiplicative gamma error model best described the population parameters from 34 patients. The pharmacokinetic parameters used in the final model were Ke (elimination rate constant from the central compartment), Vc (volume of distribution of central compartment), KCP and KPC (intercompartmental rate constants), and IC2 (the fitted amount of meropenem in the peripheral compartment). Inclusion of creatinine clearance (CLcreat) and body weight as covariates improved the model prediction (Ke = Ke0 × (Equation is included in full-text article.), Vc = Vc0 × Weight). The Ke and Vc [geometric mean (range)] of the individuals were 0.54 (0.01-2.61)/h and 9.36 (4.35-21.62) L, respectively. The probability of attaining the target, T > MIC of 100%, was higher for 3-hour infusion regimens compared with 30-minute infusion regimens for all ranges of CLcreat.

Conclusions: This study emphasizes that extended regimens of meropenem are preferable for treating infections caused by bacteria with higher MICs. The nonparametric analysis using body weight and CLcreat as covariate adequately predicted the pharmacokinetics of meropenem in critically ill patients with a wide range of renal function.

Publication types

Observational Study

MeSH terms

Anti-Bacterial Agents / administration & dosage
Anti-Bacterial Agents / blood
Anti-Bacterial Agents / pharmacokinetics
Computer Simulation
Critical Illness*
Drug Administration Schedule
Female
Humans
Infusions, Intravenous
Male
Meropenem
Monte Carlo Method
Statistics, Nonparametric
Thienamycins / administration & dosage*
Thienamycins / blood
Thienamycins / pharmacokinetics*

Substances

Anti-Bacterial Agents
Thienamycins
Meropenem