Population Pharmacokinetics of Cefuroxime in Critically Ill Patients Receiving Continuous Venovenous Hemofiltration With Regional Citrate Anticoagulation and a Phosphate-Containing Replacement Fluid

Paddy K. C. Janssen; Norbert A. Foudraine; Desiree M. T. Burgers; Kees Neef; Jos L. M. L. le Noble

doi:10.1097/FTD.0000000000000330

Population Pharmacokinetics of Cefuroxime in Critically Ill Patients Receiving Continuous Venovenous Hemofiltration With Regional Citrate Anticoagulation and a Phosphate-Containing Replacement Fluid

Paddy K. C. Janssen, Norbert A. Foudraine, Desiree M. T. Burgers, Kees Neef, Jos L. M. L. le Noble^*

^*Corresponding author for this work

Research output: Contribution to journal › Article › Academic › peer-review

Abstract

Background: Cefuroxime is frequently prescribed as an antimicrobial therapy in critically ill patients. The aim of this study was to develop a new intravenous dosing strategy for cefuroxime in critically ill patients undergoing continuous venovenous hemofiltration with regional citrate anticoagulation (RCA-CVVH) by analyzing its extracorporeal removal and pharmacokinetic (PK) parameters. Methods: Nine critically ill patients treated with intravenous cefuroxime and RCA-CVVH and a phosphate-containing replacement fluid were investigated. Arterial and effluent samples were obtained from all patients and pre-and postfilter venous blood samples were obtained from a subgroup of 5 patients. Plasma cefuroxime levels were determined by ultraperformance liquid chromatography-mass spectrometry in plasma samples collected before and after intravenous infusion of either 1500 mg cefuroxime every 12 hours or 3000 mg continuously over 24 hours. Population PK analysis and dosing simulations were performed using nonlinear mixed-effects modeling and Monte Carlo simulations. Results: The volume of distribution (VD) of cefuroxime in the central compartment, corrected for lean body mass, was 0.11 +/- 0.056 L/kgLBMc, CVVH-mediated clearance was 49.5-50.6 mL/min, the mean elimination half-life (t(1/2)) was 90 minutes (77-103), and the mean sieving coefficient was 0.89 +/- 0.01. A 2-compartment model with between-subject variability in clearance, V-D, and t(1/2) described these data adequately. Simulation of a standard dosing regimen (750 mg/12 hours) predicted failure to achieve the international target plasma cefuroxime concentration (32 mg/L). Conclusions: Cefuroxime clearance by RCA-CVVH was twice the reported clearance during standard CVVH. Our PK data predicted that a maintenance dose of 3000 mg cefuroxime, infused over 24 hours, would provide an optimal steady-state plasma concentration of 38.5 mg/L. The developed population PK model for cefuroxime has the potential to inform new dosing schedules in patients receiving cefuroxime during RCA-CVVH.

Original language	English
Pages (from-to)	699-705
Journal	Therapeutic Drug Monitoring
Volume	38
Issue number	6
DOIs	https://doi.org/10.1097/FTD.0000000000000330
Publication status	Published - Dec 2016

Keywords

cefuroxime
population pharmacokinetics
continuous venovenous hemofiltration
acute kidney injury

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10.1097/FTD.0000000000000330

Cite this

Janssen, P. K. C., Foudraine, N. A., Burgers, D. M. T., Neef, K., & le Noble, J. L. M. L. (2016). Population Pharmacokinetics of Cefuroxime in Critically Ill Patients Receiving Continuous Venovenous Hemofiltration With Regional Citrate Anticoagulation and a Phosphate-Containing Replacement Fluid. Therapeutic Drug Monitoring, 38(6), 699-705. https://doi.org/10.1097/FTD.0000000000000330

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title = "Population Pharmacokinetics of Cefuroxime in Critically Ill Patients Receiving Continuous Venovenous Hemofiltration With Regional Citrate Anticoagulation and a Phosphate-Containing Replacement Fluid",

abstract = "Background: Cefuroxime is frequently prescribed as an antimicrobial therapy in critically ill patients. The aim of this study was to develop a new intravenous dosing strategy for cefuroxime in critically ill patients undergoing continuous venovenous hemofiltration with regional citrate anticoagulation (RCA-CVVH) by analyzing its extracorporeal removal and pharmacokinetic (PK) parameters. Methods: Nine critically ill patients treated with intravenous cefuroxime and RCA-CVVH and a phosphate-containing replacement fluid were investigated. Arterial and effluent samples were obtained from all patients and pre-and postfilter venous blood samples were obtained from a subgroup of 5 patients. Plasma cefuroxime levels were determined by ultraperformance liquid chromatography-mass spectrometry in plasma samples collected before and after intravenous infusion of either 1500 mg cefuroxime every 12 hours or 3000 mg continuously over 24 hours. Population PK analysis and dosing simulations were performed using nonlinear mixed-effects modeling and Monte Carlo simulations. Results: The volume of distribution (VD) of cefuroxime in the central compartment, corrected for lean body mass, was 0.11 +/- 0.056 L/kgLBMc, CVVH-mediated clearance was 49.5-50.6 mL/min, the mean elimination half-life (t(1/2)) was 90 minutes (77-103), and the mean sieving coefficient was 0.89 +/- 0.01. A 2-compartment model with between-subject variability in clearance, V-D, and t(1/2) described these data adequately. Simulation of a standard dosing regimen (750 mg/12 hours) predicted failure to achieve the international target plasma cefuroxime concentration (32 mg/L). Conclusions: Cefuroxime clearance by RCA-CVVH was twice the reported clearance during standard CVVH. Our PK data predicted that a maintenance dose of 3000 mg cefuroxime, infused over 24 hours, would provide an optimal steady-state plasma concentration of 38.5 mg/L. The developed population PK model for cefuroxime has the potential to inform new dosing schedules in patients receiving cefuroxime during RCA-CVVH.",

keywords = "cefuroxime, population pharmacokinetics, continuous venovenous hemofiltration, acute kidney injury",

author = "Janssen, {Paddy K. C.} and Foudraine, {Norbert A.} and Burgers, {Desiree M. T.} and Kees Neef and {le Noble}, {Jos L. M. L.}",

year = "2016",

month = dec,

doi = "10.1097/FTD.0000000000000330",

language = "English",

volume = "38",

pages = "699--705",

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publisher = "LIPPINCOTT WILLIAMS & WILKINS",

number = "6",

}

Janssen, PKC, Foudraine, NA, Burgers, DMT, Neef, K & le Noble, JLML 2016, 'Population Pharmacokinetics of Cefuroxime in Critically Ill Patients Receiving Continuous Venovenous Hemofiltration With Regional Citrate Anticoagulation and a Phosphate-Containing Replacement Fluid', Therapeutic Drug Monitoring, vol. 38, no. 6, pp. 699-705. https://doi.org/10.1097/FTD.0000000000000330

Population Pharmacokinetics of Cefuroxime in Critically Ill Patients Receiving Continuous Venovenous Hemofiltration With Regional Citrate Anticoagulation and a Phosphate-Containing Replacement Fluid. / Janssen, Paddy K. C.; Foudraine, Norbert A.; Burgers, Desiree M. T. et al.
In: Therapeutic Drug Monitoring, Vol. 38, No. 6, 12.2016, p. 699-705.

Research output: Contribution to journal › Article › Academic › peer-review

TY - JOUR

T1 - Population Pharmacokinetics of Cefuroxime in Critically Ill Patients Receiving Continuous Venovenous Hemofiltration With Regional Citrate Anticoagulation and a Phosphate-Containing Replacement Fluid

AU - Janssen, Paddy K. C.

AU - Foudraine, Norbert A.

AU - Burgers, Desiree M. T.

AU - Neef, Kees

AU - le Noble, Jos L. M. L.

PY - 2016/12

Y1 - 2016/12

N2 - Background: Cefuroxime is frequently prescribed as an antimicrobial therapy in critically ill patients. The aim of this study was to develop a new intravenous dosing strategy for cefuroxime in critically ill patients undergoing continuous venovenous hemofiltration with regional citrate anticoagulation (RCA-CVVH) by analyzing its extracorporeal removal and pharmacokinetic (PK) parameters. Methods: Nine critically ill patients treated with intravenous cefuroxime and RCA-CVVH and a phosphate-containing replacement fluid were investigated. Arterial and effluent samples were obtained from all patients and pre-and postfilter venous blood samples were obtained from a subgroup of 5 patients. Plasma cefuroxime levels were determined by ultraperformance liquid chromatography-mass spectrometry in plasma samples collected before and after intravenous infusion of either 1500 mg cefuroxime every 12 hours or 3000 mg continuously over 24 hours. Population PK analysis and dosing simulations were performed using nonlinear mixed-effects modeling and Monte Carlo simulations. Results: The volume of distribution (VD) of cefuroxime in the central compartment, corrected for lean body mass, was 0.11 +/- 0.056 L/kgLBMc, CVVH-mediated clearance was 49.5-50.6 mL/min, the mean elimination half-life (t(1/2)) was 90 minutes (77-103), and the mean sieving coefficient was 0.89 +/- 0.01. A 2-compartment model with between-subject variability in clearance, V-D, and t(1/2) described these data adequately. Simulation of a standard dosing regimen (750 mg/12 hours) predicted failure to achieve the international target plasma cefuroxime concentration (32 mg/L). Conclusions: Cefuroxime clearance by RCA-CVVH was twice the reported clearance during standard CVVH. Our PK data predicted that a maintenance dose of 3000 mg cefuroxime, infused over 24 hours, would provide an optimal steady-state plasma concentration of 38.5 mg/L. The developed population PK model for cefuroxime has the potential to inform new dosing schedules in patients receiving cefuroxime during RCA-CVVH.

AB - Background: Cefuroxime is frequently prescribed as an antimicrobial therapy in critically ill patients. The aim of this study was to develop a new intravenous dosing strategy for cefuroxime in critically ill patients undergoing continuous venovenous hemofiltration with regional citrate anticoagulation (RCA-CVVH) by analyzing its extracorporeal removal and pharmacokinetic (PK) parameters. Methods: Nine critically ill patients treated with intravenous cefuroxime and RCA-CVVH and a phosphate-containing replacement fluid were investigated. Arterial and effluent samples were obtained from all patients and pre-and postfilter venous blood samples were obtained from a subgroup of 5 patients. Plasma cefuroxime levels were determined by ultraperformance liquid chromatography-mass spectrometry in plasma samples collected before and after intravenous infusion of either 1500 mg cefuroxime every 12 hours or 3000 mg continuously over 24 hours. Population PK analysis and dosing simulations were performed using nonlinear mixed-effects modeling and Monte Carlo simulations. Results: The volume of distribution (VD) of cefuroxime in the central compartment, corrected for lean body mass, was 0.11 +/- 0.056 L/kgLBMc, CVVH-mediated clearance was 49.5-50.6 mL/min, the mean elimination half-life (t(1/2)) was 90 minutes (77-103), and the mean sieving coefficient was 0.89 +/- 0.01. A 2-compartment model with between-subject variability in clearance, V-D, and t(1/2) described these data adequately. Simulation of a standard dosing regimen (750 mg/12 hours) predicted failure to achieve the international target plasma cefuroxime concentration (32 mg/L). Conclusions: Cefuroxime clearance by RCA-CVVH was twice the reported clearance during standard CVVH. Our PK data predicted that a maintenance dose of 3000 mg cefuroxime, infused over 24 hours, would provide an optimal steady-state plasma concentration of 38.5 mg/L. The developed population PK model for cefuroxime has the potential to inform new dosing schedules in patients receiving cefuroxime during RCA-CVVH.

KW - cefuroxime

KW - population pharmacokinetics

KW - continuous venovenous hemofiltration

KW - acute kidney injury

U2 - 10.1097/FTD.0000000000000330

DO - 10.1097/FTD.0000000000000330

M3 - Article

C2 - 27494946

SN - 0163-4356

VL - 38

SP - 699

EP - 705

JO - Therapeutic Drug Monitoring

JF - Therapeutic Drug Monitoring

IS - 6

ER -