Pharmacokinetic-Pharmacodynamic Correlation for Meropenem Applied to a Burn Child Using a Bioanalytical Liquid Cromatographic Method

Pharmacokinetic-Pharmacodynamic Correlation for Meropenem Applied to a Burn Child Using a Bioanalytical Liquid Cromatographic Method

Bioanalytical method for LC meropenem quantification in plasma was described. Good absolute recovery (higher than 90%), adequate linearity (0.2-50.0 μg/mL, r2=0.999), high sensitivity (LOQ: 0.2 μg/mL; LOD: 0.1μg/mL) and acceptable stability were shown. Interday/intraday precisions were 2.3%/2.0% and...

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Main Authors: Silvia R. C. J. Santos, Cristina Sanches-Giraud, Carlindo Vieira Jr., Flávio F. de Souza, David S. Gómez, Edvaldo V. Campos, Rodrigo P. de Azevedo, Marcus C. Ferreira, Jorge W. L. Nascimento
Format: Article
Language:English
Published: Formifarma, LDA. 2011-10-01
Series:Revista Portuguesa de Farmacoterapia
Subjects:
Meropenem
LC
burn child
drug plasma monitoring
pharmacokinetics-pharmacodinamics correlation
Online Access:http://revista.farmacoterapia.pt/index.php/rpf/article/view/79
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spelling doaj-6eb5fc2cf5a34a0f82e62bf588878e8a2020-11-25T00:09:27ZengFormifarma, LDA.Revista Portuguesa de Farmacoterapia1647-354X2183-73412011-10-0134412Pharmacokinetic-Pharmacodynamic Correlation for Meropenem Applied to a Burn Child Using a Bioanalytical Liquid Cromatographic MethodSilvia R. C. J. Santos0Cristina Sanches-Giraud1Carlindo Vieira Jr.2Flávio F. de Souza3David S. Gómez4Edvaldo V. Campos5Rodrigo P. de Azevedo6Marcus C. Ferreira7Jorge W. L. Nascimento8School of Pharmaceutical Sciences University of Sao Paulo – Sao Paulo/SP, BrazilSchool of Pharmaceutical Sciences University of Sao Paulo – Sao Paulo/SP, BrazilSchool of Pharmaceutical Sciences University of Sao Paulo – Sao Paulo/SP, BrazilSchool of Pharmaceutical Sciences University of Sao Paulo – Sao Paulo/SP, BrazilPlastic Surgery and Burns, Hospital das Clinicas da Faculdade de Medicina da Universidade de Sao Paulo/SP, BrazilPlastic Surgery and Burns, Hospital das Clinicas da Faculdade de Medicina da Universidade de Sao Paulo/SP, BrazilPlastic Surgery and Burns, Hospital das Clinicas da Faculdade de Medicina da Universidade de Sao Paulo/SP, BrazilPlastic Surgery and Burns, Hospital das Clinicas da Faculdade de Medicina da Universidade de Sao Paulo/SP, BrazilInstitute of Biological Sciences - Pharmacology Department, Federal University of Juiz de Fora – Juiz de Fora /MG, BrazilBioanalytical method for LC meropenem quantification in plasma was described. Good absolute recovery (higher than 90%), adequate linearity (0.2-50.0 μg/mL, r2=0.999), high sensitivity (LOQ: 0.2 μg/mL; LOD: 0.1μg/mL) and acceptable stability were shown. Interday/intraday precisions were 2.3%/2.0% and the mean accuracy was 98.9%. Case of one burn patient, 8 yrs, 30 kg, thermal/inhalation injury, 45% TBSA was reported. Meropenem was prescribed to pulmonary infection treatment and dose adjustment was performed by drug plasma monitoring (30th and 44th day of thermal accident), pharmacokinetics and pharmacokinetics-pharmacodinamics (PK-PD) modelling. On 5th and 19th day of meropenem treatment, trough drug plasma concentrations were 0.3 μg mL-1 (2.25 ga day: 0.75 g 8qh, 0.5 hour infusion) and 14 μg mL-1 (3 g a day: 1 g 8qh). Pharmacokinetics was altered on 5th day and also on 19th day, respectively: 1.3 and 3.3 hs (biological half-life); 6.4 and 1.7 mL/min.kg (plasma clearance), 0.7 and 0.5 L/kg (apparent volume of distribution). 40%fT>MIC (percentage of time above the minimum inhibitory concentration) was considered for PK-PD correlation. In conclusion, LC drug plasma monitoring was quite useful to guarantee low risk and drug efficacy. Since the pharmacokinetics is unpredictable in burn patients, the effectiveness of meropenem was reached when dose regimen of 1 g 8qh instead 0.75 g 8qh was applied to the paediatric burn patient.http://revista.farmacoterapia.pt/index.php/rpf/article/view/79MeropenemLCburn childdrug plasma monitoringpharmacokinetics-pharmacodinamics correlation
collection DOAJ
language English
format Article
sources DOAJ
author Silvia R. C. J. Santos
Cristina Sanches-Giraud
Carlindo Vieira Jr.
Flávio F. de Souza
David S. Gómez
Edvaldo V. Campos
Rodrigo P. de Azevedo
Marcus C. Ferreira
Jorge W. L. Nascimento
spellingShingle Silvia R. C. J. Santos
Cristina Sanches-Giraud
Carlindo Vieira Jr.
Flávio F. de Souza
David S. Gómez
Edvaldo V. Campos
Rodrigo P. de Azevedo
Marcus C. Ferreira
Jorge W. L. Nascimento
Pharmacokinetic-Pharmacodynamic Correlation for Meropenem Applied to a Burn Child Using a Bioanalytical Liquid Cromatographic Method
Revista Portuguesa de Farmacoterapia
Meropenem
LC
burn child
drug plasma monitoring
pharmacokinetics-pharmacodinamics correlation
author_facet Silvia R. C. J. Santos
Cristina Sanches-Giraud
Carlindo Vieira Jr.
Flávio F. de Souza
David S. Gómez
Edvaldo V. Campos
Rodrigo P. de Azevedo
Marcus C. Ferreira
Jorge W. L. Nascimento
author_sort Silvia R. C. J. Santos
title Pharmacokinetic-Pharmacodynamic Correlation for Meropenem Applied to a Burn Child Using a Bioanalytical Liquid Cromatographic Method
title_short Pharmacokinetic-Pharmacodynamic Correlation for Meropenem Applied to a Burn Child Using a Bioanalytical Liquid Cromatographic Method
title_full Pharmacokinetic-Pharmacodynamic Correlation for Meropenem Applied to a Burn Child Using a Bioanalytical Liquid Cromatographic Method
title_fullStr Pharmacokinetic-Pharmacodynamic Correlation for Meropenem Applied to a Burn Child Using a Bioanalytical Liquid Cromatographic Method
title_full_unstemmed Pharmacokinetic-Pharmacodynamic Correlation for Meropenem Applied to a Burn Child Using a Bioanalytical Liquid Cromatographic Method
title_sort pharmacokinetic-pharmacodynamic correlation for meropenem applied to a burn child using a bioanalytical liquid cromatographic method
publisher Formifarma, LDA.
series Revista Portuguesa de Farmacoterapia
issn 1647-354X
2183-7341
publishDate 2011-10-01
description Bioanalytical method for LC meropenem quantification in plasma was described. Good absolute recovery (higher than 90%), adequate linearity (0.2-50.0 μg/mL, r2=0.999), high sensitivity (LOQ: 0.2 μg/mL; LOD: 0.1μg/mL) and acceptable stability were shown. Interday/intraday precisions were 2.3%/2.0% and the mean accuracy was 98.9%. Case of one burn patient, 8 yrs, 30 kg, thermal/inhalation injury, 45% TBSA was reported. Meropenem was prescribed to pulmonary infection treatment and dose adjustment was performed by drug plasma monitoring (30th and 44th day of thermal accident), pharmacokinetics and pharmacokinetics-pharmacodinamics (PK-PD) modelling. On 5th and 19th day of meropenem treatment, trough drug plasma concentrations were 0.3 μg mL-1 (2.25 ga day: 0.75 g 8qh, 0.5 hour infusion) and 14 μg mL-1 (3 g a day: 1 g 8qh). Pharmacokinetics was altered on 5th day and also on 19th day, respectively: 1.3 and 3.3 hs (biological half-life); 6.4 and 1.7 mL/min.kg (plasma clearance), 0.7 and 0.5 L/kg (apparent volume of distribution). 40%fT>MIC (percentage of time above the minimum inhibitory concentration) was considered for PK-PD correlation. In conclusion, LC drug plasma monitoring was quite useful to guarantee low risk and drug efficacy. Since the pharmacokinetics is unpredictable in burn patients, the effectiveness of meropenem was reached when dose regimen of 1 g 8qh instead 0.75 g 8qh was applied to the paediatric burn patient.
topic Meropenem
LC
burn child
drug plasma monitoring
pharmacokinetics-pharmacodinamics correlation
url http://revista.farmacoterapia.pt/index.php/rpf/article/view/79
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