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Cefazolin plasma protein binding and its covariates in neonates
by
Kulo, A.
, Smits, A.
, Verbesselt, R.
, Naulaers, G.
, Vermeersch, P.
, Allegaert, K.
, de Hoon, J.
in
Administration, Intravenous
/ Adults
/ Anti-Bacterial Agents - administration & dosage
/ Anti-Bacterial Agents - metabolism
/ Anti-Bacterial Agents - pharmacokinetics
/ Antibacterial agents
/ Antibiotics. Antiinfectious agents. Antiparasitic agents
/ Biological and medical sciences
/ Biomedical and Life Sciences
/ Biomedicine
/ Blood Proteins - metabolism
/ Cefazolin - administration & dosage
/ Cefazolin - metabolism
/ Cefazolin - pharmacokinetics
/ Drug dosages
/ Female
/ Gram-positive bacteria
/ Humans
/ Infant
/ Infant, Newborn
/ Infectious diseases
/ Intensive care
/ Internal Medicine
/ Male
/ Medical Microbiology
/ Medical sciences
/ Neonates
/ Patients
/ Pharmacokinetics
/ Pharmacology
/ Pharmacology. Drug treatments
/ Plasma
/ Plasma - chemistry
/ Protein Binding
/ Proteins
/ Time Factors
2012
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Cefazolin plasma protein binding and its covariates in neonates
by
Kulo, A.
, Smits, A.
, Verbesselt, R.
, Naulaers, G.
, Vermeersch, P.
, Allegaert, K.
, de Hoon, J.
in
Administration, Intravenous
/ Adults
/ Anti-Bacterial Agents - administration & dosage
/ Anti-Bacterial Agents - metabolism
/ Anti-Bacterial Agents - pharmacokinetics
/ Antibacterial agents
/ Antibiotics. Antiinfectious agents. Antiparasitic agents
/ Biological and medical sciences
/ Biomedical and Life Sciences
/ Biomedicine
/ Blood Proteins - metabolism
/ Cefazolin - administration & dosage
/ Cefazolin - metabolism
/ Cefazolin - pharmacokinetics
/ Drug dosages
/ Female
/ Gram-positive bacteria
/ Humans
/ Infant
/ Infant, Newborn
/ Infectious diseases
/ Intensive care
/ Internal Medicine
/ Male
/ Medical Microbiology
/ Medical sciences
/ Neonates
/ Patients
/ Pharmacokinetics
/ Pharmacology
/ Pharmacology. Drug treatments
/ Plasma
/ Plasma - chemistry
/ Protein Binding
/ Proteins
/ Time Factors
2012
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Cefazolin plasma protein binding and its covariates in neonates
by
Kulo, A.
, Smits, A.
, Verbesselt, R.
, Naulaers, G.
, Vermeersch, P.
, Allegaert, K.
, de Hoon, J.
in
Administration, Intravenous
/ Adults
/ Anti-Bacterial Agents - administration & dosage
/ Anti-Bacterial Agents - metabolism
/ Anti-Bacterial Agents - pharmacokinetics
/ Antibacterial agents
/ Antibiotics. Antiinfectious agents. Antiparasitic agents
/ Biological and medical sciences
/ Biomedical and Life Sciences
/ Biomedicine
/ Blood Proteins - metabolism
/ Cefazolin - administration & dosage
/ Cefazolin - metabolism
/ Cefazolin - pharmacokinetics
/ Drug dosages
/ Female
/ Gram-positive bacteria
/ Humans
/ Infant
/ Infant, Newborn
/ Infectious diseases
/ Intensive care
/ Internal Medicine
/ Male
/ Medical Microbiology
/ Medical sciences
/ Neonates
/ Patients
/ Pharmacokinetics
/ Pharmacology
/ Pharmacology. Drug treatments
/ Plasma
/ Plasma - chemistry
/ Protein Binding
/ Proteins
/ Time Factors
2012
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Cefazolin plasma protein binding and its covariates in neonates
Journal Article
Cefazolin plasma protein binding and its covariates in neonates
2012
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Overview
Cefazolin (CFZ) is highly and saturably bound to human serum albumin (HSA) in adults. We aim to describe CFZ protein binding and its covariates in neonates. In neonates to whom intravenous CFZ (50 mg/kg) was administered prior to a surgical procedure, total and unbound CFZ plasma concentrations (mg/l) were determined at 0.5, 2, 4 and 8 h after CFZ administration. Linear and multiple regression analyses were used to document covariates of unbound CFZ fraction. The Wilcoxon signed-rank test was used for the paired analysis of unbound CFZ fractions. In 40 patients with a median weight of 2,767 (range 830–4,200) g and a postmenstrual age (PMA) of 39 (25–45) weeks, 131 samples were collected. The median unbound CFZ fraction was 0.39 (0.10–0.73). Linear regression of unbound CFZ fraction versus unbound CFZ plasma concentration (
R
2
= 0.39) had a slope significantly different from zero (
p
< 0.001). In a multiple regression analysis, albuminaemia, total CFZ concentration, indirect bilirubinaemia and PMA resulted in an
R
2
value of 0.496. The median unbound CFZ fraction at the peak concentration (0.46, range 0.28–0.69) was significantly higher compared to the trough level (0.36, range 0.17–0.73) (
p
< 0.001). The between- and within-patient saturability of CFZ plasma protein binding were documented in neonates. The median unbound CFZ fraction in neonates is higher than in adults and depends partly on albuminaemia, total CFZ concentration, indirect bilirubinaemia and PMA. Integration of CFZ protein binding in future pharmacokinetic/pharmacodynamic research is warranted in order to optimise neonatal CFZ dosing. We recommend protein binding assessment in the neonatal pharmacokinetic evaluation of highly protein-bound or clinically relevant drugs.
Publisher
Springer-Verlag,Springer,Springer Nature B.V
Subject
/ Adults
/ Anti-Bacterial Agents - administration & dosage
/ Anti-Bacterial Agents - metabolism
/ Anti-Bacterial Agents - pharmacokinetics
/ Antibiotics. Antiinfectious agents. Antiparasitic agents
/ Biological and medical sciences
/ Biomedical and Life Sciences
/ Cefazolin - administration & dosage
/ Cefazolin - pharmacokinetics
/ Female
/ Humans
/ Infant
/ Male
/ Neonates
/ Patients
/ Pharmacology. Drug treatments
/ Plasma
/ Proteins
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