Peer-Reviewed Journal Details
Mandatory Fields
Jullien, V,Pressler, RM,Boylan, G,Blennow, M,Marlow, N,Chiron, C,Pons, G,NEMO Consortium Neonatal Seizure T
2016
March
Journal of Clinical Pharmacology
Pilot Evaluation of the Population Pharmacokinetics of Bumetanide in Term Newborn Infants With Seizures
Validated
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Optional Fields
population pharmacokinetics neonatology central nervous system DRUG-METABOLIZING-ENZYMES CRITICALLY ILL INFANTS NEONATAL SEIZURES PHARMACODYNAMICS HYPOTHERMIA ENCEPHALOPATHY ONTOGENY EFFICACY
56
284
290
Recent experimental data suggest bumetanide as a possible therapeutic option in newborn infants with seizures after birth asphyxia. Because pharmacokinetic (PK) data are lacking in this population, who very often benefit from therapeutic cooling, which can modify the PK behavior of a drug, a PK study was conducted in term infants with seizures caused by hypoxic-ischemic encephalopathy. Fourteen infants were included, 13 of them being cooled. Forty-nine blood samples were available for the determination of the plasma concentration of bumetanide. Concentration-time data were analyzed by the use of a population approach performed with Monolix Software. Bumetanide was found to follow a 2-compartment model. The mean values were 0.063 L/h for clearance, 0.28 and 0.44 L for the central and peripheral distribution volumes, respectively, and 0.59 L/h for the distribution clearance. Birth body weight explained the interindividual variability of bumetanide clearance via an allometric model. No relationship was found between bumetanide exposure and its efficacy (reduction in seizure burden) or its toxicity (hearing loss). This study describes the first PK model of bumetanide in hypothermia-treated infants with seizures.
10.1002/jcph.596
Grant Details