Phenobarbital and midazolam suppress neonatal seizures in a noninvasive rat model of birth asphyxia, whereas bumetanide is ineffective

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Johne , M , Roemermann , K , Hampel , P , Gailus , B , Theilmann , W , Ala-Kurikka , T , Kaila , K & Loescher , W 2021 , ' Phenobarbital and midazolam suppress neonatal seizures in a noninvasive rat model of birth asphyxia, whereas bumetanide is ineffective ' , Epilepsia , vol. 62 , no. 4 , pp. 920-934 . https://doi.org/10.1111/epi.16778

Title: Phenobarbital and midazolam suppress neonatal seizures in a noninvasive rat model of birth asphyxia, whereas bumetanide is ineffective
Author: Johne, Marie; Roemermann, Kerstin; Hampel, Philip; Gailus, Bjoern; Theilmann, Wiebke; Ala-Kurikka, Tommi; Kaila, Kai; Loescher, Wolfgang
Contributor: University of Helsinki, Laboratory of Neurobiology
University of Helsinki, Physiology and Neuroscience (-2020)
Date: 2021-04
Language: eng
Number of pages: 15
Belongs to series: Epilepsia
ISSN: 0013-9580
URI: http://hdl.handle.net/10138/333660
Abstract: Objective: Neonatal seizures are the most frequent type of neurological emergency in newborn infants, often being a consequence of prolonged perinatal asphyxia. Phenobarbital is currently the most widely used antiseizure drug for treatment of neonatal seizures, but fails to stop them in similar to 50% of cases. In a neonatal hypoxia-only model based on 11-day-old (P11) rats, the NKCC1 inhibitor bumetanide was reported to potentiate the antiseizure activity of phenobarbital, whereas it was ineffective in a human trial in neonates. The aim of this study was to evaluate the effect of clinically relevant doses of bumetanide as add-on to phenobarbital on neonatal seizures in a noninvasive model of birth asphyxia in P11 rats, designed for better translation to the human term neonate. Methods: Intermittent asphyxia was induced for 30 minutes by exposing the rat pups to three 7 + 3-minute cycles of 9% and 5% O-2 at constant 20% CO2. Drug treatments were administered intraperitoneally either before or immediately after asphyxia. Results: All untreated rat pups had seizures within 10 minutes after termination of asphyxia. Phenobarbital significantly blocked seizures when applied before asphyxia at 30 mg/kg but not 15 mg/kg. Administration of phenobarbital after asphyxia was ineffective, whereas midazolam (0.3 or 1 mg/kg) exerted significant antiseizure effects when administered before or after asphyxia. In general, focal seizures were more resistant to treatment than generalized convulsive seizures. Bumetanide (0.3 mg/kg) alone or in combination with phenobarbital (15 or 30 mg/kg) exerted no significant effect on seizure occurrence. Significance: The data demonstrate that bumetanide does not increase the efficacy of phenobarbital in a model of birth asphyxia, which is consistent with the negative data of the recent human trial. The translational data obtained with the novel rat model of birth asphyxia indicate that it is a useful tool to evaluate novel treatments for neonatal seizures.
Subject: antiseizure drugs
GABA
neonates
NKCC1
CATION-CHLORIDE COTRANSPORTERS
ANTIEPILEPTIC DRUGS
BRAIN-DEVELOPMENT
HYPOXIA
PHARMACOKINETICS
PENETRATION
INTRANASAL
CHILDREN
EFFICACY
3112 Neurosciences
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