A clinical trial of enteral Levetiracetam for acute seizures in pediatric cerebral malaria

Gretchen L. Birbeck; Susan T. Herman; Edmund V. Capparelli; Fraction K. Dzinjalamala; Samah G. Abdel Baki; Macpherson Mallewa; Neema M. Toto; Douglas G. Postels; Joseph C. Gardiner; Terrie E. Taylor; Karl B. Seydel

doi:10.1186/s12887-019-1766-2

BMC Pediatrics (Nov 2019)

A clinical trial of enteral Levetiracetam for acute seizures in pediatric cerebral malaria

Gretchen L. Birbeck,
Susan T. Herman,
Edmund V. Capparelli,
Fraction K. Dzinjalamala,
Samah G. Abdel Baki,
Macpherson Mallewa,
Neema M. Toto,
Douglas G. Postels,
Joseph C. Gardiner,
Terrie E. Taylor,
Karl B. Seydel

Affiliations

Gretchen L. Birbeck: Department of Neurology, University of Rochester
Susan T. Herman: Department of Neurology, Barrow Neurological Institute
Edmund V. Capparelli: University of California San Diego, Center for Research in Paediatric and Developmental Pharmacology
Fraction K. Dzinjalamala: Malawi-Liverpool-Wellcome Trust Research Programme
Samah G. Abdel Baki: Bio-Signal Group Co.
Macpherson Mallewa: Department of Paediatrics, Queen Elizabeth Central Hospital
Neema M. Toto: Malawi-Liverpool-Wellcome Trust Research Programme
Douglas G. Postels: Department of Neurology, Children’s National Medical Center
Joseph C. Gardiner: Department of Epidemiology & Biostatistics, Michigan State University
Terrie E. Taylor: Blantyre Malaria Project
Karl B. Seydel: Blantyre Malaria Project

DOI: https://doi.org/10.1186/s12887-019-1766-2
Journal volume & issue: Vol. 19, no. 1
pp. 1 – 12

Abstract

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Abstract Background Acute seizures are common in pediatric cerebral malaria (CM), but usual care with phenobarbital risks respiratory suppression. We undertook studies of enteral levetiracetam (eLVT) to evaluate pharmacokinetics (PK), safety and efficacy including an open-label, randomized controlled trial (RCT) comparing eLVT to phenobarbital. Methods Children 24–83 months old with CM were enrolled in an eLVT dose-finding study starting with standard dose (40 mg/kg load, then 30 mg/kg Q12 hours) titrated upward until seizure freedom was attained in 75% of subjects. The RCT that followed randomized children to eLVT vs. phenobarbital for acute seizures and compared the groups on minutes with seizures based upon continuous electroencephalogram. Due to safety concerns, midway through the study children allocated to phenobarbital received the drug only if they continued to have seizures (either clinically or electrographically) after benzodiazepine treatment. Secondary outcomes were treatment failure requiring cross over, coma duration and neurologic sequelae at discharge. PK and safety assessments were also undertaken. Results Among 30 comatose CM children, eLVT was rapidly absorbed and well-tolerated. eLVT clearance was lower in patients with higher admission serum creatinine (SCr), but overall PK parameters were similar to prior pediatric PK studies. Within 4 h of the first dose, 90% reached therapeutic levels (> 20 μg/mL) and all were above 6 μg/mL. 7/7 children achieved seizure freedom on the initial eLVT dose. Comparing 23 eLVT to 21 phenobarbital patients among whom 15/21 received phenobarbital, no differences were seen for minutes with seizure, seizure freedom, coma duration, neurologic sequelae or death, but eLVT was safer (p = 0.019). Phenobarbital was discontinued in 3/15 due to respiratory side effects. Conclusion Enteral LVT offers an affordable option for seizure control in pediatric CM and is safer than phenobarbital. Trial registration NCT01660672. NCT01982812.

Published in BMC Pediatrics

ISSN: 1471-2431 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine: Pediatrics
Website: https://bmcpediatr.biomedcentral.com

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