1. Why we urgently need improved seizure and epilepsy therapies for children and neonates.
- Author
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Pressler, Ronit M. and Lagae, Lieven
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CHILDHOOD epilepsy , *PREMATURE infants , *SEIZURES (Medicine) , *INFANTS , *NEWBORN infants , *TUBEROUS sclerosis , *GOVERNMENT policy , *DRUG efficacy - Abstract
In contrast to epilepsy in adolescents and adults, neonatal seizures and early onset epilepsy poses unique challenges with significant repercussion for treatment choices. Most importantly, high seizure burden and epileptic encephalopathy are associated with developmental, behavioural and cognitive problems. The causes are multifactorial and include etiology, seizure burden, epileptic encephalopathy, but also antiseizure medication. In contrast to adults and older children only very few drugs have been licenced for infants and neonates, and after a long delay. Very recently, extrapolation of adult data has become possible as a path to speed up drug development for younger children but this is not necessarily possible for infants and neonates. With the advances in understanding the molecular basis of many epilepsies, targeted therapies become available, for example for KCNQ2 mutation related epilepsies, Dravet syndrome or tuberous sclerosis complex. Drug trials in neonates are particularly challenging because of their inconspicuous clinical presentation, the need for continuous EEG monitoring, high co-morbidity, and poor response to antiepileptic drugs. There is an urgent need for development of new drugs, evaluation of safety and efficacy of current antiseizure drugs, as well as for national policies and guidelines for the management of seizures and epilepsy in neonates and infants. This article is part of the special issue entitled 'New Epilepsy Therapies for the 21st Century – From Antiseizure Drugs to Prevention, Modification and Cure of Epilepsy'. • Treatment of early onset seizures and epilepsies pose a clinical challenge to clinicians. • Only very few drugs have been licenced due to lack of randomised controlled trials. • Systematic reviews no good evidence for the choice of treatment. • Precision medicine is so far only available for a small number of syndromes. [ABSTRACT FROM AUTHOR]
- Published
- 2020
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