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Clemizole and modulators of serotonin signalling suppress seizures in Dravet syndrome.

Authors :
Griffin, Aliesha
Griffin, Aliesha
Hamling, Kyla R
Knupp, Kelly
Hong, SoonGweon
Lee, Luke P
Baraban, Scott C
Griffin, Aliesha
Griffin, Aliesha
Hamling, Kyla R
Knupp, Kelly
Hong, SoonGweon
Lee, Luke P
Baraban, Scott C
Source :
Brain : a journal of neurology; vol 140, iss 3, 669-683; 0006-8950
Publication Year :
2017

Abstract

Dravet syndrome is a catastrophic childhood epilepsy with early-onset seizures, delayed language and motor development, sleep disturbances, anxiety-like behaviour, severe cognitive deficit and an increased risk of fatality. It is primarily caused by de novo mutations of the SCN1A gene encoding a neuronal voltage-activated sodium channel. Zebrafish with a mutation in the SCN1A homologue recapitulate spontaneous seizure activity and mimic the convulsive behavioural movements observed in Dravet syndrome. Here, we show that phenotypic screening of drug libraries in zebrafish scn1 mutants rapidly and successfully identifies new therapeutics. We demonstrate that clemizole binds to serotonin receptors and its antiepileptic activity can be mimicked by drugs acting on serotonin signalling pathways e.g. trazodone and lorcaserin. Coincident with these zebrafish findings, we treated five medically intractable Dravet syndrome patients with a clinically-approved serotonin receptor agonist (lorcaserin, Belviq®) and observed some promising results in terms of reductions in seizure frequency and/or severity. Our findings demonstrate a rapid path from preclinical discovery in zebrafish, through target identification, to potential clinical treatments for Dravet syndrome.

Details

Database :
OAIster
Journal :
Brain : a journal of neurology; vol 140, iss 3, 669-683; 0006-8950
Notes :
application/pdf, Brain : a journal of neurology vol 140, iss 3, 669-683 0006-8950
Publication Type :
Electronic Resource
Accession number :
edsoai.on1391614932
Document Type :
Electronic Resource