Jennifer C.Wong, StaceyB.B.Dutton, StephenD.Collins,
StevenSchachter and Andrew Escayg. Huperzine
A Provides Robust and Sustained Protection against Induced Seizures in Scn1a Mutant
Mice. Frontiers in Pharmacology October 2016|Volume7|Article357.
De novo loss-of-function mutations in the voltage-gated
sodium channel (VGSC) SCN1A (encoding Nav1.1) are the main cause of Dravet
syndrome (DS), a catastrophic early-life encephalopathy associated with
prolonged and recurrent early-life febrile seizures (FSs), refractory afebrile epilepsy,
cognitive and behavioral deficits, and a 15–20% mortality rate. SCN1A mutations
also lead to genetic epilepsy with febrile seizures plus (GEFS+), which is an
inherited disorder characterized by early-life FSs and the development of a
range of adult epilepsy subtypes. Current antiepileptic drugs often fail to
protect against the severe seizures and behavioral and cognitive deficits found
in patients with SCN1A mutations. To address the need for more efficacious
treatments for SCN1A-derived epilepsies, we evaluated the therapeutic potential
of Huperzine A, a naturally occurring reversible acetylcholinesterase
inhibitor. In CF1 mice, Hup A (0.56 or 1 mg/kg) was found to confer protection
against 6 Hz-, pentylenetetrazole (PTZ)-, and maximal electroshock
(MES)-induced seizures. Robust protection against 6 Hz-, MES-, and
hyperthermia-induced seizures was also achieved following Hup A administration
in mouse models of DS (Scn1a+/−) and GEFS+ (Scn1aRH/+). Furthermore, Hup
A-mediated seizure protection was sustained during 3 weeks of daily injections
in Scn1aRH/+ mutants. Finally, we determined that muscarinic and GABAA
receptors play a role in Hup A-mediated seizure protection. These findings
indicate that Hup A might provide a novel therapeutic strategy for increasing
seizure resistance in DS and GEFS+, and more broadly, in other forms of
refractory epilepsy.
Courtesy of a colleague
Courtesy of a colleague
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