Expecting the Unexpected: Lack of in Vivo Network Defects in an <i>Scn1a</i> Model of Dravet Syndrome

Hull, Jacob M.; Isom, Lori L.

doi:10.5698/1535-7511-16.6.408

Cited by 3 publications

(2 citation statements)

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“…It has also been shown that alterations in interneuronal firing seen in Scn1a +/− DS mice do not alter intrinsic network excitability in vivo (De Stasi et al 2016). According to Hull and Isom (2016), there might be other factors such as pyramidal neuron hypere xcitability that alter the network dynamics during a seizure, and pyramidal neuron function has been shown to be altered in neurons derived from induced pluripotent stem cells from Dravet patients (Liu et al 2013). For these reasons, we investigated the firing properties of pyramidal neurons in the current study, and we found increased excitability in CA3 pyramidal neurons of mutant mice that had undergone A/PFE.…”

Section: Discussionmentioning

confidence: 99%

Early-life febrile seizures worsen adult phenotypes in Scn1a mutants

Dutton

Dutt

Papale

et al. 2017

Experimental Neurology

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Mutations in the voltage-gated sodium channel (VGSC) gene SCN1A, encoding the Nav1.1 channel, are responsible for a number of epilepsy disorders including genetic epilepsy with febrile seizures plus (GEFS+) and Dravet syndrome (DS). Patients with SCN1A mutations often experience prolonged early-life febrile seizures (FSs), raising the possibility that these events may influence epileptogenesis and lead to more severe adult phenotypes. To test this hypothesis, we subjected 21-23-day-old mice expressing the human SCN1A GEFS+ mutation R1648H to prolonged hyperthermia, and then examined seizure and behavioral phenotypes during adulthood. We found that early-life FSs resulted in lower latencies to induced seizures, increased severity of spontaneous seizures, hyperactivity, and impairments in social behavior and recognition memory during adulthood. Biophysical analysis of brain slice preparations revealed an increase in epileptiform activity in CA3 pyramidal neurons along with increased action potential firing, providing a mechanistic basis for the observed worsening of adult phenotypes. These findings demonstrate the long-term negative impact of early-life FSs on disease outcomes. This has important implications for the clinical management of this patient population and highlights the need for therapeutic interventions that could ameliorate disease progression.

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Section: Discussionmentioning

confidence: 99%

Early-life febrile seizures worsen adult phenotypes in Scn1a mutants

Dutton

Dutt

Papale

et al. 2017

Experimental Neurology

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“…Voltage-gated sodium channels, such as NaV1.1, are heterotrimeric protein complexes consisting of a single large pore-forming a subunit in combination with two much smaller b subunits. 20 The noncovalently linked b1 subunit has been shown to modulate the function of the a subunits by enhancing ion flow through a subunits, and by promoting the trafficking of the a subunits from an intracellular pool to the cell surface. 21 We hypothesized that overexpression of NaVb1 would facilitate the activity of residual sodium channel subunits in Scn1a +/mice and mitigate the DS phenotype.…”

Section: Introductionmentioning

confidence: 99%

Sexually Divergent Mortality and Partial Phenotypic Rescue After Gene Therapy in a Mouse Model of Dravet Syndrome

et al. 2020

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Dravet syndrome (DS) is a neurodevelopmental genetic disorder caused by mutations in the SCN1A gene encoding the a subunit of the NaV1.1 voltage-gated sodium channel that controls neuronal action potential firing. The high density of this mutated channel in GABAergic interneurons results in impaired inhibitory neurotransmission and subsequent excessive activation of excitatory neurons. The syndrome is associated with severe childhood epilepsy, autistic behaviors, and sudden unexpected death in epilepsy. Here, we compared the rescue effects of an adeno-associated viral (AAV) vector coding for the multifunctional b1 sodium channel auxiliary subunit (AAV-NaVb1) with a control vector lacking a transgene. We hypothesized that overexpression of NaVb1 would facilitate the function of residual voltage-gated channels and improve the DS phenotype in the Scn1a +/mouse model of DS. AAV-NaVb1 was injected into the cerebral spinal fluid of neonatal Scn1a +/mice. In untreated control Scn1a +/mice, females showed a higher degree of mortality than males. Compared with Scn1a +/control mice, AAV-NaVb1-treated Scn1a +/mice displayed increased survival, an outcome that was more pronounced in females than males. In contrast, behavioral analysis revealed that male, but not female, Scn1a +/mice displayed motor hyperactivity, and abnormal performance on tests of fear and anxiety and learning and memory. Male Scn1a +/mice treated with AAV-NaVb1 showed reduced spontaneous seizures and normalization of motor activity and performance on the elevated plus maze test. These findings demonstrate sex differences in mortality in untreated Scn1a +/mice, an effect that may be related to a lower level of intrinsic inhibitory tone in female mice, and a normalization of aberrant behaviors in males after central nervous system administration of AAV-NaVb1. The therapeutic efficacy of AAV-NaVb1 in a mouse model of DS suggests a potential new long-lasting biological therapeutic avenue for the treatment of this catastrophic epilepsy.

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