<i>SCN8A</i> encephalopathy: Research progress and prospects

Meisler, Miriam H.; Helman, Guy; Hammer, Michael F.; Fureman, Brandy E.; Gaillard, William D.; Goldin, Alan L.; Hirose, Shinichi; Ishii, Atsushi; Kröner, Barbara; Lossin, Christoph; Mefford, Heather C; Parent, Jack M.; Patel, Manoj K.; Schreiber, John M.; Stewart, Randall R.; Whittemore, Vicky; Wilcox, Karen S.; Wagnon, Jacy L.; Pearl, Phillip L.; Vanderver, Adeline; Scheffer, Ingrid E.

doi:10.1111/epi.13422

Cited by 111 publications

(148 citation statements)

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“…The activity of both excitatory and inhibitory neurons is reduced in mutant mice lacking Na v 1.6, and repetitive firing of cerebellar Purkinje cells and other repetitively firing neurons is impaired (1,(4)(5)(6)(7). De novo mutations of SCN8A have been identified as an important cause of early infantile epileptic encephalopathy (EIEE) (8,9). Epileptic encephalopathy resulting from mutation of SCN8A is designated EIEE13 [Online Mendelian Inheritance in Man (OMIM) # 614558].…”

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confidence: 99%

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Neuronal hyperexcitability in a mouse model of SCN8A epileptic encephalopathy

Lopez-Santiago

Yuan

Wagnon

et al. 2017

Proc. Natl. Acad. Sci. U.S.A.

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Patients with early infantile epileptic encephalopathy (EIEE) experience severe seizures and cognitive impairment and are at increased risk for sudden unexpected death in epilepsy (SUDEP). EIEE13 [Online Mendelian Inheritance in Man (OMIM) # 614558] is caused by de novo missense mutations in the voltage-gated sodium channel gene SCN8A. Here, we investigated the neuronal phenotype of a mouse model expressing the gain-of-function SCN8A patient mutation, p.Asn1768Asp (Na v 1.6-N1768D). Our results revealed regional and neuronal subtype specificity in the effects of the N1768D mutation. Acutely dissociated hippocampal neurons from Scn8a N1768D/+ mice showed increases in persistent sodium current (I Na ) density in CA1 pyramidal but not bipolar neurons. In CA3, I Na,P was increased in both bipolar and pyramidal neurons. Measurement of action potential (AP) firing in Scn8a N1768D/+ pyramidal neurons in brain slices revealed early afterdepolarization (EAD)-like AP waveforms in CA1 but not in CA3 hippocampal or layer II/III neocortical neurons. The maximum spike frequency evoked by depolarizing current injections in Scn8a N1768D/+ CA1, but not CA3 or neocortical, pyramidal cells was significantly reduced compared with WT. Spontaneous firing was observed in subsets of neurons in CA1 and CA3, but not in the neocortex. The EAD-like waveforms of Scn8a N1768D/+ CA1 hippocampal neurons were blocked by tetrodotoxin, riluzole, and SN-6, implicating elevated persistent I Na and reverse mode Na/Ca exchange in the mechanism of hyperexcitability. Our results demonstrate that Scn8a plays a vital role in neuronal excitability and provide insight into the mechanism and future treatment of epileptogenesis in EIEE13.sodium channel | epilepsy | mouse model | action potential | Na/Ca exchange

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confidence: 99%

“…Comorbidities included intellectual disability, ataxia, and sudden unexpected death in epilepsy (SUDEP) at 15 y of age. Since then, more than 150 patients with de novo SCN8A mutations have been identified (8,11) (www.scn8a. net/Home.aspx).…”

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confidence: 99%

Neuronal hyperexcitability in a mouse model of SCN8A epileptic encephalopathy

Lopez-Santiago

Yuan

Wagnon

et al. 2017

Proc. Natl. Acad. Sci. U.S.A.

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“…In two cases, a hyperpolarizing shift in voltage dependence of channel activation was observed, also leading to hyperactivity. This gain-of-function mechanism is opposite to the situation in Dravet syndrome, where loss-of-function mutations in SCN1A are most common (Meisler et al 2016). …”

Section: Introductionmentioning

confidence: 76%

“…Approximately 1% of early infantile epileptic encephalopathies are associated with missense mutations in the SCN8A gene, and approximately 50 cases have been described in the literature (Veeramah et al 2012; Larsen et al 2015; Wagnon and Meisler 2015; Meisler et al 2016). In a few cases, the mutation was inherited from a mosaic parent, but the majority of disease-contributory mutations are de novo missense mutations (Wagnon and Meisler 2015).…”

Section: Introductionmentioning

confidence: 99%

“…EIEE13 has an average age of onset between 3 and 7 mo, and individuals present with various types of seizures, including tonic–clonic, generalized tonic, atonic, myoclonic, and focal and absence seizures, whereas febrile seizures are rare (Ohba et al 2014). There is often developmental regression, and movement disorders are present with 50% of affected individuals unable to sit or walk (Meisler et al 2016). …”

Section: Introductionmentioning

confidence: 99%

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SCN8A mutation in a child presenting with seizures and developmental delays

Malcolmson

Kleyner

Tegay

et al. 2016

Cold Spring Harb Mol Case Stud

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The SCN8A gene encodes the sodium voltage-gated channel alpha subunit 8. Mutations in this gene have been associated with early infantile epileptic encephalopathy type 13. With the use of whole-exome sequencing, a de novo missense mutation in SCN8A was identified in a 4-yr-old female who initially exhibited symptoms of epilepsy at the age of 5 mo that progressed to a severe condition with very little movement, including being unable to sit or walk on her own.

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Excitatory and inhibitory neuron defects in a mouse model of Scn1b‐linked EIEE52

Hull

O’Malley²,

Chen

et al. 2020

Ann Clin Transl Neurol

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Objective: Human variants in voltage-gated sodium channel (VGSC) α and β subunit genes are linked to developmental and epileptic encephalopathies (DEEs). Inherited, biallelic, loss-of-function variants in SCN1B, encoding the β1/β1B subunits, are linked to early infantile DEE (EIEE52). De novo, monoallelic variants in SCN1A (Nav1.1), SCN2A (Nav1.2), SCN3A (Nav1.3), and SCN8A (Nav1.6) are also linked to DEEs. While these VGSC-linked DEEs have similar presentations, they have diverse mechanisms of altered neuronal excitability. Mouse models have suggested that Scn2a-, Scn3a-, and Scn8a-linked DEE variants are, in general, gain of function, resulting in increased persistent or resurgent sodium current (I Na) and pyramidal neuron hyperexcitability. In contrast, Scn1a-linked DEE variants, in general, are loss-of-function, resulting in decreased I Na and hypoexcitability of fast-spiking interneurons. VGSC β1 subunits associate with Nav1.1, Nav1.2, Nav1.3, and Nav1.6 and are expressed throughout the brain, raising the possibility that insults to both pyramidal and interneuron excitability may drive EIEE52 pathophysiology. Methods: We investigated excitability defects in pyramidal and parvalbumin-positive (PV +) interneurons in the Scn1b −/− model of EIEE52. We also used Scn1b FL/FL mice to delete Scn1b in specific neuronal populations. Results: Scn1b −/− cortical PV + interneurons were hypoexcitable, with reduced I Na density. Scn1b −/− cortical pyramidal neurons had population-specific changes in excitability and impaired I Na density. Scn1b deletion in PV + neurons resulted in 100% lethality, whereas deletion in Emx1 + or Camk2a + neurons did not affect survival. Interpretation: This work suggests that SCN1B-linked DEE variants impact both excitatory and inhibitory neurons, leading to the increased severity of EIEE52 relative to other DEEs.

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SCN8A encephalopathy: Research progress and prospects

Cited by 111 publications

References 69 publications

Neuronal hyperexcitability in a mouse model of SCN8A epileptic encephalopathy

Neuronal hyperexcitability in a mouse model of SCN8A epileptic encephalopathy

SCN8A mutation in a child presenting with seizures and developmental delays

Excitatory and inhibitory neuron defects in a mouse model of Scn1b‐linked EIEE52

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