SCN1A
Homo sapiens
Gene Name: sodium channel, voltage-gated, type I, alpha subunit
Aliases: Na(v)1.1, FEB3; NAC1; SCN1; SMEI; HBSCI; GEFSP2; Nav1.1
Chromosome No: 2
Chromosome Band: 2q24.3
Genetic Category: Rare Single Gene variant--Syndromic-Genetic association-Functional-Rare single gene variant/Functional
Associated Syndrome(s): Dravet syndrome
Aliases: Na(v)1.1, FEB3; NAC1; SCN1; SMEI; HBSCI; GEFSP2; Nav1.1
Chromosome No: 2
Chromosome Band: 2q24.3
Genetic Category: Rare Single Gene variant--Syndromic-Genetic association-Functional-Rare single gene variant/Functional
Associated Syndrome(s): Dravet syndrome
Summary Statistics:
ASD Reports: 99
Recent Reports: 10
Annotated variants: 269
Associated CNVs: 9
Evidence score: 4
ASD Reports: 99
Recent Reports: 10
Annotated variants: 269
Associated CNVs: 9
Evidence score: 4
| Associated Disorders: |
|
Relevance to Autism
Mutations appear to give rise to Dravet Syndrome as well as distinct epilepsy-related disorders and also migraine. Missense mutations were observed in cases from multiple unrelated families, one of which presented with seizures and Asperger Syndrome (asymptomatic carriers were also seen in families, but missense variants were not observed in any of 304 controls (Osaka H et al.). Autism seems to be common amongst individuals with Dravet Syndrome but the report does not give a frequency for the 20 individuals studied (Wolff M et al.). Rare missense variants were observed in 4/299 AGRE families but none of 96 controls, and one of these variants was found previously in a child with juvenile myoclonic epilepsy (Weiss LA et al.). De novo variants in SCN1A, including multiple missense variants that were predicted to be damaging and one likely gene-disruptive variant, have been identified in ASD probands (O'Roak et al., 2011; O'Roak et al., 2012; O'Roak et al., 2012; De Rubeis et al., 2014; Yuen et al., 2017). Assessment of a cohort of 35 individuals with Dravet syndrome using standardized tools demonstrated that 11 patients (39%) had ASD according to the DSM5 classification and ADIR and ADOS2 (Ouss et al., 2018). Additional de novo missense variants in the SCN1A gene were identified in novel ASD probands from the Autism Sequencing Consortium in Satterstrom et al., 2020; subsequent TADA analysis in this report identified SCN1A as a candidate gene with a false discovery rate < 0.1.
Molecular Function
This gene encodes the large alpha subunit of the vertebrate voltage-gated sodium channel essential for the generation and propagation of action potentials, mainly in nerve and muscle.
External Links
References
Type
Title
Type of Disorder
Associated Disorders
Author, Year
Positive Association
Epilepsy, hippocampal sclerosis and febrile seizures linked by common genetic variation around SCN1A.
Epilepsy
Positive Association
De novo mutations in epileptic encephalopathies.
Epilepsy
IS, LGS, DD, ID, ASD, ADHD
Support
Sporadic autism exomes reveal a highly interconnected protein network of de novo mutations.
ASD
Support
Inherited and multiple de novo mutations in autism/developmental delay risk genes suggest a multifactorial model.
ASD
Support
Monogenic developmental and epileptic encephalopathies of infancy and childhood
DD, ID, epilepsy/seizures
ASD
Support
Clinical exome sequencing: results from 2819 samples reflecting 1000 families.
Neurodegeneration
Support
Prevalence and phenotypic impact of rare potentially damaging variants in autism spectrum disorder
ASD
Support
Exome sequencing in multiplex autism families suggests a major role for heterozygous truncating mutations.
ASD
Support
Clinical utility of multigene panel testing in adults with epilepsy and intellectual disability.
ID, epilepsy/seizures
Autistic features
Support
Expanding the genetic heterogeneity of intellectual disability.
Epilepsy/seizures, developmental regression
Support
Genetic care in geographically isolated small island communities: 8 years of experience in the Dutch Caribbean
Epilepsy/seizures
Support
Comprehensive molecular testing in patients with high functioning autism spectrum disorder.
ASD
Support
Next-Generation Sequencing in Korean Children With Autism Spectrum Disorder and Comorbid Epilepsy
ASD
ID, epilepsy/seizures
Support
Mosaic SCN1A mutations in familial partial epilepsy with antecedent febrile seizures.
Epilepsy/seizures
Support
First report on the association of SCN1A mutation, childhood schizophrenia and autism spectrum disorder without epilepsy.
ASD, SCZ
Support
Genetic and Phenotype Analysis of a Chinese Cohort of Infants and Children With Epilepsy
Epilepsy/seizures
ID
Support
The genomic landscape of balanced cytogenetic abnormalities associated with human congenital anomalies.
DD, epilepsy/seizures, microcephaly
Support
A single center experience with publicly funded clinical exome sequencing for neurodevelopmental disorders or multiple congenital anomalies
DD, ID, epilepsy/seizures
Support
Targeted resequencing in epileptic encephalopathies identifies de novo mutations in CHD2 and SYNGAP1.
Epilepsy
ID, ASD, DD
Support
The Clinical and Genetic Features of Co-occurring Epilepsy and Autism Spectrum Disorder in Chinese Children.
ASD, epilepsy/seizures
Support
Targeted sequencing and functional analysis reveal brain-size-related genes and their networks in autism spectrum disorders.
ASD
Support
Mutational Landscape of Autism Spectrum Disorder Brain Tissue
ASD
Support
Targeted DNA Sequencing from Autism Spectrum Disorder Brains Implicates Multiple Genetic Mechanisms.
ASD
Support
Utility of clinical exome sequencing in a complex Emirati pediatric cohort
Epilepsy/seizures
Support
Exome sequencing of ion channel genes reveals complex profiles confounding personal risk assessment in epilepsy.
Epilepsy
Support
Clinical genome sequencing in an unbiased pediatric cohort.
Dravet syndrome
DD, epilepsy/seizures
Support
Functional Investigation of a Neuronal Microcircuit in the CA1 Area of the Hippocampus Reveals Synaptic Dysfunction in Dravet Syndrome Mice
Dravet syndrome
Support
De novo genic mutations among a Chinese autism spectrum disorder cohort.
ASD
Support
Genome sequencing of 320 Chinese children with epilepsy: a clinical and molecular study
DD, epilepsy/seizures
Support
Generalized epilepsy with febrile seizure plus (GEFS) spectrum: Novel de novo mutation of SCN1A detected in a Malaysian patient.
Epilepsy
DD, ID
Support
Comprehensive Analysis of Rare Variants of 101 Autism-Linked Genes in a Hungarian Cohort of Autism Spectrum Disorder Patients.
ASD
Dravet syndrome
Support
Using medical exome sequencing to identify the causes of neurodevelopmental disorders: experience of two clinical units and 216 patients.
ID, epilepsy/seizures
Support
Analysis of recent shared ancestry in a familial cohort identifies coding and noncoding autism spectrum disorder variants
ASD
DD, ID, epilepsy/seizures
Support
Gene Mutation Analysis in 253 Chinese Children with Unexplained Epilepsy and Intellectual/Developmental Disabilities.
DD, ID, epilepsy/seizures
Support
Large-Scale Exome Sequencing Study Implicates Both Developmental and Functional Changes in the Neurobiology of Autism
ASD
Support
Exome sequencing in sporadic autism spectrum disorders identifies severe de novo mutations.
ASD
Support
Language Regression in an Atypical SLC6A1 Mutation.
ASD, epilepsy/seizures
Language delay, regression
Support
Genetic analysis using targeted exome sequencing of 53 Vietnamese children with developmental and epileptic encephalopathies
DD, epilepsy/seizures
Support
Exome sequencing of Pakistani consanguineous families identifies 30 novel candidate genes for recessive intellectual disability.
ID, epilepsy/seizures
Support
Clinical and genetic characteristics of patients with Doose syndrome
Epilepsy/seizures
Support
Multiplex targeted sequencing identifies recurrently mutated genes in autism spectrum disorders.
ASD
Support
Lessons Learned from Large-Scale, First-Tier Clinical Exome Sequencing in a Highly Consanguineous Population.
Epilepsy/seizures, DD, ID
Autistic features, stereotypies
Support
Genomic diagnosis for children with intellectual disability and/or developmental delay.
ID, epilepsy/seizures
Support
Critical Role of E1623 Residue in S3-S4 Loop of Nav1.1 Channel and Correlation Between Nature of Substitution and Functional Alteration
Epilepsy/seizures
DD, ID
Support
Large-scale discovery of novel genetic causes of developmental disorders.
DD, epilepsy/seizures
Support
Autism risk in offspring can be assessed through quantification of male sperm mosaicism.
ASD
Support
Nonfunctional SCN1A is common in severe myoclonic epilepsy of infancy.
Epilepsy/seizures
Support
Mosaicism of de novo pathogenic SCN1A variants in epilepsy is a frequent phenomenon that correlates with variable phenotypes.
Epilepsy/seizures
DD/ID, ASD, ADHD
Support
Clinical and Functional Features of Epilepsy-Associated In-Frame Deletion Variants in SCN1A
Epilepsy/seizures
ID, learning disability
Support
Pathogenic copy number variants and SCN1A mutations in patients with intellectual disability and childhood-onset epilepsy.
DD, ID, epilepsy/seizures
Support
Next Generation Sequencing of 134 Children with Autism Spectrum Disorder and Regression
ASD
Developmental regression, epilepsy/seizures
Support
Identification of SCN1A and PCDH19 mutations in Chinese children with Dravet syndrome.
Epilepsy
ASD, ID
Support
Neurological Diseases With Autism Spectrum Disorder: Role of ASD Risk Genes.
ASD
Dravet syndrome
Support
Whole genome sequencing resource identifies 18 new candidate genes for autism spectrum disorder
ASD
Support
Assessing Utility of Clinical Exome Sequencing in Diagnosis of Rare Idiopathic Neurodevelopmental Disorders in Indian Population
Epilepsy/seizures
DD, ID
Support
Synaptic, transcriptional and chromatin genes disrupted in autism.
ASD
Support
Re-annotation of 191 developmental and epileptic encephalopathy-associated genes unmasks de novo variants in SCN1A.
Dravet syndrome
Support
Diagnostic exome sequencing of syndromic epilepsy patients in clinical practice.
DD, epilepsy/seizures
Developmental regression
Support
Developmentally regulated impairment of parvalbumin interneuron synaptic transmission in an experimental model of Dravet syndrome
Dravet syndrome
Support
A Point Mutation in SCN1A 5' Genomic Region Decreases the Promoter Activity and Is Associated with Mild Epilepsy and Seizure Aggravation Induced by...
Epilepsy/seizures
Support
Overrepresentation of genetic variation in the AnkyrinG interactome is related to a range of neurodevelopmental disorders
ID, epilepsy/seizures
Psychomotor retardation
Support
SCN1A mutation associated with intractable myoclonic epilepsy and migraine headache.
Dravet syndrome
Epilepsy, ASD
Support
The combination of whole-exome sequencing and copy number variation sequencing enables the diagnosis of rare neurological disorders.
Epilepsy/seizures
ID
Support
Diagnostic Targeted Resequencing in 349 Patients with Drug-Resistant Pediatric Epilepsies Identifies Causative Mutations in 30 Different Genes.
Epilepsy/seizures
Dravet syndrome
Support
Autism spectrum disorder and comorbid neurodevelopmental disorders (ASD-NDDs): Clinical and genetic profile of a pediatric cohort
ASD
Epilepsy/seizures
Support
Performance comparison of bench-top next generation sequencers using microdroplet PCR-based enrichment for targeted sequencing in patients with aut...
ASD
ID, epilepsy
Support
Exome sequencing of 457 autism families recruited online provides evidence for autism risk genes
ASD
Support
High Rate of Recurrent De Novo Mutations in Developmental and Epileptic Encephalopathies.
Epilepsy/seizures
DD/ID
Support
Trio-based exome sequencing reveals a high rate of the de novo variants in intellectual disability
ID, epilepsy/seizures
Support
The contribution of protein intrinsic disorder to understand the role of genetic variants uncovered by autism spectrum disorders exome studies.
Support
A recurrent PJA1 variant in trigonocephaly and neurodevelopmental disorders
Epilepsy/seizures
ASD
Highly Cited
De novo mutations in the sodium-channel gene SCN1A cause severe myoclonic epilepsy of infancy.
Epilepsy
Highly Cited
Mutations of SCN1A, encoding a neuronal sodium channel, in two families with GEFS.
Epilepsy
Recent Recommendation
Patients with a sodium channel alpha 1 gene mutation show wide phenotypic variation.
Epilepsy
Asperger syndrome
Recent Recommendation
Low load for disruptive mutations in autism genes and their biased transmission.
ASD
Recent Recommendation
Severe myoclonic epilepsy of infants (Dravet syndrome): natural history and neuropsychological findings.
Recent Recommendation
Incorporating Functional Information in Tests of Excess De Novo Mutational Load.
Recent Recommendation
Integrated systems analysis reveals a molecular network underlying autism spectrum disorders.
ASD
Recent Recommendation
SCN1A testing for epilepsy: application in clinical practice.
Recent Recommendation
Nontruncating SCN1A mutations associated with severe myoclonic epilepsy of infancy impair cell surface expression.
Recent Recommendation
Aberrant Inclusion of a Poison Exon Causes Dravet Syndrome and Related SCN1A-Associated Genetic Epilepsies.
Dravet syndrome
Recent Recommendation
Nav1.1 localizes to axons of parvalbumin-positive inhibitory interneurons: a circuit basis for epileptic seizures in mice carrying an Scn1a gene mu...
Recent Recommendation
CRISPR/Cas9 facilitates investigation of neural circuit disease using human iPSCs: mechanism of epilepsy caused by an SCN1A loss-of-function mutation.
Rare
Variant ID
Variant Type
Allele Change
Residue Change
Inheritance Pattern
Inheritance Association
Family Type
Author, Year
GEN223R013
missense_variant
c.1625G>A
p.Arg542Gln
Familial
Paternal
Multiplex
GEN223R014
missense_variant
c.3101T>C
p.Ile1034Thr
Familial
Paternal
Multiplex
GEN223R015
missense_variant
c.3112T>C
p.Phe1038Leu
Familial
Paternal
Multiplex
GEN223R044
missense_variant
c.5962C>T
p.Arg1988Trp
Familial
Paternal and maternal
Multi-generational
GEN223R046
missense_variant
c.133G>A
p.Asp45Asn
Familial
Paternal
Multi-generational
GEN223R067
missense_variant
c.5732T>G
p.Ile1911Ser
De novo
Simplex
GEN223R078
missense_variant
c.4319C>T
p.Pro1440Leu
Unknown
Multiplex or multi-generational
GEN223R080
missense_variant
c.5768A>G
p.Gln1923Arg
Familial
Paternal
Multi-generational
GEN223R082
missense_variant
c.1811G>A
p.Arg604His
Familial
Maternal
Simplex
GEN223R087
missense_variant
c.393C>G
p.Ser131Arg
Familial
Maternal
Multi-generational
GEN223R089a
missense_variant
c.5501C>T
p.Ala1834Val
Familial
Both parents
Extended multiplex
GEN223R093
missense_variant
c.1848G>C
p.Glu616Asp
Familial
Maternal
Multi-generational
GEN223R101
frameshift_variant
c.5488_5489del
p.Gln1830ValfsTer6
De novo
Simplex
GEN223R112
splice_site_variant
c.2862+1G>T;c.2913+1G>T;c.2946+1G>T
p.?
De novo
Simplex
GEN223R113
missense_variant
c.5234C>A;c.5285C>A;c.5318C>A
p.Ser1745Tyr;p.Ser1762Tyr;p.Ser1773Tyr
De novo
Simplex
GEN223R114
missense_variant
c.2629G>C;c.2680G>C;c.2713G>C
p.Ala877Pro;p.Ala894Pro;p.Ala905Pro
De novo
Simplex
GEN223R115
stop_gained
c.2050C>T;c.2101C>T;c.2134C>T
p.Arg684Ter;p.Arg701Ter;p.Arg712Ter
De novo
Simplex
GEN223R130
intron_variant
c.4002+2165C>T
Familial
Paternal
Multi-generational
GEN223R134
intron_variant
c.4002+2503C>T
Familial
Maternal
Multi-generational
GEN223R143
frameshift_variant
c.3562delinsCC
p.Arg1188ProfsTer29
Familial
Paternal
GEN223R152
missense_variant
c.248A>G
p.Tyr83Cys
Familial
Maternal
Multi-generational
GEN223R178
frameshift_variant
c.5119_5122del
p.Phe1707ArgfsTer7
Unknown
Extended multiplex
GEN223R181
frameshift_variant
c.4553_4554del
p.Lys1518ThrfsTer18
De novo
Multiplex
GEN223R206
frameshift_variant
c.5370_5373del
p.Ser1790ArgfsTer10
De novo
Simplex
GEN223R220
missense_variant
c.5513C>T
p.Pro1838Leu
De novo
Multiplex (monozygotic twins)
GEN223R244
missense_variant
c.3926T>G
p.Leu1309Arg
Familial
Paternal
Multiplex
GEN223R248
frameshift_variant
c.4554dup
p.Pro1519ThrfsTer18
Unknown
Simplex
GEN223R250
frameshift_variant
c.5010_5013del
p.Phe1671ThrfsTer8
Unknown
Simplex
Common
Variant ID
Polymorphism
SNP ID
Allele Change
Residue Change
Population Origin
Population Stage
Author, Year
GEN223C001
intron_variant
rs7587026
c.-142+26807G>T
Minor allele, A
Discovery: 1018 MTLEHS cases, 7552 controls
Discovery
GEN223C002
intron_variant
rs7587026
c.-142+26807G>T
Minor allele, A
Replication: 959 MTLEHS cases, 3591 controls.
Replication
GEN223C003
intron_variant
rs11692675
c.264+3440A>G
Discovery: 1018 MTLEHS cases, 7552 controls; replication: 959 MTLEHS cases, 3591 controls.
Discovery
