Case Report: Novel Homozygous Likely Pathogenic SCN1A Variant With Autosomal Recessive Inheritance and Review of the Literature

Case Report: Novel Homozygous Likely Pathogenic SCN1A Variant With Autosomal Recessive Inheritance and Review of the Literature

Dominant pathogenic variations in the SCN1A gene are associated with several neuro developmental disorders with or without epilepsy, including Dravet syndrome (DS). Conversely, there are few published cases with homozygous or compound heterozygous variations in the SCN1A gene. Here, we describe two...

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Veröffentlicht in:Frontiers in neurology 2021-11, Vol.12, p.784892, Article 784892
Hauptverfasser: Marco Hernandez, Ana Victoria, Tomas Vila, Miguel, Caro Llopis, Alfonso, Monfort, Sandra, Martinez, Francisco
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autosomal recessive inheritance
Clinical Neurology
Dravet syndrome
GEFS
homozygous
Life Sciences & Biomedicine
Neurology
Neurosciences
Neurosciences & Neurology
Science & Technology
SCN1A
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Tomas Vila, Miguel
Caro Llopis, Alfonso
Monfort, Sandra
Martinez, Francisco
description Dominant pathogenic variations in the SCN1A gene are associated with several neuro developmental disorders with or without epilepsy, including Dravet syndrome (DS). Conversely, there are few published cases with homozygous or compound heterozygous variations in the SCN1A gene. Here, we describe two siblings from a consanguineous pedigree with epilepsy phenotype compatible with genetic epilepsy with febrile seizures plus (GEFS+) associated with the homozygous likely pathogenic variant (NM_001165963.1): c.4513A > C (p.Lys1505Gln). Clinical and genetic data were compared to those of other 10 previously published patients with epilepsy and variants in compound heterozygosity or homozygosity in the SCN1A gene. Most patients (11/12) had missense variants. Patients in whom the variants were located at the cytoplasmic or the extracellular domains frequently presented a less severe phenotype than those in whom they are located at the pore-forming domains. Five of the patients (41.7%) meet clinical criteria for Dravet syndrome (DS), one of them associated acute encephalopathy. Other five patients (41.7%) had a phenotype of epilepsy with febrile seizures plus familial origin, while the two remaining (17%) presented focal epileptic seizures. SCN1A-related epilepsies present in most cases an autosomal dominant inheritance; however, there is growing evidence that some genetic variants only manifest clinical symptoms when they are present in both alleles, following an autosomal recessive inheritance.
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subjects autosomal recessive inheritance
Clinical Neurology
Dravet syndrome
GEFS
homozygous
Life Sciences & Biomedicine
Neurology
Neurosciences
Neurosciences & Neurology
Science & Technology
SCN1A
title Case Report: Novel Homozygous Likely Pathogenic SCN1A Variant With Autosomal Recessive Inheritance and Review of the Literature
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