@article{10.37349/en.2025.1006120,
abstract = {Neurogenetic disorders remain genetically uncharacterized in many populations, including Libya. We report three Libyan patients from two consanguineous families with pathogenic variants in sodium channel genes. Two adult sisters (Patients 1 & 2) presented with global developmental delay and progressive spastic paraparesis without epilepsy. Whole exome sequencing identified the same heterozygous SCN8A variant (c.142G>A; p.Asp48Asn) in both sisters, classified as a variant of uncertain significance (VUS). Its occurrence in two affected siblings with a consistent phenotype and the absence of other explanatory variants provide supporting evidence for its potential pathogenicity. These cases represent the first documented instances of a suspected SCN8A-related disorder in Libya. A third, unrelated 10-year-old boy (Patient 3) with a phenotype consistent with Dravet syndrome, including refractory seizures and neurodevelopmental regression, was found to harbor a likely pathogenic heterozygous SCN1A variant (c.2113del; p.Glu705Lysfs*10). This report expands the genetic and phenotypic spectrum of neurological disorders in Libya and underscores the critical role of genetic testing, while also highlighting the need for segregation studies to achieve a definitive molecular diagnosis.},
author = {Bennour, Anwaar M. and Rajab, Ashraf M. and El-Zawawi, Heba A.},
doi = {10.37349/en.2025.1006120},
journal = {Exploration of Neuroscience},
elocation-id = {1006120},
title = {First report of SCN8A-related neurodevelopmental disorder and a case of SCN1A-related Dravet syndrome in Libya},
url = {https://www.explorationpub.com/Journals/en/Article/1006120},
volume = {4},
year = {2025}
}