| Literature DB >> 30895386 |
Barbara Castellotti1, Francesca Ragona2, Elena Freri2, Roberta Solazzi2, Stefano Ciardullo1, Giovanni Tricomi3, Anna Venerando1, Barbara Salis2, Laura Canafoglia4, Flavio Villani5, Silvana Franceschetti4, Nardo Nardocci2, Cinzia Gellera1, Jacopo C DiFrancesco6,7, Tiziana Granata8.
Abstract
Glucose transporter type 1 deficiency syndrome (Glut1 DS) is a rare neurological disorder caused by impaired glucose delivery to the brain. The clinical spectrum of Glut1 DS mainly includes epilepsy, paroxysmal dyskinesia (PD), developmental delay and microcephaly. Glut1 DS diagnosis is based on the identification of hypoglycorrhachia and pathogenic mutations of the SLC2A1 gene. Here, we report the molecular screening of SLC2A1 in 354 patients clinically suspected for Glut1 DS. From this cohort, we selected 245 patients for whom comprehensive clinical and laboratory data were available. Among them, we identified 19 patients carrying nucleotide variants of pathological significance, 5 of which were novel. The symptoms of onset, which varied from neonatal to adult age, included epilepsy, PD or non-epileptic paroxysmal manifestations. The comparison of the clinical features between the 19 SLC2A1 mutated and the 226 non-mutated patients revealed that the onset of epilepsy within the first year of life (when associated with developmental delay or other neurological manifestations), the association of epilepsy with PD and acquired microcephaly are more common in mutated subjects. Taken together, these data confirm the variability of expression of the phenotypes associated with mutation of SLC2A1 and provide useful clinical tools for the early identification of subjects highly suspected for the disease.Entities:
Keywords: Developmental delay; Epilepsy; Glut1 deficiency; Hypoglycorrhachia; Intellectual disability; Movement disorder; SLC2A1
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Year: 2019 PMID: 30895386 DOI: 10.1007/s00415-019-09280-6
Source DB: PubMed Journal: J Neurol ISSN: 0340-5354 Impact factor: 4.849