| Literature DB >> 30132828 |
Kari A Mattison1,2, Kameryn M Butler1,2, George Andrew S Inglis1,2, Oshrat Dayan3, Hanna Boussidan3, Vikas Bhambhani4, Bryan Philbrook5, Cristina da Silva6, John J Alexander1,6, Baruch I Kanner3, Andrew Escayg1,2.
Abstract
Previous reports have identified SLC6A1 variants in patients with generalized epilepsies, such as myoclonic-atonic epilepsy and childhood absence epilepsy. However, to date, none of the identified SLC6A1 variants has been functionally tested for an effect on GAT-1 transporter activity. The purpose of this study was to determine the incidence of SLC6A1 variants in 460 unselected epilepsy patients and to evaluate the impact of the identified variants on γ-aminobutyric acid (GABA)transport. Targeted resequencing was used to screen 460 unselected epilepsy patients for variants in SLC6A1. Five missense variants, one in-frame deletion, one nonsense variant, and one intronic splice-site variant were identified, representing a 1.7% diagnostic yield. Using a [3 H]-GABA transport assay, the seven identified exonic variants were found to reduce GABA transport activity. A minigene splicing assay revealed that the splice-site variant disrupted canonical splicing of exon 9 in the mRNA transcript, leading to premature protein truncation. These findings demonstrate that SLC6A1 is an important contributor to childhood epilepsy and that reduced GAT-1 function is a common consequence of epilepsy-causing SLC6A1 variants. Wiley Periodicals, Inc.Entities:
Keywords: GAT-1; absence epilepsy; epilepsy genetics; myoclonic-atonic epilepsy; γ-aminobutyric acid transport
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Year: 2018 PMID: 30132828 DOI: 10.1111/epi.14531
Source DB: PubMed Journal: Epilepsia ISSN: 0013-9580 Impact factor: 5.864