1. A missense mutation in SLC6A1 associated with Lennox-Gastaut syndrome impairs GABA transporter 1 protein trafficking and function
- Author
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Gerald Nwosu, Hai-Xia Zhu, Jie Wang, Jaclyn Eissman, Juexin Wang, Kefu Cai, Jeffrey Song, Eric Delpire, Dong Xu, Hui-Ci Liang, Wei-Ping Liao, Wangzhen Shen, Jing-Qiong Kang, Yi-Wu Shi, Xiao-Jing Li, and Yong-Hong Yi
- Subjects
Male ,0301 basic medicine ,GABA Plasma Membrane Transport Proteins ,Adolescent ,Mutant ,Mutation, Missense ,medicine.disease_cause ,Article ,Flow cytometry ,GABA transporter 1 ,03 medical and health sciences ,0302 clinical medicine ,Developmental Neuroscience ,medicine ,Animals ,Humans ,Missense mutation ,Mutation ,medicine.diagnostic_test ,biology ,Lennox Gastaut Syndrome ,Chemistry ,HEK 293 cells ,Molecular biology ,Pedigree ,Rats ,Transport protein ,Protein Transport ,HEK293 Cells ,030104 developmental biology ,Neurology ,biology.protein ,GABAergic ,030217 neurology & neurosurgery ,HeLa Cells - Abstract
Background Mutations in SLC6A1 have been associated mainly with myoclonic atonic epilepsy (MAE) and intellectual disability. We identified a novel missense mutation in a patient with Lennox-Gastaut syndrome (LGS) characterized by severe seizures and developmental delay. Methods Exome Sequencing was performed in an epilepsy patient cohort. The impact of the mutation was evaluated by 3H γ-aminobutyric acid (GABA) uptake, structural modeling, live cell microscopy, cell surface biotinylation and a high-throughput assay flow cytometry in both neurons and non neuronal cells. Results We discovered a heterozygous missense mutation (c700G to A [pG234S) in the SLC6A1 encoding GABA transporter 1 (GAT-1). Structural modeling suggests the mutation destabilizes the global protein conformation. With transient expression of enhanced yellow fluorescence protein (YFP) tagged rat GAT-1 cDNAs, we demonstrated that the mutant GAT-1(G234S) transporter had reduced total protein expression in both rat cortical neurons and HEK 293 T cells. With a high-throughput flow cytometry assay and live cell surface biotinylation, we demonstrated that the mutant GAT-1(G234S) had reduced cell surface expression. 3H radioactive labeling GABA uptake assay in HeLa cells indicated a reduced function of the mutant GAT-1(G234S). Conclusions This mutation caused instability of the mutant transporter protein, which resulted in reduced cell surface and total protein levels. The mutation also caused reduced GABA uptake in addition to reduced protein expression, leading to reduced GABA clearance, and altered GABAergic signaling in the brain. The impaired trafficking and reduced GABA uptake function may explain the epilepsy phenotype in the patient.
- Published
- 2019