Structural analysis of pathogenic missense mutations in GABRA2 and identification of a novel de novo variant in the desensitization gate

Alba Sanchis‐Juan; Marcia A. Hasenahuer; James A. Baker; Amy McTague; Katy Barwick; Manju A. Kurian; Sofia T. Duarte; NIHR BioResource; Keren J. Carss; Janet Thornton; F. Lucy Raymond

doi:10.1002/mgg3.1106

Molecular Genetics & Genomic Medicine (Jul 2020)

Structural analysis of pathogenic missense mutations in GABRA2 and identification of a novel de novo variant in the desensitization gate

Alba Sanchis‐Juan,
Marcia A. Hasenahuer,
James A. Baker,
Amy McTague,
Katy Barwick,
Manju A. Kurian,
Sofia T. Duarte,
NIHR BioResource,
Keren J. Carss,
Janet Thornton,
F. Lucy Raymond

Affiliations

Alba Sanchis‐Juan: Department of Haematology University of Cambridge NHS Blood and Transplant Centre Cambridge UK
Marcia A. Hasenahuer: European Molecular Biology Laboratory European Bioinformatics Institute Wellcome Genome Campus Hinxton, Cambridge UK
James A. Baker: European Molecular Biology Laboratory European Bioinformatics Institute Wellcome Genome Campus Hinxton, Cambridge UK
Amy McTague: Developmental Neurosciences Great Ormond Street Institute of Child Health University College London London UK
Katy Barwick: Developmental Neurosciences Great Ormond Street Institute of Child Health University College London London UK
Manju A. Kurian: Developmental Neurosciences Great Ormond Street Institute of Child Health University College London London UK
Sofia T. Duarte: Hospital Dona Estefânia Centro Hospitalar de Lisboa Central Lisbon Portugal
NIHR BioResource
Keren J. Carss: Department of Haematology University of Cambridge NHS Blood and Transplant Centre Cambridge UK
Janet Thornton: European Molecular Biology Laboratory European Bioinformatics Institute Wellcome Genome Campus Hinxton, Cambridge UK
F. Lucy Raymond: NIHR BioResource Cambridge University Hospitals NHS Foundation Trust Cambridge Biomedical Campus Cambridge UK

DOI: https://doi.org/10.1002/mgg3.1106
Journal volume & issue: Vol. 8, no. 7
pp. n/a – n/a

Abstract

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Abstract Background Cys‐loop receptors control neuronal excitability in the brain and their dysfunction results in numerous neurological disorders. Recently, six missense variants in GABRA2, a member of this family, have been associated with early infantile epileptic encephalopathy (EIEE). We identified a novel de novo missense variant in GABRA2 in a patient with EIEE and performed protein structural analysis of the seven variants. Methods The novel variant was identified by trio whole‐genome sequencing. We performed protein structural analysis of the seven variants, and compared them to previously reported pathogenic mutations at equivalent positions in other Cys‐loop receptors. Additionally, we studied the distribution of disease‐associated variants in the transmembrane helices of these proteins. Results The seven variants are in the transmembrane domain, either close to the desensitization gate, the activation gate, or in inter‐subunit interfaces. Six of them have pathogenic mutations at equivalent positions in other Cys‐loop receptors, emphasizing the importance of these residues. Also, pathogenic mutations are more common in the pore‐lining helix, consistent with this region being highly constrained for variation in control populations. Conclusion Our study reports a novel pathogenic variant in GABRA2, characterizes the regions where pathogenic mutations are in the transmembrane helices, and underscores the value of considering sequence, evolutionary, and structural information as a strategy for variant interpretation of novel missense mutations.

Published in Molecular Genetics & Genomic Medicine

ISSN: 2324-9269 (Online)
Publisher: Wiley
Country of publisher: United States
LCC subjects: Science: Biology (General): Genetics
Website: https://onlinelibrary.wiley.com/journal/23249269

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