Literature DB >> 31056671

Altered inhibitory synapses in de novo GABRA5 and GABRA1 mutations associated with early onset epileptic encephalopathies.

Ciria C Hernandez1,2, Wenshu XiangWei3,4, Ningning Hu1, Dingding Shen5,6, Wangzhen Shen1, Andre H Lagrange1,7, Yujia Zhang8, Lifang Dai8, Changhong Ding8, Zhaohui Sun9, Jiasheng Hu10, Hongmin Zhu10, Yuwu Jiang3,4, Robert L Macdonald1.   

Abstract

We performed next generation sequencing on 1696 patients with epilepsy and intellectual disability using a gene panel with 480 epilepsy-related genes including all GABAA receptor subunit genes (GABRs), and we identified six de novo GABR mutations, two novel GABRA5 mutations (c.880G>T, p.V294F and c.1238C>T, p.S413F), two novel GABRA1 mutations (c.778C>T, p.P260S and c.887T>C, p.L296S/c.944G>T, p.W315L) and two known GABRA1 mutations (c.335G>A, p.R112Q and c.343A>G, p.N115D) in six patients with intractable early onset epileptic encephalopathy. The α5(V294F and S413F) and α1(P260S and L296S/W315L) subunit residue substitutions were all in transmembrane domains, while the α1(R112Q and N115R) subunit residue substitutions were in the N-terminal GABA binding domain. Using multidisciplinary approaches, we compared effects of mutant GABAA receptor α5 and α1 subunits on the properties of recombinant α5β3γ2 and α1β3γ2 GABAA receptors in both neuronal and non-neuronal cells and characterized their effects on receptor clustering, biogenesis and channel function. GABAA receptors containing mutant α5 and α1 subunits all had reduced cell surface and total cell expression with altered endoplasmic reticulum processing, impaired synaptic clustering, reduced GABAA receptor function and decreased GABA binding potency. Our study identified GABRA5 as a causative gene for early onset epileptic encephalopathy and expands the mutant GABRA1 phenotypic spectrum, supporting growing evidence that defects in GABAergic neurotransmission contribute to early onset epileptic encephalopathy phenotypes.
© The Author(s) (2019). Published by Oxford University Press on behalf of the Guarantors of Brain. All rights reserved. For Permissions, please email: journals.permissions@oup.com.

Entities:  

Keywords:  zzm321990 GABRA1zzm321990 ; zzm321990 GABRA5zzm321990 ; GABAA receptors; GABAergic synapses; encephalopathy

Mesh:

Substances:

Year:  2019        PMID: 31056671      PMCID: PMC6598634          DOI: 10.1093/brain/awz123

Source DB:  PubMed          Journal:  Brain        ISSN: 0006-8950            Impact factor:   13.501


  60 in total

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Journal:  Ann Neurol       Date:  2015-03-28       Impact factor: 10.422

3.  GABRA1 and STXBP1: novel genetic causes of Dravet syndrome.

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Authors:  C N Connolly; B J Krishek; B J McDonald; T G Smart; S J Moss
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Authors:  C Essrich; M Lorez; J A Benson; J M Fritschy; B Lüscher
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Review 7.  Understanding Genotypes and Phenotypes in Epileptic Encephalopathies.

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10.  The Ensembl gene annotation system.

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Journal:  Database (Oxford)       Date:  2016-06-23       Impact factor: 3.451

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  13 in total

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2.  Encephalitis patient-derived monoclonal GABAA receptor antibodies cause epileptic seizures.

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3.  Genetic Association of Epilepsy and Anti-Epileptic Drugs Treatment in Jordanian Patients.

Authors:  Laith N Al-Eitan; Islam M Al-Dalala; Afrah K Elshammari; Wael H Khreisat; Aseel F Nimiri; Adan H Alnaamneh; Hanan A Aljamal; Mansour A Alghamdi
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4.  Successful use of perampanel in GABRA1-related myoclonic epilepsy with photosensitivity.

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5.  Rare variants in the GABAA receptor subunit ε identified in patients with a wide spectrum of epileptic phenotypes.

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7.  Activity- and sleep-dependent regulation of tonic inhibition by Shisa7.

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8.  Manganese exposure in juvenile C57BL/6 mice increases glial inflammatory responses in the substantia nigra following infection with H1N1 influenza virus.

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9.  Dravet syndrome-associated mutations in GABRA1, GABRB2 and GABRG2 define the genetic landscape of defects of GABAA receptors.

Authors:  Ciria C Hernandez; XiaoJuan Tian; Ningning Hu; Wangzhen Shen; Mackenzie A Catron; Ying Yang; Jiaoyang Chen; Yuwu Jiang; Yuehua Zhang; Robert L Macdonald
Journal:  Brain Commun       Date:  2021-03-11

10.  Side chain similarity comparisons for integrated drug repositioning and potential toxicity assessments in epidemic response scenarios: The case for COVID-19.

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