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Literature DB >> 30615093

Neuronal mechanisms of mutations in SCN8A causing epilepsy or intellectual disability.

Yuanyuan Liu¹, Julian Schubert¹, Lukas Sonnenberg², Katherine L Helbig³, Christina E Hoei-Hansen⁴, Mahmoud Koko¹, Maert Rannap¹, Stephan Lauxmann^1,2, Mahbubul Huq⁵, Michael C Schneider⁶, Katrine M Johannesen^7,8, Gerhard Kurlemann⁹, Elena Gardella^7,8, Felicitas Becker¹, Yvonne G Weber¹, Jan Benda², Rikke S Møller^7,8, Holger Lerche¹.

Abstract

Ion channel mutations can cause distinct neuropsychiatric diseases. We first studied the biophysical and neurophysiological consequences of four mutations in the human Na+ channel gene SCN8A causing either mild (E1483K) or severe epilepsy (R1872W), or intellectual disability and autism without epilepsy (R1620L, A1622D). Only combined electrophysiological recordings of transfected wild-type or mutant channels in both neuroblastoma cells and primary cultured neurons revealed clear genotype-phenotype correlations. The E1483K mutation causing mild epilepsy showed no significant biophysical changes, whereas the R1872W mutation causing severe epilepsy induced clear gain-of-function biophysical changes in neuroblastoma cells. However, both mutations increased neuronal firing in primary neuronal cultures. In contrast, the R1620L mutation associated with intellectual disability and autism-but not epilepsy-reduced Na+ current density in neuroblastoma cells and expectedly decreased neuronal firing. Interestingly, for the fourth mutation, A1622D, causing severe intellectual disability and autism without epilepsy, we observed a dramatic slowing of fast inactivation in neuroblastoma cells, which induced a depolarization block in neurons with a reduction of neuronal firing. This latter finding was corroborated by computational modelling. In a second series of experiments, we recorded three more mutations (G1475R, M1760I, G964R, causing intermediate or severe epilepsy, or intellectual disability without epilepsy, respectively) that revealed similar results confirming clear genotype-phenotype relationships. We found intermediate or severe gain-of-function biophysical changes and increases in neuronal firing for the two epilepsy-causing mutations and decreased firing for the loss-of-function mutation causing intellectual disability. We conclude that studies in neurons are crucial to understand disease mechanisms, which here indicate that increased or decreased neuronal firing is responsible for distinct clinical phenotypes.

Entities: Disease Gene Mutation Species

Mesh：

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Year: 2019 PMID： 30615093 DOI： 10.1093/brain/awy326

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

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Cited

24 in total

1. Effects of Deltamethrin Acute Exposure on Nav1.6 Channels and Medium Spiny Neurons of the Nucleus Accumbens.

Authors: Cynthia M Tapia; Oluwarotimi Folorunso; Aditya K Singh; Kathleen McDonough; Fernanda Laezza
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2. NBI-921352, a first-in-class, Na_V1.6 selective, sodium channel inhibitor that prevents seizures in Scn8a gain-of-function mice, and wild-type mice and rats.

Authors: J P Johnson; Thilo Focken; Kuldip Khakh; Parisa Karimi Tari; Celine Dube; Samuel J Goodchild; Jean-Christophe Andrez; Girish Bankar; David Bogucki; Kristen Burford; Elaine Chang; Sultan Chowdhury; Richard Dean; Gina de Boer; Shannon Decker; Christoph Dehnhardt; Mandy Feng; Wei Gong; Michael Grimwood; Abid Hasan; Angela Hussainkhel; Qi Jia; Stephanie Lee; Jenny Li; Sophia Lin; Andrea Lindgren; Verner Lofstrand; Janette Mezeyova; Rostam Namdari; Karen Nelkenbrecher; Noah Gregory Shuart; Luis Sojo; Shaoyi Sun; Matthew Taron; Matthew Waldbrook; Diana Weeratunge; Steven Wesolowski; Aaron Williams; Michael Wilson; Zhiwei Xie; Rhena Yoo; Clint Young; Alla Zenova; Wei Zhang; Alison J Cutts; Robin P Sherrington; Simon N Pimstone; Raymond Winquist; Charles J Cohen; James R Empfield
Journal: Elife Date: 2022-03-02 Impact factor: 8.140

3. SCN8A epileptic encephalopathy mutations display a gain-of-function phenotype and divergent sensitivity to antiepileptic drugs.

Authors: Qian-Bei Guo; Li Zhan; Hai-Yan Xu; Zhao-Bing Gao; Yue-Ming Zheng
Journal: Acta Pharmacol Sin Date: 2022-07-27 Impact factor: 7.169

Review 4. Rational Small Molecule Treatment for Genetic Epilepsies.

Authors: Ethan M Goldberg
Journal: Neurotherapeutics Date: 2021-08-24 Impact factor: 6.088

Review 5. Diagnostic Considerations in the Epilepsies-Testing Strategies, Test Type Advantages, and Limitations.

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Journal: Neurotherapeutics Date: 2021-09-16 Impact factor: 6.088

6. Functional analysis of three Na_v1.6 mutations causing early infantile epileptic encephalopathy.

Authors: Laura Solé; Jacy L Wagnon; Michael M Tamkun
Journal: Biochim Biophys Acta Mol Basis Dis Date: 2020-09-08 Impact factor: 5.187

7. Biallelic inherited SCN8A variants, a rare cause of SCN8A-related developmental and epileptic encephalopathy.

Authors: Eric R Wengert; Cathrine E Tronhjem; Jacy L Wagnon; Katrine M Johannesen; Hayley Petit; Ilona Krey; Anusha U Saga; Payal S Panchal; Samantha M Strohm; Jörn Lange; Susanne B Kamphausen; Guido Rubboli; Johannes R Lemke; Elena Gardella; Manoj K Patel; Miriam H Meisler; Rikke S Møller
Journal: Epilepsia Date: 2019-10-17 Impact factor: 5.864

Neuronal mechanisms of mutations in SCN8A causing epilepsy or intellectual disability.

1. Effects of Deltamethrin Acute Exposure on Nav1.6 Channels and Medium Spiny Neurons of the Nucleus Accumbens.

2. NBI-921352, a first-in-class, Na_V1.6 selective, sodium channel inhibitor that prevents seizures in Scn8a gain-of-function mice, and wild-type mice and rats.

3. SCN8A epileptic encephalopathy mutations display a gain-of-function phenotype and divergent sensitivity to antiepileptic drugs.

Review 4. Rational Small Molecule Treatment for Genetic Epilepsies.

Review 5. Diagnostic Considerations in the Epilepsies-Testing Strategies, Test Type Advantages, and Limitations.

6. Functional analysis of three Na_v1.6 mutations causing early infantile epileptic encephalopathy.

7. Biallelic inherited SCN8A variants, a rare cause of SCN8A-related developmental and epileptic encephalopathy.

Review 8. Sodium channelopathies in neurodevelopmental disorders.

Review 9. Sodium channelopathies of skeletal muscle and brain.

Review 10. Dendritic Integration Dysfunction in Neurodevelopmental Disorders.

Neuronal mechanisms of mutations in SCN8A causing epilepsy or intellectual disability.

1. Effects of Deltamethrin Acute Exposure on Nav1.6 Channels and Medium Spiny Neurons of the Nucleus Accumbens.

2. NBI-921352, a first-in-class, NaV1.6 selective, sodium channel inhibitor that prevents seizures in Scn8a gain-of-function mice, and wild-type mice and rats.

3. SCN8A epileptic encephalopathy mutations display a gain-of-function phenotype and divergent sensitivity to antiepileptic drugs.

Review 4. Rational Small Molecule Treatment for Genetic Epilepsies.

Review 5. Diagnostic Considerations in the Epilepsies-Testing Strategies, Test Type Advantages, and Limitations.

6. Functional analysis of three Nav1.6 mutations causing early infantile epileptic encephalopathy.

7. Biallelic inherited SCN8A variants, a rare cause of SCN8A-related developmental and epileptic encephalopathy.

Review 8. Sodium channelopathies in neurodevelopmental disorders.

Review 9. Sodium channelopathies of skeletal muscle and brain.

Review 10. Dendritic Integration Dysfunction in Neurodevelopmental Disorders.

2. NBI-921352, a first-in-class, Na_V1.6 selective, sodium channel inhibitor that prevents seizures in Scn8a gain-of-function mice, and wild-type mice and rats.

6. Functional analysis of three Na_v1.6 mutations causing early infantile epileptic encephalopathy.