The gain of function <i>SCN1A</i> disorder spectrum: novel epilepsy phenotypes and therapeutic implications-Reference-Cited by-同舟云学术

The gain of function SCN1A disorder spectrum: novel epilepsy phenotypes and therapeutic implications

Published:2022-06-13 Issue:11 Volume:145 Page:3816-3831
ISSN:0006-8950
Container-title:Brain
language:en
Short-container-title:

Author:

Brunklaus Andreas¹²^ORCID,Brünger Tobias³,Feng Tony¹²,Fons Carmen⁴,Lehikoinen Anni⁵,Panagiotakaki Eleni⁶,Vintan Mihaela-Adela⁷,Symonds Joseph¹²^ORCID,Andrew James²,Arzimanoglou Alexis⁴⁶,Delima Sarah⁸,Gallois Julie⁹,Hanrahan Donncha¹⁰,Lesca Gaetan¹¹,MacLeod Stewart²,Marjanovic Dragan¹²,McTague Amy¹³¹⁴,Nuñez-Enamorado Noemi¹⁵,Perez-Palma Eduardo¹⁶,Scott Perry M¹⁷,Pysden Karen¹⁸,Russ-Hall Sophie J¹⁹,Scheffer Ingrid E¹⁹²⁰²¹,Sully Krystal²²²³,Syrbe Steffen²⁴,Vaher Ulvi²⁵,Velayutham Murugan²⁶,Vogt Julie²⁷,Weiss Shelly²⁸,Wirrell Elaine²⁹,Zuberi Sameer M¹²^ORCID,Lal Dennis³³⁰³¹³²,Møller Rikke S¹²³³,Mantegazza Massimo³⁴³⁵³⁶^ORCID,Cestèle Sandrine³⁴³⁵

Affiliation:

1. Institute of Health and Wellbeing, University of Glasgow , Glasgow , UK

2. The Paediatric Neurosciences Research Group, Royal Hospital for Children, Member of the ERN EpiCARE , Glasgow , UK

3. Cologne Center for Genomics, University of Cologne , Cologne , Germany

4. Pediatric Neurology Department, CIBERER-ISCIII, Sant Joan de Déu Universitary Hospital, Institut de Recerca Sant Joan de Déu, Member of the ERN EpiCARE , Barcelona , Spain

5. Pediatric Neurology Department, Kuopio University Hospital, Member of the ERN EpiCARE , Kuopio , Finland

6. Department of Paediatric Clinical Epileptology, sleep disorders and functional neurology, Member of the ERN EpiCARE, University Hospitals of Lyon (HCL) and Inserm U1028/CNRS UMR5292 , Lyon , France

7. ‘Iuliu Hatieganu’ University of Medicine and Pharmacy, Faculty of Medicine, Department of Neuroscience, Neurology and Pediatric Neurology , Victor Babes, 43, 400012 Cluj-Napoca , Romania

8. Indiana University School of Medicine, IU Health Riley Hospital for Children, Department of Neurology, Division of Pediatric Neurology , Indianapolis, IN , USA

9. Louisiana State University Health Sciences Center School of Medicine , New Orleans, LA , USA

10. Department of Paediatric Neurology, Royal Belfast Hospital for Sick Children , Belfast , UK

11. Department of Medical Genetics, Lyon University Hospital, Member of the ERN EpiCARE , Université Claude Bernard Lyon 1, Lyon , France

12. The Danish Epilepsy Centre, Member of the ERN EpiCARE , Dianalund , Denmark

13. Developmental Neurosciences, UCL Great Ormond Street Institute of Child Health , London , UK

14. Department of Neurology, Great Ormond Street Hospital for Children, Member of the ERN EpiCARE , London , UK

15. Pediatric Neurology Department, 12 Octubre Universitary Hospital , Madrid , Spain

16. Universidad del Desarrollo, Centro de Genética y Genómica, Facultad de Medicina Clínica Alemana , Santiago , Chile

17. Jane and John Justin Neurosciences Center, Cook Children’s Medical Center , Ft Worth, TX , USA

18. Paediatric Neurology Department, Leeds Teaching Hospitals, Leeds General Infirmary , Leeds , UK

19. Epilepsy Research Centre, Department of Medicine, University of Melbourne, Austin Health , Melbourne , Australia

20. Florey Institute of Neuroscience and Mental Health , Melbourne , Australia

21. Murdoch Children’s Research Institute and Department of Paediatrics, University of Melbourne, Royal Children’s Hospital , Melbourne , Australia

22. Baylor College of Medicine , Houston, TX , USA

23. Texas Children’s Hospital , Houston, TX , USA

24. Division of Pediatric Epileptology, Center for Pediatrics and Adolescent Medicine, University Hospital Heidelberg , Heidelberg , Germany

25. Children’s Clinic of Tartu University Hospital, Faculty of Medicine of Tartu University, Member of the ERN EpiCARE , Tartu , Estonia

26. Birmingham Children’s Hospital , Birmingham , UK

27. West Midlands Regional Genetics Service, Birmingham Women’s and Children’s Hospital , Birmingham , UK

28. Division of Neurology, SickKids, University of Toronto , Toronto , Canada

29. Divisions of Epilepsy and Child and Adolescent Neurology, Department of Neurology, Mayo Clinic , Rochester, MN , USA

30. Genomic Medicine Institute, Lerner Research Institute, Cleveland Clinic , Cleveland, OH , USA

31. Epilepsy Center, Neurological Institute, Cleveland Clinic , Cleveland, OH , USA

32. Stanley Center for Psychiatric Genetics, Broad Institute of MIT and Harvard , Cambridge, MA , USA

33. Department of Regional Health Research, University of Southern Denmark , Odense , Denmark

34. Université Côte d’Azur , 06560 Valbonne-Sophia Antipolis , France

35. CNRS UMR7275, Institute of Molecular and Cellular Pharmacology (IPMC) , 06560 Valbonne-Sophia Antipolis , France

36. Inserm , 06560 Valbonne-Sophia Antipolis , France

Abstract

Abstract Brain voltage-gated sodium channel NaV1.1 (SCN1A) loss-of-function variants cause the severe epilepsy Dravet syndrome, as well as milder phenotypes associated with genetic epilepsy with febrile seizures plus. Gain of function SCN1A variants are associated with familial hemiplegic migraine type 3. Novel SCN1A-related phenotypes have been described including early infantile developmental and epileptic encephalopathy with movement disorder, and more recently neonatal presentations with arthrogryposis. Here we describe the clinical, genetic and functional evaluation of affected individuals. Thirty-five patients were ascertained via an international collaborative network using a structured clinical questionnaire and from the literature. We performed whole-cell voltage-clamp electrophysiological recordings comparing sodium channels containing wild-type versus variant NaV1.1 subunits. Findings were related to Dravet syndrome and familial hemiplegic migraine type 3 variants. We identified three distinct clinical presentations differing by age at onset and presence of arthrogryposis and/or movement disorder. The most severely affected infants (n = 13) presented with congenital arthrogryposis, neonatal onset epilepsy in the first 3 days of life, tonic seizures and apnoeas, accompanied by a significant movement disorder and profound intellectual disability. Twenty-one patients presented later, between 2 weeks and 3 months of age, with a severe early infantile developmental and epileptic encephalopathy and a movement disorder. One patient presented after 3 months with developmental and epileptic encephalopathy only. Associated SCN1A variants cluster in regions of channel inactivation associated with gain of function, different to Dravet syndrome variants (odds ratio = 17.8; confidence interval = 5.4–69.3; P = 1.3 × 10−7). Functional studies of both epilepsy and familial hemiplegic migraine type 3 variants reveal alterations of gating properties in keeping with neuronal hyperexcitability. While epilepsy variants result in a moderate increase in action current amplitude consistent with mild gain of function, familial hemiplegic migraine type 3 variants induce a larger effect on gating properties, in particular the increase of persistent current, resulting in a large increase of action current amplitude, consistent with stronger gain of function. Clinically, 13 out of 16 (81%) gain of function variants were associated with a reduction in seizures in response to sodium channel blocker treatment (carbamazepine, oxcarbazepine, phenytoin, lamotrigine or lacosamide) without evidence of symptom exacerbation. Our study expands the spectrum of gain of function SCN1A-related epilepsy phenotypes, defines key clinical features, provides novel insights into the underlying disease mechanisms between SCN1A-related epilepsy and familial hemiplegic migraine type 3, and identifies sodium channel blockers as potentially efficacious therapies. Gain of function disease should be considered in early onset epilepsies with a pathogenic SCN1A variant and non-Dravet syndrome phenotype.

Funder

Dravet Syndrome Foundation

BMBF

NIH

Publisher

Oxford University Press (OUP)

Subject

Neurology (clinical)

Link

https://academic.oup.com/brain/advance-article-pdf/doi/10.1093/brain/awac210/44046742/awac210.pdf

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