Benign Infantile Seizures and Paroxysmal Dyskinesia Caused by an SCN8A Mutation

Elena Gardella; Felicitas Becker; Rikke S. Moller; Julian Schubert; Johannes R. Lemke; Line H. G. Larsen; Hans Eiberg; Michael Nothnagel; Holger Thiele; Janine Altmueller; Steffen Syrbe; Andreas Merkenschlager; Thomas Bast; Bernhard Steinhoff; Peter Nuernberg; Yuan Mang; Louise Bakke Moller; Pia Gellert; Sarah E. Heron; Leanne M. Dibbens; Sarah Weckhuysen; Hans Atli Dahl; Saskia Biskup; Niels Tommerup; Helle Hjalgrim; Holger Lerche; Sandor Beniczky; Yvonne G. Weber

doi:10.1002/ana.24580

Benign Infantile Seizures and Paroxysmal Dyskinesia Caused by an SCN8A Mutation

Elena Gardella, Felicitas Becker, Rikke S. Moller, Julian Schubert, Johannes R. Lemke, Line H. G. Larsen, Hans Eiberg, Michael Nothnagel, Holger Thiele, Janine Altmueller, Steffen Syrbe, Andreas Merkenschlager, Thomas Bast, Bernhard Steinhoff, Peter Nuernberg, Yuan Mang, Louise Bakke Moller, Pia Gellert, Sarah E. Heron, Leanne M. DibbensSarah Weckhuysen, Hans Atli Dahl, Saskia Biskup, Niels Tommerup, Helle Hjalgrim, Holger Lerche, Sandor Beniczky, Yvonne G. Weber

103 Citations (Scopus)

Abstract

Objective: Benign familial infantile seizures (BFIS), paroxysmal kinesigenic dyskinesia (PKD), and their combination-known as infantile convulsions and paroxysmal choreoathetosis (ICCA)-are related autosomal dominant diseases. PRRT2 (proline-rich transmembrane protein 2 gene) has been identified as the major gene in all 3 conditions, found to be mutated in 80 to 90% of familial and 30 to 35% of sporadic cases.

Methods: We searched for the genetic defect in PRRT2-negative, unrelated families with BFIS or ICCA using whole exome or targeted gene panel sequencing, and performed a detailed cliniconeurophysiological workup.

Results: In 3 families with a total of 16 affected members, we identified the same, cosegregating heterozygous missense mutation (c.4447G> A; p.E1483K) in SCN8A, encoding a voltage-gated sodium channel. A founder effect was excluded by linkage analysis. All individuals except 1 had normal cognitive and motor milestones, neuroimaging, and interictal neurological status. Fifteen affected members presented with afebrile focal or generalized tonic-clonic seizures during the first to second year of life; 5 of them experienced single unprovoked seizures later on. One patient had seizures only at school age. All patients stayed otherwise seizure-free, most without medication. Interictal electroencephalogram (EEG) was normal in all cases but 2. Five of 16 patients developed additional brief paroxysmal episodes in puberty, either dystonic/dyskinetic or "shivering" attacks, triggered by stretching, motor initiation, or emotional stimuli. In 1 case, we recorded typical PKD spells by video-EEG-polygraphy, documenting a cortical involvement.

Interpretation: Our study establishes SCN8A as a novel gene in which a recurrent mutation causes BFIS/ICCA, expanding the clinical-genetic spectrum of combined epileptic and dyskinetic syndromes.

Original language	English
Journal	Annals of Neurology
Volume	79
Issue number	3
Pages (from-to)	428-436
ISSN	0364-5134
DOIs	https://doi.org/10.1002/ana.24580
Publication status	Published - 1 Mar 2016

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Gardella, E., Becker, F., Moller, R. S., Schubert, J., Lemke, J. R., Larsen, L. H. G., Eiberg, H., Nothnagel, M., Thiele, H., Altmueller, J., Syrbe, S., Merkenschlager, A., Bast, T., Steinhoff, B., Nuernberg, P., Mang, Y., Moller, L. B., Gellert, P., Heron, S. E., ... Weber, Y. G. (2016). Benign Infantile Seizures and Paroxysmal Dyskinesia Caused by an SCN8A Mutation. Annals of Neurology, 79(3), 428-436. https://doi.org/10.1002/ana.24580

Gardella, E, Becker, F, Moller, RS, Schubert, J, Lemke, JR, Larsen, LHG, Eiberg, H, Nothnagel, M, Thiele, H, Altmueller, J, Syrbe, S, Merkenschlager, A, Bast, T, Steinhoff, B, Nuernberg, P, Mang, Y, Moller, LB, Gellert, P, Heron, SE, Dibbens, LM, Weckhuysen, S, Dahl, HA, Biskup, S, Tommerup, N, Hjalgrim, H, Lerche, H, Beniczky, S & Weber, YG 2016, 'Benign Infantile Seizures and Paroxysmal Dyskinesia Caused by an SCN8A Mutation', Annals of Neurology, vol. 79, no. 3, pp. 428-436. https://doi.org/10.1002/ana.24580

@article{d27cad24a5174651af3b7e4894b21a4c,

title = "Benign Infantile Seizures and Paroxysmal Dyskinesia Caused by an SCN8A Mutation",

abstract = "Objective: Benign familial infantile seizures (BFIS), paroxysmal kinesigenic dyskinesia (PKD), and their combination-known as infantile convulsions and paroxysmal choreoathetosis (ICCA)-are related autosomal dominant diseases. PRRT2 (proline-rich transmembrane protein 2 gene) has been identified as the major gene in all 3 conditions, found to be mutated in 80 to 90% of familial and 30 to 35% of sporadic cases.Methods: We searched for the genetic defect in PRRT2-negative, unrelated families with BFIS or ICCA using whole exome or targeted gene panel sequencing, and performed a detailed cliniconeurophysiological workup.Results: In 3 families with a total of 16 affected members, we identified the same, cosegregating heterozygous missense mutation (c.4447G> A; p.E1483K) in SCN8A, encoding a voltage-gated sodium channel. A founder effect was excluded by linkage analysis. All individuals except 1 had normal cognitive and motor milestones, neuroimaging, and interictal neurological status. Fifteen affected members presented with afebrile focal or generalized tonic-clonic seizures during the first to second year of life; 5 of them experienced single unprovoked seizures later on. One patient had seizures only at school age. All patients stayed otherwise seizure-free, most without medication. Interictal electroencephalogram (EEG) was normal in all cases but 2. Five of 16 patients developed additional brief paroxysmal episodes in puberty, either dystonic/dyskinetic or {"}shivering{"} attacks, triggered by stretching, motor initiation, or emotional stimuli. In 1 case, we recorded typical PKD spells by video-EEG-polygraphy, documenting a cortical involvement.Interpretation: Our study establishes SCN8A as a novel gene in which a recurrent mutation causes BFIS/ICCA, expanding the clinical-genetic spectrum of combined epileptic and dyskinetic syndromes.",

author = "Elena Gardella and Felicitas Becker and Moller, {Rikke S.} and Julian Schubert and Lemke, {Johannes R.} and Larsen, {Line H. G.} and Hans Eiberg and Michael Nothnagel and Holger Thiele and Janine Altmueller and Steffen Syrbe and Andreas Merkenschlager and Thomas Bast and Bernhard Steinhoff and Peter Nuernberg and Yuan Mang and Moller, {Louise Bakke} and Pia Gellert and Heron, {Sarah E.} and Dibbens, {Leanne M.} and Sarah Weckhuysen and Dahl, {Hans Atli} and Saskia Biskup and Niels Tommerup and Helle Hjalgrim and Holger Lerche and Sandor Beniczky and Weber, {Yvonne G.}",

year = "2016",

month = mar,

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doi = "10.1002/ana.24580",

language = "English",

volume = "79",

pages = "428--436",

journal = "Annals of Neurology",

issn = "0364-5134",

publisher = "JohnWiley & Sons, Inc.",

number = "3",

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TY - JOUR

T1 - Benign Infantile Seizures and Paroxysmal Dyskinesia Caused by an SCN8A Mutation

AU - Gardella, Elena

AU - Becker, Felicitas

AU - Moller, Rikke S.

AU - Schubert, Julian

AU - Lemke, Johannes R.

AU - Larsen, Line H. G.

AU - Eiberg, Hans

AU - Nothnagel, Michael

AU - Thiele, Holger

AU - Altmueller, Janine

AU - Syrbe, Steffen

AU - Merkenschlager, Andreas

AU - Bast, Thomas

AU - Steinhoff, Bernhard

AU - Nuernberg, Peter

AU - Mang, Yuan

AU - Moller, Louise Bakke

AU - Gellert, Pia

AU - Heron, Sarah E.

AU - Dibbens, Leanne M.

AU - Weckhuysen, Sarah

AU - Dahl, Hans Atli

AU - Biskup, Saskia

AU - Tommerup, Niels

AU - Hjalgrim, Helle

AU - Lerche, Holger

AU - Beniczky, Sandor

AU - Weber, Yvonne G.

PY - 2016/3/1

Y1 - 2016/3/1

N2 - Objective: Benign familial infantile seizures (BFIS), paroxysmal kinesigenic dyskinesia (PKD), and their combination-known as infantile convulsions and paroxysmal choreoathetosis (ICCA)-are related autosomal dominant diseases. PRRT2 (proline-rich transmembrane protein 2 gene) has been identified as the major gene in all 3 conditions, found to be mutated in 80 to 90% of familial and 30 to 35% of sporadic cases.Methods: We searched for the genetic defect in PRRT2-negative, unrelated families with BFIS or ICCA using whole exome or targeted gene panel sequencing, and performed a detailed cliniconeurophysiological workup.Results: In 3 families with a total of 16 affected members, we identified the same, cosegregating heterozygous missense mutation (c.4447G> A; p.E1483K) in SCN8A, encoding a voltage-gated sodium channel. A founder effect was excluded by linkage analysis. All individuals except 1 had normal cognitive and motor milestones, neuroimaging, and interictal neurological status. Fifteen affected members presented with afebrile focal or generalized tonic-clonic seizures during the first to second year of life; 5 of them experienced single unprovoked seizures later on. One patient had seizures only at school age. All patients stayed otherwise seizure-free, most without medication. Interictal electroencephalogram (EEG) was normal in all cases but 2. Five of 16 patients developed additional brief paroxysmal episodes in puberty, either dystonic/dyskinetic or "shivering" attacks, triggered by stretching, motor initiation, or emotional stimuli. In 1 case, we recorded typical PKD spells by video-EEG-polygraphy, documenting a cortical involvement.Interpretation: Our study establishes SCN8A as a novel gene in which a recurrent mutation causes BFIS/ICCA, expanding the clinical-genetic spectrum of combined epileptic and dyskinetic syndromes.

AB - Objective: Benign familial infantile seizures (BFIS), paroxysmal kinesigenic dyskinesia (PKD), and their combination-known as infantile convulsions and paroxysmal choreoathetosis (ICCA)-are related autosomal dominant diseases. PRRT2 (proline-rich transmembrane protein 2 gene) has been identified as the major gene in all 3 conditions, found to be mutated in 80 to 90% of familial and 30 to 35% of sporadic cases.Methods: We searched for the genetic defect in PRRT2-negative, unrelated families with BFIS or ICCA using whole exome or targeted gene panel sequencing, and performed a detailed cliniconeurophysiological workup.Results: In 3 families with a total of 16 affected members, we identified the same, cosegregating heterozygous missense mutation (c.4447G> A; p.E1483K) in SCN8A, encoding a voltage-gated sodium channel. A founder effect was excluded by linkage analysis. All individuals except 1 had normal cognitive and motor milestones, neuroimaging, and interictal neurological status. Fifteen affected members presented with afebrile focal or generalized tonic-clonic seizures during the first to second year of life; 5 of them experienced single unprovoked seizures later on. One patient had seizures only at school age. All patients stayed otherwise seizure-free, most without medication. Interictal electroencephalogram (EEG) was normal in all cases but 2. Five of 16 patients developed additional brief paroxysmal episodes in puberty, either dystonic/dyskinetic or "shivering" attacks, triggered by stretching, motor initiation, or emotional stimuli. In 1 case, we recorded typical PKD spells by video-EEG-polygraphy, documenting a cortical involvement.Interpretation: Our study establishes SCN8A as a novel gene in which a recurrent mutation causes BFIS/ICCA, expanding the clinical-genetic spectrum of combined epileptic and dyskinetic syndromes.

U2 - 10.1002/ana.24580

DO - 10.1002/ana.24580

M3 - Journal article

C2 - 26677014

SN - 0364-5134

VL - 79

SP - 428

EP - 436

JO - Annals of Neurology

JF - Annals of Neurology

IS - 3

ER -

Benign Infantile Seizures and Paroxysmal Dyskinesia Caused by an SCN8A Mutation

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