BACKGROUND: Familial hemiplegic migraine is an autosomal dominant severe subtype of migraine with aura characterised by some degree of hemiparesis during the attacks. So far, mutations in two genes regulating ion translocation-CACNA1A and ATP1A2-have been identified in pedigrees with this disease. METHODS: To identify additional genes for familial hemiplegic migraine, we did a genome-wide linkage analysis of two disease pedigrees without mutations in CACNA1A and ATP1A2. Ion channel genes in the candidate interval were analysed for mutations, and the functional consequences of the recorded sequence alteration were determined. FINDINGS: We identified a novel locus for familial hemiplegic migraine on chromosome 2q24. Sequencing of candidate genes in this region revealed a heterozygous missense mutation (Gln1489Lys) in the neuronal voltage-gated sodium channel gene SCN1A, mutations of which have been associated with epilepsy. This same mutation was present in three families with familial hemiplegic migraine. It results in a charge-altering aminoacid exchange in the so-called hinged-lid domain of the protein, which is critical for fast inactivation of the channel. Whole-cell recordings in transiently transfected tsA201 cells expressing the highly homologous SCN5A sodium channel showed that the mutation induces a two-fold to four-fold accelerated recovery from fast inactivation without altering any of the other channel parameters investigated. INTERPRETATION: Dysfunction of the neuronal sodium channel SCN1A can cause familial hemiplegic migraine. Our findings have implications for the understanding of migraine aura. Moreover, our study reinforces the molecular links between migraine and epilepsy, two common paroxysmal disorders.
BACKGROUND: Familial hemiplegic migraine is an autosomal dominant severe subtype of migraine with aura characterised by some degree of hemiparesis during the attacks. So far, mutations in two genes regulating ion translocation-CACNA1A and ATP1A2-have been identified in pedigrees with this disease. METHODS: To identify additional genes for familial hemiplegic migraine, we did a genome-wide linkage analysis of two disease pedigrees without mutations in CACNA1A and ATP1A2. Ion channel genes in the candidate interval were analysed for mutations, and the functional consequences of the recorded sequence alteration were determined. FINDINGS: We identified a novel locus for familial hemiplegic migraine on chromosome 2q24. Sequencing of candidate genes in this region revealed a heterozygous missense mutation (Gln1489Lys) in the neuronal voltage-gated sodium channel gene SCN1A, mutations of which have been associated with epilepsy. This same mutation was present in three families with familial hemiplegic migraine. It results in a charge-altering aminoacid exchange in the so-called hinged-lid domain of the protein, which is critical for fast inactivation of the channel. Whole-cell recordings in transiently transfected tsA201 cells expressing the highly homologous SCN5A sodium channel showed that the mutation induces a two-fold to four-fold accelerated recovery from fast inactivation without altering any of the other channel parameters investigated. INTERPRETATION: Dysfunction of the neuronal sodium channel SCN1A can cause familial hemiplegic migraine. Our findings have implications for the understanding of migraine aura. Moreover, our study reinforces the molecular links between migraine and epilepsy, two common paroxysmal disorders.
Authors: Padhraig Gormley; Mitja I Kurki; Marjo Eveliina Hiekkala; Kumar Veerapen; Paavo Häppölä; Adele A Mitchell; Dennis Lal; Priit Palta; Ida Surakka; Mari Anneli Kaunisto; Eija Hämäläinen; Salli Vepsäläinen; Hannele Havanka; Hanna Harno; Matti Ilmavirta; Markku Nissilä; Erkki Säkö; Marja-Liisa Sumelahti; Jarmo Liukkonen; Matti Sillanpää; Liisa Metsähonkala; Seppo Koskinen; Terho Lehtimäki; Olli Raitakari; Minna Männikkö; Caroline Ran; Andrea Carmine Belin; Pekka Jousilahti; Verneri Anttila; Veikko Salomaa; Ville Artto; Markus Färkkilä; Heiko Runz; Mark J Daly; Benjamin M Neale; Samuli Ripatti; Mikko Kallela; Maija Wessman; Aarno Palotie Journal: Neuron Date: 2018-05-03 Impact factor: 17.173
Authors: V Anttila; M Kallela; G Oswell; M A Kaunisto; D R Nyholt; E Hamalainen; H Havanka; M Ilmavirta; J Terwilliger; E Sobel; L Peltonen; J Kaprio; M Farkkila; M Wessman; A Palotie Journal: Am J Hum Genet Date: 2006-05-10 Impact factor: 11.025
Authors: Ronald G Lafrenière; M Zameel Cader; Jean-François Poulin; Isabelle Andres-Enguix; Maryse Simoneau; Namrata Gupta; Karine Boisvert; François Lafrenière; Shannon McLaughlan; Marie-Pierre Dubé; Martin M Marcinkiewicz; Sreeram Ramagopalan; Olaf Ansorge; Bernard Brais; Jorge Sequeiros; Jose Maria Pereira-Monteiro; Lyn R Griffiths; Stephen J Tucker; George Ebers; Guy A Rouleau Journal: Nat Med Date: 2010-09-26 Impact factor: 53.440
Authors: Carla C M Chen; Kerrie L Mengersen; Jonathan M Keith; Nicholas G Martin; Dale R Nyholt Journal: Hum Genet Date: 2009-03-19 Impact factor: 4.132