XB-ART-51334
Nat Genet
2013 Sep 01;459:1067-72.
Show Gene links
Show Anatomy links
Mutations in GRIN2A cause idiopathic focal epilepsy with rolandic spikes.
Lemke JR
,
Lal D
,
Reinthaler EM
,
Steiner I
,
Nothnagel M
,
Alber M
,
Geider K
,
Laube B
,
Schwake M
,
Finsterwalder K
,
Franke A
,
Schilhabel M
,
Jähn JA
,
Muhle H
,
Boor R
,
Van Paesschen W
,
Caraballo R
,
Fejerman N
,
Weckhuysen S
,
De Jonghe P
,
Larsen J
,
Møller RS
,
Hjalgrim H
,
Addis L
,
Tang S
,
Hughes E
,
Pal DK
,
Veri K
,
Vaher U
,
Talvik T
,
Dimova P
,
Guerrero López R
,
Serratosa JM
,
Linnankivi T
,
Lehesjoki AE
,
Ruf S
,
Wolff M
,
Buerki S
,
Wohlrab G
,
Kroell J
,
Datta AN
,
Fiedler B
,
Kurlemann G
,
Kluger G
,
Hahn A
,
Haberlandt DE
,
Kutzer C
,
Sperner J
,
Becker F
,
Weber YG
,
Feucht M
,
Steinböck H
,
Neophythou B
,
Ronen GM
,
Gruber-Sedlmayr U
,
Geldner J
,
Harvey RJ
,
Hoffmann P
,
Herms S
,
Altmüller J
,
Toliat MR
,
Thiele H
,
Nürnberg P
,
Wilhelm C
,
Stephani U
,
Helbig I
,
Lerche H
,
Zimprich F
,
Neubauer BA
,
Biskup S
,
von Spiczak S
.
???displayArticle.abstract???
Idiopathic focal epilepsy (IFE) with rolandic spikes is the most common childhood epilepsy, comprising a phenotypic spectrum from rolandic epilepsy (also benign epilepsy with centrotemporal spikes, BECTS) to atypical benign partial epilepsy (ABPE), Landau-Kleffner syndrome (LKS) and epileptic encephalopathy with continuous spike and waves during slow-wave sleep (CSWS). The genetic basis is largely unknown. We detected new heterozygous mutations in GRIN2A in 27 of 359 affected individuals from 2 independent cohorts with IFE (7.5%; P = 4.83 × 10(-18), Fisher's exact test). Mutations occurred significantly more frequently in the more severe phenotypes, with mutation detection rates ranging from 12/245 (4.9%) in individuals with BECTS to 9/51 (17.6%) in individuals with CSWS (P = 0.009, Cochran-Armitage test for trend). In addition, exon-disrupting microdeletions were found in 3 of 286 individuals (1.0%; P = 0.004, Fisher's exact test). These results establish alterations of the gene encoding the NMDA receptor NR2A subunit as a major genetic risk factor for IFE.
???displayArticle.pubmedLink??? 23933819
???displayArticle.link??? Nat Genet
Species referenced: Xenopus
Genes referenced: grin2a
GO keywords: glutamate receptor activity
???displayArticle.disOnts??? childhood electroclinical syndrome [+]
???displayArticle.omims??? EPILEPSY, FOCAL, WITH SPEECH DISORDER AND WITH OR WITHOUT IMPAIRED INTELLECTUAL DEVELOPMENT; FESD
???attribute.lit??? ???displayArticles.show???
|
|
|
Figure 1: Structural and functional consequences of the missense mutation in GRIN2A encoding p.Ala243Val. Functional analysis of the missense alteration p.Ala243Val (index subject 1) showed a significant reduction in high-affinity Zn2+ inhibition, whereas current amplitude, glutamate and glycine affinities and relative open-state probability remained unchanged. (a) Topology model of an NR1 and an NR2A subunit. The position of p.Ala243Val is indicated by a star in the NR2A subunit consisting of an N-terminal domain (NTD), the ligand-binding domain (LBD) including the S1 and S2 peptide segments, three transmembrane segments (M1âM3), a re-entrant pore loop (P) and an intracellular C-terminal domain (CTD). Ala243 lies within the Zn2+-binding NTD in NR2A. (b) Model of the NR2A NTD (cyan) together with an adjacent NR1 NTD (green). An enlarged view shows Ala243 within the Zn2+-binding NR2A NTD. (c) Pharmacological characterization of the apparent agonist affinities of wild-type and mutant NMDA receptors. Glutamate dose-response curves of wild-type NR1-NR2A (black triangles) and mutant NR1âNR2A Ala243Val (red squares) NMDA receptors were measured upon heterologous expression in Xenopus laevis oocytes by two-electrode voltage clamping (TEVC; n = 5). Similar glutamate and glycine (data not shown) concentrations were required for a half-maximal response (EC50); representative dose-response curves are shown for wild-type and mutant receptors. I/Imax is the relative current, normalized to the maximal inducible current (in μA). (d) Maximal current responses and kinetics of the open-channel blocker MK-801 for wild-type and mutant NMDA receptors show similar channel activity. The maximal agonist-inducible currents and rate kinetics of MK-801âmediated inhibition were used to determine the relative open-state probability (Po) of wild-type NR1-NR2A compared to mutant NR1âNR2A Ala243Val NMDA receptors. Data are shown as mean + s.d. (e) Inhibition of agonist-evoked currents by low concentrations of Zn2+ at wild-type and mutant NMDA receptors. Currents for NR1-NR2A, NR1-NR2AâNR2A Ala243Val and NR1âNR2A Ala243Val receptors show a gradual loss of high-affinity inhibition by 0.1 μM Zn2+ (n = 5; P < 0.01, Student's t test). Traces show currents for the NMDA receptors in the absence (black) and presence (red) of 0.1 μM Zn2+. |
|
Figure 2: Pedigrees of affected individuals with available family information. Analysis of possible segregation of the respective mutation in family members could be performed for index subject 2 and for 19 of 27 mutation carriers in cohorts II and III where DNA samples were available from family members. The respective GRIN2A mutation segregated with a variable phenotype of seizures, pathologic EEG patterns and/or intellectual disability in family members. A few individuals carried the familial mutation but did not present any clinical features, indicating incomplete penetrance of the mutations or mosaicism. However, subclinical phenotypes (for example, EEG patterns) have not been investigated in these individuals. Pedigree 87-4 suggests phenocopy in the proband's brother. WT, wild type. |
References [+] :
Bali,
Autosomal dominant inheritance of centrotemporal sharp waves in rolandic epilepsy families.
2007, Pubmed
Bali, Autosomal dominant inheritance of centrotemporal sharp waves in rolandic epilepsy families. 2007, Pubmed
Balu, Glutamate receptor composition of the post-synaptic density is altered in genetic mouse models of NMDA receptor hypo- and hyperfunction. 2011, Pubmed
Berg, Revised terminology and concepts for organization of seizures and epilepsies: report of the ILAE Commission on Classification and Terminology, 2005-2009. 2010, Pubmed
Claes, The SCN1A variant database: a novel research and diagnostic tool. 2009, Pubmed
Di Maio, Thiol oxidation and altered NR2B/NMDA receptor functions in in vitro and in vivo pilocarpine models: implications for epileptogenesis. 2013, Pubmed
Endele, Mutations in GRIN2A and GRIN2B encoding regulatory subunits of NMDA receptors cause variable neurodevelopmental phenotypes. 2010, Pubmed
Engel, A proposed diagnostic scheme for people with epileptic seizures and with epilepsy: report of the ILAE Task Force on Classification and Terminology. 2001, Pubmed
Fernández, The tower of Babel: survey on concepts and terminology in electrical status epilepticus in sleep and continuous spikes and waves during sleep in North America. 2013, Pubmed
Franke, Sequence variants in IL10, ARPC2 and multiple other loci contribute to ulcerative colitis susceptibility. 2008, Pubmed
Frasca, Misplaced NMDA receptors in epileptogenesis contribute to excitotoxicity. 2011, Pubmed
Ghasemi, The NMDA receptor complex as a therapeutic target in epilepsy: a review. 2011, Pubmed
Gobbi, The spectrum of idiopathic Rolandic epilepsy syndromes and idiopathic occipital epilepsies: from the benign to the disabling. 2006, Pubmed
Helbig, 15q13.3 microdeletions increase risk of idiopathic generalized epilepsy. 2009, Pubmed
Henson, Genetic deletion of NR3A accelerates glutamatergic synapse maturation. 2012, Pubmed
Hughes, A review of the relationships between Landau-Kleffner syndrome, electrical status epilepticus during sleep, and continuous spike-waves during sleep. 2011, Pubmed
Kingwell, Epilepsy: GRIN2A mutations identified as key genetic drivers of epilepsy-aphasia spectrum disorders. 2013, Pubmed
Lacey, Enhanced NMDA receptor-dependent thalamic excitation and network oscillations in stargazer mice. 2012, Pubmed
Lathrop, Strategies for multilocus linkage analysis in humans. 1984, Pubmed
Lemke, Targeted next generation sequencing as a diagnostic tool in epileptic disorders. 2012, Pubmed
Lesca, Epileptic encephalopathies of the Landau-Kleffner and continuous spike and waves during slow-wave sleep types: genomic dissection makes the link with autism. 2012, Pubmed
Marini, Idiopathic epilepsies with seizures precipitated by fever and SCN1A abnormalities. 2007, Pubmed
Marini, The genetics of Dravet syndrome. 2011, Pubmed
Neubauer, Centrotemporal spikes in families with rolandic epilepsy: linkage to chromosome 15q14. 1998, Pubmed
Niimura, Changes in phosphorylation of the NMDA receptor in the rat hippocampus induced by status epilepticus. 2005, Pubmed
Pal, Pleiotropic effects of the 11p13 locus on developmental verbal dyspraxia and EEG centrotemporal sharp waves. 2010, Pubmed
Paoletti, Molecular basis of NMDA receptor functional diversity. 2011, Pubmed
Reutlinger, Deletions in 16p13 including GRIN2A in patients with intellectual disability, various dysmorphic features, and seizure disorders of the rolandic region. 2010, Pubmed
Schmermund, Assessment of clinically silent atherosclerotic disease and established and novel risk factors for predicting myocardial infarction and cardiac death in healthy middle-aged subjects: rationale and design of the Heinz Nixdorf RECALL Study. Risk Factors, Evaluation of Coronary Calcium and Lifestyle. 2002, Pubmed
Stephani, Typical semiology of benign childhood epilepsy with centrotemporal spikes (BCECTS). 2000, Pubmed
Strug, Centrotemporal sharp wave EEG trait in rolandic epilepsy maps to Elongator Protein Complex 4 (ELP4). 2009, Pubmed
Vadlamudi, Analyzing the etiology of benign rolandic epilepsy: a multicenter twin collaboration. 2006, Pubmed
Wang, PennCNV: an integrated hidden Markov model designed for high-resolution copy number variation detection in whole-genome SNP genotyping data. 2007, Pubmed
Weckx, novoSNP, a novel computational tool for sequence variation discovery. 2005, Pubmed