Medicine (Austin & Northern Health) - Research Publications

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Author: Scheffer, Ingrid × Author: MCMAHON, JACINTA × Start date: 2013 × End date: 2013 ×

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    Mutations in TNK2 in Severe Autosomal Recessive Infantile Onset Epilepsy
    Hitomi, Y ; Heinzen, EL ; Donatello, S ; Dahl, H-H ; Damiano, JA ; McMahon, JM ; Berkovic, SF ; Scheffer, IE ; Legros, B ; Rai, M ; Weckhuysen, S ; Suls, A ; De Jonghe, P ; Pandolfo, M ; Goldstein, DB ; Van Bogaert, P ; Depondt, C (WILEY, 2013-09)
    We identified a small family with autosomal recessive, infantile onset epilepsy and intellectual disability. Exome sequencing identified a homozygous missense variant in the gene TNK2, encoding a brain-expressed tyrosine kinase. Sequencing of the coding region of TNK2 in 110 patients with a similar phenotype failed to detect further homozygote or compound heterozygote mutations. Pathogenicity of the variant is supported by the results of our functional studies, which demonstrated that the variant abolishes NEDD4 binding to TNK2, preventing its degradation after epidermal growth factor stimulation. Definitive proof of pathogenicity will require confirmation in unrelated patients.
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    Targeted resequencing in epileptic encephalopathies identifies de novo mutations in CHD2 and SYNGAP1
    Carvill, GL ; Heavin, SB ; Yendle, SC ; McMahon, JM ; O'Roak, BJ ; Cook, J ; Khan, A ; Dorschner, MO ; Weaver, M ; Calvert, S ; Malone, S ; Wallace, G ; Stanley, T ; Bye, AME ; Bleasel, A ; Howell, KB ; Kivity, S ; Mackay, MT ; Rodriguez-Casero, V ; Webster, R ; Korczyn, A ; Afawi, Z ; Zelnick, N ; Lerman-Sagie, T ; Lev, D ; Moller, RS ; Gill, D ; Andrade, DM ; Freeman, JL ; Sadleir, LG ; Shendure, J ; Berkovic, SF ; Scheffer, IE ; Mefford, HC (NATURE PUBLISHING GROUP, 2013-07)
    Epileptic encephalopathies are a devastating group of epilepsies with poor prognosis, of which the majority are of unknown etiology. We perform targeted massively parallel resequencing of 19 known and 46 candidate genes for epileptic encephalopathy in 500 affected individuals (cases) to identify new genes involved and to investigate the phenotypic spectrum associated with mutations in known genes. Overall, we identified pathogenic mutations in 10% of our cohort. Six of the 46 candidate genes had 1 or more pathogenic variants, collectively accounting for 3% of our cohort. We show that de novo CHD2 and SYNGAP1 mutations are new causes of epileptic encephalopathies, accounting for 1.2% and 1% of cases, respectively. We also expand the phenotypic spectra explained by SCN1A, SCN2A and SCN8A mutations. To our knowledge, this is the largest cohort of cases with epileptic encephalopathies to undergo targeted resequencing. Implementation of this rapid and efficient method will change diagnosis and understanding of the molecular etiologies of these disorders.
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    Mutations in PRRT2 are not a common cause of infantile epileptic encephalopathies
    Heron, SE ; Ong, YS ; Yendle, SC ; McMahon, JM ; Berkovic, SF ; Scheffer, IE ; Dibbens, LM (WILEY, 2013-05)
    Heterozygous mutations in PRRT2 have recently been identified as the major cause of autosomal dominant benign familial infantile epilepsy (BFIE), infantile convulsions with choreoathetosis syndrome (ICCA), and paroxysmal kinesigenic dyskinesia (PKD). Homozygous mutations in PRRT2 have also been reported in two families with intellectual disability (ID) and seizures. Heterozygous mutations in the genes KCNQ2 and SCN2A cause the two other autosomal dominant seizure disorders of infancy: benign familial neonatal epilepsy and benign familial neonatal-infantile epilepsy. Mutations in KCNQ2 and SCN2A also contribute to severe infantile epileptic encephalopathies (IEEs) in which seizures and intellectual disability co-occur. We therefore hypothesized that PRRT2 mutations may also underlie cases of IEE. We examined PRRT2 for heterozygous, compound heterozygous or homozygous mutations to determine their frequency in causing epileptic encephalopathies (EEs). Two hundred twenty patients with EEs with onset by 2 years were phenotyped. An assay for the common PRRT2 c.649-650insC mutation and high resolution-melt analysis for mutations in the remaining exons of PRRT2 were performed. Neither the common mutation nor any other pathogenic variants in PRRT2 were detected in the 220 patients. Our findings suggest that mutations in PRRT2 are not a common cause of IEEs.