Suggestive evidence for a new locus for epilepsy with heterogeneous phenotypes on chromosome 17q
Autor: | Matti Koivikko, Reijo Laaksonen, Maria Kousi, Lyne Chahine, Malgorzata Labuda, Massimo Pandolfo, Asta Laiho, Kalle O.J. Simola, Auli Siren, Anne Polvi, Juhani T. Soini, Anna-Elina Lehesjoki, Eva Andermann, Anna-Kaisa Anttonen, Sarah Bourgoin, Kari Hirvonen |
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Rok vydání: | 2010 |
Předmět: |
Adult
Male Candidate gene Adolescent Genotype DNA Mutational Analysis Locus (genetics) Biology Ion Channels Childhood absence epilepsy Genetic linkage Febrile seizure medicine Humans Copy-number variation Child Aged Oligonucleotide Array Sequence Analysis Family Health Genetics Epilepsy Gene Expression Profiling Chromosome Mapping Middle Aged medicine.disease Penetrance Phenotype Neurology Child Preschool Mutation Female Neurology (clinical) Lod Score Chromosomes Human Pair 17 Comparative genomic hybridization |
Zdroj: | Epilepsy Research. 88:65-75 |
ISSN: | 0920-1211 |
DOI: | 10.1016/j.eplepsyres.2009.09.022 |
Popis: | Summary Purpose To characterize the clinical features and molecular genetic background in a family with various epilepsy phenotypes including febrile seizures, childhood absence epilepsy, and possible temporal lobe epilepsy. Methods Clinical data were collected. DNA and RNA were extracted from peripheral blood. A genome-wide microsatellite marker scan was performed and regions with a multipoint location score ≥1.5 were fine mapped. Functional candidate genes identified from databases and by comparing gene expression profiles of genes between affected and unaffected individuals were sequenced. Copy number variation was evaluated with array-based comparative genomic hybridization. Results The seizure phenotype was benign. Inheritance was consistent with an autosomal dominant model and reduced penetrance. The highest two-point LOD score of 2.8 was identified at marker D17S1606 in a 37cM interval on chromosome 17q12-q24. Loci on 5q11.2 and on 18p11-q11, showed LOD scores ≥1.5 after fine mapping. Sequencing of nine ion-channel genes and two ( RPIP8 and SLC25A39 ) differentially expressed genes from 17q12-q24, as well as IMPA2 from 18p11-q11 did not reveal a pathogenic alteration. No clinically relevant copy number variation was identified. Conclusions Our findings suggest complex inheritance of seizure susceptibility in the family with contribution from three loci, including a possible new locus on chromosome 17q. The underlying molecular defects remain unknown. |
Databáze: | OpenAIRE |
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