Haplotype and linkage disequilibrium analysis to characterise a region in the calcium channel gene CACNA1A associated with idiopathic generalised epilepsy

Chioza, Barry and Osei-Lah, Abena and Nashef, Lina and Suarez-Merino, Blanca and Wilkie, Hazel and Sham, Pak and Knight, Jo and Asherson, Philip and Makoff, Andrew J (2002) Haplotype and linkage disequilibrium analysis to characterise a region in the calcium channel gene CACNA1A associated with idiopathic generalised epilepsy. European Journal of Human Genetics, 10 (12). pp. 857-864. ISSN 1018-4813

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Abstract

Idiopathic generalised epilepsy (IGE) is a common form of epilepsy, including several defined and overlapping syndromes, and likely to be due to the combined actions of mutations in several genes. In a recent study we investigated the calcium channel gene CACNA1A for involvement in IGE, unselected for syndrome, by means of association studies using several polymorphisms within the gene. We reported a highly significant case/control association with a silent single nucleotide polymorphism (SNP) in exon 8 that we confirmed by within-family analyses. In this present study we screened the gene for novel SNPs within 25 kb of exon 8, which have enabled us to define the critical region of CACNA1A in predisposing to IGE. Several intronic SNPs were identified and three, within 1.5 kb of exon 8 and in strong linkage disequilibrium with each other and with the original SNP, were significantly associated with IGE (P=0.00029, P=0.0015 and P=0.010). The associations were not limited to an IGE syndrome or other subgroup. Another SNP, 25 kb away, in intron 6 was also significantly associated with IGE (P=0.0057) but is not in linkage disequilibrium with the SNPs around exon 8. Haplotype predictions revealed even more significant associations (3-marker haplotype: P<10(-6)). Logistic regression showed that all the data can be explained by two of the SNPs, which is consistent with two functionally significant variants being responsible for all five associations, although a single variant cannot be excluded. The functionally significant variant(s) are unlikely to be exonic and suggests an effect on expression or alternative splicing.

Item Type:
Journal Article
Journal or Publication Title:
European Journal of Human Genetics
Uncontrolled Keywords:
/dk/atira/pure/subjectarea/asjc/2700/2716
Subjects:
?? ADOLESCENTADULTBASE SEQUENCECALCIUM CHANNELSCHILDCHILD, PRESCHOOLCHROMATOGRAPHY, HIGH PRESSURE LIQUIDDNA MUTATIONAL ANALYSISEPILEPSY, GENERALIZEDFEMALEGENE FREQUENCYHAPLOTYPESHUMANSLINKAGE DISEQUILIBRIUMMALEMIDDLE AGEDMOLECULAR SEQUENCE DATAGENETICSGENETI ??
ID Code:
79923
Deposited By:
Deposited On:
07 Jun 2016 09:26
Refereed?:
Yes
Published?:
Published
Last Modified:
21 Sep 2023 02:03