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Publication : Mutations in the Cacnl1a4 calcium channel gene are associated with seizures, cerebellar degeneration, and ataxia in tottering and leaner mutant mice.

First Author  Doyle J Year  1997
Journal  Mamm Genome Volume  8
Issue  2 Pages  113-20
PubMed ID  9060410 Mgi Jnum  J:38910
Mgi Id  MGI:86296 Doi  10.1007/s003359900369
Citation  Doyle J, et al. (1997) Mutations in the Cacnl1a4 calcium channel gene are associated with seizures, cerebellar degeneration, and ataxia in tottering and leaner mutant mice. Mamm Genome 8(2):113-20
abstractText  Tottering and leaner, two mutations of the mouse tottering locus, have been studied extensively as models for human epilepsy, Here we describe the isolation, mapping, and expression analysis of Cacnl1a4, a gene encoding the alpha subunit of a proposed P-type calcium channel, and also report the physical mapping and expression patterns of the orthologous human gene. DNA sequencing and gene expression data demonstrate that Cacnl1a4 mutations are the primary cause of seizures and ataxia in tottering and leaner mutant mice, and suggest that tottering locus mutations and human diseases, episodic ataxia 2 and familial hemiplegic migraine, represent mutations in mouse and human versions of the same channel-encoding gene.
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