Journal article
A Cav3.2 T-type calcium channel point mutation has splice-variant-specific effects on function and segregates with seizure expression in a polygenic rat model of absence epilepsy
KL Powell, SM Cain, C Ng, S Sirdesai, LS David, M Kyi, E Garcia, JR Tyson, CA Reid, M Bahlo, SJ Foote, TP Snutch, TJ O'Brien
Journal of Neuroscience | SOC NEUROSCIENCE | Published : 2009
Abstract
Low-voltage-activated, or T-type, calcium (Ca2+) channels are believed to play an essential role in the generation of absence seizures in the idiopathic generalized epilepsies (IGEs). We describe a homozygous, missense, single nucleotide (G to C) mutation in the Cav3.2 T-type Ca2 2+ channel gene (Cacna1h) in the genetic absence epilepsy rats from Strasbourg (GAERS) model of IGE. The GAERS Cav3.2 mutation (gcm) produces an arginine to proline (R1584P) substitution in exon 24 of Cacna1h, encoding a portion of the III-IV linker region in Cav3.2. gcm segregates codominantly with the number of seizures and time in seizure activity in progeny of an F1 intercross. We have further identified two maj..
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Grants
Awarded by National Health and Medical Research Council
Awarded by Canadian Institutes of Health Research Grant
Funding Acknowledgements
This work was supported by National Health and Medical Research Council Grants 406640 (T.J.O., S.J.F.) and 454655 (C. A. R.), the Molly McDonnell Foundation Scholarship (K. L. P.), and Canadian Institutes of Health Research Grant 10677 (T. P. S.). T. P. S. is a Tier 1 Canada Research Chair in Biotechnology and Genomics-Neurobiology.