Cacna1g is a genetic modifier of epilepsy caused by mutation of voltage‐gated sodium channel Scn2a

Summary More than 1,200 mutations in neuronal voltage‐gated sodium channel (VGSC) genes have been identified in patients with several epilepsy syndromes. A common feature of genetic epilepsies is variable expressivity among individuals with the same mutation. The Scn2aQ54 transgenic mouse model has...

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Bibliographic Details
Published inEpilepsia (Copenhagen) Vol. 57; no. 6; pp. e103 - e107
Main Authors Calhoun, Jeffrey D., Hawkins, Nicole A., Zachwieja, Nicole J., Kearney, Jennifer A.
Format Journal Article
LanguageEnglish
Published United States Wiley Subscription Services, Inc 01.06.2016
Subjects
Animals
Calcium Channels, T-Type - genetics
Calcium Channels, T-Type - metabolism
Disease Models, Animal
Epilepsy
Epilepsy - genetics
Epilepsy - physiopathology
Gene Expression Regulation - genetics
Genetics
Genotype
Humans
Mice
Mice, Inbred C57BL
Mice, Transgenic
Mouse model
Mutation
Mutation - genetics
NAV1.2 Voltage-Gated Sodium Channel - genetics
Phenotype
Rodents
Seizures
Voltage‐gated calcium channels
Voltage‐gated ion channels
Genetics
Voltage-gated calcium channels
Mouse model
Voltage-gated ion channels
Seizures
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Summary:Summary More than 1,200 mutations in neuronal voltage‐gated sodium channel (VGSC) genes have been identified in patients with several epilepsy syndromes. A common feature of genetic epilepsies is variable expressivity among individuals with the same mutation. The Scn2aQ54 transgenic mouse model has a mutation in Scn2a that results in spontaneous epilepsy. Scn2aQ54 phenotype severity varies depending on the genetic strain background, making it a useful model for identifying and characterizing epilepsy modifier genes. Scn2aQ54 mice on the [C57BL/6JxSJL/J]F1 background exhibit earlier seizure onset, elevated spontaneous seizure frequency, and decreased survival compared to Scn2aQ54 mice congenic on the C57BL/6J strain. Genetic mapping and RNA‐Seq analysis identified Cacna1g as a candidate modifier gene at the Moe1 locus, which influences Scn2aQ54 phenotype severity. In this study, we evaluated the modifier potential of Cacna1g, encoding the Cav3.1 voltage‐gated calcium channel, by testing whether transgenic alteration of Cacna1g expression modifies severity of the Scn2aQ54 seizure phenotype. Scn2aQ54 mice exhibited increased spontaneous seizure frequency with elevated Cacna1g expression and decreased seizure frequency with decreased Cacna1g expression. These results provide support for Cacna1g as an epilepsy modifier gene and suggest that modulation of Cav3.1 may be an effective therapeutic strategy.
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ISSN:0013-9580
1528-1167
DOI:10.1111/epi.13390