Mapping of a FEB3 homologous febrile seizure locus on mouse chromosome 2 containing candidate genes Scn1a and Scn3a

Publication date

2016-12

Authors

Hessel, Ellen V S
van Lith, Hein A
Wolterink-Donselaar, I. G.
de Wit, Marina
Groot Koerkamp, Marian J A
Holstege, Frank C PISNI 000000014099129X
Kas, Martien JISNI 000000039367038X
Fernandes, Cathy
de Graan, Pierre N EISNI 0000000391979201

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Advisors

Supervisors

Document Type

Article

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License

taverne

Abstract

Febrile seizures (FS) are the most common seizure type in children. Recurrent FS are a risk factor for developing temporal lobe epilepsy later in life and are known to have a strong genetic component. Experimental FS (eFS) can be elicited in mice by warm-air induced hyperthermia. We used this model to screen the chromosome substitution strain (CSS) panel derived from C57BL/6J and A/J for FS susceptibility and identified C57BL/6J-Chr2(A) /NaJ (CSS2), as the strain with the strongest FS susceptibility phenotype. The aim of this study was to map FS susceptibility loci and select candidate genes on mouse chromosome 2. We generated an F2 population by intercrossing the hybrids (F1) that were derived from CSS2 and C57BL/6J mice. All CSS2-F2 individuals were genotyped and phenotyped for eFS susceptibility, and QTL analysis was performed. Candidate gene selection was based on bioinformatics analyses and differential brain expression between CSS2 and C57BL/6J strains determined by microarray analysis. Genetic mapping of the eFS susceptibility trait identified two significant loci: FS-QTL2a (LOD-score 3.6) and FS-QTL2b (LOD-score 6.2). FS-QTL2a contained 44 genes expressed in the brain at post natal day 14. Four of these (Arl6ip6, Cytip, Fmnl2 Ifih1) contained a non-synonymous SNP comparing CSS2 and C57BL/6J, six genes (March7, Nr4a2, Gpd2, Grb14, Scn1a, Scn3a) were differentially expressed between these strains. A region within FS-QTL2a is homologous to the human FEB3 locus. The fact that we identify mouse FS-QTL2a with high FEB3 homology is strong support for the validity of the eFS mouse model to study genetics of human FS. 

Keywords

chromosome substitution strain, hyperthermia, quantitatve trait loci, temporal lobe epilepsy, Taverne, Journal Article

Citation

Hessel, E V S, van Lith, H A, Wolterink-Donselaar, I G, de Wit, M, Groot Koerkamp, M J A, Holstege, F C P, Kas, M J H, Fernandes, C & de Graan, P N E 2016, 'Mapping of a FEB3 homologous febrile seizure locus on mouse chromosome 2 containing candidate genes Scn1a and Scn3a', European Journal of Neuroscience, vol. 44, no. 11, pp. 2950–2957 . https://doi.org/10.1111/ejn.13420