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Deletion of a non-canonical regulatory sequence causes loss of Scn1a expression and epileptic phenotypes in mice
- Haigh, Jessica L;
- Adhikari, Anna;
- Copping, Nycole A;
- Stradleigh, Tyler;
- Wade, A Ayanna;
- Catta-Preta, Rinaldo;
- Su-Feher, Linda;
- Zdilar, Iva;
- Morse, Sarah;
- Fenton, Timothy A;
- Nguyen, Anh;
- Quintero, Diana;
- Agezew, Samrawit;
- Sramek, Michael;
- Kreun, Ellie J;
- Carter, Jasmine;
- Gompers, Andrea;
- Lambert, Jason;
- Canales, Cesar P;
- Pennacchio, Len A;
- Visel, Axel;
- Dickel, Diane E;
- Silverman, Jill L;
- Nord, Alex S
- et al.
Published Web Location
https://doi.org/10.1101/766634Abstract
Genes with multiple co-active promoters appear common in brain, yet little is known about functional requirements for these potentially redundant genomic regulatory elements. SCN1A, which encodes the Na V 1.1 sodium channel alpha subunit, is one such gene with two co-active promoters. Mutations in SCN1A are associated with epilepsy, including Dravet Syndrome (DS). The majority of DS patients harbor coding mutations causing SCN1A haploinsufficiency, however putative causal non-coding promoter mutations have been identified. To determine the functional role of one of these potentially redundant Scn1a promoters, we focused on the non-coding Scn1a 1b regulatory region, previously described as a non-canonical alternative transcriptional start site. Mice harboring a deletion of the extended evolutionarily-conserved 1b non-coding interval exhibited surprisingly severe reductions of Scn1a and Na V 1.1 expression in brain with accompanying electroencephalographic seizures and behavioral deficits. This work identified the 1b region as a critical disease-relevant regulatory element and provides evidence that non-canonical and seemingly redundant promoters can have essential function.
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