Behavioral phenotyping of young Scn1a haploinsufficient mice

Behavioral phenotyping of young Scn1a haploinsufficient mice

•Scn1a-A1783V haploinsufficient mice display age-dependent phenotypic alterations.•The course of behavioral patterns confirmed the overall face validity of the model.•Validated composite measure scheme confirmed for severity assessment in young mice. Dravet syndrome is a rare, severe, infancy-onset...

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Bibliographic Details
Published in:Epilepsy & behavior Vol. 136; p. 108903
Main Authors: Reiber, Maria, Miljanovic, Nina, Schönhoff, Katharina, Palme, Rupert, Potschka, Heidrun
Format: Journal Article
Language:English
Published: United States Elsevier Inc 01-11-2022
Subjects:
Adolescence
Adolescent
Animals
Disease Models, Animal
Dravet syndrome
Epilepsies, Myoclonic
Epilepsy
Genetic mouse model
Humans
Mice
Mutation
Mutation, Missense
NAV1.1 Voltage-Gated Sodium Channel - genetics
Severity assessment
Genetic mouse model
Adolescence
Severity assessment
Epilepsy
Dravet syndrome
3R
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Summary:•Scn1a-A1783V haploinsufficient mice display age-dependent phenotypic alterations.•The course of behavioral patterns confirmed the overall face validity of the model.•Validated composite measure scheme confirmed for severity assessment in young mice. Dravet syndrome is a rare, severe, infancy-onset epileptic encephalopathy associated with a high premature mortality. In most patients, Dravet syndrome is caused by a heterozygous loss-of-function mutation in the SCN1A gene encoding the alpha 1 subunit of the sodium channel. Of the variety of SCN1A variants identified in patients with Dravet syndrome, SCN1A missense mutations occur in one-third of cases. The novel Scn1a-A1783V mouse model of Dravet syndrome carries the human Ala1783Val missense variant. Recently, the behavioral phenotype of Scn1a-A1783V haploinsufficient adult mice has been characterized, which may provide a valuable basis for assessment of novel therapeutic approaches. However, there is still limited information on the developmental course of behavioral alterations in the Scn1a-A1783V mouse model, which is of particular relevance for conclusions about face validity and severity classification of the model. Based on reference data from young wildtype mice, we analyzed selected behavioral parameters and fecal corticosterone metabolites in the Scn1a-A1783V mouse model during post-weaning development. Differences in the preference for a sweet saccharin solution between Dravet mice and wildtype mice were observed once mice reached sexual maturity. Nest building behavior was already influenced by the Scn1a genotype during prepubescence. Sexually mature Dravet mice showed a significantly reduced burrowing performance as compared to their wildtype littermates. In the open-field test, pronounced hyperactivity and increased thigmotactic behavior were evident in prepubescent and sexually mature Dravet mice. Analysis of Irwin scores revealed several genotype-dependent changes in handling-associated parameters during the course of adolescence. The information obtained provides insight into the age-dependence of behavioral patterns in the novel Scn1a-A1783V mouse model of Dravet syndrome. In addition, the dataset confirms the suitability of the applied behavioral composite measure scheme for evidence-based assessment of cumulative severity in genetic mouse lines.
ISSN:1525-5050
1525-5069
DOI:10.1016/j.yebeh.2022.108903