Phenotypic analysis of catastrophic childhood epilepsy genes.
Aliesha GriffinColleen CarpenterJing LiuRosalia PaternoBrian GroneKyla HamlingMaia MoogMatthew T DindayFrancisco FigueroaMana AnvarChinwendu OnonujuTony QuScott C BarabanPublished in: Communications biology (2021)
Genetic engineering techniques have contributed to the now widespread use of zebrafish to investigate gene function, but zebrafish-based human disease studies, and particularly for neurological disorders, are limited. Here we used CRISPR-Cas9 to generate 40 single-gene mutant zebrafish lines representing catastrophic childhood epilepsies. We evaluated larval phenotypes using electrophysiological, behavioral, neuro-anatomical, survival and pharmacological assays. Local field potential recordings (LFP) were used to screen ∼3300 larvae. Phenotypes with unprovoked electrographic seizure activity (i.e., epilepsy) were identified in zebrafish lines for 8 genes; ARX, EEF1A, GABRB3, GRIN1, PNPO, SCN1A, STRADA and STXBP1. We also created an open-source database containing sequencing information, survival curves, behavioral profiles and representative electrophysiology data. We offer all zebrafish lines as a resource to the neuroscience community and envision them as a starting point for further functional analysis and/or identification of new therapies.
Keyphrases
- genome wide
- crispr cas
- genome wide identification
- copy number
- high throughput
- bioinformatics analysis
- endothelial cells
- dna methylation
- venous thromboembolism
- healthcare
- genome editing
- genome wide analysis
- free survival
- machine learning
- single cell
- early life
- health information
- temporal lobe epilepsy
- drosophila melanogaster
- electronic health record
- drug induced
- case control
- human health