Humanization of Drosophila Gαo to Model GNAO1 Paediatric Encephalopathies.
Mikhail SavitskyGonzalo P SolisMikhail KryuchkovVladimir L KatanaevPublished in: Biomedicines (2020)
Several hundred genes have been identified to contribute to epilepsy-the disease affecting 65 million people worldwide. One of these genes is GNAO1 encoding Gαo, the major neuronal α-subunit of heterotrimeric G proteins. An avalanche of dominant de novo mutations in GNAO1 have been recently described in paediatric epileptic patients, suffering, in addition to epilepsy, from motor dysfunction and developmental delay. Although occurring in amino acids conserved from humans to Drosophila, these mutations and their functional consequences have only been poorly analysed at the biochemical or neuronal levels. Adequate animal models to study the molecular aetiology of GNAO1 encephalopathies have also so far been lacking. As the first step towards modeling the disease in Drosophila, we here describe the humanization of the Gαo locus in the fruit fly. A two-step CRISPR/Cas9-mediated replacement was conducted, first substituting the coding exons 2-3 of Gαo with respective human GNAO1 sequences. At the next step, the remaining exons 4-7 were similarly replaced, keeping intact the gene Cyp49a1 embedded in between, as well as the non-coding exons, exon 1 and the surrounding regulatory sequences. The resulting flies, homozygous for the humanized GNAO1 loci, are viable and fertile without any visible phenotypes; their body weight, locomotion, and longevity are also normal. Human Gαo-specific antibodies confirm the endogenous-level expression of the humanized Gαo, which fully replaces the Drosophila functions. The genetic model we established will make it easy to incorporate encephalopathic GNAO1 mutations and will permit intensive investigations into the molecular aetiology of the human disease through the powerful toolkit of Drosophila genetics.
Keyphrases
- endothelial cells
- genome wide
- crispr cas
- body weight
- induced pluripotent stem cells
- intensive care unit
- emergency department
- pluripotent stem cells
- end stage renal disease
- newly diagnosed
- oxidative stress
- poor prognosis
- peritoneal dialysis
- drosophila melanogaster
- gene expression
- copy number
- amino acid
- ejection fraction
- patient reported outcomes
- brain injury
- binding protein