NDUFS7 variant in dogs with Leigh syndrome and its functional validation in a Drosophila melanogaster model.
Matthias ChristenAnne GregorRodrigo Gutierrez QuintanaJos Jacqueline BongersAngie RuppJacques PenderisG Diane SheltonVidhya JagannathanChristiane ZweierTosso LeebPublished in: Scientific reports (2024)
Two Jack-Russell Terrier × Chihuahua mixed-breed littermates with Leigh syndrome were investigated. The dogs presented with progressive ataxia, dystonia, and increased lactate levels. Brain MRI showed characteristic bilateral symmetrical T2 hyperintense lesions, histologically representing encephalomalacia. Muscle histopathology revealed accumulation of mitochondria. Whole genome sequencing identified a missense variant in a gene associated with human Leigh syndrome, NDUFS7:c.535G > A or p.(Val179Met). The genotypes at the variant co-segregated with the phenotype in the investigated litter as expected for a monogenic autosomal recessive mode of inheritance. We investigated the functional consequences of the missense variant in a Drosophila melanogaster model by expressing recombinant wildtype or mutant canine NDUFS7 in a ubiquitous knockdown model of the fly ortholog ND-20. Neither of the investigated overexpression lines completely rescued the lethality upon knockdown of the endogenous ND-20. However, a partial rescue was found upon overexpression of wildtype NDUFS7, where pupal lethality was moved to later developmental stages, which was not seen upon canine mutant overexpression, thus providing additional evidence for the pathogenicity of the identified variant. Our results show the potential of the fruit fly as a model for canine disease allele validation and establish NDUFS7:p.(Val179Met) as causative variant for the investigated canine Leigh syndrome.
Keyphrases
- drosophila melanogaster
- case report
- atomic force microscopy
- intellectual disability
- endothelial cells
- transcription factor
- multiple sclerosis
- early onset
- skeletal muscle
- computed tomography
- magnetic resonance imaging
- tyrosine kinase
- mitochondrial dna
- autism spectrum disorder
- contrast enhanced
- escherichia coli
- cell death
- magnetic resonance
- copy number
- deep brain stimulation
- gene expression
- subarachnoid hemorrhage
- functional connectivity
- risk assessment
- climate change
- high resolution
- cerebral ischemia
- induced pluripotent stem cells
- reactive oxygen species
- duchenne muscular dystrophy
- human health