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Peer-reviewed veterinary case report

Bullmastiffs with brain disease linked to mitochondrial gene variant

By Christen, Matthias et al.·Published in Animal genetics·2022·Institute of Genetics·View original on PubMed

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Original publication title: Mitochondrial fission factor (MFF) frameshift variant in Bullmastiffs with mitochondrial fission encephalopathy.

Species:
dog
Brain & nervesDogs

Plain-English summary

Two young Bullmastiffs, around 6 months old, were brought in for problems with their balance and behavior. They showed signs of a brain disorder, and MRI scans revealed specific lesions in their brains. Genetic testing identified a harmful mutation in the MFF gene, which is linked to a similar condition in humans called mitochondrial fission encephalopathy. This mutation appears to be the cause of the neurological issues in these dogs. Unfortunately, there is no cure, but understanding the genetic basis can help in managing the condition and advising owners.

People also search for: Bullmastiff neurological problems · dog balance issues · mitochondrial fission encephalopathy in dogs · genetic testing for dogs · Bullmastiff behavior changes

Abstract

Familial cerebellar ataxia with hydrocephalus in Bullmastiffs was described almost 40 years ago as a monogenic autosomal recessive trait. We investigated two young Bullmastiffs showing similar clinical signs. They developed progressive gait and behavioural abnormalities with an onset at around 6 months of age. Neurological assessment was consistent with a multifocal brain disease. Magnetic resonance imaging of the brain showed intra-axial bilateral symmetrical focal lesions localised to the cerebellar nuclei. Based on the juvenile age, nature of neurological deficits and imaging findings, an inherited disorder of the brain was suspected. We sequenced the genome of one affected Bullmastiff. The data were compared with 782 control genomes of dogs from diverse breeds. This search revealed a private homozygous frameshift variant in the MFF gene in the affected dog, XM_038574000.1:c.471_475delinsCGCTCT, that is predicted to truncate 55% of the wild type MFF open reading frame, XP_038429928.1: p.(Glu158Alafs*14). Human patients with pathogenic MFF variants suffer from 'encephalopathy due to defective mitochondrial and peroxisomal fission 2'. Archived samples from two additional affected Bullmastiffs related to the originally described cases were obtained. Genotypes in a cohort of four affected and 70 unaffected Bullmastiffs showed perfect segregation with the disease phenotype. The available data together with information from previous disease reports allow classification of the investigated MFF frameshift variant as pathogenic and probably causative defect of the observed neurological phenotype. In analogy to the human phenotype, we propose to rename this disease 'mitochondrial fission encephalopathy (MFE)'.

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Original publication on PubMed: https://pubmed.ncbi.nlm.nih.gov/36085405/