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Peer-reviewed veterinary case report

Hereditary ataxia causes gait problems and seizures in Jack Russell

By Wessmann, Annette et al.·Published in Journal of veterinary internal medicine·2004·Queen Mother Hospital for Animals, United Kingdom·View original on PubMed

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Original publication title: Hereditary ataxia in the Jack Russell Terrier--clinical and genetic investigations.

Species:
dog

Plain-English summary

A Jack Russell Terrier with hereditary ataxia showed symptoms like difficulty walking and uncoordinated movements starting as early as 2 to 9 months old. Some affected dogs also experienced seizures and breathing problems. Researchers studied 35 dogs and found that the condition is likely inherited through multiple genes rather than a single one. While there is no cure, understanding the genetic basis can help owners be aware of the risks and manage their pet's condition.

People also search for: Jack Russell Terrier ataxia symptoms · dog seizures treatment · hereditary ataxia in dogs · Jack Russell breathing problems · dog gait disturbance causes

Abstract

Hereditary ataxia in the Jack Russell Terrier (JRT) is characterized by a gait disturbance with symmetric generalized ataxia and hypermetric and spastic movements. Histopathology shows a disease of the entire central nervous system, predominantly an axonopathy. In the present study, 35 clinically affected dogs were examined. Gait abnormalities began at 2-9 months of age. Generalized seizures occurred in 13 dogs in addition to the ataxia, and 7 dogs developed respiratory distress. Brain stem auditory-evoked potentials (BAEPs) were abnormal in 4 of 8 examined dogs, in which only waves I and II were detected. Abnormal BAEPs suggest the possibility of hereditary ataxia in the JRT. Investigations regarding the mode of inheritance were performed by complex segregation analyses on 3 pedigrees with a total of 115 JRTs (27 clinically affected dogs and 88 unaffected littermates and ancestors). Different modes of inheritance were tested, including monogenic, mixed, and polygenic models, as well as a model with environmental effects only. Models with genetic effects explained the data significantly better than the environmental model. The monogenic model had to be rejected in this study because of an insufficient match of data when compared to that of the most general model. The polygenic and mixed major gene models explained the pedigree data best and therefore have to be regarded as possible hypotheses for the mode of inheritance of hereditary ataxia in the JRT. The polygenic model proved best suited to explain the segregation pattern in the JRT, because it had the fewest number of parameters.

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Original publication on PubMed: https://pubmed.ncbi.nlm.nih.gov/15320590/