Peer-reviewed veterinary case report
Lafora disease causing seizures in miniature Wirehaired Dachshunds
By Swain, Lindsay et al.·Published in PloS one·2017·Fitzpatrick Referrals Orthopedics and Neurology, United Kingdom·View original on PubMed →
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Original publication title: Lafora disease in miniature Wirehaired Dachshunds.
- Species:
- dog
Plain-English summary
A 7-year-old miniature Wirehaired Dachshund was diagnosed with Lafora disease, a genetic condition that causes myoclonic seizures (sudden muscle jerks) and other neurological symptoms. The dog initially showed signs of reflex myoclonus, which is when the muscles twitch in response to stimuli, and later developed other issues like generalized seizures, impaired vision, and even aggression. Unfortunately, the condition worsened over time, leading to more severe symptoms that were harder to manage. While there is no cure, understanding the disease better could help in developing more effective treatments in the future.
People also search for: Dachshund myoclonic seizures · Lafora disease in dogs · dog neurological symptoms treatment
Abstract
Lafora disease (LD) is an autosomal recessive late onset, progressive myoclonic epilepsy with a high prevalence in the miniature Wirehaired Dachshund. The disease is due to a mutation in the Epm2b gene which results in intracellular accumulation of abnormal glycogen (Lafora bodies). Recent breed-wide testing suggests that the carrier plus affected rate may be as high as 20%. A characteristic feature of the disease is spontaneous and reflex myoclonus; however clinical signs and disease progression are not well described. A survey was submitted to owners of MWHD which were homozygous for Epm2b mutation (breed club testing program) or had late onset reflex myoclonus and clinical diagnosis of LD. There were 27 dogs (11 male; 16 female) for analysis after young mutation-positive dogs that had yet to develop disease were excluded. Average age of onset of clinical signs was 6.94 years (3.5-12). The most common initial presenting sign was reflex and spontaneous myoclonus (77.8%). Other presenting signs included hypnic myoclonus (51.9%) and generalized seizures (40.7%). Less common presenting signs include focal seizures, "jaw smacking", "fly catching", "panic attacks", impaired vision, aggression and urinary incontinence. All these clinical signs may appear, and then increase in frequency and intensity over time. The myoclonus in particular becomes more severe and more refractory to treatment. Signs that developed later in the disease include dementia (51.9%), blindness (48.1%), aggression to people (25.9%) and dogs (33.3%), deafness (29.6%) and fecal (29.6%) and urinary (37.0%) incontinence as a result of loss of house training (disinhibited type behavior). Further prospective study is needed to further characterize the canine disease and to allow more specific therapeutic strategies and to tailor therapy as the disease progresses.
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Search related cases →Original publication on PubMed: https://pubmed.ncbi.nlm.nih.gov/28767715/