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Peer-reviewed veterinary case report

COX-2 inhibitor added to treat drug-resistant epilepsy in dogs

By Fischer, Andrea et al.·Published in Frontiers in veterinary science·2022·Clinic of Small Animal Medicine, Germany·View original on PubMed

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Original publication title: Cyclooxygenase-2 Inhibition as an Add-On Strategy in Drug Resistant Epilepsy-A Canine Translational Study.

Species:
dog

Plain-English summary

A group of dogs with drug-resistant epilepsy, specifically those not responding to phenobarbital, were given an additional medication called firocoxib to see if it could help reduce their seizures. Out of 11 dogs that completed the study, only 2 showed a significant decrease in their seizure frequency, particularly those who had the most frequent seizures to begin with. While the treatment was generally well-tolerated, the low success rate suggests that firocoxib may not be effective for most dogs with this type of epilepsy. More research is needed to determine if this treatment could work for dogs with very high seizure rates.

People also search for: dog epilepsy treatment · firocoxib for seizures in dogs · why is my dog having seizures

Abstract

Drug-resistant epilepsy is a common complaint in dogs and affects up to 30% of dogs with idiopathic epilepsy. Experimental data suggest that targeting cyclooxygenase-2 (COX-2) mediated signaling might limit excessive excitability and prevent ictogenesis. Moreover, the role of COX-2 signaling in the seizure-associated induction of P-glycoprotein has been described. Thus, targeting this pathway may improve seizure control based on disease-modifying effects as well as enhancement of brain access and efficacy of the co-administered antiseizure medication. The present open-label non-controlled pilot study investigated the efficacy and tolerability of a COX-2 inhibitor (firocoxib) add-on therapy in a translational natural occurring chronic epilepsy animal model (client-owned dogs with phenobarbital-resistant idiopathic epilepsy). The study cohort was characterized by frequent tonic-clonic seizures and cluster seizures despite adequate phenobarbital treatment. Enrolled dogs (= 17) received a firocoxib add-on therapy for 6 months. Tonic-clonic seizure and cluster seizure frequencies were analyzed at baseline (6 months) months during the study (6 months). The responders were defined by a substantial reduction of tonic-clonic seizure and cluster seizure frequency (≥50%). In total, eleven dogs completed the study and were considered for the statistical analysis. Two dogs (18%, 2/11) were classified as responders based on their change in seizure frequency. Interestingly, those two dogs had the highest baseline seizure frequency. The overall tolerability was good. However, given the low percentage of responders, the present data do not support an overall considerable efficacy of COX-2 inhibitor add-on therapy to overcome naturally occurring phenobarbital-resistant epilepsy in dogs. Further translational evaluation should only be considered in the canine patients with a very high baseline seizure density.

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Original publication on PubMed: https://pubmed.ncbi.nlm.nih.gov/35464372/