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Peer-reviewed veterinary case report

Phenobarbitone side effects in epileptic cats and how common they are

By Marsh, Oliver et al.·Published in Journal of Feline Medicine and Surgery·2020·Neurology and Neurosurgery Service, Centre for Small Animal Studies, Animal Health Trust, Newmarket, UK, United Kingdom·View original on Crossref

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Original publication title: Prevalence and clinical characteristics of phenobarbitone-associated adverse effects in epileptic cats

Species:
cat
Brain & nervesCats

Plain-English summary

A group of 77 cats with epilepsy were treated with phenobarbitone, a common medication, to control their seizures. Nearly half of these cats experienced side effects, with the most common being sedation and unsteady movements. The likelihood of these side effects increased with higher doses of phenobarbitone and when a second seizure medication was added. Most side effects appeared within the first month of treatment but were usually temporary. One cat had a rare and severe reaction that resolved after stopping the medication.

People also search for: cat epilepsy medication side effects · phenobarbitone sedation in cats · cat seizure treatment options

Abstract

Objectives The study objective was to investigate the prevalence and clinical characteristics of phenobarbitone-associated adverse effects in epileptic cats. Methods The medical records of two veterinary referral clinics from 2007 to 2017 were searched for cats fulfilling the inclusion criteria of a diagnosis of epilepsy, treatment with phenobarbitone and available follow-up information on the occurrence of adverse effects. Follow-up information was obtained from the medical records of the primary veterinarian and referral institutions and a questionnaire completed by the cats’ owners. Results Seventy-seven cats met the inclusion criteria. Fifty-eight were affected by idiopathic epilepsy and 19 by structural epilepsy. One or more of the following adverse effects were reported in 47% of the cats: sedation (89%); ataxia (53%); polyphagia (22%); polydipsia (6%); polyuria (6%); and anorexia (6%). Logistic regression analyses revealed significant associations between adverse effect occurrence and both phenobarbitone starting dosage and administration of a second antiepileptic drug (AED). For each 1 mg/kg q12h increment of phenobarbitone, the likelihood of adverse effects increased 3.1 times. When a second AED was used, the likelihood of adverse effects increased 3.2 times. No association was identified between epilepsy aetiology and adverse effect occurrence. An idiosyncratic adverse effect, characterised by severe neutropenia and granulocytic hypoplasia, was diagnosed in one cat. This resolved following phenobarbitone discontinuation. Conclusions and relevance The prevalence of phenobarbitone-associated adverse effects was 47%. Sedation and ataxia were most common. These are type A adverse effects and are predictable from phenobarbitone’s known pharmacological properties. In the majority of cases, adverse effects occurred within the first month of treatment and were transient. Idiosyncratic (type B) adverse effects, which were not anticipated given the known properties of the drug, occurred in one cat. Increased phenobarbitone starting dosage and the addition of a second AED were significantly associated with the occurrence of adverse effects.

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Original publication on Crossref: https://doi.org/10.1177/1098612x20924925