Peer-reviewed veterinary case report
Collie with MDR1 mutation had severe reaction to butorphanol
By Tyler S. Nelson et al.·Published in Frontiers in Veterinary Science·2025·Department of Pharmacology and Therapeutics, Center for Advanced Pain Therapeutics and Research (CaPToR), McKnight Brain Institute, College of Medicine, University of Florida, Gainesville, FL, United States, CH·View original on DOAJ →
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Original publication title: Case Report: Adverse reaction to butorphanol in a Collie homozygous for the ABCB1-1∆ (MDR1) mutation
- Species:
- dog
Plain-English summary
A 5-year-old male Collie with a genetic mutation (ABCB1-1∆) that makes him sensitive to certain medications developed severe side effects after receiving a pain medication called butorphanol. He showed signs of sedation, unsteady movements, excessive drooling, and even seizures. Despite receiving supportive care, his symptoms lasted for about 40 hours, requiring continuous treatment with naloxone to help him recover. This case highlights the importance of genetic testing for drug sensitivities in certain dog breeds to prevent such dangerous reactions in the future.
People also search for: Collie drug sensitivity · butorphanol side effects in dogs · seizure treatment for dogs · ABCB1-1∆ mutation in dogs
Abstract
Certain dog breeds, particularly herding breeds like Collies, are predisposed to drug sensitivity due to the ABCB1-1∆ (previously known as MDR1) mutation, which disrupts P-glycoprotein (P-gp) function. This mutation impairs drug efflux at the blood–brain barrier, leading to increased susceptibility to neurotoxic effects. While adverse reactions to P-gp substrate drugs such as macrocyclic lactones and chemotherapeutics are well documented, opioid sensitivity remains poorly understood. This case report documents a Collie that developed severe neurotoxicity, including profound sedation, ataxia, hypersalivation, and seizures, following a single 0.2 mg/kg dose of butorphanol. Symptoms persisted despite supportive care, requiring continuous naloxone administration for approximately 40 h before significant improvement. Neurotoxicological effects may have been exacerbated by metoclopramide and maropitant, known P-gp substrates. This case underscores the need for further research into opioid pharmacokinetics in ABCB1-1∆ mutant dogs and highlights the importance of genetic screening in veterinary practice. To enhance patient safety, integration of automated alerts within electronic medical record systems is recommended to flag high-risk drugs for at-risk breeds, providing real-time warnings, dosing adjustments, and monitoring guidance. These measures could reduce adverse drug reactions and improve clinical outcomes in genetically susceptible dogs.
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Search related cases →Original publication on DOAJ: https://doi.org/10.3389/fvets.2025.1603375