Peer-reviewed veterinary case report
New COX-2 inhibitor reduces joint inflammation in dogs with synovitis
By McCann, Margaret E et al.·Published in American journal of veterinary research·2004·Departments of Animal Health Research, United States·View original on PubMed →
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Original publication title: In vitro effects and in vivo efficacy of a novel cyclooxygenase-2 inhibitor in dogs with experimentally induced synovitis.
- Species:
- dog
Plain-English summary
A group of healthy mixed-breed and Beagle dogs were given a new medication called ML-1,785,713 to see if it could help with lameness caused by urate crystal-induced synovitis (inflammation in the joints). The medication was effective whether given before or after the onset of symptoms, reducing pain and improving movement. This new drug is highly selective for targeting the COX-2 enzyme, which may make it safer than traditional anti-inflammatory medications that affect both COX-1 and COX-2. Overall, ML-1,785,713 showed promise as a treatment option for dogs with joint inflammation.
People also search for: dog joint pain treatment · Beagle lameness medication · new anti-inflammatory for dogs · urate crystal synovitis in dogs
Abstract
OBJECTIVE: To determine cyclooxygenase-2 (COX-2) selectivity, pharmacokinetic properties, and in vivo efficacy of ML-1,785,713 in dogs. ANIMALS: 21 healthy male and female mixed-breed dogs and 24 healthy male Beagles. PROCEDURE: Selectivity of ML-1,785,713 for inhibiting COX-2 was determined by comparing the potency for inhibiting cyclooxygenase-1 (COX-1) with that of COX-2 in canine blood. Pharmacokinetic properties were determined after i.v. (2 mg/kg) and oral (8 mg/kg) administration in female mixed-breed dogs. In vivo efficacy was evaluated in male mixed-breed dogs with urate crystal-induced synovitis. Prophylactic efficacy was evaluated by administering ML-1,785,713 two hours before induction of synovitis whereas therapeutic efficacy was determined by administering ML-1,785,713 one hour after induction of synovitis. RESULTS: Blood concentrations that resulted in 50% inhibition of COX-1 and COX-2 activity in vitro were 119.1 microM and 0.31 microM, respectively, and selectivity ratio for inhibiting COX-2 relative to COX-1 was 384. ML-1,785,713 had high oral bioavailability (101%), low systemic clearance (77 mL/min/kg), and an elimination half-life of 5.9 hours. ML-1,785,713 was efficacious when administered prophylactically and therapeutically to dogs with urate crystal-induced synovitis. CONCLUSIONS AND CLINICAL RELEVANCE: ML-1,785,713 is a novel, potent COX-2 inhibitor that is the most selective COX-2 inhibitor described for use in dogs to date. ML-1,785,713 has oral bioavailability and low systemic clearance that is comparable to other non-steroidal anti-inflammatory drugs. It is effective after prophylactic and therapeutic administration in attenuating lameness in dogs with urate crystal-induced synovitis. Drugs that specifically inhibit COX-2 and not COX-1 at therapeutic doses may have an improved tolerability profile, compared with nonselective non-steroidal anti-inflammatory drugs.
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Search related cases →Original publication on PubMed: https://pubmed.ncbi.nlm.nih.gov/15077695/