| name | nsaid-safety |
| description | NSAID comparison (meloxicam, carprofen, deracoxib, firocoxib, robenacoxib), species-specific dosing, GI ulceration risk factors, renal monitoring protocols, corticosteroid washout requirements, COX-1 vs. COX-2 selectivity. |
NSAID Safety
Overview
Evidence-based NSAID selection, dosing by species, contraindication recognition, and safety monitoring protocols. Includes COX-1 vs. COX-2 selectivity comparison, renal/GI risk stratification, and drug interaction management.
When to Use
- User prescribes NSAID or assesses drug safety for concurrent NSAID use
- User needs NSAID selection, dosing verification, or renal/GI monitoring plan
- Keywords: NSAID, meloxicam, carprofen, deracoxib, firocoxib, robenacoxib, GI ulcer, renal, COX, anti-inflammatory, contraindication, drug interaction
NSAID Comparison Table
| Drug | Species | Dose | Route | Frequency | COX Selectivity | Comments |
|---|
| Meloxicam | Dog | 0.1-0.2 mg/kg | PO/IV/SC | Daily | COX-2 preferential | Longer half-life (12-18h); IV/SC option; first-line many practices |
| Cat | 0.1 mg/kg | PO/SC/IV | Daily | COX-2 preferential | CONTROVERSIAL dosing: 0.3-0.5 mg/kg q48h alternative; GI risk lower than dogs at low dose; renal monitoring mandatory |
| Rabbit | 0.6-1 mg/kg | PO/SC | BID | COX-2 preferential | Limited data; anecdotal use; monitor renal/GI closely |
| Carprofen | Dog | 2-4 mg/kg | PO/IV | BID-TID | COX-2 preferential (mild) | Rapid GI absorption; shorter half-life (8 hours); hepatotoxicity rare but reported |
| Cat | 1-2 mg/kg | PO/IV | BID | COX-2 preferential (mild) | Limited feline data; less commonly used in cats; GI ulceration risk higher than meloxicam |
| Deracoxib | Dog | 1-2 mg/kg | PO | Daily | COX-2 selective | Food-dependent absorption (give with food); 5-7 day max acute, 30 days chronic (FDA restriction) |
| Firocoxib | Dog | 5 mg/kg | PO | Daily | COX-2 highly selective | Equine label (5 mg/kg); less GI ulceration than carprofen; excellent for orthopedic pain; expensive |
| Horse | 0.1 mg/kg IV/5 mg/kg PO | PO/IV | Daily | COX-2 highly selective | Superior to phenylbutazone in some studies; longer plasma half-life |
| Robenacoxib | Dog/Cat | 1-2 mg/kg | SC/IV | Daily × 4-10 days | COX-2 selective | Short-term use primarily; less renal effects at short durations; expensive; limited US availability |
COX-1 vs. COX-2 Selectivity
COX-1 Functions: Gastric mucosal protection (prostaglandins), platelet aggregation, renal hemodynamics, tissue homeostasis
- Inhibition consequence: GI ulceration, platelet dysfunction, renal perfusion reduction
COX-2 Functions: Inflammation, fever, pain; also renal and gastric roles in chronic settings
- Selectivity advantage: Lower GI ulceration risk; some renal protective effects at lower doses
Clinical Implication: COX-2 selective agents (meloxicam, firocoxib, deracoxib, robenacoxib) safer GI profiles than less-selective agents (carprofen) in short-term use; long-term use blunts selectivity advantage
GI Ulceration Risk Factors
Intrinsic Risk (patient factors):
- Age (geriatric >7 years; puppies/kittens immature mucosa)
- Concurrent disease (inflammatory bowel disease, gastric ulcer history, neoplasia)
- Hepatic/renal disease (reduced clearance, decreased perfusion)
- Hypoproteinemia (<5.0 g/dL; reduced gastric mucosa protection)
- Dehydration (reduced gastric blood flow)
- NSAIDs increase risk 4-6× in dogs; cats lower baseline risk but elevation if predisposed
Extrinsic Risk (drug factors):
- High NSAID dose
- Prolonged duration (risk increases after 2-4 weeks)
- Concurrent corticosteroid use (synergistic ulceration risk; contraindicated)
- Concurrent anticoagulant (inhibited platelet aggregation)
- Multiple NSAIDs (avoid combining even "safer" pairs)
Gastroduodenal Complications:
- Grade 1: Gastric mucosal erythema, no erosion; asymptomatic
- Grade 2: Erosions <3 mm; vomiting possible
- Grade 3-4: Ulcers >3 mm, perforation risk; hematemesis, melena, severe pain
Renal Monitoring Protocol
Baseline Assessment (before NSAID initiation):
- Serum creatinine, BUN, urine specific gravity (USG)
- Contraindicate NSAID if: Cr >1.8 mg/dL (dogs), >1.6 mg/dL (cats); pre-existing renal disease; dehydration present
During Therapy:
- Recheck BUN/creatinine at 7-10 days if new NSAID (acute phase kidney injury risk peaks early)
- Repeat at 2-4 weeks if continuing >2 weeks duration
- For chronic NSAIDs (months+): Check q3-6 months
Renal NSAID Mechanism:
- Decrease renal perfusion (COX-2 inhibition reduces renal vasodilation)
- Acute kidney injury risk in hypovolemic/dehydrated states
- Chronic risk: Progressive glomerulosclerosis with prolonged high-dose use
Discontinuation Indications:
- Creatinine increase >0.5 mg/dL from baseline
- BUN >40 mg/dL without other explanation
- Evidence of acute kidney injury (azotemia + clinical signs)
- Oliguria/polyuria development
Species-Specific Dosing and Considerations
Dogs
- Standard dose: Meloxicam 0.1-0.2 mg/kg daily; carprofen 2-4 mg/kg BID
- Geriatric/renal disease: Reduce to minimum effective dose; meloxicam 0.1 mg/kg daily preferred (less renal impact)
- Post-operative: Start pre-operatively (pre-emptive analgesia); continue 5-7 days minimum
- Chronic orthopedic disease: Long-term meloxicam acceptable with monitoring; consider adjuvant agents (gabapentin, joint supplements) to minimize NSAID requirements
Cats
- Meloxicam controversy: AAHA (2017) recommends 0.1 mg/kg daily (same as dogs); some practitioners prefer 0.3-0.5 mg/kg q48h
- Rationale: Feline renal physiology; lower baseline GI risk; extrarenal NSAID metabolism; palatability of sustained dosing
- Conservative approach: 0.1 mg/kg daily with renal monitoring remains safest evidence-based recommendation
- GI risk: Cats more sensitive to severe GI ulceration than dogs despite lower overall baseline
- Renal monitoring: Mandatory (USG, BUN, creatinine baseline and q2-4 weeks)
- Chronic use: Short-term (acute pain, <2 weeks) preferred; long-term requires strong indication and close monitoring
Rabbits/Small Mammals
- Meloxicam: 0.6-1 mg/kg PO/SC BID common dosing (limited species-specific data)
- GI stasis risk: Meloxicam may reduce appetite/motility; ensure adequate hydration and hay intake
- Carprofen: Anecdotal use; minimal data; generally avoided
- Monitoring: Renal monitoring less standardized; assess appetite, fecal output, hydration
Horses
- Firocoxib: 5 mg/kg daily PO (approved label); superior to phenylbutazone (PBZ, older standard) in some pain models
- Phenylbutazone: Traditional (4.4 mg/kg daily max); longer-term GI ulceration risk; now second-line
- Monitoring: Renal dysfunction less common in horses; GI ulceration still risk
- Maximum duration: 30 days typically recommended (extended use controversial)
Corticosteroid + NSAID Interaction
Mechanism: Corticosteroids inhibit phospholipase A2 (blocks arachidonic acid release); NSAIDs inhibit COX; combined blockade → synergistic GI ulceration
Contraindication: Absolute: Do NOT combine systemic corticosteroid + NSAID concurrently
- Washout period: Discontinue corticosteroid ≥1 week before initiating NSAID OR discontinue NSAID ≥1 week before corticosteroid
Exception: Topical corticosteroids (ophthalmic, dermal) + systemic NSAID generally safe (minimal systemic absorption)
Alternative: Use NSAID + adjuvant analgesic (gabapentin, tramadol) instead of corticosteroid if possible
Drug Interactions and Contraindications
NSAIDs + Anticoagulants (warfarin, apixaban): Increased bleeding risk; avoid if possible; if necessary, use lowest NSAID dose, monitor INR closely
NSAIDs + ACE Inhibitors (enalapril, lisinopril): Combined renal perfusion reduction; acceptable in euvolemic patients; contraindicated if dehydrated
NSAIDs + Diuretics: Reduced renal perfusion; monitor renal function closely; ensure adequate hydration
NSAIDs + Methotrexate: Reduced MTX clearance; potential toxicity; monitor closely
Absolute Contraindications:
- Acute/chronic kidney disease (Cr >1.8 dogs, >1.6 cats without specialist guidance)
- Severe hepatic disease
- Active GI ulceration (confirmed or high suspicion)
- Platelet dysfunction disorders
- Concurrent corticosteroid (system non-topical)
- Hypersensitivity/allergy history
GI Protection Strategies
H2 Blockers (famotidine 0.5-1 mg/kg q12h):
- Reduces gastric acid; modest ulceration prevention
- Minimal evidence for routine prophylaxis in short-term NSAID use
- Consider if: Geriatric, pre-existing GI disease, high-risk NSAID choice
Proton Pump Inhibitors (omeprazole 0.5-1 mg/kg q24h):
- Superior acid suppression to H2 blockers
- Limited evidence for routine prophylaxis short-term
- Consider if: High-risk patient, previous NSAID intolerance, chronic NSAID use
Misoprostol (2-5 mcg/kg q6-8h): Prostaglandin analog; promotes gastric mucosa protection
- Reduced diarrhea (side effect) in cats; avoid if GI dysmotility risk
- Limited practical use due to dosing frequency
Evidence: Routine GI protection not recommended for short-term (<2 weeks) NSAID use in low-risk patients; consider for high-risk or chronic use
Monitoring and Patient Selection Workflow
- Assess renal function baseline: Serum creatinine, BUN, USG; exclude if abnormal
- Assess GI risk: History of ulceration, concurrent medications, age, dehydration status
- Select appropriate NSAID: COX-2 selective (meloxicam, firocoxib) preferred over less-selective agents; meloxicam for cats with renal monitoring
- Verify no corticosteroid within 1 week: Washout period essential
- Establish monitoring plan: Recheck creatinine/BUN at 7-10 days if new prescription; q2-4 weeks if chronic; assess appetite/vomiting at each visit
- Educate owner: Signs of GI ulceration (vomiting, melena, anorexia); signs of renal disease (polyuria, polydipsia, lethargy); importance of monitoring
Limitations
- Baseline renal assessment: Many animals have subclinical renal disease (eGFR reduced despite normal creatinine); urine protein assessment (UP:C) not routine in screening
- NSAID selectivity: Clinical significance of COX-1 vs. COX-2 selectivity debated; all NSAIDs carry GI/renal risk at higher doses or longer duration
- Feline meloxicam dosing: Significant controversy; "safe" dose remains undefined; individual variation large
- GI protection efficacy: Limited high-quality evidence for routine prophylaxis; many protection strategies add cost without proven benefit in short-term use
- Chronic NSAID use: Long-term safety data limited; adjuvant agents (gabapentin, joint supplements) may reduce NSAID requirements but evidence variable
- Referral: Complex polypharmacy, unexplained renal elevation during NSAID therapy, or refractory pain → internist/pain specialist consideration
