Comprehensive DDI risk assessment with evidence-based clinical guidance.
User: "Analyze drug interactions between warfarin and amoxicillin"
Agent: Creates `DDI_risk_report_warfarin_amoxicillin.md` with:
- Bidirectional mechanism analysis
- Risk score: 55/100 (Moderate)
- Management: Monitor INR at day 3-5
- Evidence: ★★★ (FDA label + clinical studies)
User: "Assess interactions for: warfarin, lisinopril, metoprolol, omeprazole, amlodipine, furosemide"
Agent: Creates `DDI_risk_report_polypharmacy.md` with:
- 15 pairwise interactions analyzed
- DDI matrix showing all combinations
- Polypharmacy risk score: 38/100
- Top 3 priority interactions with management
User: "Which statin is safest with diltiazem and erythromycin?"
Agent: Analyzes all statins and recommends:
- PREFERRED: Pravastatin or rosuvastatin (no CYP3A4 interaction)
- AVOID: Simvastatin, lovastatin (contraindicated)
- Evidence table with risk scores for each statin
Always analyzes both directions:
- Drug A → Drug B (A affects B)
- Drug B → Drug A (B affects A)
Effects are often asymmetric (e.g., ketoconazole affects simvastatin, but not vice versa).
Score = Mechanism(30) + Evidence(25) + Clinical Impact(25) + Prevalence(10) + Reversibility(10)
80-100: Critical (contraindicated)
60-79: High (avoid if possible)
40-59: Moderate (monitor/adjust)
20-39: Low (minimal action)
0-19: Negligible
- ★★★ = FDA label, RCT, clinical guidelines
- ★★☆ = Clinical studies, PK studies, case series
- ★☆☆ = Case reports, theoretical mechanisms
- ☆☆☆ = Computational predictions only
Pharmacokinetic (PK):
- CYP450 enzyme interactions (CYP3A4, 2D6, 2C9, 2C19, 1A2)
- Drug transporter interactions (P-gp, OATs, OCTs, BCRP, OATPs)
- Protein binding displacement
Pharmacodynamic (PD):
- Additive/synergistic effects (e.g., two anticoagulants)
- Antagonistic effects (e.g., beta-blocker + beta-agonist)
- QTc prolongation (additive cardiac risk)
- CNS depression (additive sedation)
- Serotonin syndrome risk
For each DDI, provides:
- Avoid combination (if Major/contraindicated)
- Alternative drug recommendations
- Dose adjustments
- Timing separation strategies
- Monitoring parameters (labs, vital signs, symptoms)
- Patient counseling points
✅ Use for:
- Two-drug interaction analysis
- Polypharmacy risk assessment (3+ drugs)
- Alternative drug recommendations (lower DDI risk)
- QTc prolongation risk (multiple drugs)
- Clinical decision support for prescribing
- Patient safety reviews
- Medication reconciliation
❌ Don't use for:
- Single drug safety profile → use
tooluniverse-drug-research - Drug mechanism only → use
tooluniverse-drug-research - Pharmacogenomics → use PGx-specific analysis
- Disease-drug associations → use disease-focused skills
- Create report file FIRST with all section headers
- Populate progressively as data is gathered
- User sees complete report, not search process
- Actionable clinical guidance, not just theory
- Evidence-based recommendations
- Alternative drugs when DDI risk is high
- Clear monitoring parameters
- Patient-friendly counseling language
- All sections must exist
- Explicit "No interaction found" when appropriate
- Document tool failures
- Cite data sources throughout
| Analysis Path | Primary Tools |
|---|---|
| Drug ID | rxnorm_get_drugs_by_name, DailyMed_search_spls, PubChem_get_CID_by_compound_name |
| CYP interactions | ADMETAI_predict_CYP_interactions, DailyMed_get_spl_sections_by_setid |
| FDA warnings | DailyMed_get_spl_sections_by_setid (contraindications, boxed_warning, drug_interactions) |
| Clinical evidence | PubMed_search_articles, search_clinical_trials |
| Post-marketing | FAERS_count_reactions_by_drug_event |
| Alternatives | DGIdb_get_drug_gene_interactions, DailyMed_search_spls |
DDI_risk_report_[DRUG1]_[DRUG2].md
0. Drug Identification
1. Interaction Mechanisms (CYP, Transporters, PD)
2. FDA Label & Regulatory Warnings
3. Clinical Evidence & Literature
4. Post-Marketing Surveillance (FAERS)
5. Severity Classification & Risk Scoring
6. Clinical Management Strategies
7. Summary & Clinical Action Plan
DDI_risk_report_polypharmacy.md
- DDI matrix (all pairwise combinations)
- Polypharmacy risk score
- Top priority interactions
- Cumulative monitoring plan
- Simplification opportunities
See EXAMPLES.md for 7 detailed scenarios:
- Warfarin + Amoxicillin - CYP/gut flora interaction
- Simvastatin + Ketoconazole - Major contraindicated DDI
- Polypharmacy (6 drugs) - Complex elderly regimen
- QTc prolongation - Multiple psychiatric drugs
- Alternative recommendations - Safer statin selection
- Drug-food interaction - Tacrolimus + grapefruit
- Timing separation - Levothyroxine + calcium
Before finalizing DDI report:
✅ All drug names resolved to standard identifiers
✅ Bidirectional analysis completed (A→B and B→A)
✅ All mechanism types assessed (CYP, transporters, PD)
✅ FDA label warnings extracted
✅ Clinical literature searched
✅ Evidence grades assigned (★★★, ★★☆, ★☆☆)
✅ Risk score calculated (0-100)
✅ Severity classified (Major/Moderate/Minor)
✅ Primary management recommendation provided
✅ Alternative drugs suggested (if Major DDI)
✅ Monitoring parameters defined
✅ Patient counseling points included
✅ All sections completed (no [Analyzing...] placeholders)
✅ Data sources cited throughout
When all criteria met → Ready for Clinical Use
- Major: High risk, life-threatening. Avoid combination
- Moderate: Significant risk. Monitor closely, dose adjust
- Minor: Limited risk. Minimal action needed
- 80-100: Critical - contraindicated
- 60-79: High - avoid if alternatives exist
- 40-59: Moderate - monitor and adjust
- 20-39: Low - minimal precautions
- 0-19: Negligible
- Avoid combination (Major DDI)
- Use alternative drug
- Dose adjustment
- Timing separation
- Intensive monitoring
- Patient education
Reports include:
- Distribution of evidence grades (% ★★★, ★★☆, ★☆☆)
- Source coverage (FDA labels, PubMed, FAERS)
- Data recency and limitations
- FAERS does not support direct co-medication queries (requires manual review)
- Some theoretical interactions lack clinical validation
- Alternative drug recommendations limited to same therapeutic class
- Non-US regulatory data (EMA, PMDA) not available via public APIs
See SKILL.md for:
- Complete implementation guide
- Tool call sequences
- Error handling patterns
- Bidirectional analysis algorithms
- Risk scoring formulas
- Alternative drug selection logic
Validate skill with:
- Two-drug pairs (10+ examples)
- Polypharmacy (3 scenarios, 5-8 drugs each)
- Edge cases (no interaction, contraindicated, food-drug)
- Bidirectional asymmetry (e.g., A→B but not B→A)
This skill provides decision support information based on FDA labels, clinical literature, and pharmacology databases. It is NOT a substitute for clinical judgment, patient-specific assessment, or consultation with a pharmacist. Always verify critical DDI information with authoritative sources and consider individual patient factors (age, renal/hepatic function, comorbidities, concomitant medications beyond those analyzed).
Skill Version: 1.0 Last Updated: 2026-02-09 ToolUniverse Compatibility: v0.3.0+ Key Dependencies: DailyMed, PubMed, ADMET-AI, FAERS, RxNorm
For questions or feedback, see main ToolUniverse documentation.