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Management of Drug Interactions

Management of Drug Interactions

Management of Drug Interactions

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General Principles - Interaction Game Plan

  • Goal: Minimize patient harm from drug-drug interactions (DDIs).

  • Core Strategy: A systematic, proactive approach is crucial.

  • Key Actions:

    • Avoid: If possible, use non-interacting alternatives.
    • Adjust: Modify dose, frequency, or timing.
    • Monitor: Closely observe for adverse drug reactions (ADRs) or therapeutic failure; consider therapeutic drug monitoring (TDM).
    • Discontinue: Stop one of the interacting drugs if risks outweigh benefits.
  • Patient Education: Essential for adherence and early reporting of issues.

⭐ Most clinically significant interactions involve drugs with a narrow therapeutic index or those affecting critical pathways. 📌 Common enzyme inducers (e.g., Rifampicin, Phenytoin, Carbamazepine) and inhibitors (e.g., Ketoconazole, Erythromycin, Ritonavir) are frequent culprits.

Proactive Management - Prevent & Predict

  • Comprehensive Medication History:
    • Rx, OTC, herbals, supplements.
    • Allergies, past ADRs.
  • Medication Reconciliation:
    • Essential at care transitions.
  • Identify High-Risk:
    • Patients: Elderly, polypharmacy, organ dysfunction (renal/hepatic), NTI drug therapy.
    • Drugs: NTI (e.g., warfarin, digoxin, phenytoin), key enzyme inducers (e.g., rifampicin) & inhibitors (e.g., azoles).

    ⭐ Cytochrome P450 (CYP450) enzyme system metabolizes ~70-80% of clinical drugs; its inhibition/induction is a key cause of pharmacokinetic drug interactions.

  • Utilize Decision Support:
    • CPOE with CDSS alerts.
    • Drug interaction databases.
    • Beers, STOPP/START criteria (elderly).
  • Pharmacogenomic (PGx) Testing:
    • For specific gene-drug pairs (e.g., $CYP2C19$ & clopidogrel).
  • Patient Education:
    • Stress adherence, reporting new issues. Precision medicine in polypharmacy challenges and approachesoka

Reactive Management - Detect & Correct

  • Suspicion & Confirmation:
    • Detailed history (all drugs, diet, herbals).
    • Clinical exam for ADR/interaction signs.
    • Lab tests: drug levels, organ function (LFTs, RFTs).
  • Causality Assessment:
    • Use Naranjo Algorithm or WHO-UMC criteria.
    • Assess temporal link: onset post-drug, dechallenge (improvement), rechallenge (recurrence).
  • Identify Interacting Drugs:
    • Review all current medications (Rx, OTC, herbals).
    • Consult drug interaction databases (e.g., Micromedex, Lexicomp).
  • Corrective Actions (Severity-dependent):
    • Stop drug if severe/life-threatening.
    • Reduce dose of one/both drugs; monitor.
    • Substitute with non-interacting alternative.
    • Monitor closely if drugs essential.
    • Stagger administration times if appropriate.
  • Documentation & Reporting:
    • Document interaction & management in patient records.
    • Report significant ADRs/interactions to PvPI.

⭐ Naranjo Algorithm score >9 indicates a definite ADR; 5-8 probable; 1-4 possible; 0 doubtful.

Patient & System Factors - Holistic Handling

  • Patient-Specific Considerations:
    • Age extremes (elderly, neonates): altered pharmacokinetics/dynamics.
    • Genetic factors (e.g., CYP450 polymorphisms): influences drug metabolism.
    • Comorbidities (renal/hepatic impairment): affects drug elimination.
    • Polypharmacy: significantly ↑ interaction risk; review regularly.
    • Patient education & adherence: key to prevention.
  • System-Level Strategies:
    • Medication reconciliation: critical during care transitions.
    • Clinical Decision Support Systems (CDSS): utilize for interaction screening.
    • Multidisciplinary team approach: involve pharmacists.
    • Clear, unambiguous prescribing practices.
    • Robust ADR & interaction reporting systems.

⭐ Polypharmacy (concurrent use of ≥5 drugs) is a major predictor of adverse drug interactions, especially in geriatric patients.

High‑Yield Points - ⚡ Biggest Takeaways

  • Dose adjustment is a key strategy to manage drug interactions.
  • Monitor therapy closely, especially for drugs with narrow therapeutic windows.
  • Substitute interacting drugs with safer alternatives when possible.
  • Separate administration times to minimize pharmacokinetic interactions.
  • Discontinue one drug if the interaction is unavoidable and severe.
  • Be vigilant for CYP450 enzyme inducers/inhibitors and their impact.
  • Educate patients about potential interaction symptoms for prompt reporting.

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