Methadone
Methadone
Generic Name
Methadone
Mechanism
- Mu‑opioid receptor agonist – provides analgesia and substitution therapy through sustained activation of central mu receptors.
- NMDA receptor antagonist – reduces tolerance and opioid‑induced hyperalgesia.
- Serotonin & norepinephrine reuptake inhibition – contributes to analgesic and mood‑stabilizing effects.
- Long‑acting pharmacodynamics → steady plasma concentration, reducing craving and withdrawal symptoms.
Pharmacokinetics
- Absorption – oral bioavailability 65–80 %; delayed peak (1–4 h).
- Distribution – large volume of distribution (~400 L), lipophilic, >90 % protein‑bound (mainly albumin).
- Metabolism – hepatic CYP3A4, CYP2B6, CYP2C19; first‑pass effect significant.
- Half‑life – 8–48 h (average 24 h); highly variable with steady‑state achieved in 3–4 weeks.
- Elimination – 60–70 % fecal (biliary), remainder renal in the form of metabolites.
Indications
- Treatment of opioid dependence (maintenance/withdrawal).
- Chronic pain management in patients intolerant to short‑acting opioids.
- Adjunct for opioid‑related neuropathic pain and non‑opioid analgesia in specialized settings.
Contraindications
- QT prolongation or arrhythmia (QTC >480 ms, ventricular tachycardia).
- Severe hepatic dysfunction (ALT > 3× ULN).
- Concurrent use of CYP3A4 inhibitors or serotonergic agents (risk of serotonin syndrome, cardiac toxicity).
- Hypersensitivity to methadone or components.
- Pregnancy – category D; avoid unless benefit outweighs risk.
Dosing
| Context | Initial Dose (oral) | Titration | Maintenance |
| Opioid withdrawal | 30 mg | Increment 5–10 mg every 2 h until withdrawal resolves | 30–60 mg daily split 2–3 times |
| Opioid dependence | 60–120 mg | Increase 5–10 mg weekly to reach 120–150 mg | 60–120 mg divided 2–3 times/d |
| Chronic pain | 10–30 mg | 5–10 mg/day increments over 1–2 wk | 20–80 mg divided 2–3 times/d |
• Administer with food to reduce GI upset but beware delayed absorption.
• Check QTc baseline, ≥2 wk after titration, and at any dose change.
• Reformulated tablets prevent “dose‑splitting” errors.
Monitoring
- Baseline: CBC, CMP, liver enzymes, QTc, opioid urine screen.
- During therapy:
- QTc at baseline, 2 wk, then quarterly; immediately if symptoms.
- Drug levels only in special cases (treatment failure, detox).
- Renal & hepatic function quarterly.
- Physical exam: weight, vital signs, pain score, signs of withdrawal or overdose.
- Education: patient advised on constipation management, safe storage, and dosage adherence.
Clinical Pearls
- Titration Pace – err on the slow side; a 15‑mg increase per week is safer than 30 mg, decreasing withdrawal and QT risk.
- Avoid Liquid Methadone – if formulation is available, use tablet/gel to prevent dosing errors.
- Drug‑Drug Interactions:
- Strong CYP3A4 inhibitors (ketoconazole, clarithromycin) can double blood levels; consider dose reduction.
- Serotonergic drugs + methadone = serotonin‑syndrome risk; monitor agitation, hyperthermia, autonomic instability.
- Pregnancy & Lactation – use only if no alternatives; monitor neonate for respiratory depression.
- Withdrawal Assessment – use Clinical Opiate Withdrawal Scale (COWS); methadone may mask symptoms; be vigilant for low pain thresholds.
- Toxicology Screening – methadone is lipophilic; urine screens may be negative early – confirm with plasma if suspicion persists.
--
• Key Takeaway
Methadone’s unique long‑acting mu‑agonist action, NMDA antagonism, and serotonergic effects make it a cornerstone for opioid dependence and complex pain regimens—but careful titration, cardiac monitoring, and vigilance for drug interactions are essential to minimize toxicity.