Lofexidine | Pharmacology Mentor

Generic Name

Lofexidine

Selective α₂‑adrenergic receptor agonist that activates pre‑synaptic inhibitory autoreceptors in the locus coeruleus.
↓ Sympathetic outflow → ↓ norepinephrine release.
Inhibits “central noradrenergic hyperactivity” that drives withdrawal signs (rigidity, diaphoresis, lacrimation, tachycardia).
Provides symptomatic control (e.g., tremor, sweating) without the pronounced hypotension of non‑selective α‑agonists.

Parameter	Typical Value
Absorption	Oral bioavailability ≈ 15% (first‑pass)
Cₘₐₓ	1–1.5 h post‑dose (rapid onset)
Half‑life (t½)	3–4 h (short, supports BID dosing)
Metabolism	Primarily CYP2D6 → active metabolites; 15%‑20% unchanged
Elimination	Urine: ~80 % unchanged; kidney & biliary routes
Protein binding	45 %
Drug interactions	↑↑CYP2D6 inhibitors (e.g., fluoxetine) ↑ plasma levels; caution with other α‑agonists or β‑blockers

> Key point: Lofexidine is safe in mild‑to‑moderate hepatic or renal impairment; dose adjustment required only in severe renal/ hepatic disease.

Approved: *Short‑term (≤ 72 h) management of opioid withdrawal* in adults.
Off‑label (studied): Adjunct analgesia for neuropathic pain; not a first‑line analgesic.

Contraindication / Warning	Rationale
Hypersensitivity to lofexidine, other α₂‑agonists, or excipients	Allergic reactions
Severe cardiovascular disease (eg. advanced heart block, uncontrolled hypotension)	Risk of exacerbated bradycardia/Hypotension
Severe hepatic impairment	↓ metabolism → ↑ exposure
Concurrent use of strong CYP2D6 inhibitors	↑ systemic exposure → increased adverse events
Co‑administration with other CNS depressants (benzodiazepines, opioids)	Additive hypotension/bradycardia
Pregnancy Category C – Use only if benefits outweigh risks	Fetal safety data limited
Pediatric (< 12 yr) – Not indicated	Safety profile not established

Situation	Dose	Titration	Administration
Initial	0.1 mg PO BID (≥ 4 h apart)	Increase by 0.1 mg every 8 h up to max 0.6 mg/day if needed	Oral (tablet)
Max	0.3 mg PO Q4H (not > 0.6 mg/day)	Stop if BP < 90 mmHg or HR < 45 bpm	Oral
Renal impairment (CrCl 15‑30 mL/min)	0.05 mg BID	Titrate more slowly	Oral
Severe hepatic impairment	Hold or use with extreme caution	•	•

• Initiate 1 h after opioid cessation or when withdrawal signs appear.
• Typically discontinued after 48–72 h once withdrawal is controlled.

Vital signs (BP, HR) q2–4 h during initiation/ titration.
COWS (Clinical Opioid Withdrawal Scale) or equivalent to gauge symptom relief.
Liver function if pre‑existing hepatic disease; re‑check after 1–2 weeks of therapy.
Renal function if dose adjustments required.
Signs of allergic reaction: rash, swelling, wheezing.

Titration is key: A 0.1 mg increment every 8 h keeps bradycardia risk low while quickly alleviating withdrawal.
Lofexidine vs. clonidine: Lofexidine has less CNS sedation, lower risk of nausea & constipation, and a shorter half‑life—ideal for abrupt withdrawal protocols.
CYP2D6 polymorphisms affect clearance; poor metabolizers may show exaggerated hypotension—monitor more closely.
Concurrent benzodiazepines are often used for anxiety; avoid overlapping α‑agonists (e.g., clonidine) to reduce additive CV depressant effects.
Withdrawal assessment: Even mild hypotension can precipitate fainting in patients who have been withdrawing (dehydrated). Encourage adequate hydration.
Adjunct analgesia: While not labeled for pain, low‑dose lofexidine (≤ 0.1 mg BID) has shown limited benefit for neuropathic pain—use cautiously and monitor tolerability.

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• *References: FDA label (2023), Goodman & Gilman’s Pharmacological Basis of Therapy (13th ed.), Clinical Pharmacokinetics of Lofexidine 2023.*