Acyclovir
Selective activation
Generic Name
Selective activation
Mechanism
- Selective activation by viral thymidine kinase to acyclovir monophosphate (viral specific).
- Host cellular kinases convert it to the triphosphate form.
- The triphosphate competitively inhibits viral DNA polymerase and incorporates into nascent DNA strands, causing chain termination.
- High selectivity for infected cells reduces host toxicity.
Pharmacokinetics
| Parameter | Typical Value | Notes |
| Bioavailability | 10–30 % (PO) | Reduced by food; 95 % at 200 mg doses. |
| Volume of distribution | 0.3–0.4 L/kg | Low tissue penetration; limited brain CSF (<4 %). |
| Metabolism | None (direct renal excretion) | No CYP450 interaction. |
| Elimination half‑life | ~2–3 h (PO) | 5–8 h with IV; shorter in renal impairment. |
| Kidney clearance | Major route | Dose adjustment based on CrCl. |
Indications
- Herpes simplex (HSV‑1/2) ulcers, genital herpes, and encephalitis.
- Varicella‑zoster disease (chronic, post‑herpetic neuralgia).
- Immunocompromised patients with disseminated HSV or VZV.
- Prophylaxis for transplant recipients or severe immunosuppression.
Contraindications
- Severe renal impairment (CrCl < 30 mL/min) – requires dose adjustment.
- Known hypersensitivity to acyclovir or guanosine analogues.
- Pregnancy Category B – use only if clearly indicated.
- Potential for crystalluria in high doses or rapid IV infusion → hydrate and slow infusion rate.
Dosing
- Adult (PO):
- HSV/Genital: 400 mg TID for 7–10 days.
- VZV: 200 mg QID for 7–12 days.
- Prophylaxis (immunocompromised): 400 mg BID to 1 g BID.
- IV (Adults):
- HSV encephalitis: 5 mg/kg IV q8h for 5–14 days.
- VZV dissemination: 10 mg/kg IV q8h.
- Children: Adjust by weight (5 mg/kg PO q8h or IV q8h).
- Hydrate > 1 L/d for IV to prevent crystalluria.
Adverse Effects
- Common:
- GI upset, rash, headache.
- Cramps, mild renal impairment.
- Serious:
- Renal tubular dysfunction → acute kidney injury or Fanconi syndrome.
- Neurotoxicity (confusion, seizures) at high IV doses or in renal failure.
- Clostridium difficile colitis.
Monitoring
- Renal function: CrCl before starting, then every 3 days during IV courses > 7 days.
- Urinalysis: for crystals or hematuria during IV therapy.
- Neurologic assessment: monitor for confusion or seizures.
- Blood counts: if used long‑term in immunocompromised pts.
Clinical Pearls
- “Crystallinity can kill”: Aggressive hydration (≥1 L/d) and slow IV infusion (≥20 min) mitigate renal crystal formation.
- Dosing in CrCl ≤ 30 mL/min: Divide daily dose into 2–3 smaller doses to maintain trough concentrations.
- Commercial formulations: Foscarnet is an alternative for acyclovir‑resistant strains; choose when nephrotoxicity is anticipated.
- Bioavailability boost: 200 mg PO q6h achieves similar plasma levels to 400 mg PO t.i.d, useful in pediatric settings.
- Activate quickly: In HSV encephalitis, start IV acyclovir within 12 h of symptom onset; delay > 48 h worsens outcomes.
Key Takeaway: Acyclovir’s viral‑specific activation, low systemic toxicity, and clear PK profile make it the frontline agent for HSV/VZV infections, but vigilant renal monitoring and hydration are essential to prevent crystal‑induced nephropathy.
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• References
1. DiLabio MA, Marra G. A