Ganciclovir: Difference between revisions
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== Dosing == |
== Dosing == |
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* If non-obese (BMI <30), use total body weight; if obese (BMI ≥30), use adjusted body weight |
* If non-obese (BMI <30), use total body weight; if obese (BMI ≥30), use [[adjusted body weight]] |
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=== Adult Dosing === |
=== Adult Dosing === |
Latest revision as of 18:44, 9 January 2024
Background
- Guanosine nucleoside analogue similar to acyclovir
- Indications: CMV after hematopoietic stem cell transplantation, CMV after solid organ transplantation, Congenital CMV, Cytomegalovirus, Herpesviridae, Macacine alphaherpesvirus 1, Post-transplant acute limbic encephalitis
Mechanism of Action
- Analog of deoxyguanosine, competes with deoxyguanosine to inhibit viral DNA polymerase
Mechanisms of Resistance
- Resistance in CMV
- Most often conferred by mutations of UL97 kinase, which is required in order to phosphorylate ganciclovir into its active form
- Can also develop through mutations in the target UL54 DNA polymerase
Spectrum of Activity
Pharmacokinetics and Pharmacodynamics
- Oral bioavailability 6-8%
- CNS penetration 24-67% of serum levels
Dosing
- If non-obese (BMI <30), use total body weight; if obese (BMI ≥30), use adjusted body weight
Adult Dosing
- Induction dose: 5 mg/kg q12h
- Maintenance dose: 5 mg/kg q24h or 6 mg/kg 5x/week
Pediatric Dosing
- Ganciclovir 5-6 mg/kg IV q12h
Safety
- Major toxicity is cytopenias
- Usually develops in first one to two weeks of treatment
- Contraindicated when neutrophils <0.5 cells/mL or platelets <25 cells/mL
Drug-Drug Interactions
- Zidovudine, didanosine, probenecid, and imipenem-cilastatin (increases risk of seizures)