| Structure/Class |
- DNA polymerase inhibitor
|
| Pharmacodynamics |
- It is a prodrug that requires activation by viral thymidine kinase before become active.
- It then functions by inhibiting viral DNA polymerase, preventing replication of viral DNA.
- Spectrum of activity as follows: HSV-1, HSV-2 and VZV. No in vivo activity against EBV/CMV and HHV-6.
- Therefore, indications as follows:
- Herpes simplex encephalitis
- Neonatal HSV
- Serious HSV/VZV infections, especially in the immunocompromised
- Resistance is due to reduction in viral thymidine kinase or the alteration of DNA polymerase binding site. If there is a reduction in the viral thymidine kinase, then the virus will have cross resistance to valacyclovir, ganciclovir and famciclovir.
|
| Absorption/administration |
- PO or IV. Bioavailability is very low.
|
| Distribution |
- Readily distributes into most tissues and body fluids, with CSF concentrations approximately 20-50%.
|
| Metabolism |
- Not metabolized – it is excreted unchanged in the urine.
|
| Excretion |
- T ½ of 2.5 hours, which is prolonged in renal failure.
|
| Adverse events |
|
| Dosing/administration |
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| Toxicology |
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| Withdrawal syndrome |
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| Special notes |
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