Zhimeng Wu, J. Drach, M. Prichard
Aug 1, 2009
Citations
1
Influential Citations
18
Citations
Quality indicators
Journal
Antiviral Chemistry and Chemotherapy
Abstract
Background: Following the example of L-valine prodrugs of antiviral nucleoside analogues, L-valine ester of cyclopropavir (valcyclopropavir) was synthesized. Methods: The known tetrahydropyranylcyclopropavir was transformed to N-(tert-butoxycarbonyl)-L-valine ester, which was deprotected to valcyclopropavir. Results: Stability of valcyclopropavir towards hydrolysis at pH 7.0 roughly corresponded to that of valganciclovir. Valcyclopropavir inhibited replication of human cytomegalovirus (HCMV, Towne and AD169 strains) to approximately the same extent as the parent drug cyclopropavir. Pharmacokinetic studies in mice established that the oral bioavailability of valcyclopropavir was 95%. Conclusions: The prodrug valcyclopropavir offers some improved therapeutic parameters over the parent compound cyclopropavir.