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Research Article

Ocular penetration of acyclovir and its peptide prodrugs valacyclovir and val-valacyclovir following systemic administration in rabbits: An evaluation using ocular microdialysis and LC-MS

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Pages 243-252 | Published online: 02 Jul 2009
 

Abstract

Purpose. To investigate the ocular penetration of acyclovir and its prodrugs following systemic administration and to elucidate the mechanism of penetration. Methods. Hydrophilic peptide prodrugs of acyclovir were infused intravenously in New Zealand albino rabbits over 45 min at a dose equivalent to 30 mmoles/kg acyclovir. Aqueous and vitreous humor samples were obtained utilizing ocular microdialysis and blood samples were obtained from the mid ear vein using a cannula. Results. The plasma bioavailability for acyclovir, valacyclovir and val-valacyclovir were similar with area under curve values being 896.24 (±143.58), 776.54 (±197.52), 824.69 (±217.43) min.µmoles/L respectively. Anterior segment area under curve values were 53.70 (±35.58), 139.85 (±9.43) and 291.05 (±88.13) min.µmoles/L respectively while the mean residence time values were 46.47 (±24.94), 76.30 (±7.24) and 188.39 (±80.73) min respectively. Vitreous levels of the prodrugs were not measurable. Conclusions. The valine and valine-valine ester prodrugs of ACV penetrated the anterior segment of the eye much better than acyclovir alone, probably via a carrier mediated transport mechanism.

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