Liposomal ophthalmic drug delivery system. II. Dihydrostreptomycin sulfate

Abstract

The carrier ability of liposomes for a model hydrophilic compound vas investigated in the rabbit eye. Dihydrostreptomycin sulfate was encapsulated in various types of liposomes, i.e. large and small uni- and multilamellar vesicles having either positive or neutral surface charge. An aqueous solution served as control preparation. Results indicated that liposomal encapsulation reduced the ocular drug con- centration. Addition of empty liposomes to the control solution did not alter drug levels in most of the ocular tissues. Among the liposomal preparations the large multi- and unilamellar vesicles provided higher drug concentration in all ocular tissue than the small unilamellar ones. Introduction of a positive charge on liposome surface enhanced liposome-conjunctiva interactions. The results suggest that liposomal encapsulation alters drug disposition in the eye lepending on the type of liposomes and the physicochemical properties of the encapsulated drug. In the case of the dihydrostreptomycin sulfate and possibly other hydrophilic drugs the liposomal encapsulation provides no advantages as far as drug delivery is concerned.