Journal of Pharmaceutics & Drug Delivery ResearchISSN: 2325-9604

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Liposomal voriconazole (VOR) formulation for improved ocular delivery


Tais Gratieri

University of Brasilia, Brazil

: J Pharm Drug Deliv Res

Abstract


Treating infectious eye diseases topically requires a drug delivery system capable of overcoming the eye’s defense mechanisms, which efficiently reduce the drug residence time right after its administration, therefore reducing absorption. In order to try to surpass such administration issues and improve life quality for patients with fungal keratitis, liposomal voriconazol (VOR) formulations were prepared. Formulations were composed of soy phosphatidylcholine (PC) containing or not 1, 2-dioleoyl-3- trimethylammonium-propane (DOTAP) and cholesterol. Liposomes were characterized by their drug entrapment efficiency (EE), drug recovery (DR), average diameter (size) and polydispersivity index (PdI). In vitro mucosal interaction and irritancy levels, ex vivo permeation, as well as the short-term stability were also assessed. Liposomal VOR formulation produced with 7.2:40 mM VOR:PC showed to be the most promising formulation: Mean size of 116.6±5.9 nm, narrow PdI (0.17±0.06), negative zeta potential (~ -7 mV) and over 80% of EE and yield, remaining stable for at least 30 days in solution and 90 days after lyophilization. This formulation was classified as ‘non-irritant’ after HET-CAM’s test and was able to deliver about 47.85±5.72 μg/cm2 of VOR into porcine cornea after 30 min of permeation test. Such drug levels are higher than the minimal inhibitory concentrations (MIC) of several fungi species isolated from clinical cases of corneal keratitis. Overall results suggest VOR can be effectively incorporated in liposomes for potential topical treatment of fungal keratitis. This work was supported by CNPq, CAPES, FAPDF and L’Oreal-UNESCO for the Women in Science Awards.

Biography


Email: tgratieri@gmail.com

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