Core-Shell Arginine-Containing Chitosan Microparticles for Enhanced Transcorneal Permeation of Drugs |
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| Authors: | Nicolò Mauro Giulia Di Prima Paola Varvarà Mariano Licciardi Gennara Cavallaro Gaetano Giammona |
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| Affiliation: | 1. Department of “Scienze e Tecnologie Biologiche, Chimiche e Farmaceutiche” (STEBICEF), Laboratory of Biocompatible Polymers, University of Palermo, Via Archirafi, 32, 90123 Palermo, Italy;2. Fondazione Umberto Veronesi, Piazza Velasca 5, 20122 Milano, Italy;3. Institute of Biophysics, Italian National Research Council, Via Ugo La Malfa 153, 90146 Palermo, Italy |
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| Abstract: | Chitosan oligosaccharide (C) was functionalized with l-arginine (A) and short hydrocarbon chains (C8) to design an amphiphilic copolymer, henceforth CAC8, leading to microparticles (MPs) consisting of an arginine-decorated hydrophilic shell and inner hydrophobic domains allowing the encapsulation of high amount hydrophobic drugs such as sorafenib tosylate (>10% w/w). l-arginine side chains were selected in order to impart the final MPs enhanced transcorneal penetration properties, thus overcoming the typical biological barriers which hamper the absorption of drugs upon topical ocular administration. The mucoadhesive properties and drug release profile of the CAC8 MPs (CAC8-MPs) were studied, showing that CAC8-MPs can strongly interact with mucin, and thus gradually release their payload in situ to potentially improve the bioavailability of the drug after topical administration. In vitro transcorneal studies also showed that CAC8-MPs are endowed with effective permeation enhancer ability combined with negligible toxicity. |
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| Keywords: | chitosan amphiphilic copolymer microparticles mucoadhesion ocular administration |
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