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In vitro characterization of chitosan gels for buccal delivery of celecoxib: influence of a penetration enhancer. | LitMetric

In vitro characterization of chitosan gels for buccal delivery of celecoxib: influence of a penetration enhancer.

AAPS PharmSciTech

Faculdade de Farmácia, Laboratório de Pesquisa e Desenvolvimento Farmacotécnico, Departamento de Medicamentos, Universidade Federal do Rio de Janeiro, Brazil.

Published: March 2012

Celecoxib (Cx) shows high efficacy in the treatment of osteoarthritis and rheumatoid arthritis as a result of its high specificity for COX-2, without gastrolesivity or interference with platelet function at therapeutic concentrations. Besides of anti-inflammatory effects, Cx also has a potential role for oral cancer chemoprevention. For these conditions, oral administration in long-term treatment is a concern due to its systemic side effects. However, local application at the site of injury (e.g., buccal inflammation conditions or chemoprevention of oral cancer) is a promising way to reduce its toxicity. In this study, the in vitro characterization of mucoadhesive chitosan (CHT) gels associated to Azone® was assessed to explore the potential buccal mucosal administration of Cx in this tissue. Rheological properties of gels were analyzed by a rheometer with cone-plate geometry. In vitro Cx release and permeability studies used artificial membranes and pig cheek mucosa, respectively. Mucoadhesion were measured with a universal test machine. CHT gels (3.0%) containing 2.0% or 3.0% Az showed more appropriate characteristics compared to the others: pH values, rheology, higher amount of Cx retained in the mucosa, and minimal permeation through mucosa, besides the highest mucoadhesion values, ideal for buccal application. Moreover, the flux (J) and amounts of drug released decreased with increased CHT and Az concentrations. CHT gels (3.0%) associated with 2.0% or 3.0% Az may be considered potential delivery systems for buccal administration of Cx.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3299462PMC
http://dx.doi.org/10.1208/s12249-011-9725-8DOI Listing

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