Dynamic Ex Vivo Porcine Eye Model to Measure Ophthalmic Drug Penetration under Simulated Lacrimal Flow

Author:

Barbalho Geisa N.1ORCID,Falcão Manuel A.1,Lopes Jefferson M. S.2,Lopes Júlia M.1,Contarato Jonad L. A.1,Gelfuso Guilherme M.1ORCID,Cunha-Filho Marcilio1ORCID,Gratieri Tais1ORCID

Affiliation:

1. Laboratory of Food, Drugs, and Cosmetics (LTMAC), University of Brasilia, Brasília 70910-900, DF, Brazil

2. Physics Department, Federal University of Pará, Belém 66075-110, PA, Brazil

Abstract

Animal models are still used in the research and development of ophthalmic drug products, mainly due to the difficulty in simulating natural physiological conditions with in vitro models, as there is a lack of dynamic protection mechanisms. Therefore, developing alternative ophthalmic models that evaluate drug penetration in the cornea while applying dynamic protection barriers is a contemporary challenge. This study aimed to develop a dynamic ex vivo model using porcine eyes with a simulated lacrimal flow to evaluate the performance of pharmaceutical drug products. A glass donor cell to support a simulated tear flow was designed, optimized, and custom-made. The system was challenged with different formulations (with fluconazole) including excipients with different viscosities (poloxamer 407) and mucoadhesive properties (chitosan). The results were compared to those obtained from a conventional excised cornea model mounted in Franz-type diffusion cells. The dynamic model could differentiate formulations, while the static model did not, overestimating ex vivo drug penetrated amounts. Hence, the dynamic model with simulated tear flow showed to be a simple and promising new alternative method for the drug penetration of ophthalmic formulations that ultimately can reduce the number of animals used in research.

Funder

Brazilian funding agencies FAP-DF (Fundação de Apoio à Pesquisa do Distrito Federal, Brazil

DPI/DPG University of Brasilia

Publisher

MDPI AG

Subject

Pharmaceutical Science

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