Understanding dexamethasone kinetics in the rabbit tear fluid: Drug release and clearance from solution, suspension and hydrogel formulations

地塞米松 自愈水凝胶 药代动力学 化学 剂型 生物利用度 体内 色谱法 吸收(声学) 药理学 医学 材料科学 有机化学 复合材料 生物技术 内分泌学 生物
作者
Anusha Balla,Marika Ruponen,Annika Valtari,Elisa Toropainen,Marjo Tuomainen,Carmen Alvarez‐Lorenzo,Eva M. del Amo,Arto Urtti,Kati‐Sisko Vellonen
出处
期刊:European Journal of Pharmaceutics and Biopharmaceutics [Elsevier]
卷期号:172: 53-60 被引量:14
标识
DOI:10.1016/j.ejpb.2022.01.005
摘要

Rapid precorneal loss of topically applied eye drops limits ocular drug absorption. Controlling release and precorneal residence properties of topical formulations may improve ocular drug bioavailability and duration of action. In this study, we evaluated in vivo ocular pharmacokinetics of dexamethasone in rabbits after application of a drug solution (0.01%), suspension (Maxidex® 0.1%), and hydrogels of 2-hydroxyethyl methacrylate (HEMA) and acrylic acid (AAc) copolymers. The rabbits received a single eyedrop (solution or suspension) or dexamethasone-loaded hydrogel topically. Dexamethasone in tear fluid was sampled with glass capillaries and quantitated by LC-MS/MS. Higher dexamethasone exposure (AUC) in the tear fluid was observed with the suspension (≈3.6-fold) and hydrogel (12.8-fold) as compared to the solution. During initial 15 min post-application, the highest AUC of dissolved dexamethasone was seen after hydrogel application (368 min*µg/mL) followed by suspension (109.9 min*µg/mL) and solution (28.7 min*µg/mL. Based on kinetic simulations, dexamethasone release from hydrogels in vivo and in vitro is comparable. Our data indicate that prolonged exposure of absorbable dexamethasone in tear fluid is reached with hydrogels and suspensions. Pharmacokinetic understanding of formulation behavior in the lacrimal fluid helps in the design of dexamethasone delivery systems with improved ocular absorption and prolonged duration of action.

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