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Characterization of Ocular Pharmacokinetics of Beta-Blockers Using a Diffusion Model After Instillation
Authors:Yamamura  Kenzo  Sasaki  Hitoshi  Nakashima  Mikiro  Ichikawa  Masataka  Mukai  Takahiro  Nishida  Koyo  Nakamura  Junzo
Institution:(1) School of Pharmaceutical Sciences, Nagasaki University, 1-14 Bunkyo-machi, Nagasaki City, Japan;(2) Department of Hospital Pharmacy, Nagasaki University School of Medicine, 1-7-1 Sakamoto, Nagasaki City, Japan
Abstract:Purpose. To characterize the ocular pharmacokinetics of beta-blockers (timolol and tilisolol) after instillation in the albino rabbit using a mathematical model that includes a diffusion process. Methods. The disposition of fluorescein isothiocyanate-dextran (FITC-dextran, molecular weight 4400), timolol, and tilisolol was determined in tear fluid and aqueous humor after instillation or ocular injection in rabbits. The in vivo penetration parameters were estimated by fitting the concentration-time profiles to the Laplace equations based on a diffusion model using MULTI(FILT) program. Thein vivo permeability of drugs was measured across cornea using a two-chamber diffusion cell. Results. Concentration-time profiles of drugs in the tear fluid after instillation showed a monoexponential curve. Although a monoexponential curve was observed in the aqueous humor concentration of FITC-dextran after injection into the aqueous chamber, timolol and tilisolol showed a biexponential curve. On the basis of these results, anin vivo pharmacokinetic model was developed for estimation of penetration parameters. The in vitro partition parameters were higher than those of the in vivo parameters. Conclusions. The ocular absorption of timolol and tilisolol was characterized using an in vivo pharmacokinetic model and in vivo penetration parameters.
Keywords:diffusion model  drug delivery system  ocular penetration  pharmacokinetics
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