Release kinetics of liposome-encapsulated ganciclovir after intravitreal injection in rabbits

被引:1
作者
LeBourlais, C
Chevanne, F
Ropert, P
Bretagne, G
Acar, L
Zia, H
Sado, PA
Needham, T
Leverge, R
机构
[1] UNIV RHODE ISL,COLL PHARM,DEPT PHARMACEUT,KINGSTON,RI 02881
[2] CHRU,SERV OPHTALMOL,RENNES,FRANCE
关键词
ganciclovir; intravitreal; liposomes; ophthalmic drug delivery system; AIDS; antiviral agent; controlled release;
D O I
暂无
中图分类号
O69 [应用化学];
学科分类号
081704 ;
摘要
This study was undertaken to establish experimentally whether the intravitreal application of liposomally-entrapped ganciclovir could prolong intraocular therapeutic levels when it is compared to the intravitreal injection of a simple solution of the drug. New Zealand white rabbits were given an intravitreal injection of the drug solution and of liposome-encapulated ganciclovir. The intravitreal clearance of ganciclovir was determined after a single injection of either the drug solution (200 mu g/0.1 mL) or the liposomally-entrapped (with 41% load; 82 mu g drug load and 118 mu g free) ganciclovir. The ganciclovir vitreal concentrations were measured at various time intervals for a period up to 43 days using an HPLC method. The results of this study clearly demonstrated that prolonged intravitreal drug levels (above the mean inhibitory dose of cytomegalovirus of 1 mu g/mL) after administration of the liposome-entrapped ganciclovir and estimated to continue beyond 30-43 days. The injection of the 200 mu g/0.1 mt of drug solution showed a mean vitreous concentration which was higher than the ID50 only for 55 h. The disappearance rate constant for the liposome-encapsulated injections was approximately 22 x slower than simple drug solution injections (controls). No evidence of retinal toxicity was found by clinical or light microscopy examination of the treated eyes.
引用
收藏
页码:473 / 480
页数:8
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