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用于青光眼滤过手术的载有5-氟尿嘧啶的聚甲基丙烯酸羟乙酯引流植入物:装置设计与体外释放动力学

5-FU loaded pHEMA drainage implants for glaucoma-filtering surgery: device design and in vitro release kinetics.

作者信息

Gökce M, Akata R F, Kiremitçi-Gümüşderelioğlu M

机构信息

Chemical Engineering Department, Hacettepe University, Beytepe, Ankara, Turkey.

出版信息

Biomaterials. 1996 May;17(9):941-9. doi: 10.1016/0142-9612(96)83290-x.

Abstract

Implantable monolithic and reservoir-like water-swellable drainage devices were developed for the subconjunctival sustained release of 5-fluorouracil (5-FU) in glaucoma-filtering surgery. A water-swellable matrix was formed of a copolymer of 2-hydroxyethyl methacrylate (HEMA) with different amounts of ethylene glycol dimethacrylate (EGDMA). Drug incorporation was done before polymerization and cross-linking. Briefly, to prepare the monolithic device the monomer-drug mixture is compression moulded into a 10 mm cylinder of 1 mm length. Furthermore, reservoir-like devices were obtained by coating the monolithic devices with a highly cross-linked polymer of HEMA (pHEMA) composition. The pHEMA devices containing 5-FU or not were well characterized by means of dynamic swelling studies, structural and thermal analysis. The release of 5-FU from these implants was studied in vitro. The rate of drug release was controlled by changing the drug loading (i.e. 10 mg or 20 mg 5-FU per device), cross-linking density of polymer matrix and type of implantable device, i.e. monolithic or reservoir-like device. While monolithic devices are releasing total releasable 5-FU during the first 10 h, reservoir-like devices prolong 5-FU release for up to 120 h. The 5-FU diffusion coefficient in swollen devices (Ds,s) is in the order of 10(-8) cm2 s-1 (approximately 10 times smaller than Dw,g values) and it is dependent on the cross-linking density of polymeric matrix and device load. These preliminary results suggested that 20 mg 5-FU-loaded reservoir-like devices may be a potentially effective system to deliver 5-FU into the subconjunctiva.

摘要

为了在青光眼滤过手术中实现5-氟尿嘧啶(5-FU)在结膜下的持续释放,研发了可植入的整体式和储库式水膨胀引流装置。水膨胀基质由不同量乙二醇二甲基丙烯酸酯(EGDMA)与甲基丙烯酸2-羟乙酯(HEMA)的共聚物形成。药物在聚合和交联之前加入。简要地说,为制备整体式装置,将单体-药物混合物压制成10毫米长、1毫米直径的圆柱体。此外,通过用HEMA(pHEMA)组成的高度交联聚合物涂覆整体式装置来获得储库式装置。通过动态溶胀研究、结构和热分析对含或不含5-FU的pHEMA装置进行了充分表征。对这些植入物中5-FU的释放进行了体外研究。通过改变药物负载量(即每个装置含10毫克或20毫克5-FU)、聚合物基质的交联密度和可植入装置的类型(即整体式或储库式装置)来控制药物释放速率。整体式装置在最初10小时内释放全部可释放的5-FU,而储库式装置将5-FU释放延长至120小时。5-FU在溶胀装置中的扩散系数(Ds,s)约为10(-8)平方厘米每秒(比Dw,g值小约10倍),并且它取决于聚合物基质的交联密度和装置负载。这些初步结果表明,负载20毫克5-FU的储库式装置可能是一种将5-FU递送至结膜下的潜在有效系统。

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