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利用分子印迹软性隐形眼镜开发眼部给药系统。

Development of ocular drug delivery systems using molecularly imprinted soft contact lenses.

作者信息

Tashakori-Sabzevar Faezeh, Mohajeri Seyed Ahmad

机构信息

Pharmaceutical Research Center, School of Pharmacy, Mashhad University of Medical Sciences , Mashhad , Iran.

出版信息

Drug Dev Ind Pharm. 2015 May;41(5):703-13. doi: 10.3109/03639045.2014.948451. Epub 2014 Aug 12.

Abstract

Recently, significant advances have been made in order to optimize drug delivery to ocular tissues. The main problems in ocular drug delivery are poor bioavailability and uncontrollable drug delivery of conventional ophthalmic preparations (e.g. eye drops). Hydrogels have been investigated since 1965 as new ocular drug delivery systems. Increase of hydrogel loading capacity, optimization of drug residence time on the ocular surface and biocompatibility with the eye tissue has been the main focus of previous studies. Molecular imprinting technology provided the opportunity to fulfill the above-mentioned objectives. Molecularly imprinted soft contact lenses (SCLs) have high potentials as novel drug delivery systems for the treatment of eye disorders. This technique is used for the preparation of polymers with specific binding sites for a template molecule. Previous studies indicated that molecular imprinting technology could be successfully applied for the preparation of SCLs as ocular drug delivery systems. Previous research, particularly in vivo studies, demonstrated that molecular imprinting is a versatile and effective method in optimizing the drug release behavior and enhancing the loading capacity of SCLs as new ocular drug delivery systems. This review highlights various potentials of molecularly imprinted contact lenses in enhancing the drug-loading capacity and controlling the drug release, compared to other ocular drug delivery systems. We have also studied the effects of contributing factors such as the type of comonomer, template/functional monomer molar ratio, crosslinker concentration in drug-loading capacity, and the release properties of molecularly imprinted hydrogels.

摘要

近年来,为优化眼部组织的药物递送已取得显著进展。眼部药物递送的主要问题是传统眼科制剂(如滴眼液)的生物利用度低和药物递送不可控。自1965年以来,水凝胶就作为新型眼部药物递送系统进行了研究。提高水凝胶载药量、优化药物在眼表的停留时间以及与眼组织的生物相容性一直是以往研究的主要重点。分子印迹技术为实现上述目标提供了契机。分子印迹软性隐形眼镜(SCL)作为治疗眼部疾病的新型药物递送系统具有很大潜力。该技术用于制备具有针对模板分子的特异性结合位点的聚合物。以往研究表明,分子印迹技术可成功应用于制备作为眼部药物递送系统的SCL。以往的研究,尤其是体内研究表明,分子印迹是优化药物释放行为和提高作为新型眼部药物递送系统的SCL载药量的一种通用且有效的方法。与其他眼部药物递送系统相比,本综述重点介绍了分子印迹隐形眼镜在提高载药量和控制药物释放方面的各种潜力。我们还研究了共聚单体类型、模板/功能单体摩尔比、交联剂浓度等影响因素对载药量以及分子印迹水凝胶释放性能的影响。

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