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γ-环糊精水凝胶用于潜在眼部应用的交沙霉素的缓释。

γ-Cyclodextrin hydrogel for the sustained release of josamycin for potential ocular application.

机构信息

Institute for Biomedical Engineering, Rostock University Medical Center, Rostock, Germany.

Department of Ophthalmology, Rostock University Medical Center, Rostock, Germany.

出版信息

Drug Deliv. 2024 Dec;31(1):2361168. doi: 10.1080/10717544.2024.2361168. Epub 2024 Jun 20.

Abstract

Glaucoma is the leading cause of blindness worldwide. However, its surgical treatment, in particular via trabeculectomy, can be complicated by fibrosis. In current clinical practice, application of the drug, Mitomycin C, prevents or delays fibrosis, but can lead to additional side effects, such as bleb leakage and hypotony. Previous drug screening and testing has identified the known antibiotic, josamycin, as a possible alternative antifibrotic medication with potentially fewer side effects. However, a suitable ocular delivery mechanism for the hydrophobic drug to the surgical site does not yet exist. Therefore, the focus of this paper is the development of an implantable drug delivery system for sustained delivery of josamycin after glaucoma surgery based on crosslinked γ-cyclodextrin. γ-Cyclodextrin is a commonly used solubilizer which was shown to complex with josamycin, drastically increasing the drug's solubility in aqueous solutions. A simple γ-cyclodextrin crosslinking method produced biocompatible hydrogels well-suited for implantation. The crosslinked γ - cyclodextrin retained the ability to form complexes with josamycin, resulting in a 4-fold higher drug loading efficiency when compared to linear dextran hydrogels, and prolonged drug release over 4 days.

摘要

青光眼是全球致盲的主要原因。然而,其手术治疗,特别是通过小梁切除术,可能会出现纤维化并发症。在当前的临床实践中,应用丝裂霉素 C 药物可以预防或延缓纤维化,但也会导致其他副作用,如滤泡渗漏和低眼压。先前的药物筛选和测试已经确定了已知的抗生素,交沙霉素,作为一种潜在的具有较少副作用的替代抗纤维化药物。然而,对于疏水药物在手术部位的合适眼部给药机制尚未存在。因此,本文的重点是开发一种基于交联 γ-环糊精的植入式药物输送系统,用于在青光眼手术后持续输送交沙霉素。γ-环糊精是一种常用的增溶剂,已被证明可与交沙霉素形成复合物,极大地增加了药物在水溶液中的溶解度。一种简单的 γ-环糊精交联方法产生了适合植入的生物相容性水凝胶。交联的 γ-环糊精保留了与交沙霉素形成复合物的能力,与线性葡聚糖水凝胶相比,药物负载效率提高了 4 倍,药物释放时间延长了 4 天以上。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/50bc/11191840/fb27fa3a22cc/IDRD_A_2361168_UF0001_C.jpg

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