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丝素蛋白作为一种用于药物控释的有机聚合物。

Silk fibroin as an organic polymer for controlled drug delivery.

作者信息

Hofmann S, Foo C T Wong Po, Rossetti F, Textor M, Vunjak-Novakovic G, Kaplan D L, Merkle H P, Meinel L

机构信息

Drug Formulation and Delivery, ETH Zurich, 8093 Zurich, Switzerland.

出版信息

J Control Release. 2006 Mar 10;111(1-2):219-27. doi: 10.1016/j.jconrel.2005.12.009. Epub 2006 Feb 3.

DOI:10.1016/j.jconrel.2005.12.009
PMID:16458987
Abstract

The pharmaceutical utility of silk fibroin (SF) materials for drug delivery was investigated. SF films were prepared from aqueous solutions of the fibroin protein polymer and crystallinity was induced and controlled by methanol treatment. Dextrans of different molecular weights, as well as proteins, were physically entrapped into the drug delivery device during processing into films. Drug release kinetics were evaluated as a function of dextran molecular weight, and film crystallinity. Treatment with methanol resulted in an increase in beta-sheet structure, an increase in crystallinity and an increase in film surface hydrophobicity determined by FTIR, X-ray and contact angle techniques, respectively. The increase in crystallinity resulted in the sustained release of dextrans of molecular weights ranging from 4 to 40 kDa, whereas for less crystalline films sustained release was confined to the 40 kDa dextran. Protein release from the films was studied with horseradish peroxidase (HRP) and lysozyme (Lys) as model compounds. Enzyme release from the less crystalline films resulted in a biphasic release pattern, characterized by an initial release within the first 36 h, followed by a lag phase and continuous release between days 3 and 11. No initial burst was observed for films with higher crystallinity and subsequent release patterns followed linear kinetics for HRP, or no substantial release for Lys. In conclusion, SF is an interesting polymer for drug delivery of polysaccharides and bioactive proteins due to the controllable level of crystallinity and the ability to process the biomaterial in biocompatible fashion under ambient conditions to avoid damage to labile compounds to be delivered.

摘要

研究了丝素蛋白(SF)材料在药物递送方面的药用价值。丝素蛋白膜由丝素蛋白聚合物水溶液制备而成,通过甲醇处理诱导并控制其结晶度。在制成薄膜的过程中,不同分子量的葡聚糖以及蛋白质被物理包裹在药物递送装置中。药物释放动力学作为葡聚糖分子量和薄膜结晶度的函数进行了评估。甲醇处理导致β-折叠结构增加、结晶度增加以及薄膜表面疏水性增加,分别通过傅里叶变换红外光谱(FTIR)、X射线和接触角技术测定。结晶度的增加导致分子量范围为4至40 kDa的葡聚糖持续释放,而对于结晶度较低的薄膜,持续释放仅限于40 kDa的葡聚糖。以辣根过氧化物酶(HRP)和溶菌酶(Lys)作为模型化合物研究了蛋白质从薄膜中的释放。酶从结晶度较低的薄膜中释放呈现双相释放模式,其特征是在最初36小时内有初始释放,随后是一个滞后阶段,在第3天至第11天之间持续释放。对于结晶度较高的薄膜,未观察到初始爆发,随后的释放模式对于HRP遵循线性动力学,对于Lys则没有大量释放。总之,由于结晶度水平可控,并且能够在环境条件下以生物相容的方式加工生物材料以避免对要递送的不稳定化合物造成损害,SF是一种用于多糖和生物活性蛋白质药物递送的有趣聚合物。

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