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用于可控胰岛素递送的功能化可注射水凝胶

Functionalized injectable hydrogels for controlled insulin delivery.

作者信息

Huynh Dai P, Nguyen Minh K, Pi Bong S, Kim Min S, Chae Su Y, Lee Kang C, Kim Bong S, Kim Sung W, Lee Doo S

机构信息

Department of Polymer Science and Engineering, Sungkyunkwan University, Suwon, Gyeonggi 440-746, Republic of Korea.

出版信息

Biomaterials. 2008 Jun;29(16):2527-34. doi: 10.1016/j.biomaterials.2008.02.016. Epub 2008 Mar 10.

DOI:10.1016/j.biomaterials.2008.02.016
PMID:18329707
Abstract

The concept of this research is using poly(beta-amino ester) (PAE) as a duo-functional group for synthesis of the novel sensitive injectable hydrogel for controlled drug/protein delivery. Firstly, PAE made of 1,4-butanediol diacrylate and 4,4'-trimethylene dipiperidine is used as a pH-sensitive moiety to conjugate to the temperature-sensitive biodegradable triblock copolymer of poly(ethylene glycol)-poly(epsilon-caprolactone) (PCL-PEG-PCL) to manufacture pH/temperature-sensitive injectable hydrogel of pentablock copolymer PAE-PCL-PEG-PCL-PAE. Furthermore, the cationic nature of PAE is used as the second function to make the ionic complexes with anionic biomolecule loaded into the hydrogel such as insulin. As a result, the release of drug/protein from this hydrogel device can be controlled by the degradation of copolymer. Sol-gel phase transition behavior of PAE-PCL-PEG-PCL-PAE block copolymer was investigated; the results showed that the aqueous media of the pentablock copolymer changed from a sol to a gel phase with increasing temperature and pH. The effect of anionic biomolecule such as insulin on sol-gel phase transition, degradation of the complex gel of the material with insulin was studied in vitro. Then the schematic of the ionic complexes between positive charges in PAE and the negatively charges in protein was simulated. In addition, the mechanism of controlled release behavior of insulin from the complex gel was supposed, which includes the chemically-controlled and diffusion-controlled stages. To prove the simulations, the cumulative release of the protein from the complex gel was investigated in vitro with different methods. Furthermore, the pharmacokinetic release of insulin from the complex gel in vivo on male Sprague-Dawley (SD) rats was compared with that from triblock copolymer hydrogel of PCL-PEG-PCL.

摘要

本研究的概念是使用聚(β-氨基酯)(PAE)作为双功能基团,合成用于药物/蛋白质控释的新型敏感可注射水凝胶。首先,由1,4-丁二醇二丙烯酸酯和4,4'-三亚甲基二哌啶制成的PAE用作pH敏感部分,与聚(乙二醇)-聚(ε-己内酯)(PCL-PEG-PCL)的温度敏感可生物降解三嵌段共聚物共轭,以制备五嵌段共聚物PAE-PCL-PEG-PCL-PAE的pH/温度敏感可注射水凝胶。此外,PAE的阳离子性质用作第二个功能,与负载在水凝胶中的阴离子生物分子(如胰岛素)形成离子复合物。结果,药物/蛋白质从该水凝胶装置中的释放可以通过共聚物的降解来控制。研究了PAE-PCL-PEG-PCL-PAE嵌段共聚物的溶胶-凝胶相变行为;结果表明,随着温度和pH值的升高,五嵌段共聚物的水性介质从溶胶相转变为凝胶相。体外研究了阴离子生物分子如胰岛素对溶胶-凝胶相变、该材料与胰岛素的复合凝胶降解的影响。然后模拟了PAE中正电荷与蛋白质中负电荷之间离子复合物的示意图。此外,推测了胰岛素从复合凝胶中控制释放行为的机制,包括化学控制和扩散控制阶段。为了验证模拟结果,采用不同方法体外研究了复合凝胶中蛋白质的累积释放。此外,还比较了复合凝胶中胰岛素在雄性Sprague-Dawley(SD)大鼠体内的药代动力学释放与PCL-PEG-PCL三嵌段共聚物水凝胶的药代动力学释放。

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