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使用低分子量凝胶剂水凝胶包封和释放喹啉衍生物

Entrapment and release of quinoline derivatives using a hydrogel of a low molecular weight gelator.

作者信息

Friggeri Arianna, Feringa Ben L, van Esch Jan

机构信息

Biomade Technology Foundation, Nijenborgh 4, 9747 AG Groningen, The Netherlands.

出版信息

J Control Release. 2004 Jun 18;97(2):241-8. doi: 10.1016/j.jconrel.2004.03.012.

DOI:10.1016/j.jconrel.2004.03.012
PMID:15196751
Abstract

Gels of low molecular weight gelators (LMWGs) are self-assembled, thermoreversible, viscoelastic materials which can also be rendered sensitive to light, pH or chemical substances by simple chemical modifications. In addition, the ability of some of these LMWGs to gelate water (hydrogelators) makes these gels interesting, new materials for drug delivery applications. In this paper, for the first time, a release study from LMWG gels is presented. This study concerns the release of small (model) drug molecules: 8-aminoquinoline (AQ) and 2-hydroxyquinoline (HQ), from gels of N,N'-dibenzoyl-L-cystine (DBC). DBC forms stable, clear gels in water, 150 mM NaCl solution and PBS (phosphate-buffered saline at pH 7.4) with gel-to-sol transition temperatures (Tgs) of 40-120 degrees C, depending on the gelator concentration (from 2.23 to 22.3 mM). The release of HQ from DBC gels was found to be approximately seven times faster than that of AQ and the initial release of the latter follows the kinetics of gel degradation. These observations indicate that AQ is preferentially retained in the gel, presumably as a result of stronger interactions with the gelator molecules (i.e. DBC-COO-+ H3N-AQ). These results indicate the potential of LMWG gels as delivery vehicles for small drug molecules and also show that the release profiles for such systems can be fine-tuned by the correct choice of gelator-drug combination.

摘要

低分子量凝胶剂(LMWGs)凝胶是自组装的、热可逆的、粘弹性材料,通过简单的化学修饰还可使其对光、pH值或化学物质敏感。此外,其中一些LMWGs形成水凝胶(水凝胶剂)的能力使这些凝胶成为用于药物递送应用的有趣新材料。本文首次展示了对LMWG凝胶的释放研究。该研究涉及小(模型)药物分子:8-氨基喹啉(AQ)和2-羟基喹啉(HQ)从N,N'-二苯甲酰-L-胱氨酸(DBC)凝胶中的释放。DBC在水、150 mM NaCl溶液和PBS(pH 7.4的磷酸盐缓冲盐水)中形成稳定、澄清的凝胶,凝胶-溶胶转变温度(Tgs)为40-120摄氏度,具体取决于凝胶剂浓度(2.23至22.3 mM)。发现HQ从DBC凝胶中的释放速度比AQ快约七倍,且后者的初始释放遵循凝胶降解动力学。这些观察结果表明,AQ优先保留在凝胶中,可能是由于与凝胶剂分子(即DBC-COO- + H3N-AQ)的相互作用更强。这些结果表明LMWG凝胶作为小药物分子递送载体的潜力,并且还表明通过正确选择凝胶剂-药物组合可以微调此类系统的释放曲线。

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