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首页> 外文期刊>International Journal of Pharmaceutics >Polymer-cysteamine conjugates: new mucoadhesive excipients for drug delivery?
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Polymer-cysteamine conjugates: new mucoadhesive excipients for drug delivery?

机译:聚合物-半胱胺结合物:用于药物递送的新型粘膜粘附赋形剂?

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In the present study, the features of two new thiolated polymers--the so-called thiomers--were investigated. Mediated by a carbodiimide cysteamine was covalently attached to sodium carboxymethylcellulose (Na-CMC) and neutralised polycarbophil (Na-PCP). Depending on the weight-ratio polymer to cysteamine during the coupling reaction, the resulting CMC-cysteamine conjugate and PCP-cysteamine conjugate showed in maximum 43 +/- 15 and 138 +/- 22 micromole thiol groups per g polymer (mean +/- S.D.; n=3), respectively, which were used for further characterisation. Tensile studies carried out with the CMC-cysteamine conjugate on freshly excised porcine intestinal mucosa displayed no significantly (P<0.01) improved mucoadhesion, whereas, the mucoadhesive properties of the PCP-cysteamine conjugate were increased 2.5-fold compared with the unmodified polymer. The swelling behaviour of the CMC-cysteamine conjugate was uninfluenced by the covalent attachment of the sulfhydryl compound. In contrast the swelling behaviour of the PCP-cysteamine conjugate was improved significantly (P<0.01) versus unmodified PCP. Furthermore, in aqueous solutions the disintegration time of tablets based on the CMC- and PCP-cysteamine conjugates was prolonged 1.5 and 3.2-fold, respectively, in comparison to tablets containing the corresponding unmodified polymers. According to these results, especially the PCP-cysteamine conjugate represents a promising new pharmaceutical excipient for various drug delivery systems.
机译:在本研究中,研究了两种新的硫醇化聚合物(所谓的硫代聚合物)的特征。由碳二亚胺半胱胺介导的共价连接到羧甲基纤维素钠(Na-CMC)和中和的聚卡波非(Na-PCP)。取决于偶联反应期间聚合物与半胱胺的重量比,所得的CMC-半胱胺共轭物和PCP-半胱胺共轭物显示每克聚合物最大43 +/- 15和138 +/- 22微摩尔硫醇基团(平均值+/- SD; n = 3),分别用于进一步表征。用CMC-半胱胺缀合物对新鲜切除的猪肠粘膜进行的拉伸研究显示,粘膜粘附没有明显改善(P <0.01),而与未修饰的聚合物相比,PCP-半胱胺缀合物的粘膜粘附特性​​提高了2.5倍。巯基化合物的共价连接不会影响CMC-半胱胺共轭物的溶胀行为。相反,与未修饰的PCP相比,PCP-半胱胺缀合物的溶胀行为得到了显着改善(P <0.01)。此外,与含有相应的未修饰的聚合物的片剂相比,在水溶液中基于CMC-和PCP-半胱胺缀合物的片剂的崩解时间分别延长了1.5倍和3.2倍。根据这些结果,尤其是PCP-半胱胺缀合物代表了用于各种药物递送系统的有希望的新药物赋形剂。

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