首页> 美国卫生研究院文献>International Journal of Nanomedicine >Ketoprofen-loaded polymer carriers in bigel formulation: an approach to enhancing drug photostability in topical application forms
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Ketoprofen-loaded polymer carriers in bigel formulation: an approach to enhancing drug photostability in topical application forms

机译:Bigel配方中负载酮洛芬的聚合物载体:在局部应用形式中增强药物光稳定性的方法

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摘要

The purpose of the study was to investigate the stability and biopharmaceutical characteristics of ketoprofen, loaded in polymeric carriers, which were included into a bigel in a semisolid dosage form. The polymer carriers with in situ-included ketoprofen were obtained by emulsifier-free emulsion polymerization of the monomers in aqueous medium or a solution of the polymers used. The morphological characteristics of the carriers, the in vitro release and the photochemical stability of ketoprofen were evaluated. The model with optimal characteristics was included in a bigel formulation. The bigel was characterized in terms of pH, rheological behavior, spreadability, and in vitro drug release. Acute skin toxicity, antinociceptive activity, anti-inflammatory activity, and antihyperalgesic effects of the prepared bigel with ketoprofen-loaded polymer carrier were evaluated. The carriers of ketoprofen were characterized by a high yield and drug loading. The particle size distribution varied widely according to the polymer used, and a sustained release was provided for up to 6 hours. The polymer mixture poly(vinyl acetate) and hydroxypropyl cellulose as a drug carrier, alone or included in the bigel composition, improved the photostability of the drug compared with unprotected ketoprofen. The bigel with ketoprofen-loaded particles provided sustained release of the drug and had optimal rheological parameters. In vivo experiments on the bigel showed no skin inflammation or irritation. Four hours after its application, a well-defined analgesic, anti-inflammatory, and antihyperalgesic effect was registered. The polymer mixture of poly(vinyl acetate) and hydroxypropyl cellulose as a carrier of ketoprofen and the bigel in which it was included provided an enhanced photostability and sustained drug release.
机译:该研究的目的是研究负载在聚合物载体中的酮洛芬的稳定性和生物药物特性,该载体以半固体剂型包含在双药中。通过在水性介质或所用聚合物的溶液中进行单体的无乳化剂乳液聚合来获得具有原位包含酮洛芬的聚合物载体。评价了载体的形态特征,酮洛芬的体外释放和光化学稳定性。具有最佳特性的模型包含在bigel公式中。该比吉尔在pH,流变行为,铺展性和体外药物释放方面具有特征。评价了制备的含酮洛芬的聚合物载体的bigel的急性皮肤毒性,抗伤害感受活性,抗炎活性和抗痛觉过敏作用。酮洛芬的载体具有高收率和载药量的特点。粒度分布根据所用聚合物的不同而有很大差异,并提供了长达6小时的持续释放。与未保护的酮洛芬相比,单独或包括在bigel组合物中的聚合物混合物聚乙酸乙烯酯和羟丙基纤维素作为药物载体,改善了药物的光稳定性。具有酮洛芬负载颗粒的双环提供了药物的持续释放,并具有最佳的流变参数。在Bigel上的体内实验显示没有皮肤发炎或刺激。施用四小时后,记录到了明确的止痛,抗炎和抗痛觉过敏作用。聚(乙酸乙烯酯)和羟丙基纤维素的聚合物混合物作为酮洛芬的载体,并且其中包括的双环提供增强的光稳定性和持续的药物释放。

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