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首页> 外文期刊>International Journal of Pharmaceutical Sciences Review and Research >Development and In-Vitro Evaluation of Sustained Release Gastroretentive Microspheric Drug Delivery System of Ciprofloxacin Hydrochloride
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Development and In-Vitro Evaluation of Sustained Release Gastroretentive Microspheric Drug Delivery System of Ciprofloxacin Hydrochloride

机译:盐酸环丙沙​​星缓释胃肠滞留微球给药系统的开发和体外评价

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The goal of this paper is to develop an alginate-based matrix device to control the release rate of a very poorly soluble drug such as nimesulide for 12h. The molecular weight and degree of substitution of the polymer were determined by capillary viscometry and conductimetry, respectively. The compaction behavior was determined using the Heckel and Leuenberger analyses. The intrinsic dissolution was conducted on an Apparatus II dissolutor using a pH 6.8 phosphate buffer. Matrixes containing 100 mg of nimesulide and different levels of sodium alginate and electrolytes or surfactants were made on a single punch tablet machine. Matrixes containing benzalconium chloride at levels >300mg improved the solubility and the release profile of nimesulide. Conversely, sorbitan laurate, sodium lauryl sulfate and electrolytes such as sodium chloride failed to improve the release rate of nimesulide from the hydrophilic matrix. The release characteristics of nimesulide from these matrixes were best described by the Korschmeyer- Peppas model. The alginate-based system containing benzalconium chloride has a potential to improve and control the release characteristics of nimesulide within 12h.
机译:本文的目的是开发一种基于藻酸盐的基质装置,以控制难溶性药物(如尼美舒利)的释放速率,持续12h。分别通过毛细管粘度测定法和电导率测定法测定聚合物的分子量和取代度。使用Heckel和Leuenberger分析确定压实行为。固有溶解是使用pH 6.8磷酸盐缓冲液在仪器II溶解器上进行的。在单冲片机上制备包含100 mg尼美舒利和不同含量的海藻酸钠以及电解质或表面活性剂的基质。含量大于300mg的苯扎氯铵的基质改善了尼美舒利的溶解度和释放特性。相反,脱水山梨糖醇月桂酸酯,十二烷基硫酸钠和诸如氯化钠的电解质不能提高尼美舒利从亲水性基质中的释放速率。尼美舒利从这些基质中的释放特征最好用Korschmeyer-Peppas模型来描述。含有苯扎氯铵的藻酸盐基体系具有改善和控制尼美舒利在12小时内释放特性的潜力。

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