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SAS 工艺包载阿莫西林微球的聚合物包膜。

Polymer encapsulation of amoxicillin microparticles by SAS process.

机构信息

Department of Chemical Engineering and Food Technology, University of Cádiz , Puerto Real (Cádiz) , Spain.

出版信息

J Microencapsul. 2014;31(1):16-22. doi: 10.3109/02652048.2013.799242. Epub 2013 May 23.

Abstract

Encapsulation of amoxicillin (AMC) with ethyl cellulose (EC) by a supercritical antisolvent process (SAS) was investigated. AMC microparticles obtained previously by an SAS process were used as host particles and EC, a biodegradable polymer used for the controlled release of drugs, was chosen as the coating material. In this work, a suspension of AMC microparticles in a solution of ethyl cellulose in dichloromethane (DCM) was sprayed through a nozzle into supercritical CO2. Scanning electron microscopy (SEM), X-ray photoelectron spectroscopy (XPS) and HPLC analyses were carried out. The effects of AMC:EC ratio, the initial polymer concentration of the solution, temperature and pressure on the encapsulation process were investigated. Although all the experiments led to powder precipitation, the AMC encapsulation was achieved in only half of the cases, particularly when the lower drug:polymer ratios were assayed. In general, it was observed that the percentages of AMC present in the precipitates were higher on increasing the AMC:EC ratio. In these cases composites rather than encapsulates were obtained. The in vitro release profiles of the resulting materials were evaluated in order to ascertain whether composites can be used as encapsulated systems for drug delivery systems.

摘要

采用超临界抗溶剂法(SAS)将阿莫西林(AMC)包封在乙基纤维素(EC)中。先前通过 SAS 工艺获得的 AMC 微球被用作宿主颗粒,而 EC 是一种用于药物控制释放的可生物降解聚合物,被选为包覆材料。在这项工作中,将 AMC 微球在二氯甲烷(DCM)中的乙基纤维素溶液悬浮液通过喷嘴喷入超临界 CO2 中。进行了扫描电子显微镜(SEM)、X 射线光电子能谱(XPS)和 HPLC 分析。考察了 AMC:EC 比、溶液初始聚合物浓度、温度和压力对包封过程的影响。尽管所有实验都导致了粉末沉淀,但只有在一半的情况下实现了 AMC 的包封,特别是在测定较低的药物:聚合物比时。一般来说,随着 AMC:EC 比的增加,沉淀中存在的 AMC 百分比更高。在这些情况下,得到的是复合材料而不是包封物。评估了所得材料的体外释放曲线,以确定复合材料是否可以用作药物传递系统的包封系统。

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