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In Situ Incorporation of Praziquantel in Polymer Microparticles through Suspension Polymerization for Treatment of Schistosomiasis

机译:通过悬浮聚合法将吡喹酮原位掺入聚合物微粒中以治疗血吸虫病

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摘要

Schistosomiasis is one of the major public health problems worldwide. Even though this is a common illness among preschool children in poor countries, treatment is carried out mainly through the administration of praziquantel tablets, which has some disadvantages, such as the strong bitter taste. As an alternative to overcome this problem, the development of new encapsulated praziquantel formulations is demanded. For this reason, suspension polymerizations are carried out for the in situ encapsulation of praziquantel into polymer microparticles, using methyl methacrylate (MMA) and cationic compounds (diethylaminoethyl methacrylate, DEAEMA, and dimethylaminoethyl methacrylate, DMAEMA) as comonomers. This technique allows for the preparation of polymer microparticles with high encapsulation efficiencies (90%) with characteristic sizes ranging from 0.5 to 1500 mu m. Drug release profiles show that praziquantel is released from poly(methyl methacrylate) microparticles slowly due to the existence of strong diffusional resistance. On the other hand, the addition of cationic comonomers renders polymer particles sensitive to pH variations, allowing for faster release of praziquantel in acidic environments, as found in the stomach.
机译:血吸虫病是全球主要的公共卫生问题之一。尽管这是贫穷国家学龄前儿童中的常见疾病,但治疗主要还是通过吡喹酮片来进行的,吡喹酮片具有一些缺点,例如浓烈的苦味。作为克服该问题的替代方案,需要开发新的封装的吡喹酮制剂。为此,使用甲基丙烯酸甲酯(MMA)和阳离子化合物(甲基丙烯酸二乙氨基乙酯,DEAEMA和甲基丙烯酸二甲氨基乙酯,DMAEMA)作为共聚单体,进行悬浮聚合以将吡喹酮原位包封到聚合物微粒中。该技术允许制备具有0.5至1500μm的特征尺寸的高封装效率(> 90%)的聚合物微粒。药物释放曲线表明吡喹酮由于存在较强的扩散阻力而从聚甲基丙烯酸甲酯微粒中缓慢释放出来。另一方面,阳离子共聚单体的添加使聚合物颗粒对pH值变化敏感,从而使吡喹酮在酸性环境下(如在胃中)更快地释放。

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