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首页> 外文期刊>Biological & pharmaceutical bulletin >Evaluation of poly(vinyl alcohol)-gel spheres containing chitosan as dosage form to control gastrointestinal transit time of drugs.
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Evaluation of poly(vinyl alcohol)-gel spheres containing chitosan as dosage form to control gastrointestinal transit time of drugs.

机译:评估以壳聚糖为剂型的聚乙烯醇凝胶球体,以控制药物在胃肠道中的传播时间。

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Two types of poly(vinyl alcohol)-gel spheres were prepared with chitosan (CS/PVA-GS) and without chitosan (PVA-GS), and comparative studies were performed using these gel spheres (GSs). No change in particle size was observed by the addition of chitosan: nearly 45% of both particles were in the 5-10 microm range. In an in vivo gastrointestinal transit test, CS/PVA-GS prolonged the small-intestinal transit time more than PVA-GS. In an in vitro intestinal perfusion study, the mean transit time of these GSs was markedly reduced by pretreatment of the intestinal surface with a mucolytic agent, N-acetyl-L-cysteine, suggesting that the mucous layer on the intestinal surface plays an important role in controlling the transit rate of these GSs. The oral administration of aminophylline (theophylline) and ampicillin as model drugs incorporated in PVA-GS and CS/PVA-GS was examined in rats. While theophylline absorption from PVA-GS was not affected by the addition of chitosan, the improvement of ampicillin absorption by PVA-GS was enhanced by the chitosan combination.
机译:使用壳聚糖(CS / PVA-GS)和不使用壳聚糖(PVA-GS)制备了两种类型的聚乙烯醇-凝胶球,并使用这些凝胶球(GSs)进行了比较研究。通过加入壳聚糖,未观察到粒径变化:两种颗粒中几乎有45%在5-10微米范围内。在体内胃肠道转运试验中,CS / PVA-GS比PVA-GS延长了小肠转运时间。在体外肠道灌注研究中,通过使用粘液溶解剂N-乙酰基-L-半胱氨酸预处理肠道表面,这些GS的平均运输时间明显缩短,这表明肠道表面的黏液层起着重要的作用。控制这些GS的通过率。在大鼠中检查了氨茶碱(茶碱)和氨苄青霉素作为掺入PVA-GS和CS / PVA-GS中的模型药物的口服给药。虽然添加壳聚糖不会影响PVA-GS对茶碱的吸收,但壳聚糖组合可增强PVA-GS对氨苄青霉素吸收的改善。

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