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Bioavailability Enhancement of Paclitaxel via a Novel Oral Drug Delivery System: Paclitaxel-Loaded Glycyrrhizic Acid Micelles

机译:通过新型口服药物递送系统增强紫杉醇的生物利用度:载有紫杉醇的甘草酸胶束

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摘要

Paclitaxel (PTX, taxol), a classical antitumor drug against a wide range of tumors, shows poor oral bioavailability. In order to improve the oral bioavailability of PTX, glycyrrhizic acid (GA) was used as the carrier in this study. This was the first report on the preparation, characterization and the pharmacokinetic study in rats of PTX-loaded GA micelles The PTX-loaded micelles, prepared with ultrasonic dispersion method, displayed small particle sizes and spherical shapes. Differential scanning calorimeter (DSC) thermograms indicated that PTX was entrapped in the GA micelles and existed as an amorphous state. The encapsulation efficiency was about 90%, and the drug loading rate could reach up to 7.90%. PTX-loaded GA micelles displayed a delayed drug release compared to Taxol in the in vitro release experiment. In pharmacokinetic study via oral administration, the area under the plasma concentration-time curve (AUC(0 -> 24 h)) of PTX-loaded GA micelles was about six times higher than that of Taxol (p < 0.05). The significant oral absorption enhancement of PTX from PTX-loaded GA micelles could be largely due to the increased absorption in jejunum and colon intestine. All these results suggested that GA would be a promising carrier for the oral delivery of PTX.
机译:紫杉醇(PTX,紫杉酚)是一种针对多种肿瘤的经典抗肿瘤药物,口服生物利用度较差。为了提高PTX的口服生物利用度,本研究以甘草酸(GA)为载体。这是有关PTX负载的GA胶束在大鼠体内的制备,表征和药代动力学研究的第一篇报道。用超声分散法制备的PTX负载的胶束具有较小的粒径和球形。差示扫描量热仪(DSC)热分析图表明,PTX被困在GA胶束中,并以非晶态存在。包封率约为90%,载药率可达7.90%。在体外释放实验中,与紫杉醇相比,载有PTX的GA胶束显示出延迟的药物释放。在口服给药的药代动力学研究中,PTX加载的GA胶束的血浆浓度-时间曲线下面积(AUC(0-> 24 h))比紫杉醇高约六倍(p <0.05)。从载有PTX的GA胶束中PTX的口服吸收显着增强可能主要是由于空肠和结肠肠道吸收的增加。所有这些结果表明,GA将是PTX口服给药的有希望的载体。

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