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首页> 外文期刊>Journal of drug targeting >Preparation of liposomes containing zedoary turmeric oil using freeze-drying of liposomes via TBA/water cosolvent systems and evaluation of the bioavailability of the oil
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Preparation of liposomes containing zedoary turmeric oil using freeze-drying of liposomes via TBA/water cosolvent systems and evaluation of the bioavailability of the oil

机译:通过TBA /水助溶剂系统冻干脂质体,制备含Zedoary姜黄油的脂质体,并评估该油的生物利用度

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摘要

The purpose of this study was to enhance the absorption of zedoary turmeric oil (ZTO) in vivo and develop new formulations of a water-insoluble oily drug. This study described a method for preparing ZTO liposomes, which involved freeze-drying (FD) of liposomes with TBA/water cosolvent systems. The TBA/ water cosolvent systems were used to investigate a feasible method of liposomes manufacture; the two factors, sugar/lipid mass ratio and TBA content (concentration), of the preparation process were evaluated in this study. The results showed that the addition of TBA content could significantly enhance the sublimation of ice resulting in short FD cycles time, and reduce the entrapment efficiency of liposomes. In addition, the residual TBA solvents levels were determined to be less than 0.37% under all optimum formulations and processing conditions. Several physical properties of liposomes were examined by H-600 transmission electron microscope (TEM) and zetamaster analyser system.The results revealed that the liposomes were smooth and spherical with an average particle size of 457+-7.8nm and the zeta potential was more than 3.65 Mv. The bioavailability of the liposomes was evaluated in rabbits, compared with the conventional self-emulsifying formulation for oral administration. Compared with the conventional self-emulsifying formulation, the plasma concentration-time profiles with improved sustained-release characteristics were achieved after oral administration of the liposomes with a bioavailability of 257.7% (a good strategy for improving the bioavailability of an oily drug). In conclusion, the present experimental findings clearly demonstrated the usefulness of ZTO liposome vesicles in improving therapeutic efficacy by enhancing oral bioavailability. Our study offered an alternative method for designing sustained-release preparations of oily drugs.
机译:这项研究的目的是增强Zedoary姜黄油(ZTO)在体内的吸收,并开发一种不溶于水的油性药物的新配方。这项研究描述了一种制备ZTO脂质体的方法,该方法涉及使用TBA /水助溶剂系统冻干(FD)脂质体。使用TBA /水助溶剂系统研究脂质体生产的可行方法。本研究评估了糖/脂质质量比和TBA含量(浓度)这两个因素。结果表明,TBA含量的添加可以显着增强冰的升华,从而缩短FD循环时间,并降低脂质体的包封效率。此外,在所有最佳配方和加工条件下,残留的TBA溶剂含量均确定为小于0.37%。通过H-600透射电子显微镜(TEM)和zetamaster分析仪系统对脂质体的几种物理性质进行了研究,结果表明脂质体是光滑球形的,平均粒径为457 + -7.8nm,zeta电位大于3.65英里与用于口服的常规自乳化制剂相比,评估了在兔中脂质体的生物利用度。与常规的自乳化制剂相比,口服给予脂质体的血浆浓度-时间曲线具有改善的缓释特性,其生物利​​用度为257.7%(改善油性药物生物利用度的好策略)。总之,本实验发现清楚地证明了ZTO脂质体囊泡通过增强口服生物利用度来改善治疗效果的有效性。我们的研究为设计油性药物的缓释制剂提供了另一种方法。

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