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[肺靶向阿奇霉素脂质体的制备及其在小鼠体内的组织分布]

[Preparation of lung targeting azithromycin liposomes and its tissue distribution in mice].

作者信息

Wang Jian-song, Zhu Jia-bi, Lu Rui-qin, Shen Wei

机构信息

Institute of Pharmaceutics, China Pharmaceutical University, Nanjing 210009, China.

出版信息

Yao Xue Xue Bao. 2005 Mar;40(3):274-8.

Abstract

AIM

To prepare lung targeting azithromycin cationic liposomes and to observe its tissue distribution in mice.

METHODS

The azithromycin cationic liposomes were prepared by thin film method with freeze-thawing steps. HPLC method was established and validated for the determination of azithromycin in tissues of mice.

RESULTS

The particle size of the liposomes was 6.582 microm with zeta potential of +19.5 mV. The entrapment efficiency was more than 75%. The liposomes was stable in 6 months stored at 4 degrees C. The release in vitro was characterized by Higuchi equation. Azithromycin liposomes and free azithromycin solution were injected intravenously at a dose of 80 mg x kg(-1) to mice. Compared with solution, liposomes were characterized by slower clearance, increased half-life and the AUC increased by 7.4 fold in lung.

CONCLUSION

Thin film method with freeze-thawing steps could increase the entrapment efficiency and increase the particle size of azithromycin liposomes. After modification of lipid membrane with stearylamine, the cationic liposomes were prepared. The azithromycin concentration and AUC increased in lung after iv administration to mice of the cationic liposomes. This offered a good information for preparing liposomes targeting on the lung.

摘要

目的

制备肺靶向阿奇霉素阳离子脂质体并观察其在小鼠体内的组织分布。

方法

采用薄膜法结合冻融步骤制备阿奇霉素阳离子脂质体。建立并验证了用高效液相色谱法测定小鼠组织中阿奇霉素的方法。

结果

脂质体粒径为6.582微米,ζ电位为+19.5毫伏。包封率大于75%。脂质体在4℃储存6个月稳定。体外释放符合Higuchi方程。将阿奇霉素脂质体和游离阿奇霉素溶液以80毫克·千克⁻¹的剂量静脉注射给小鼠。与溶液相比,脂质体的特点是清除较慢、半衰期延长,肺中的AUC增加了7.4倍。

结论

薄膜法结合冻融步骤可提高阿奇霉素脂质体的包封率并增大粒径。用硬脂胺修饰脂质膜后制备了阳离子脂质体。静脉注射给小鼠阳离子脂质体后,肺中阿奇霉素浓度和AUC增加。这为制备肺靶向脂质体提供了良好的信息。

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