首页> 外文期刊>International Journal of Pharmaceutics >Preparation, characterization, and biodistribution of letrozole loaded PLGA nanoparticles in Ehrlich Ascites tumor bearing mice.
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Preparation, characterization, and biodistribution of letrozole loaded PLGA nanoparticles in Ehrlich Ascites tumor bearing mice.

机译:载有来曲唑的PLGA纳米颗粒在携带Ehrlich腹水的荷瘤小鼠中的制备,表征和生物分布。

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摘要

Letrozole (LTZ) incorporated PLGA nanoparticles were prepared by solvent displacement technique and characterized by transmission electron microscopy, poly-dispersity index and zeta potential measurement. Radiolabeling of free LTZ and LTZ-loaded PLGA NPs was performed with technetium-99m with high labeling efficiency. The labeled complex showed good in vitro stability as verified by DTPA challenge test. The labeled complexes also showed significant in vivo stability when incubated in rat serum for 24 h. Biodistribution studies of (99m)Tc-labeled complexes were performed after intravenous administration in normal mice and Ehrlich Ascites tumor bearing mice. Compared to free LTZ, LTZ-loaded PLGA NPs exhibited significantly lower uptake by the organs of RES. The tumor concentration of LTZ-loaded PLGA NPs was 4.65 times higher than that of free LTZ at 4 h post-injection. This study indicates the capability of PLGA nanopartcles in enhancing the tumor uptake of letrozole.
机译:通过溶剂置换技术制备了掺入来曲唑(LTZ)的PLGA纳米粒子,并通过透射电子显微镜,多分散指数和ζ电势测量进行了表征。使用tech 99m进行游离LTZ和装载LTZ的PLGA NP的放射性标记,标记效率很高。标记的复合物显示出良好的体外稳定性,如DTPA激发试验所证实。当在大鼠血清中孵育24小时时,标记的复合物也显示出显着的体内稳定性。 (99m)Tc标记的复合物的生物分布研究是在正常小鼠和携带Ehrlich腹水的荷瘤小鼠中静脉内给药后进行的。与自由LTZ相比,装载LTZ的PLGA NP表现出RES器官的摄取显着降低。注射LTH的PLGA NPs在注射后4 h的肿瘤浓度是游离LTZ的4.65倍。这项研究表明PLGA纳米颗粒增强来曲唑对肿瘤的吸收能力。

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