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首页> 外文期刊>Journal of pharmaceutical sciences. >Biodistribution and pharmacokinetic analysis of long-circulating thiolated gelatin nanoparticles following systemic administration in breast cancer-bearing mice.
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Biodistribution and pharmacokinetic analysis of long-circulating thiolated gelatin nanoparticles following systemic administration in breast cancer-bearing mice.

机译:荷瘤小鼠全身给药后长循环硫代明胶纳米颗粒的生物分布和药代动力学分析。

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The objective of the present study was to modify thiolated gelatin nanoparticles with poly(ethylene glycol) (PEG) chains and examine their long circulating and tumor-targeting properties in vivo in an orthotopic a human breast adenocarcinoma xenograft model. The crosslinked nanoparticle systems were characterized to have a size of 150-250 nm with rapid payload release properties in a highly reducing environment. Upon PEG modification, the nanoparticle size increased to 300-350 nm in diameter. The presence of PEG chains on the surface was confirmed by characterization with electron spectroscopy for chemical analysis. The in vivo long-circulating potential, biodistribution and passive tumor targeting of the controls, and PEG-modified thiolated gelatin nanoparticles were evaluated by injecting indium-111 (111In)-labeled nanoparticles into breast tumor (MDA-MB-435)-bearing nude mice. Upon modification with PEG, the nanoparticles were found to have longer circulation times, with the plasma and tumor half-lives of 15.3 and 37.8 h, respectively. The results also showed preferential localization of thiolated nanoparticles in the tumor mass. The resulting nanoparticulate systems with long circulation properties could be used to target encapsulated drugs and genes to tumors passively by utilizing the enhanced permeability and retention effect of the tumor vasculature.
机译:本研究的目的是在原位人类乳腺癌细胞异种移植模型中,用聚乙二醇(PEG)链修饰硫醇化明胶纳米颗粒,并检查它们在体内的长循环和肿瘤靶向特性。交联的纳米粒子系统的特征是具有150-250 nm的尺寸,在高度还原的环境中具有快速的有效负载释放特性。 PEG修饰后,纳米粒子的直径增加到300-350 nm。通过用于电子分析的电子光谱表征证实了表面上PEG链的存在。通过将铟(111In)标记的纳米颗粒注射到带有乳腺肿瘤(MDA-MB-435)的裸鼠体内,评估了对照组和PEG修饰的硫醇化明胶纳米颗粒的体内长循环潜力,生物分布和被动靶向肿瘤老鼠。经PEG修饰后,发现纳米粒子具有更长的循环时间,血浆和肿瘤的半衰期分别为15.3和37.8小时。结果还显示,硫醇化纳米颗粒在肿瘤块中优先定位。通过利用增强的肿瘤脉管系统的通透性和保留作用,具有长循环特性的所得纳米颗粒系统可用于将包封的药物和基因被动地靶向肿瘤。

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