首页> 外文期刊>Journal of drug targeting >Altered organ accumulation of oligonucleotides using polyethyleneimine grafted with poly(ethylene oxide) or pluronic as carriers.
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Altered organ accumulation of oligonucleotides using polyethyleneimine grafted with poly(ethylene oxide) or pluronic as carriers.

机译:使用聚乙烯亚胺与聚乙烯亚胺接枝用聚乙烯亚胺(环氧乙烷)或PLURONIC作为载体的改变器官积累。

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摘要

Passive targeting provides a simple strategy based on natural properties of the carriers to deliver DNA molecules to desired compartments. Polyethylenimine (PEI) is a potent non-viral system that has been known to deliver efficiently both plasmids and oligonucleotides (ODNs) in vitro. However, in vivo systemic administration of DNA/PEI complexes has encountered significant difficulties because these complexes are toxic and have low biodistribution in target tissues. This study evaluates PEI grafted with poly(ethylene oxide) (PEO(8K)-g-PEI(2K)) and PEI grafted with non-ionic amphiphilic block copolymer, Pluronic P85 (P85-g-PEI(2K)) as carriers for systemic delivery of ODNs. Following i.v. injection an antisense ODN formulated with PEO(8K)-g-PEI(2K) accumulated mainly in kidneys, while the same ODN formulated with P85-g-PEI(2K) was found almost exclusively in the liver. Furthermore, in the case of the animals injected with the P85-g-PEI(2K)-based complexes most of the ODN was found in hepatocytes, while only a minor portion of ODN was found in the lymphocyte/monocyte populations. The results of this study suggest that formulating ODN with PEO(8K)-g-PEI(2K) and P85-g-PEI(2K) carriers allows targeting of the ODN to the liver or kidneys, respectively. The variation in the tissue distribution of ODN observed with the two carriers is probably due to the different hydrophilic-lipophilic balance of the polyether chains grafted to PEI in these molecules. Therefore, polyether-grafted PEI carriers provide a simple way to enhance ODN accumulation in a desired compartment without the need of a specific targeting moiety.
机译:被动靶向提供了一种基于载体的自然特性的简单策略,以将DNA分子递送到所需隔室。聚乙烯亚胺(PEI)是一种有效的非病毒系统,已知在体外有效地提供质粒和寡核苷酸(ODN)。然而,在体内的DNA / PEI复合物施用DNA / PEI复合物中遇到了显着的困难,因为这些配合物有毒并且在靶组织中具有低生物分布。该研究评估了用聚(环氧乙烷)(PEO(8K)-G-PEI(2K))和用非离子两亲嵌段共聚物,Pluronic P85(P85-G-PEI(2K))接枝的PEI作为载体系统性交付ODN。遵循I.v.注射用PEO(8K)-G-PEI(2K)配制的反义ODN主要在肾脏中累积,而在肝脏中几乎仅发现用P85-G-PEI(2K)配制的相同ODN。此外,在注入P85-G-PEI(2K)的动物的情况下,基于肝细胞的大部分ODN在肝细胞中发现,而在淋巴细胞/单核细胞群中仅发现一小部分ODN。该研究的结果表明,使用PEO(8K)-G-PEI(2K)和P85-G-PEI(2K)载体的ODN分别允许分别针对肝脏或肾脏的靶向。用两种载体观察到的ODN组织分布的变化可能是由于在这些分子中移植到PEI的聚醚链的不同亲水性 - 亲脂性平衡。因此,聚醚接枝的PEI载体提供了一种简单的方法,以增强所需隔室中的ODN积累而不需要特异的靶向部分。

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