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The effect of molar mass and degree of hydroxyethylation on the controlled shielding and deshielding of hydroxyethyl starch-coated polyplexes

机译:摩尔质量和羟乙基化程度对羟乙基淀粉包覆的复合物的可控屏蔽和去屏蔽的影响

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PEGylation is currently the gold-standard in shielding cationic DNA-polyplexes against non-specific interaction with blood components. However, it reduces cellular uptake and transfection, in what is known as the "PEG-dilemma". In an approach to solve this problem we developed hydroxyethyl starch (HES)-shielded polyplexes which get deshielded under the action of alpha amylase (AA). In this study, the effect of molar mass and degree of hydroxyethylation on the shielding and deshielding of the polyplexes as well as their in vivo performance were investigated. For this purpose, a battery of HES-polyethylenimine (PEI) conjugates was synthesized, and their rate and extent of biodegradation were investigated using asymmetric flow-field flow fractionation (AF4) and quartz-crystal microbalance with dissipation (QCM-D). Additionally, the transfection efficiency of the polyplexes was tested in Neuro2A cells and tumor-bearing mice. AF4 and QCM results show a rapid degradation for HES with lower degrees of hydroxyethylation. Meanwhile, in vitro transfection experiments showed a better shielding for higher HES molar masses, as well as deshielding with a significant boost in transfection upon addition of AA. Finally, in vivo experiments showed that the biodegradable HES markedly reduced the non-specific lung transcription of the polyplexes, but maintained gene expression in the tumor, contrary to the non-degradable HES and PEG controls, which reduced both tumor and lung expression. This study shows that by controlling the molecular characteristics of HES it is possible to engineer the shielding and deshielding properties of the polyplexes for more efficient gene delivery. (C) 2013 Elsevier Ltd. All rights reserved.
机译:聚乙二醇化目前是屏蔽阳离子DNA多聚体与血液成分之间非特异性相互作用的金标准。但是,它减少了细胞摄取和转染,这就是所谓的“ PEG困境”。在解决该问题的方法中,我们开发了羟乙基淀粉(HES)保护的多链体,该复合体在α淀粉酶(AA)的作用下被去屏蔽。在这项研究中,研究了摩尔质量和羟乙基化程度对多链体的屏蔽和去屏蔽及其体内性能的影响。为此,合成了一组HES-聚乙烯亚胺(PEI)共轭物,并使用不对称流场流动分馏(AF4)和带耗散的石英晶体微天平(QCM-D)研究了它们的生物降解速率和程度。此外,在Neuro2A细胞和荷瘤小鼠中测试了多链体的转染效率。 AF4和QCM结果显示,羟乙基化程度较低的HES会迅速降解。同时,体外转染实验显示,对较高的HES摩尔质量有更好的屏蔽作用,并且在添加AA的情况下对转染有明显的促进作用。最后,体内实验表明,与不可降解的HES和PEG对照物同时降低肿瘤和肺部表达的情况相反,可生物降解的HES显着降低了多链体的非特异性肺转录,但维持了肿瘤中的基因表达。这项研究表明,通过控制HES的分子特性,可以设计多链体的屏蔽和去屏蔽特性,以实现更有效的基因传递。 (C)2013 Elsevier Ltd.保留所有权利。

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