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基于丙二酸酰胺骨架的新型阳离子脂质体:转染效率和细胞毒性性质。

Novel cationic lipids based on malonic acid amides backbone: transfection efficacy and cell toxicity properties.

机构信息

Institute of Pharmacy, Department of Biochemical Pharmacy, Martin-Luther-University, Wolfgang-Langenbeck-Strasse 4, 06120 Halle (Saale), Germany.

出版信息

Bioconjug Chem. 2010 Apr 21;21(4):696-708. doi: 10.1021/bc9004624.

Abstract

Gene delivery using nonviral approaches has been extensively studied as a basic tool for intracellular gene transfer. Despite intensive research activity, the aim of creating a vector which meets all necessary demands has still not been reached. One possibility to solve the nonviral vector associated problem of low transfection efficacy is the development of new cationic amphiphiles. Therefore, the non-glycerol-based cationic lipids 1-9 have been synthesized and tested for in vitro gene delivery experiments. The backbone structure of the lipids consists of a malonic acid diamide with two long hydrophobic chains. The degree of saturation of the hydrophobic chains and the structure of the polar cationic headgroup were varied. The preparation follows an easy process and facilitates the trouble-free insertion of different alkyl chains. By studying in vitro gene delivery an increase of transfection efficacy was observed when using at least one unsaturated alkyl chain in the hydrophobic part and lysine or bis(2-aminoethyl)aminoethylamid as hydrophilic headgroup. This leads to cationic lipids exhibiting comparable or even higher transfection efficacies compared to the commercially available LipofectAmine and SuperFect.

摘要

使用非病毒方法进行基因传递已被广泛研究作为细胞内基因转移的基本工具。尽管研究活动很活跃,但仍未达到创建满足所有必要要求的载体的目标。解决非病毒载体转染效率低的问题的一种可能性是开发新的阳离子两亲物。因此,已经合成了非基于甘油的阳离子脂质 1-9 并测试了它们的体外基因传递实验。脂质的骨架结构由具有两个长疏水性链的丙二酸二酰胺组成。疏水性链的饱和度和极性阳离子头基的结构都有所不同。该制备方法简单,便于轻松插入不同的烷基链。通过研究体外基因传递,当在疏水性部分中使用至少一个不饱和烷基链和赖氨酸或双(2-氨基乙基)氨基乙基酰胺作为亲水头基时,观察到转染效率的增加。这导致阳离子脂质表现出与市售的 LipofectAmine 和 SuperFect 相当或甚至更高的转染效率。

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