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首页> 外文期刊>Journal of Materials Chemistry, B. materials for biology and medicine >Synthesis of alpha-amino-lipophosphonates as cationic lipids or co-lipids for DNA transfection in dendritic cells
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Synthesis of alpha-amino-lipophosphonates as cationic lipids or co-lipids for DNA transfection in dendritic cells

机译:作为阳离子脂质的合成α-氨基 - 脂磷酸盐或树突细胞中DNA转染的共脂质

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Cationic lipid/co-lipid combinations have been extensively explored in gene delivery as alternatives to viral vectors. To be established as a gold standard of chemical vectors, considerable improvement in their transfection efficiency is however required. Herein, we report a simple procedure to synthesize new cationic lipids and co-lipids for the DNA transfection of dendritic cells (DCs). Seven alpha-amino-lipophosphonates featuring two aza-heterocycles with protonable sites (imidazole or pyridine) were synthesized and used as co-lipids in liposomes with cationic lipids. For each liposome, the cationic lipid is either an imidazolium lipophosphoramidate (lipid 2) or an alpha-amino-lipophosphonate containing a basic tertiary aliphatic amine in the polar head group (lipid 3b). The cationic lipids either with new co-lipids or DOPE formed positively charged nano-sized stable liposomes that effectively interact with plasmid DNA (pDNA) to produce lipoplexes. Membrane fusion studies showed that alpha-amino-phosphonates featuring an imidazole moiety in the polar head group exhibited higher fusion at pH 5.5 than pH 7.4. This study suggests that the best formulations for the transfection of DCs (based on the % transfected cells and the intensity of EGFP-based fluorescence) are lipid 2 associated with either 3a, 3d or DOPE and cationic lipid 3b formulated with 3a or DOPE as a helper lipid. Furthermore, lipid 3a could be used as an alternative to DOPE as a helper lipid. Overall, these results indicate that novel imidazole containing alpha-aminophosphonates can serve as effective transfection agents for DC-based vaccines.
机译:在基因递送中被广泛探索阳离子脂/共脂质组合作为病毒载体的替代品。然而,建立为化学载体的黄金标准,然而,需要相当大的转染效率的改善。在此,我们报告了一种简单的方法,用于合成用于树突细胞(DCS)的DNA转染的新阳离子脂质和共脂质。七种α-氨基 - 脂族磷酸酯以两种Aza-杂环为具有蛋白质位点(咪唑或吡啶),并用作脂质脂质的脂质体中的共脂质。对于每个脂质体,阳离子脂质是咪唑鎓脂磷酰胺(脂质2)或含有在极性头部(脂质3B)中的碱性叔脂胺的α-氨基 - 脂磷酸盐。阳离子脂质用新的共脂质或涂料形成带正电荷的纳米尺寸稳定的脂质体,其有效地与质粒DNA(PDNA)相互作用以产生唇膜。膜融合研究表明,α-氨基 - 膦酸盐在极性头部组中具有咪唑部分的氨基膦酸盐在pH5.5的pH 5.5处表现出更高的熔融。该研究表明,DC转染的最佳配方(基于百分比转染的细胞和EGFP的荧光强度)是与3A,3D或涂料和用3A或涂料配制的阳离子脂质3B相关的脂质2帮手脂质。此外,脂质3a可用作作为辅助脂质的替代物的替代物。总体而言,这些结果表明含有α-氨基膦酸盐的新型咪唑可以用作基于DC的疫苗的有效转染剂。

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