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首页> 外文期刊>International Journal of Genetics and Genomics >The Insertion Timing of PEGylated Lipids to Galactosylated Lipoplexes Is Important for Liver-Selective Transfection in Mice
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The Insertion Timing of PEGylated Lipids to Galactosylated Lipoplexes Is Important for Liver-Selective Transfection in Mice

机译:聚乙二醇化脂质向半乳糖化脂质复合体的插入时间对于小鼠肝脏选择性转染很重要

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In the present study, we demonstrated the importance of PEGylation timing of galactosylated liposome/plasmid DNA (pDNA) complexes (lipoplexes) for liver-selective transfection in mice. Because a fenestrated endothelium can be a barrier for penetration of lipoplexes though sinusoids, the particle size of lipoplexes is one of the determining factors for in vivo liver parenchymal cell (hepatocyte, PC)-selective transfection. Here, we found that syn-insertion, as a novel PEGylation timing, was useful to control the particle size of galactosylated lipoplexes. Syn-insertion of PEGylated lipids was performed by simple mixing of pDNA solution containing PEGylated lipids and dispersion of the cationic liposomes. Both syn- and pre-insertion of PEGylated lipids decreased the particle size of lipoplexes, whereas post-insertion did not. Moreover, syn-insertion of PEGylated lipids to galactosylated lipoplexes improved liver selectivity and the PCon-parenchymal cell ratio of transgene expression after intravenous injection in mice. Hence, these data will be valuable for the design and preparation of PEGylated lipoplexes for gene targeting.
机译:在本研究中,我们证明了半乳糖基化脂质体/质粒DNA(pDNA)复合物(lipoplexes)的PEG化时间对于小鼠肝选择性转染的重要性。因为有孔的内皮可能是脂质复合物通过正弦波渗透的障碍,所以脂质复合物的粒径是体内肝实质细胞(肝细胞,PC)选择性转染的决定因素之一。在这里,我们发现同位插入作为一种新的聚乙二醇化时机,可用于控制半乳糖基化脂质复合物的粒径。通过简单地混合含有PEG化脂质的pDNA溶液和分散阳离子脂质体来进行PEG化脂质的同插入。聚乙二醇化脂质的顺式插入和插入前均可降低脂质复合物的粒径,而插入后则不会。此外,在小鼠静脉内注射后,将聚乙二醇化脂质与半乳糖基化脂质复合物的共插入改善了肝选择性和转基因表达的PC /非实质细胞比率。因此,这些数据对于用于基因靶向的聚乙二醇化脂复合物的设计和制备将是有价值的。

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