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Screening PEGylated polyethylenimine derivatives for safe and efficient delivery of gene materials

机译:筛选聚乙二醇化聚乙烯亚胺衍生物以安全有效地传递基因材料

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Gene-based therapy has broad and important clinical applications, and the non-viral vector delivery of exogenous nucleic acids is commonly used for gene therapy. Among the numerous gene delivery vectors, the cationic polymer vectors are considered to be the most promising materials for gene delivery and gene therapy. In this study, we chemically modified a novel cross-linked PEI derivative PEI-Et through PEGylation, as PEGylation can reduce the cytotoxicity of PEI-Et by shielding the excess positive surface charge of PEI-Et. To screen out an optimal molar ratio of PEI-Et to PEG for efficient delivery of gene materials, we first synthesized three kinds of PEG-Et cationic polymers with different molar ratios (1 : 1, 2 : 1, 1 : 2) of PEI-Et to PEG, then we prepared and characterized the PEG-Et/DNA complexes and PEG-Et/siRNA complexes, and finally we tested the cytotoxicity and transfection efficiency of the PEG-Et/DNA complexes as well as the gene silencing efficiency of the PEG-Et/siRNA complexes. The results suggest that the gene vector PEG-Et 1 : 1 (with a 1 : 1 molar ratio of PEI-Et to PEG) was the best among the three types of PEG-Et (PEG-Et 1 : 1, PEG-Et 2 : 1, and PEG-Et 1 : 2) for condensing DNA and siRNA into nanoparticles, as it has significant lower cytotoxicity, higher gene transfection and siRNA silencing efficiency.
机译:基于基因的疗法具有广泛而重要的临床应用,并且外源核酸的非病毒载体递送通常用于基因疗法。在众多基因递送载体中,阳离子聚合物载体被认为是用于基因递送和基因治疗的最有希望的材料。在这项研究中,我们通过PEG化对一种新型的交联PEI衍生物PEI-Et进行了化学修饰,因为PEG化可以通过屏蔽PEI-Et的过量正表面电荷来降低PEI-Et的细胞毒性。为了筛选出PEI-Et与PEG的最佳摩尔比以有效传递基因材料,我们首先合成了三种PEI不同摩尔比(1:1、2:1、1:2)的PEG-Et阳离子聚合物-Et对PEG,然后我们制备并表征了PEG-Et / DNA复合物和PEG-Et / siRNA复合物,最后我们测试了PEG-Et / DNA复合物的细胞毒性和转染效率以及基因沉默效率。 PEG-Et / siRNA复合物。结果表明,在三种类型的PEG-Et(PEG-Et 1:1,PEG-Et)中,基因载体PEG-Et 1:1(PEI-Et与PEG的摩尔比为1:1)是最好的2:1和PEG-Et 1:2)用于将DNA和siRNA浓缩成纳米颗粒,因为它具有较低的细胞毒性,较高的基因转染和siRNA沉默效率。

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