Dual-targeting non-viral vector based on polyethylenimine improves gene transfer efficiency

被引:12
作者
Li, D.
Tang, G. P.
Li, J. Z.
Kong, Y.
Huang, H. L.
Min, L. J.
Zhou, J.
Shen, F. P.
Wang, Q. Q.
Yu, H.
机构
[1] Zhejiang Univ, Inst Immunol, Hangzhou 310058, Peoples R China
[2] Zhejiang Univ, Inst Chem Biol & Pharmaceut Chem, Hangzhou 310028, Peoples R China
关键词
polyethylenimine; FGF receptors; integrins; targeting; gene transfer;
D O I
10.1163/156856207780852532
中图分类号
R318 [生物医学工程];
学科分类号
0831 ;
摘要
Polyethylenimine (PEI) is the polymer most commonly used for transferring plasmids into eukaryotes, but its gene-transfer efficiency is lower compared to viral vectors. Receptors targeting PEI combined with ligands can enhance efficiency of gene transfer into the corresponding receptor-positive cells. Using the double-receptor-mediated pathway of viral infection, in this study we synthesized a novel non-viral vector based on PEI combined with two peptides recognizing FGF receptors (peptide YC25) and integrins (peptide CP9) on the cell surface. The dual targeting vector showed a physicochemical character similar to that of PEI, such as pDNA formation, particle size, zeta potential and lower toxicity. In vitro gene transfer showed that the dual-receptor targeted vector (YC25-PEI-CP9) exhibited a markedly higher transgene efficiency in cell lines with positive expression of FGF receptors and integrins, compared with single-peptide-modified PEI or unmodified PEI. In the cells with only integrin-positive expression, YC25-PEI-CP9 mediated a higher transgene expression than PEI but lower than CP9-PEI. The corresponding free peptides could inhibit the transgene efficiency of the peptide-coupled PEI. In vivo gene transfer in tumor-bearing nude mice also demonstrated that the dual-targeting vectors showed a significantly enhanced transfection efficiency in tumors with positive expression of FGF receptors and integrins. The synthesized polymer YC25-PEI-CP9 has the prospect to act as a novel kind of non-viral vector in gene therapy.
引用
收藏
页码:545 / 560
页数:16
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