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| Preparation of PLL-PEG-PLL and its application to DNA encapsulation | |
| 引用本文: | YANG Zigang1,ZHOU Fen1,YUAN Jianjun1,MA Lixin2,ZHAI Chao2 & CHENG Shiyuan1 1. School of Chemistry and Materials Science,Hubei University,Wuhan 430062,China, 2. School of Life Science,Hubei University,Wuhan 430062,China. Preparation of PLL-PEG-PLL and its application to DNA encapsulation[J]. 中国科学B辑(英文版), 2006, 49(4): 357-362. DOI: 10.1007/s11426-006-2006-9 |
| 作者姓名: | YANG Zigang1 ZHOU Fen1 YUAN Jianjun1 MA Lixin2 ZHAI Chao2 & CHENG Shiyuan1 1. School of Chemistry and Materials Science Hubei University Wuhan 430062 China 2. School of Life Science Hubei University Wuhan 430062 China |
| 作者单位: | YANG Zigang1,ZHOU Fen1,YUAN Jianjun1,MA Lixin2,ZHAI Chao2 & CHENG Shiyuan1 1. School of Chemistry and Materials Science,Hubei University,Wuhan 430062,China; 2. School of Life Science,Hubei University,Wuhan 430062,China |
| 摘 要: | With the successful sequencing of Human Genome, it would be possible to cure all diseases by gene ther- apy in the near future. However, one of the major problems in gene therapy is the development of gene vectors. To date, there are two kinds of gene vectors, namely, viral and non-viral gene vectors. Viruses are widely used as vectors in gene therapy, with the trans- fection efficiency being relatively high, but they have the safety problems such as immunogenicity, non- biocompatibility and … |
| 收稿时间: | 2005-07-02 |
| 修稿时间: | 2005-11-10 |
Preparation of PLL-PEG-PLL and its application to DNA encapsulation |
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| YANG Zigang,ZHOU Fen,YUAN Jianjun,MA Lixin,ZHAI Chao,CHENG Shiyuan. Preparation of PLL-PEG-PLL and its application to DNA encapsulation[J]. Science in China(Chemistry), 2006, 49(4): 357-362. DOI: 10.1007/s11426-006-2006-9 | |
| Authors: | YANG Zigang ZHOU Fen YUAN Jianjun MA Lixin ZHAI Chao CHENG Shiyuan |
| Affiliation: | 1. School of Chemistry and Materials Science, Hubei University, Wuhan 430062, China 2. School of Life Science, Hubei University, Wuhan 430062, China |
| Abstract: | PLL-PEG-PLL was synthesized by deprotection of the amino group of PLL(Z)-PEG-PLL(Z). The properties of the polyion complex (PIC) micelles comprising of PLL-PEG-PLL and DNA were investigated. The results showed that the core of PIC was formed by PLL and DNA through electrostatic interactions, and PEG was shell of PIC, so PIC micelles in aqueous medium were homogenous with no precipitation even under the neutral condition, and PIC had the characteristic of stability, which were very important in gene therapy. At the same time, the results showed PLL-PEG-PLL could condense DNA, longer PLL blocks were generally more effective at condensation, and the nuclease resistance of DNA was increased remarkably. PIC was spherical with diameter of 10–35 nm, which could be easily taken up by cells. Transfection experiments in vitro showed that the DNA encapsulated could be expressed in the cell line SF9. |
| Keywords: | poly(L-Lysine) poly(ethylene glycol) block copolymer DNA polyion complex micelles (PIC) |
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