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生物素触发生物素化聚乙烯亚胺上聚乙二醇-抗生物素蛋白的释放可增强体外基因表达。

Biotin-triggered release of poly(ethylene glycol)-avidin from biotinylated polyethylenimine enhances in vitro gene expression.

作者信息

Xiong May P, Forrest M Laird, Karls Angela L, Kwon Glen S

机构信息

Division of Pharmaceutical Sciences, School of Pharmacy, University of Wisconsin, 777 Highland Avenue, Madison, Wisconsin 53705-2222, USA.

出版信息

Bioconjug Chem. 2007 May-Jun;18(3):746-53. doi: 10.1021/bc0602883. Epub 2007 Mar 22.

DOI:10.1021/bc0602883
PMID:17375897
Abstract

Covalently poly(ethylene glycol) (PEG)-ylated polyethylenimine (PEI)/pDNA complexes display prolonged blood circulation profiles compared with PEI/pDNA complexes, but such PEGylated particles may not be suitable for tumor targeting due to low interaction with cell membranes, low internalization, and low gene expression. Noncovalent PEGylation of cationic particles via PEG-avidin/biotin-PEI is an attempt to bridge the gap between the positive attributes of PEG (prolonged particle circulation) and the positive attributes of nontoxic cationic polymers (enhanced cell interactions) for greater gene expression. Our polymer, 2PEG-avidin/biotin-PEI8, forms salt-stable particles ( approximately 100 nm) under physiologic conditions with a minimum of two 2PEG-avidin molecules bound per polymer chain (biotin-PEI8, 8 biotins/PEI). Following 10 days of incubation with 3000-fold excess biotin, 2PEG-avidin completely dissociated from biotin-PEI8, and gene expression was increased 2.1-32-fold in various cell lines when the desirable transfection feature of the cationic polymer was retained. This new PEGylation approach has implications for generally improving the clinical aspect of gene delivery via a two-step therapeutic strategy: (1) intravenous injection of noncovalent PEG-avidin/biotin-polycation nanoparticles for prolonged circulation, followed by (2) temporal release of PEG-avidin from biotin-polycation through either endogenous biotin or intravenous injection of biotin.

摘要

与聚乙烯亚胺(PEI)/质粒DNA(pDNA)复合物相比,共价聚乙二醇(PEG)化的聚乙烯亚胺(PEI)/pDNA复合物具有更长的血液循环时间,但由于与细胞膜的相互作用低、内化率低和基因表达低,这种PEG化颗粒可能不适用于肿瘤靶向。通过PEG-抗生物素蛋白/生物素-PEI对阳离子颗粒进行非共价PEG化,试图弥合PEG的积极特性(延长颗粒循环时间)和无毒阳离子聚合物的积极特性(增强细胞相互作用)之间的差距,以实现更高的基因表达。我们的聚合物2PEG-抗生物素蛋白/生物素-PEI8在生理条件下形成盐稳定颗粒(约100纳米),每个聚合物链至少结合两个2PEG-抗生物素蛋白分子(生物素-PEI8,8个生物素/PEI)。在用过量3000倍的生物素孵育10天后,2PEG-抗生物素蛋白与生物素-PEI8完全解离,当保留阳离子聚合物的理想转染特性时,各种细胞系中的基因表达增加了2.1至32倍。这种新的PEG化方法对于通过两步治疗策略总体改善基因递送的临床应用具有重要意义:(1)静脉注射非共价PEG-抗生物素蛋白/生物素-聚阳离子纳米颗粒以延长循环时间,随后(2)通过内源性生物素或静脉注射生物素从生物素-聚阳离子中暂时释放PEG-抗生物素蛋白。

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