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通过整合素介导的内吞作用途径利用合成病毒样颗粒进行基因转移。

Gene transfer with synthetic virus-like particles via the integrin-mediated endocytosis pathway.

作者信息

Erbacher P, Remy J S, Behr J P

机构信息

Laboratoire de Chimie Génétique, UMR 7514 CNRS/Université Louis Pasteur de Strasbourg, Faculté de Pharmacie, Illkirch, France.

出版信息

Gene Ther. 1999 Jan;6(1):138-45. doi: 10.1038/sj.gt.3300783.

DOI:10.1038/sj.gt.3300783
PMID:10341886
Abstract

The interaction between cationic DNA-containing particles and cell surface anionic proteoglycans is an efficient means of entering cultured cells. Therapeutic in vivo gene delivery levels, however, require binding to less ubiquitous molecules. In an effort to follow adenovirus, thiol-derivatized polyethylenimine (PEI) was conjugated to the integrin-binding peptide CYGGRGDTP via a disulfide bridge. The most extensively conjugated derivative (5.5% of the PEI amine functions) showed physical properties of interest for systemic gene delivery. In the presence of excess PEI-RGD, plasmid DNA was condensed into a rather homogeneous population of 30-100 nm toroidal particles as revealed by electron microscopy images in 150 mM salt. Their surface charge was close to neutrality as a consequence of the shielding effect of the prominent zwitterionic peptide residues. Transfection efficiency of integrin-expressing epithelial (HeLa) and fibroblast (MRC5) cells was increased by 10- to 100-fold as compared with PEI, even in serum. This large enhancement factor was lost when aspartic acid was replaced by glutamic acid in the targeted peptide sequence (RGD/RGE), confirming the involvement of integrins in transfection. PEI-RGD/DNA complexes thus share with adenovirus constitutive properties such as size and a centrally protected DNA core, and 'early' properties, i.e. cell entry mediated by integrins and acid-triggered endosome escape.

摘要

含阳离子DNA的颗粒与细胞表面阴离子蛋白聚糖之间的相互作用是进入培养细胞的有效方式。然而,体内治疗性基因递送水平需要与不那么普遍存在的分子结合。为了模仿腺病毒,将巯基衍生化的聚乙烯亚胺(PEI)通过二硫键与整合素结合肽CYGGRGDTP偶联。偶联程度最高的衍生物(占PEI胺官能团的5.5%)表现出对全身基因递送有意义的物理性质。在过量的PEI-RGD存在下,质粒DNA被浓缩成相当均匀的30-100nm环形颗粒群体,这在150mM盐的电子显微镜图像中得以揭示。由于突出的两性离子肽残基的屏蔽作用,它们的表面电荷接近中性。与PEI相比,即使在血清存在的情况下,表达整合素的上皮细胞(HeLa)和成纤维细胞(MRC5)的转染效率也提高了10到100倍。当靶向肽序列(RGD/RGE)中的天冬氨酸被谷氨酸取代时,这种大的增强因子就会丧失,这证实了整合素参与了转染过程。因此,PEI-RGD/DNA复合物与腺病毒具有共同的组成特性,如大小和受中央保护的DNA核心,以及“早期”特性,即由整合素介导的细胞进入和酸触发的内体逃逸。

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