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一种源自HIV gp41的肽在增强合成基因和小干扰RNA递送载体的细胞内运输中的应用。

Application of an HIV gp41-derived peptide for enhanced intracellular trafficking of synthetic gene and siRNA delivery vehicles.

作者信息

Kwon Ester J, Bergen Jamie M, Pun Suzie H

机构信息

Department of Bioengineering, University of Washington, 1705 NE Pacific Street, Seattle, Washington 98195, USA.

出版信息

Bioconjug Chem. 2008 Apr;19(4):920-7. doi: 10.1021/bc700448h. Epub 2008 Apr 1.

Abstract

Endosomal release is an efficiency-limiting step for many nonviral gene delivery vehicles. In this work, nonviral gene delivery vehicles were modified with a membrane-lytic peptide taken from the endodomain of HIV gp41. Peptide was covalently linked to polyethylenimine (PEI) and the peptide-modified polymer was complexed with DNA. The resulting nanoparticles were shown to have similar physicochemical properties as complexes formed with unmodified PEI. The gp41-derived peptide demonstrated significant lytic activity both as free peptide and when conjugated to PEI. Significant increases in transgene expression were achieved in HeLa cells when compared to unmodified polyplexes at low polymer to DNA ratios. Additionally, peptide-modified polyplexes mediated significantly enhanced siRNA delivery compared to unmodified polyplexes. Despite increases in transgene expression and siRNA knockdown, there was no increase in internalization or binding of modified carriers as determined by flow cytometry. The hypothesis that the gp41-derived peptide increases the endosomal escape of vehicles is supported by confocal microscopy imaging of DNA distributions in transfected cells. This work demonstrates the use of a lytic peptide for improved trafficking of nonviral gene delivery vehicles.

摘要

内体释放是许多非病毒基因递送载体的一个效率限制步骤。在这项工作中,非病毒基因递送载体用取自HIV gp41胞内结构域的膜裂解肽进行了修饰。该肽与聚乙烯亚胺(PEI)共价连接,并且肽修饰的聚合物与DNA复合。结果表明,所得纳米颗粒具有与用未修饰的PEI形成的复合物相似的物理化学性质。gp41衍生肽无论是作为游离肽还是与PEI偶联时都表现出显著的裂解活性。与低聚合物与DNA比例下的未修饰多聚体相比,在HeLa细胞中实现了转基因表达的显著增加。此外,与未修饰的多聚体相比,肽修饰的多聚体介导的siRNA递送显著增强。尽管转基因表达增加且siRNA敲低,但通过流式细胞术测定,修饰载体的内化或结合并未增加。转染细胞中DNA分布的共聚焦显微镜成像支持了gp41衍生肽增加载体的内体逃逸这一假设。这项工作证明了使用裂解肽来改善非病毒基因递送载体的运输。

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