将成簇配体结合工程化到非病毒载体中:以αvβ3靶向为例。

Engineering clustered ligand binding into nonviral vectors: alphavbeta3 targeting as an example.

作者信息

Ng Quinn K T, Sutton Marie K, Soonsawad Pan, Xing Li, Cheng Holland, Segura Tatiana

机构信息

Department of Chemical and Biomolecular Engineering, University of California at Los Angeles, Los Angeles, California 90024, USA.

出版信息

Mol Ther. 2009 May;17(5):828-36. doi: 10.1038/mt.2009.11. Epub 2009 Feb 24.

Abstract

The development of techniques to efficiently deliver genes using nonviral approaches can broaden the application of gene delivery in medical applications without the safety concerns associated with viral vectors. Here, we designed a clustered integrin-binding platform to enhance the efficiency and targetability of nonviral gene transfer to HeLa cells with low and high densities of alpha(v)beta(3) integrin receptors. Arg-Gly-Asp (RGD) nanoclusters were formed using gold nanoparticles functionalized with RGD peptides and used to modify the surface of DNA/poly(ethylene imine) (PEI) polyplexes. DNA/PEI polyplexes with attached RGD nanoclusters resulted in either 5.4- or 35-fold increase in gene transfer efficiency over unmodified polyplexes for HeLa cells with low- or high-integrin surface density, respectively. The transfection efficiency obtained with the commercially available vector jetPEI-RGD was used for comparison as a vector without clustered binding. JetPEI-RGD exhibited a 1.2-fold enhancement compared to unmodified jetPEI in cells with high densities of alpha(v)beta(3) integrin receptors. The data presented here emphasize the importance of the RGD conformational arrangement on the surface of the polyplex to achieve efficient targeting and gene transfer, and provide an approach to introduce clustering to a wide variety of nanoparticles for gene delivery.

摘要

利用非病毒方法高效递送基因的技术发展,可以拓宽基因递送在医学应用中的应用范围,而无需担心与病毒载体相关的安全问题。在此,我们设计了一个簇状整合素结合平台,以提高非病毒基因转移至具有低密度和高密度α(v)β(3)整合素受体的HeLa细胞的效率和靶向性。使用用RGD肽功能化的金纳米颗粒形成Arg-Gly-Asp(RGD)纳米簇,并用于修饰DNA/聚(乙烯亚胺)(PEI)多聚体的表面。对于具有低整合素或高整合素表面密度的HeLa细胞,附着有RGD纳米簇的DNA/PEI多聚体分别比未修饰的多聚体在基因转移效率上提高了5.4倍或35倍。将市售载体jetPEI-RGD作为无簇状结合的载体进行比较。在具有高密度α(v)β(3)整合素受体的细胞中,JetPEI-RGD与未修饰的jetPEI相比,表现出1.2倍的增强。此处呈现的数据强调了多聚体表面RGD构象排列对于实现有效靶向和基因转移的重要性,并提供了一种将簇状结构引入多种用于基因递送的纳米颗粒的方法。

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