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通过REDV肽修饰的聚乙二醇-三甲基壳聚糖将微小RNA-126靶向递送至血管内皮细胞。

Targeted delivery of microRNA-126 to vascular endothelial cells via REDV peptide modified PEG-trimethyl chitosan.

作者信息

Zhou Fang, Jia Xiaoling, Yang Qingmao, Yang Yang, Zhao Yunhui, Fan Yubo, Yuan Xiaoyan

机构信息

School of Materials Science and Engineering, and Tianjin Key Laboratory of Composite and Functional Materials, Tianjin University, Tianjin 300072, China.

出版信息

Biomater Sci. 2016 May 26;4(5):849-56. doi: 10.1039/c5bm00629e. Epub 2016 Apr 8.

DOI:10.1039/c5bm00629e
PMID:27055482
Abstract

Manipulation of gene expression by means of microRNAs (miRNAs) is one of the emerging strategies to treat cardiovascular and cancer diseases. Nevertheless, efficient delivery of miRNAs to a specific vascular tissue is limited. In this work, a short peptide Arg-Glu-Asp-Val (REDV) was linked to trimethyl chitosan (TMC) via a bifunctional poly(ethylene glycol) (PEG) linker for the targeted delivery of microRNA-126 (miRNA-126) to vascular endothelial cells (VECs). The morphology, serum stability and cytotoxicity of the polyplex/miRNA complexes, namely, TMC/miRNA, TMC-g-PEG/miRNA and TMC-g-PEG-REDV/miRNA, were investigated along with the cellular uptake, proliferation and in vitro miRNA transfection efficiency. By REDV modification, the TMC-g-PEG-REDV/miRNA complex showed negligible cytotoxicity, increased expression of miRNA-126 and enhanced VEC proliferation compared with the TMC/miRNA and TMC-g-PEG/miRNA complexes. In particular, the approaches adopted for the miRNA delivery and targeted peptide REDV modification promote the selective uptake and the growth of VECs over vascular smooth muscle cells. It was suggested that the REDV peptide-modified TMC-g-PEG polyplex could be potentially used as a miRNA carrier in artificial blood vessels for rapid endothelialization.

摘要

通过微小RNA(miRNA)来操纵基因表达是治疗心血管疾病和癌症的新兴策略之一。然而,将miRNA有效递送至特定血管组织存在局限性。在本研究中,一种短肽精氨酸-谷氨酸-天冬氨酸-缬氨酸(REDV)通过双功能聚乙二醇(PEG)连接子与三甲基壳聚糖(TMC)相连,用于将微小RNA-126(miRNA-126)靶向递送至血管内皮细胞(VECs)。研究了多聚体/miRNA复合物,即TMC/miRNA、TMC-g-PEG/miRNA和TMC-g-PEG-REDV/miRNA的形态、血清稳定性和细胞毒性,以及细胞摄取、增殖和体外miRNA转染效率。与TMC/miRNA和TMC-g-PEG/miRNA复合物相比,通过REDV修饰,TMC-g-PEG-REDV/miRNA复合物显示出可忽略不计的细胞毒性、miRNA-126表达增加以及VEC增殖增强。特别是,用于miRNA递送和靶向肽REDV修饰的方法促进了VECs相对于血管平滑肌细胞的选择性摄取和生长。研究表明,REDV肽修饰的TMC-g-PEG多聚体有可能作为人工血管中用于快速内皮化的miRNA载体。

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