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壳聚糖基基因递送至周围神经系统的靶向载体。

Chitosan-based gene delivery vectors targeted to the peripheral nervous system.

机构信息

INEB, Instituto de Engenharia Biomédica, Divisão de Biomateriais, Universidade do Porto, Rua do Campo Alegre 823, 4150-180 Porto, Portugal.

出版信息

J Biomed Mater Res A. 2010 Dec 1;95(3):801-10. doi: 10.1002/jbm.a.32874.

DOI:10.1002/jbm.a.32874
PMID:20734332
Abstract

A non-toxic, targeted, simple and efficient system that can specifically transfect peripheral sensorial neurons can pave the way towards the development of new therapeutics for the treatment of peripheral neuropathies. In this study chitosan (CH), a biodegradable polymer, was used as the starting material in the design of a multicomponent vector targeted to the peripheral nervous system (PNS). Polycation-DNA complexes were optimized using imidazole- and thiol-grafted CH (CHimiSH), in order to increase transfection efficiency and allow the formation of ligand conjugated nanocomplexes, respectively. The 50 kDa non-toxic fragment from the tetanus toxin (HC), shown to interact specifically with peripheral neurons and undergo retrograde transport, was grafted to the binary complex via a bi-functional poly(ethylene glycol) (HC-PEG) reactive for the thiol moieties present in the complex surface. The targeting of the developed nanocomplexes was assessed by means of internalization and transfection studies in the ND7/23 (neuronal) vs. NIH 3T3 (fibroblast) cell lines. Targeted transfection was further confirmed in dorsal root ganglion dissociated primary cultures. A versatile, multi-component nanoparticle system that successfully targets and transfects neuronal cell lines, as well as dorsal root ganglia (DRG) primary neuron cultures was obtained for the 1.0 (w/w) HC-PEG/DNA formulation.

摘要

一种无毒、靶向、简单且高效的系统,能够特异性转染周围感觉神经元,为开发治疗周围神经病变的新疗法铺平道路。在这项研究中,壳聚糖 (CH) 作为一种可生物降解的聚合物,被用作针对周围神经系统 (PNS) 的多组分载体设计的起始材料。使用咪唑和巯基接枝壳聚糖 (CHimiSH) 优化聚阳离子-DNA 复合物,以分别提高转染效率并允许形成配体共轭的纳米复合物。破伤风毒素 (HC) 的无毒 50 kDa 片段已被证明与周围神经元特异性相互作用并经历逆行运输,通过双功能聚(乙二醇)(HC-PEG)与二元复合物中的巯基反应基团连接到二元复合物上。通过 ND7/23(神经元)与 NIH 3T3(成纤维细胞)细胞系的内化和转染研究评估了开发的纳米复合物的靶向性。在背根神经节分离的原代培养物中进一步证实了靶向转染。对于 1.0(w/w)HC-PEG/DNA 制剂,获得了一种多功能的多组分纳米颗粒系统,该系统能够成功靶向和转染神经元细胞系以及背根神经节 (DRG) 原代神经元培养物。

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