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Local gene delivery via endovascular stents coated with dodecylated chitosan–plasmid DNA nanoparticles

机译:通过覆有十二烷基化壳聚糖-质粒DNA纳米颗粒的血管内支架进行局部基因递送

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摘要

Development of efficacious therapeutic strategies to prevent and inhibit the occurrences of restenosis after percutaneous transluminal coronary angioplasty is critical for the treatment of cardiovascular diseases. In this study, the feasibility and efficiency of stents coated with dodecylated chitosan–plasmid DNA nanoparticles (DCDNPs) were evaluated as scaffolds for localized and prolonged delivery of reporter genes into the diseased blood vessel wall. Dodecylated chitosan–plasmid DNA complexes formed stable positive charged nanospheres with mean diameter of approximately 90–180 nm and zeta potential of +28 ± 3 mV. As prepared DCDNPs were spray-coated on stents, a thin layer of dense DCDNPs was successfully distributed onto the metal struts of the endovascular stents as demonstrated by scanning electron microscopy. The DCDNP stents were characterized for the release kinetics of plasmid DNA, and further evaluated for gene delivery and expression both in vitro and in vivo. In cell culture, DCDNP stents containing plasmid EGFP-C1 exhibited high level of GFP expression in cells grown on the stent surface and along the adjacent area. In animal studies, reporter gene activity was observed in the region of the artery in contact with the DCDNP stents, but not in adjacent arterial segments or distal organs. The DCDNP stent provides a very promising strategy for cardiovascular gene therapy.
机译:开发有效的治疗策略来预防和抑制经皮腔内冠状动脉成形术后再狭窄的发生对心血管疾病的治疗至关重要。在这项研究中,评估了十二烷基化壳聚糖质粒DNA纳米颗粒(DCDNPs)涂层支架的可行性和有效性,以作为将报告基因局部和长期递送至患病血管壁的支架。十二烷基化的壳聚糖-质粒DNA复合物形成稳定的带正电的纳米球,平均直径约为90-180 nm,ζ电位为+28±3 mV。将制备的DCDNPs喷涂在支架上后,薄薄的致密DCDNPs成功地分布在血管内支架的金属支杆上,如扫描电子显微镜所证明的那样。 DCDNP支架的特征在于质粒DNA的释放动力学,并进一步评估了体内和体外的基因传递和表达。在细胞培养中,含有质粒EGFP-C1的DCDNP支架在支架表面和邻近区域生长的细胞中表现出高水平的GFP表达。在动物研究中,在与DCDNP支架接触的动脉区域观察到报告基因活性,但在相邻的动脉节段或远端器官中未观察到。 DCDNP支架为心血管基因治疗提供了非常有前途的策略。

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