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Multifunctional nanomedicine platform for cancer specific delivery of siRNA by superparamagnetic iron oxide nanoparticles-dendrimer complexes.

机译:多功能纳米医学平台,可通过超顺磁性氧化铁纳米颗粒-树状聚合物复合物实现siRNA的癌症特异性递送。

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摘要

The ability of Superparamagnetic Iron Oxide (SPIO) nanoparticles and Poly(Propyleneimine) generation 5 dendrimers (PPI G5) to cooperatively provoke siRNA complexation was investigated in order to develop a targeted, multifunctional siRNA delivery system for cancer therapy. Poly(ethylene glycol) (PEG) coating and cancer specific targeting moiety (LHRH peptide) have been incorporated into SPIO-PPI G5-siRNA complexes to enhance serum stability and selective internalization by cancer cells. Such a modification of siRNA nanoparticles enhanced its internalization into cancer cells and increased the efficiency of targeted gene suppression in vitro. Moreover, the developed siRNA delivery system was capable of sufficiently enhancing in vivo antitumor activity of an anticancer drug (Cisplatin). The proposed approach demonstrates potential for the creation of targeted multifunctional nanomedicine platforms with the ability to deliver therapeutic siRNA specifically to cancer cells in order to prevent severe adverse side effects on healthy tissues and in situ monitoring of the therapeutic outcome using clinically relevant imaging techniques.
机译:研究了超顺磁性氧化铁(SPIO)纳米粒子和聚(丙亚胺)5树枝状聚合物(PPI G5)协同激发siRNA络合的能力,以开发用于癌症治疗的靶向,多功能siRNA递送系统。聚(乙二醇)(PEG)涂层和癌症特异性靶向部分(LHRH肽)已被掺入SPIO-PPI G5-siRNA复合物中,以增强血清的稳定性和癌细胞的选择性内在化。 siRNA纳米粒子的这种修饰增强了其内化到癌细胞中的能力,并提高了体外靶向基因抑制的效率。而且,开发的siRNA递送系统能够充分增强抗癌药(顺铂)的体内抗肿瘤活性。所提出的方法证明了创建具有针对性的多功能纳米医学平台的潜力,该平台具有将治疗性siRNA特异地递送至癌细胞的能力,从而可以防止对健康组织的严重不良副作用,并使用临床相关的成像技术原位监测治疗结果。

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