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首页> 外文期刊>Pharmaceutical research >Hyaluronic acid/chitosan-g-poly(ethylene glycol) nanoparticles for gene therapy: an application for pDNA and siRNA delivery.
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Hyaluronic acid/chitosan-g-poly(ethylene glycol) nanoparticles for gene therapy: an application for pDNA and siRNA delivery.

机译:用于基因治疗的透明质酸/壳聚糖-g-聚(乙二醇)纳米粒子:pDNA和siRNA递送的应用。

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摘要

PURPOSE: To design hyaluronic acid (HA) and chitosan-g-poly(ethylene glycol) (CS-g-PEG) nanoparticles intended for a broad range of gene delivery applications. METHODS: Nanoparticles formulated at different HA/CS-g-PEG mass ratios were developed to associate either pDNA or siRNA. The physico-chemical characteristics, morphology, association efficiency and nuclease protection ability of the nanocarriers were compared for these two molecules. Their biological performance, including transfection effciency, nanoparticle cellular uptake and citotoxicity, was assesed. RESULTS: The resulting nanoparticles showed an adequate size (between 130 and 180 nm), and their surface charge could be modulated according to the nanoparticle composition (from +30 mV to -20 mV). All prototypes exhibited a greater association efficiency and nuclease protection for pDNA than for siRNA. However, cell culture experiments evidenced that HA/CS-g-PEG nanoparticles were effective carriers for the delivery of both, siRNA and pDNA, eliciting a biological response with minimal cytotoxicity. Moreover, experiments performed in the HEK-EGFP-Snail1 cell line showed the potential of the HA/CS-g-PEG nanoparticles to silence the expression of the Snail1 transcription factor, an important mediator in tumor progression. CONCLUSIONS: HA/CS-g-PEG nanoparticles can be easily modulated for the delivery of different types of gene molecules, offering great potential for gene therapy applications, as evidenced by their biological performance.
机译:目的:设计透明质酸(HA)和壳聚糖-g-聚(乙二醇)(CS-g-PEG)纳米粒子,旨在广泛的基因传递应用。方法:开发了以不同的HA / CS-g-PEG质量比配制的纳米颗粒,以结合pDNA或siRNA。比较了这两个分子的纳米载体的理化特性,形态,缔合效率和核酸酶保护能力。评估了它们的生物学性能,包括转染效率,纳米颗粒细胞摄取和细胞毒性。结果:所得纳米粒子显示出适当的尺寸(介于130至180 nm之间),并且其表面电荷可以根据纳米粒子的组成(从+30 mV至-20 mV)进行调节。与siRNA相比,所有原型都对pDNA表现出更大的缔合效率和核酸酶保护作用。但是,细胞培养实验证明,HA / CS-g-PEG纳米颗粒是siRNA和pDNA传递的有效载体,引发了最小的细胞毒性的生物学反应。此外,在HEK-EGFP-Snail1细胞系中进行的实验表明,HA / CS-g-PEG纳米颗粒可能会沉默Snail1转录因子的表达,而Snail1转录因子是肿瘤进展中的重要介体。结论:HA / CS-g-PEG纳米粒子可以很容易地调节以递送不同类型的基因分子,为它们的生物学性能提供了巨大的潜力,可用于基因治疗应用。

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