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首页> 外文期刊>Journal of Controlled Release: Official Journal of the Controlled Release Society >Prolonged gene silencing by combining siRNA nanogels and photochemical internalization
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Prolonged gene silencing by combining siRNA nanogels and photochemical internalization

机译:通过结合siRNA纳米凝胶和光化学内化作用延长基因沉默

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摘要

Small interfering RNAs (siRNAs) show potential for the treatment of a wide variety of pathologies with a known genetic origin through sequence-specific gene silencing. However, siRNAs do not have favorable drug-like properties and need to be packaged into nanoscopic carriers that are designed to guide the siRNA to the cytoplasm of the target cell. In this report biodegradable cationic dextran nanogels are used to deliver siRNA across the intracellular barriers. For the majority of non-viral siRNA carriers studied so far, endosomal confinement is identified as the most prominent hurdle, limiting the full gene silencing potential. Thus, there is a major interest in methods that are able to enhance endosomal escape of siRNA to improve its intracellular bioavailability. Photochemical internalization (PCI) is a method that employs amphiphilic photosensitizers to destabilize endosomal vesicles. We show that applying PCI at a later time-point post-transfection significantly prolonged the knockdown of the target protein only in case the siRNA was carried by nanogels and not when a liposomal carrier was used. Combining siRNA nanogels and PCI creates new possibilities to prolong gene silencing by using intracellular vesicles as depots for siRNA and applying PCI at the time when maintaining the RNAi effect becomes critical.
机译:小型干扰RNA(siRNA)通过序列特异性基因沉默显示了具有已知遗传起源的多种病理学治疗潜力。但是,siRNA不具有良好的类药物特性,需要包装到纳米载体中,这些载体旨在将siRNA引导至靶细胞的细胞质。在该报告中,可生物降解的阳离子葡聚糖纳米凝胶用于跨细胞内屏障递送siRNA。对于迄今为止研究的大多数非病毒siRNA携带者,将内体禁闭确定为最突出的障碍,限制了全基因沉默的潜力。因此,对能够增强siRNA的内体逸出以改善其细胞内生物利用度的方法引起了极大的兴趣。光化学内在化(PCI)是一种使用两亲性光敏剂去破坏内体囊泡的方法。我们表明,仅在siRNA由纳米凝胶携带的情况下,而不是在使用脂质体载体的情况下,在转染后的较晚时间点应用PCI显着延长了靶蛋白的敲低时间。 siRNA纳米凝胶和PCI的结合创造了新的可能性,可以通过使用细胞内囊泡作为siRNA的贮库来延长基因沉默,并在维持RNAi效应的关键时刻应用PCI。

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