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Hybrid inorganic-organic capsules for efficient intracellular delivery of novel siRNAs against influenza A (H1N1) virus infection

机译:杂合无机-有机胶囊可有效地在细胞内递送新型siRNA以抵抗甲型流感(H1N1)病毒感染

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摘要

The implementation of RNAi technology into the clinical practice has been significantly postponing due to the issues regarding to the delivery of naked siRNA predominantly to target cells. Here we report the approach to enhance the efficiency of siRNA delivery by encapsulating the siRNA into new carrier systems which are obtained via the combination of widely used layer-by-layer technique and in situ modification by sol-gel chemistry. We used three types of siRNAs (NP-717, NP-1155 and NP-1496) in encapsulated form as new therapeutic agents against H1N1 influenza virus infection. By employing the hybrid microcontainers for the siRNA encapsulation we demonstrate the reduction of viral nucleoprotein (NP) level and inhibition of influenza virus production in infected cell lines (MDCK and A549). The obtained hybrid carriers based on assembled biodegradable polyelectrolytes and sol-gel coating possess several advantages such as a high cell uptake efficiency, low toxicity, efficient intracellular delivery of siRNAs and the protection of siRNAs from premature degradation before reaching the target cells. These findings underpin a great potential of versatile microencapsulation technology for the development of anti-viral RNAi delivery systems against influenza virus infection.
机译:由于主要将裸siRNA传递至靶细胞的问题,RNAi技术在临床实践中的实施已大大推迟。在这里,我们报告了通过将siRNA封装到新的载体系统中来增强siRNA传递效率的方法,这些载体系统是通过广泛使用的逐层技术和通过溶胶-凝胶化学原位修饰而获得的。我们以封装形式使用了三种类型的siRNA(NP-717,NP-1155和NP-1496)作为抗H1N1流感病毒感染的新治疗剂。通过将杂种微容器用于siRNA封装,我们证明了感染细胞系(MDCK和A549)中病毒核蛋白(NP)水平的降低和流感病毒产生的抑制作用。基于组装的可生物降解的聚电解质和溶胶-凝胶涂层获得的杂合载体具有几个优点,例如高细胞吸收效率,低毒性,有效的siRNA细胞内递送以及保护siRNA避免到达目标细胞之前的过早降解。这些发现为开发针对流感病毒感染的抗病毒RNAi递送系统奠定了广泛的微囊化技术的巨大潜力。

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