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Inhibition of influenza A virus matrix and nonstructural gene expression using RNA interference

机译:利用RNA干扰抑制流感病毒基质和非结构基因表达

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Influenza antiviral drugs that use protein inhibitors can lose their efficacy as resistant strains emerge. As an alternative strategy, we investigated the use of small interfering RNA molecules (siRNAs) by characterizing three siRNAs (M747, M776 and M832) targeting the influenza matrix 2 gene and three (NS570, NS595 and NS615) targeting the nonstructural protein 1 and 2 genes. We also re-examined two previously reported siRNAs, M331 and M950, which target the matrix 1 and 2 genes. Treatment with M331-, M776-, M832-, and M950-siRNAs attenuated influenza titer. M776-siRNA treated cells had 29.8% less infectious virus than cells treated with the previously characterized siRNA, M950. NS570-, NS595- and NS615-siRNAs reduced nonstructural protein 1 and 2 expression and enhanced type I interferon expression by 50%. Combination siRNA treatment attenuated 20.9% more infectious virus than single siRNA treatment. Our results suggest a potential use for these siRNAs as an effective anti-influenza virus therapy. Published by Elsevier Inc.
机译:使用蛋白质抑制剂的流感抗病毒药物可以失去它们的疗效,因为抗性菌株出现。作为一种替代策略,我们通过表征靶向非结构蛋白1和2的三种siRNA(M747,2776和M832)来研究使用小干扰RNA分子(SIRNA)的使用小干扰RNA分子(SIRNA),靶向非结构蛋白1和2的三种(NS570,NS595和NS615)基因。我们还重新检查了两种先前报告的SIRNA,M331和M950,其靶向基质1和2基因。用M331,M776-,M832-和M950-SIRNA治疗抑制流感滴度。 M776-siRNA处理的细胞比用先前特征的siRNA,M950处理的细胞具有29.8%的感染病毒。 NS570-,NS595和NS615-SIRNA减少了非结构蛋白1和2表达和增强的I型干扰素表达50%。组合siRNA治疗比单次siRNA治疗更高的传染性病毒衰减20.9%。我们的结果表明这些siRNA作为有效的抗流感病毒治疗的潜在用途。 elsevier公司出版

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