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Inhibition of hepatitis C virus replication and expression by small interfering RNA targeting host cellular genes.

机译:通过靶向宿主细胞基因的小干扰RNA抑制丙型肝炎病毒的复制和表达。

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Small interfering RNA (siRNA) is a powerful tool for functional genomics and gene therapy. Viral replication and gene expression are strongly inhibited by siRNA treatment of infected mammalian cells. However, the high sequence specificity of siRNAs, combined with prolonged treatment, promote the emergence of siRNA-resistant virus variants, especially among viruses that encode a polymerase lacking proofreading capabilities, indicating that the antiviral properties of specific siRNAs are not as effective as expected. To investigate the silencing effect of siRNAs against selected host cellular proteins that promote replication of hepatitis C virus (HCV), several siRNAs against human VAMP-associated protein (hVAP-A), La antigen and polypyrimidine-tract-binding protein (PTB) were evaluated. The data show that several siRNAs markedly decreased the expression levels of corresponding cellular genes that inhibited HCV replication in Huh-7 cells. These treatments were also shown to have no impact upon cell viability. These findings provide an alternative approach for blocking HCV replication. Hence, combination therapies with siRNAs against both the virus and host genes that support virus replication are likely to be a potent approach in the treatment of chronic hepatitis C.
机译:小干扰RNA(siRNA)是功能基因组学和基因治疗的强大工具。 siRNA处理感染的哺乳动物细胞会强烈抑制病毒的复制和基因表达。但是,siRNA的高序列特异性与长期治疗相结合,促进了siRNA抗性病毒变体的出现,特别是在编码聚合酶缺乏校对能力的病毒中,这表明特定siRNA的抗病毒特性没有预期的有效。为了研究siRNA对选定的促进丙型肝炎病毒(HCV)复制的宿主细胞蛋白的沉默作用,分别针对人VAMP相关蛋白(hVAP-A),La抗原和多嘧啶束结合蛋白(PTB)的几种siRNA进行了沉默。评估。数据显示,几种siRNA显着降低了抑制Huh-7细胞中HCV复制的相应细胞基因的表达水平。还显示这些处理对细胞活力没有影响。这些发现为阻断HCV复制提供了另一种方法。因此,针对病毒和支持病毒复制的宿主基因的siRNA联合疗法可能是治疗慢性丙型肝炎的有效方法。

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