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首页> 外文期刊>Virus Research: An International Journal of Molecular and Cellular Virology >Vaccinia virus double-stranded RNA-binding protein E3 does not interfere with siRNA-mediated gene silencing in mammalian cells.
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Vaccinia virus double-stranded RNA-binding protein E3 does not interfere with siRNA-mediated gene silencing in mammalian cells.

机译:牛痘病毒双链RNA结合蛋白E3不会干扰哺乳动物细胞中siRNA介导的基因沉默。

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摘要

Vaccinia virus (VACV) evolved several strategies to evade antiviral cellular defence. The vaccinia virus E3 protein for example binds and sequesters double stranded RNA (dsRNA) and counteracts interferon action. We were interested to find out whether and to what extend E3 interferes with RNA silencing mediated by short interfering RNA (siRNA) in mammalian cells. We could show that the expression of a VACV-encoded marker gene can be efficiently inhibited by siRNA independently of the presence of the E3 protein. In addition, expression of E3 had no impact on RNA polymerase III promoter-derived shRNA-induced silencing of a cellular gene in human cells. Both VACV early and late gene expression could be inhibited by siRNA. Furthermore, downregulation of the expression of the E3L gene itself by siRNA in VACV infected cells produced the previously described phenotype of a knock-out virus, which illustrates the power of siRNA for vaccinia virus gene function analysis.
机译:牛痘病毒(VACV)进化出几种策略来逃避抗病毒细胞防御。牛痘病毒E3蛋白例如结合并隔离双链RNA(dsRNA),并抵消干扰素的作用。我们有兴趣找出E3是否以及在哺乳动物细胞中扩展由短干扰RNA(siRNA)介导的RNA沉默。我们可以证明,独立于E3蛋白的存在,siRNA可以有效抑制VACV编码的标记基因的表达。另外,E3的表达对RNA聚合酶III启动子衍生的shRNA诱导的人细胞中细胞基因的沉默没有影响。 siRNA可以抑制VACV早期和晚期基因表达。此外,在VACV感染的细胞中,siRNA对E3L基因自身表达的下调产生了先前描述的敲除病毒的表型,这说明了siRNA在牛痘病毒基因功能分析中的作用。

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