University of Stuttgart, Institute of Industrial Genetics, Allmandring, Stuttgart, Germany.
J Virol Methods. 2009 May;157(2):211-8. doi: 10.1016/j.jviromet.2009.01.012. Epub 2009 Jan 31.
RNA interference (RNAi) has been shown to be suitable to inhibit viruses in experimental setups and is considered a promising antiviral strategy that is currently being tested in various clinical trials. The present study provides an approach to design siRNAs with high potency against a virus-specific target gene. In recent years, several outbreaks of aseptic meningitis caused by an echovirus 30 (EV-30) infection have been described. Based on an initial set of 30 in silico designed siRNAs, six siRNAs targeting the 3D RNA-dependent RNA-Polymerase (3D(Pol)) of EV-30 were selected. All but one of them showed high efficiency in both, reporter and virus assays. A second aim of the study was to re-investigate the relevance of the decay-accelerating factor (DAF, also known as CD55) as cellular entry receptor of EV-30 by means of RNAi, a question which had been under debate in previous studies. Knockdown of DAF inhibited drastically infection by EV-30 indicating that DAF plays an important role either as an attachment factor or as a receptor.
RNA 干扰 (RNAi) 已被证明可在实验环境中抑制病毒,被认为是一种有前途的抗病毒策略,目前正在各种临床试验中进行测试。本研究提供了一种针对病毒特异性靶基因设计高效 siRNA 的方法。近年来,已描述了多起因肠道病毒 30 (EV-30) 感染引起的无菌性脑膜炎爆发。基于最初的 30 个计算机设计的 siRNA,选择了 6 个针对 EV-30 的 3D RNA 依赖性 RNA 聚合酶 (3D(Pol)) 的 siRNA。除了一个之外,其余的在报告基因和病毒检测中均显示出高效性。该研究的第二个目的是通过 RNAi 重新研究衰变加速因子 (DAF,也称为 CD55) 作为 EV-30 的细胞进入受体的相关性,这是之前的研究中存在争议的问题。DAF 的敲低大大抑制了 EV-30 的感染,表明 DAF 作为附着因子或受体发挥重要作用。
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