首页> 外文期刊>Antiviral Research >Inoculation of newborn mice with non-coding regions of foot-and-mouth disease virus RNA can induce a rapid, solid and wide-range protection against viral infection.
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Inoculation of newborn mice with non-coding regions of foot-and-mouth disease virus RNA can induce a rapid, solid and wide-range protection against viral infection.

机译:用口蹄疫病毒RNA的非编码区接种新生小鼠可以诱导快速,稳定和广泛的保护,以抵抗病毒感染。

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摘要

We have recently described the ability of in vitro-transcribed RNAs, mimicking structural domains in the 5' and 3' non-coding regions (NCRs) of the foot-and-mouth disease virus (FMDV) genome, to trigger the innate immune response in porcine cultured cells and mice. In this work, the antiviral effect exerted in vivo by these small synthetic non-infectious RNA molecules was analyzed extensively. The susceptibility of transfected newborn Swiss mice to FMDV challenge was tested using a wide range of viral doses. The level of protection depended on the specific RNA inoculated and was dose-dependent. The RNA giving the best protection was the internal ribosome entry site (IRES), followed by the transcripts corresponding to the S fragment. The time course of resistance to FMDV of the RNA-transfected mice was studied. Our results show the efficacy of these RNAs to prevent viral infection as well as to contain ongoing FMDV infection in certain time intervals. Protection proved to be independent of the serotype of FMDV used for challenge. These results support the potential use of the FMDV NCR transcripts as both prophylactic and therapeutic molecules for new FMDV control strategies.
机译:我们最近描述了模仿口蹄疫病毒(FMDV)基因组5'和3'非编码区(NCR)中结构域的体外转录RNA触发先天免疫应答的能力。在猪培养的细胞和小鼠中。在这项工作中,广泛地分析了这些小的合成非感染性RNA分子在体内产生的抗病毒作用。使用多种病毒剂量测试了转染的新生瑞士小鼠对FMDV攻击的敏感性。保护水平取决于所接种的特定RNA,并且是剂量依赖性的。提供最佳保护的RNA是内部核糖体进入位点(IRES),其次是与S片段相对应的转录本。研究了RNA转染小鼠对FMDV的抗性的时间过程。我们的结果表明,这些RNA可以预防病毒感染,并能在一定的时间间隔内抑制持续的FMDV感染。事实证明,保护作用与用于挑战的FMDV血清型无关。这些结果支持FMDV NCR转录本作为新的FMDV控制策略的预防和治疗分子的潜在用途。

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