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A glance at subgenomic flavivirus RNAs and microRNAs in flavivirus infections

机译:浅谈黄病毒感染中的亚基因组黄病毒RNA和microRNA

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摘要

The family Flaviviridae comprises a wide variety of viruses that are distributed worldwide, some of which are associated with high rates of morbidity and mortality. There are neither vaccines nor antivirals for most flavivirus infections, reinforcing the importance of research on different aspects of the viral life cycle. During infection, cytoplasmic accumulation of RNA fragments mainly originating from the 3′ UTRs, which have been designated subgenomic flavivirus RNAs (sfRNAs), has been detected. It has been shown that eukaryotic exoribonucleases are involved in viral sfRNA production. Additionally, viral and human small RNAs (sRNAs) have also been found in flavivirus-infected cells, especially microRNAs (miRNAs). miRNAs were first described in eukaryotic cells and in a mature and functional state present as single-stranded 18–24 nt RNA fragments. Their main function is the repression of translation through base pairing with cellular mRNAs, besides other functions, such as mRNA degradation. Canonical miRNA biogenesis involves Drosha and Dicer, however miRNA can also be generated by alternative pathways. In the case of flaviviruses, alternative pathways have been suggested. Both sfRNAs and miRNAs are involved in viral infection and host cell response modulation, representing interesting targets of antiviral strategies. In this review, we focus on the generation and function of viral sfRNAs, sRNAs and miRNAs in West Nile, dengue, Japanese encephalitis, Murray Valley encephalitis and yellow fever infections, as well as their roles in viral replication, translation and cell immune response evasion. We also give an overview regarding other flaviviruses and the generation of cellular miRNAs during infection.
机译:黄病毒科包括分布在世界各地的多种病毒,其中一些与高发病率和高死亡率有关。对于大多数黄病毒而言,既没有疫苗也没有抗病毒药,这加强了对病毒生命周期不同方面进行研究的重要性。在感染过程中,已经检测到主要来源于3'UTR的RNA片段的胞质积累,这些片段被称为亚基因组黄病毒RNA(sfRNA)。已经显示,真核外核糖核酸酶参与病毒sfRNA的产生。此外,还发现在黄病毒感染的细胞,尤其是微RNA(miRNA)中发现了病毒和人类小RNA(sRNA)。 miRNA首先在真核细胞中被描述,并且以单链18-24nt RNA片段的形式存在于成熟和功能状态。它们的主要功能是通过与细胞mRNA的碱基配对来抑制翻译,此外还具有其他功能,例如mRNA降解。规范的miRNA生物发生涉及Drosha和Dicer,但是miRNA也可以通过替代途径生成。对于黄病毒,已经提出了替代途径。 sfRNA和miRNA均参与病毒感染和宿主细胞应答调节,代表了抗病毒策略的重要靶标。在这篇综述中,我们重点研究西尼罗河,登革热,日本脑炎,墨累谷脑炎和黄热病感染中病毒sfRNA,sRNA和miRNA的产生和功能,以及它们在病毒复制,翻译和细胞免疫应答逃避中的作用。我们还概述了其他黄病毒和感染过程中细胞miRNA的产生。

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