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Strategies of highly pathogenic RNA viruses to block dsRNA detection by RIG-I-like receptors: Hide, mask, hit

机译:高致病性RNA病毒通过RIG-I样受体阻断dsRNA检测的策略:皮,口罩,命中

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摘要

Double-stranded RNA (dsRNA) is synthesized during the course of infection by RNA viruses as a byproduct of replication and transcription and acts as a potent trigger of the host innate antiviral response. In the cytoplasm of the infected cell, recognition of the presence of viral dsRNA as a signature of "non-self" nucleic acid is carried out by RIG-I-like receptors (RLRs), a set of dedicated helicases whose activation leads to the production of type I interferon α/β (IFN-α/β). To overcome the innate antiviral response, RNA viruses encode suppressors of IFN-α/β induction, which block RLRs recognition of dsRNA by means of different mechanisms that can be categorized into: (i) dsRNA binding and/or shielding ("hide"), (ii) dsRNA termini processing ("mask") and (iii) direct interaction with components of the RLRs pathway ("hit"). In light of recent functional, biochemical and structural findings, we review the inhibition mechanisms of RLRs recognition of dsRNA displayed by a number of highly pathogenic RNA viruses with different disease phenotypes such as haemorrhagic fever (Ebola, Marburg, Lassa fever, Lujo, Machupo, Junin, Guanarito, Crimean-Congo, Rift Valley fever, dengue), severe respiratory disease (influenza, SARS, Hendra, Hantaan, Sin Nombre, Andes) and encephalitis (Nipah, West Nile).
机译:双链RNA(dsRNA)是在RNA病毒感染过程中作为复制和转录的副产物而合成的,并可以有效触发宿主固有的抗病毒反应。在受感染细胞的细胞质中,通过RIG-I-样受体(RLR)识别病毒dsRNA的存在是“非自身”核酸的标志,这是一组专用解旋酶,其激活导致I型干扰素α/β(IFN-α/β)的产生。为了克服先天的抗病毒反应,RNA病毒编码IFN-α/β诱导的抑制剂,该抑制剂通过不同的机制阻断RLR对dsRNA的识别,这些机制可分为:(i)dsRNA结合和/或屏蔽(“隐藏”) ,(ii)dsRNA末端加工(“遮罩”)和(iii)与RLRs途径的成分直接相互作用(“命中”)。根据最近的功能,生化和结构研究结果,我们综述了RLRs对dsRNA的抑制机制,该抑制作用由许多具有不同疾病表型的高致病性RNA病毒(如出血热(埃博拉,马尔堡,拉萨热,卢霍,马修波,胡宁,瓜纳里托,克里米亚-刚果,裂谷热,登革热,严重呼吸道疾病(流感,SARS,亨德拉,汉坦,辛诺布勒,安第斯山脉)和脑炎(尼帕,西尼罗河)。

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