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首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >Self RNA Sensing by RIG-I-like Receptors in Viral Infection and Sterile Inflammation
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Self RNA Sensing by RIG-I-like Receptors in Viral Infection and Sterile Inflammation

机译:病毒感染和无菌炎症中的钻井平均受体感测

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摘要

The innate immune system uses pattern recognition receptors to survey the intracellular and extracellular environment for signs of infection. Viral infection is detected through the presence of viral nucleic acids in infected cells. Pattern recognition receptor activation by viral nucleic acids induces the expression and secretion of type I IFNs (IFN-Is), important mediators of antiviral immunity. RIG-I-like receptors (RLRs) are RNA sensors that detect viral RNA in the cytosol and induce an IFN-I response. Viral RNAs contain features that set them apart from host RNAs, allowing RLRs to discriminate between cellular/ self and viral/non-self RNA. The notion emerged that self RNAs can also engage RLRs and modulate the IFN-I response, indicating that the distinction between self and non-self RNA is not watertight. We review how self RNAs regulate RLR activation and the IFN-I response during viral infection and how recognition of self RNAs by RLRs is implicated in autoinflammatory disorders and cancer.
机译:先天免疫系统使用模式识别受体来调查细胞内和细胞外环境进行感染的迹象。通过在感染细胞中存在病毒核酸来检测病毒感染。病毒核酸的模式识别受体激活诱导I I型IFNS(IFN-IS)的表达和分泌,抗病毒免疫的重要介质。钻机-I样受体(RLRS)是检测细胞溶质中病毒RNA的RNA传感器,并诱导IFN-I反应。病毒RNA包含与主机RNA相比设置它们的特征,允许RLR区分细胞/自我和病毒/非自动RNA。出现了自我RNA的概念也可以接合RLR并调制IFN-I响应,表明自我和非自动RNA之间的区别不潜水。我们回顾了自我RNA如何调节RLR激活和病毒感染期间的IFN-I反应以及如何通过RLRS识别自身rNA,涉及自身炎症疾病和癌症。

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