抗辐射细胞和辐射敏感细胞的TLR/RLH信号协同作用对于抵御水疱性口炎病毒感染至关重要。
Concomitant TLR/RLH signaling of radioresistant and radiosensitive cells is essential for protection against vesicular stomatitis virus infection.
作者信息
Spanier Julia, Lienenklaus Stefan, Paijo Jennifer, Kessler Annett, Borst Katharina, Heindorf Sabrina, Baker Darren P, Kröger Andrea, Weiss Siegfried, Detje Claudia N, Staeheli Peter, Kalinke Ulrich
机构信息
Institute for Experimental Infection Research, TWINCORE, Centre for Experimental and Clinical Infection Research, a joint venture between the Helmholtz Centre for Infection Research, Braunschweig, and the Hannover Medical School, 30625 Hannover, Germany;
Department of Molecular Immunology, Helmholtz Centre for Infection Research, 38124 Braunschweig, Germany;
出版信息
J Immunol. 2014 Sep 15;193(6):3045-54. doi: 10.4049/jimmunol.1400959. Epub 2014 Aug 15.
Several studies indicated that TLR as well as retinoic acid-inducible gene I-like helicase (RLH) signaling contribute to vesicular stomatitis virus (VSV)-mediated triggering of type I IFN (IFN-I) responses. Nevertheless, TLR-deficient MyD88(-/-)Trif(-/-) mice and RLH-deficient caspase activation and recruitment domain adaptor inducing IFN-β (Cardif)(-/-) mice showed only marginally enhanced susceptibility to lethal VSV i.v. infection. Therefore, we addressed whether concomitant TLR and RLH signaling, or some other additional mechanism, played a role. To this end, we generated MyD88(-/-)Trif(-/-)Cardif(-/-) (MyTrCa(-/-)) mice that succumbed to low-dose i.v. VSV infection with similar kinetics as IFN-I receptor-deficient mice. Three independent approaches (i.e., analysis of IFN-α/β serum levels, experiments with IFN-β reporter mice, and investigation of local IFN-stimulated gene induction) revealed that MyTrCa(-/-) mice did not mount IFN-I responses following VSV infection. Of note, treatment with rIFN-α protected the animals, qualifying MyTrCa(-/-) mice as a model to study the contribution of different immune cell subsets to the production of antiviral IFN-I. Upon adoptive transfer of wild-type plasmacytoid dendritic cells and subsequent VSV infection, MyTrCa(-/-) mice displayed significantly reduced viral loads in peripheral organs and showed prolonged survival. On the contrary, adoptive transfer of wild-type myeloid dendritic cells did not have such effects. Analysis of bone marrow chimeric mice revealed that TLR and RLH signaling of radioresistant and radiosensitive cells was required for efficient protection. Thus, upon VSV infection, plasmacytoid dendritic cell-derived IFN-I primarily protects peripheral organs, whereas concomitant TLR and RLH signaling of radioresistant stroma cells as well as of radiosensitive immune cells is needed to effectively protect against lethal disease.
多项研究表明,Toll样受体(TLR)以及视黄酸诱导基因I样解旋酶(RLH)信号通路有助于水泡性口炎病毒(VSV)介导的I型干扰素(IFN-I)反应的触发。然而,缺乏TLR的MyD88(-/-)Trif(-/-)小鼠和缺乏RLH的半胱天冬酶激活和募集结构域衔接蛋白诱导IFN-β(Cardif)(-/-)小鼠对致死性VSV静脉内感染的易感性仅略有增加。因此,我们探讨了TLR和RLH信号通路的协同作用或其他一些额外机制是否发挥了作用。为此,我们培育了MyD88(-/-)Trif(-/-)Cardif(-/-)(MyTrCa(-/-))小鼠,这些小鼠在静脉内感染低剂量VSV后会死亡,其动力学与缺乏IFN-I受体的小鼠相似。三种独立的方法(即分析IFN-α/β血清水平、用IFN-β报告基因小鼠进行实验以及研究局部IFN刺激基因的诱导)表明,MyTrCa(-/-)小鼠在VSV感染后不会产生IFN-I反应。值得注意的是,用重组IFN-α治疗可保护这些动物,这使MyTrCa(-/-)小鼠成为研究不同免疫细胞亚群对抗病毒IFN-I产生贡献的模型。在过继转移野生型浆细胞样树突状细胞并随后进行VSV感染后,MyTrCa(-/-)小鼠外周器官中的病毒载量显著降低,存活时间延长。相反,过继转移野生型髓样树突状细胞则没有这种效果。对骨髓嵌合小鼠的分析表明,抗辐射和辐射敏感细胞的TLR和RLH信号通路对于有效保护是必需的。因此,在VSV感染后,浆细胞样树突状细胞衍生的IFN-I主要保护外周器官,而抗辐射基质细胞以及辐射敏感免疫细胞的TLR和RLH信号通路协同作用对于有效预防致死性疾病是必要的。
Zotero 插件