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Structures of Arenaviral Nucleoproteins with Triphosphate dsRNA Reveal a Unique Mechanism of Immune Suppression

机译:带有三磷酸dsRNA的腔室病毒核蛋白的结构揭示了独特的免疫抑制机制。

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摘要

A hallmark of severe Lassa fever is the generalized immune suppression, the mechanism of which is poorly understood. Lassa virus (LASV) nucleoprotein (NP) is the only known 3′-5′ exoribonuclease that can suppress type I interferon (IFN) production possibly by degrading immune-stimulatory RNAs. How this unique enzymatic activity of LASV NP recognizes and processes RNA substrates is unknown. We provide an atomic view of a catalytically active exoribonuclease domain of LASV NP (LASV NP-C) in the process of degrading a 5′ triphosphate double-stranded (ds) RNA substrate, a typical pathogen-associated molecular pattern molecule, to induce type I IFN production. Additionally, we provide for the first time a high-resolution crystal structure of an active exoribonuclease domain of Tacaribe arenavirus (TCRV) NP. Coupled with the in vitro enzymatic and cell-based interferon suppression assays, these structural analyses strongly support a unified model of an exoribonuclease-dependent IFN suppression mechanism shared by all known arenaviruses. New knowledge learned from these studies should aid the development of therapeutics against pathogenic arenaviruses that can infect hundreds of thousands of individuals and kill thousands annually.
机译:严重的拉沙热的标志是普遍的免疫抑制,其机制尚不清楚。拉萨病毒(LASV)核蛋白(NP)是唯一已知的3'-5'核糖核酸外切酶,可以抑制I型干扰素(IFN)的产生,可能是通过降解免疫刺激性RNA来抑制的。 LASV NP的这种独特的酶促活性如何识别和加工RNA底物尚不清楚。我们提供了在降解5'三磷酸双链(ds)RNA底物(一种典型的病原体相关分子模式分子)的过程中,LASV NP(LASV NP-C)具有催化活性的核酸外切酶结构域的原子视图。我产生IFN。此外,我们首次提供了Tacaribe arenavirus(TCRV)NP的活性外切核糖核酸酶结构域的高分辨率晶体结构。结合体外酶促和基于细胞的干扰素抑制测定,这些结构分析强有力地支持了所有已知的类鼻病毒共有的依赖外核糖核酸酶的干扰素抑制机制的统一模型。从这些研究中获得的新知识应有助于抗病原性沙门氏病毒的治疗方法的发展,这种病毒可感染成千上万的人,每年造成数千人死亡。

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