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病毒 RNA 激活免疫系统 OAS/RNAse L 途径的分子基础和特异性。

Molecular Bases and Specificity behind the Activation of the Immune System OAS/RNAse L Pathway by Viral RNA.

机构信息

Université Paris Cité and CNR, ITODYS, F-75006 Paris, France.

Université de Lorraine and CNRS, LPCT UMR 7019, F-54000 Nancy, France.

出版信息

Viruses. 2024 Aug 2;16(8):1246. doi: 10.3390/v16081246.

Abstract

The first line of defense against invading pathogens usually relies on innate immune systems. In this context, the recognition of exogenous RNA structures is primordial to fight, notably, against RNA viruses. One of the most efficient immune response pathways is based on the sensing of RNA double helical motifs by the oligoadenylate synthase (OAS) proteins, which in turn triggers the activity of RNase L and, thus, cleaves cellular and viral RNA. In this contribution, by using long-range molecular dynamics simulations, complemented with enhanced sampling techniques, we elucidate the structural features leading to the activation of OAS by interaction with a model double-strand RNA oligomer mimicking a viral RNA. We characterize the allosteric regulation induced by the nucleic acid leading to the population of the active form of the protein. Furthermore, we also identify the free energy profile connected to the active vs. inactive conformational transitions in the presence and absence of RNA. Finally, the role of two RNA mutations, identified as able to downregulate OAS activation, in shaping the protein/nucleic acid interface and the conformational landscape of OAS is also analyzed.

摘要

先天免疫系统通常是抵御入侵病原体的第一道防线。在这种情况下,识别外源 RNA 结构对于抵御 RNA 病毒尤为重要。最有效的免疫反应途径之一是基于寡聚腺苷酸合成酶 (OAS) 蛋白对 RNA 双螺旋结构的感应,这反过来又触发了 RNase L 的活性,从而切割细胞和病毒 RNA。在本研究中,我们使用长程分子动力学模拟,并辅以增强采样技术,阐明了与模拟病毒 RNA 的双链 RNA 寡聚物相互作用导致 OAS 激活的结构特征。我们描述了核酸诱导的变构调节,导致蛋白活性形式的形成。此外,我们还确定了在存在和不存在 RNA 的情况下,活性与非活性构象转变相关的自由能分布。最后,还分析了两种 RNA 突变(能够下调 OAS 的激活)在塑造蛋白/核酸界面和 OAS 的构象景观中的作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/86b9/11359028/b0efa6ea66e9/viruses-16-01246-g001.jpg

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