Screening Legionella effectors for antiviral effects reveals Rab1 GTPase as a proviral factor coopted for tombusvirus replication.

中华核医学与分子影像杂志 Pub Date : 2019-10-22 Epub Date: 2019-10-07 DOI:10.1073/pnas.1911108116
Jun-Ichi Inaba, Kai Xu, Nikolay Kovalev, Harish Ramanathan, Craig R Roy, Brett D Lindenbach, Peter D Nagy
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引用次数: 20

Abstract

Bacterial virulence factors or effectors are proteins targeted into host cells to coopt or interfere with cellular proteins and pathways. Viruses often coopt the same cellular proteins and pathways to support their replication in infected cells. Therefore, we screened the Legionella pneumophila effectors to probe virus-host interactions and identify factors that modulate tomato bushy stunt virus (TBSV) replication in yeast surrogate host. Among 302 Legionella effectors tested, 28 effectors affected TBSV replication. To unravel a coopted cellular pathway in TBSV replication, the identified DrrA effector from Legionella was further exploited. We find that expression of DrrA in yeast or plants blocks TBSV replication through inhibiting the recruitment of Rab1 small GTPase and endoplasmic reticulum-derived COPII vesicles into the viral replication compartment. TBSV hijacks Rab1 and COPII vesicles to create enlarged membrane surfaces and optimal lipid composition within the viral replication compartment. To further validate our Legionella effector screen, we used the Legionella effector LepB lipid kinase to confirm the critical proviral function of PI(3)P phosphoinositide and the early endosomal compartment in TBSV replication. We demonstrate the direct inhibitory activity of LegC8 effector on TBSV replication using a cell-free replicase reconstitution assay. LegC8 inhibits the function of eEF1A, a coopted proviral host factor. Altogether, the identified bacterial effectors with anti-TBSV activity could be powerful reagents in cell biology and virus-host interaction studies. This study provides important proof of concept that bacterial effector proteins can be a useful toolbox to identify host factors and cellular pathways coopted by (+)RNA viruses.

筛选军团菌的抗病毒效应因子发现,Rab1 GTPase 是一种可用于墓穴病毒复制的病毒因子。
细菌毒力因子或效应物是一种靶向宿主细胞的蛋白质,用于共用或干扰细胞蛋白质和途径。病毒通常会利用相同的细胞蛋白和途径来支持其在受感染细胞中的复制。因此,我们筛选了嗜肺军团菌效应因子,以探究病毒与宿主之间的相互作用,并确定调节番茄矮花叶病毒(TBSV)在酵母代宿主中复制的因子。在测试的 302 种军团菌效应因子中,有 28 种效应因子会影响 TBSV 的复制。为了揭示 TBSV 复制过程中的协同细胞通路,我们进一步研究了军团菌中已发现的 DrrA 效应子。我们发现,在酵母或植物中表达 DrrA 会抑制 Rab1 小 GTPase 和内质网衍生 COPII 囊泡进入病毒复制区,从而阻止 TBSV 复制。TBSV 劫持 Rab1 和 COPII 囊泡,在病毒复制区内形成扩大的膜表面和最佳的脂质成分。为了进一步验证军团菌效应物筛选结果,我们使用军团菌效应物 LepB 脂质激酶证实了 PI(3)P 磷脂在 TBSV 复制过程中的关键性病毒功能和早期内体区。我们利用无细胞复制酶重组试验证明了 LegC8 效应子对 TBSV 复制的直接抑制活性。LegC8 可抑制 eEF1A 的功能,eEF1A 是一种共用的病毒宿主因子。总之,所发现的具有抗 TBSV 活性的细菌效应物可以成为细胞生物学和病毒-宿主相互作用研究的有力试剂。这项研究提供了一个重要的概念证明,即细菌效应蛋白可以作为一个有用的工具箱,用于识别被 (+)RNA 病毒共用的宿主因子和细胞通路。
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来源期刊
中华核医学与分子影像杂志
中华核医学与分子影像杂志 核医学,分子影像
自引率
0.00%
发文量
5088
期刊介绍: Chinese Journal of Nuclear Medicine and Molecular Imaging (CJNMMI) was established in 1981, with the name of Chinese Journal of Nuclear Medicine, and renamed in 2012. As the specialized periodical in the domain of nuclear medicine in China, the aim of Chinese Journal of Nuclear Medicine and Molecular Imaging is to develop nuclear medicine sciences, push forward nuclear medicine education and basic construction, foster qualified personnel training and academic exchanges, and popularize related knowledge and raising public awareness. Topics of interest for Chinese Journal of Nuclear Medicine and Molecular Imaging include: -Research and commentary on nuclear medicine and molecular imaging with significant implications for disease diagnosis and treatment -Investigative studies of heart, brain imaging and tumor positioning -Perspectives and reviews on research topics that discuss the implications of findings from the basic science and clinical practice of nuclear medicine and molecular imaging - Nuclear medicine education and personnel training - Topics of interest for nuclear medicine and molecular imaging include subject coverage diseases such as cardiovascular diseases, cancer, Alzheimer’s disease, and Parkinson’s disease, and also radionuclide therapy, radiomics, molecular probes and related translational research.
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