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本文引用的文献

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Rapid, Seamless Generation of Recombinant Poxviruses using Host Range and Visual Selection.利用宿主范围和视觉筛选快速、无缝地产生重组痘病毒
J Vis Exp. 2020 May 24(159). doi: 10.3791/61049.
2
Species-specific inhibition of capripoxvirus replication by host antiviral protein kinase R.宿主抗病毒蛋白激酶 R 特异性抑制羊痘病毒复制。
Ann N Y Acad Sci. 2019 Feb;1438(1):3-17. doi: 10.1111/nyas.13976. Epub 2018 Nov 1.
3
Bovine Vaccinia: Insights into the Disease in Cattle.牛痘病:对牛群疾病的深入了解。
Viruses. 2018 Mar 9;10(3):120. doi: 10.3390/v10030120.
4
A Single Amino Acid Dictates Protein Kinase R Susceptibility to Unrelated Viral Antagonists.单个氨基酸决定蛋白激酶R对无关病毒拮抗剂的敏感性。
PLoS Pathog. 2016 Oct 25;12(10):e1005966. doi: 10.1371/journal.ppat.1005966. eCollection 2016 Oct.
5
Opposing Roles of Double-Stranded RNA Effector Pathways and Viral Defense Proteins Revealed with CRISPR-Cas9 Knockout Cell Lines and Vaccinia Virus Mutants.利用CRISPR-Cas9基因敲除细胞系和痘苗病毒突变体揭示双链RNA效应途径和病毒防御蛋白的相反作用
J Virol. 2016 Aug 12;90(17):7864-79. doi: 10.1128/JVI.00869-16. Print 2016 Sep 1.
6
Myxoma virus M156 is a specific inhibitor of rabbit PKR but contains a loss-of-function mutation in Australian virus isolates.黏液瘤病毒M156是兔PKR的特异性抑制剂,但在澳大利亚病毒分离株中存在功能丧失突变。
Proc Natl Acad Sci U S A. 2016 Apr 5;113(14):3855-60. doi: 10.1073/pnas.1515613113. Epub 2016 Feb 22.
7
Review: Capripoxvirus Diseases: Current Status and Opportunities for Control.综述:山羊痘病毒病:现状与防控机遇
Transbound Emerg Dis. 2017 Jun;64(3):729-745. doi: 10.1111/tbed.12444. Epub 2015 Nov 13.
8
Ectopic expression of vaccinia virus E3 and K3 cannot rescue ectromelia virus replication in rabbit RK13 cells.痘苗病毒E3和K3的异位表达无法挽救兔RK13细胞中鼠痘病毒的复制。
PLoS One. 2015 Mar 3;10(3):e0119189. doi: 10.1371/journal.pone.0119189. eCollection 2015.
9
Seroprevalence of Rift Valley fever and lumpy skin disease in African buffalo (Syncerus caffer) in the Kruger National Park and Hluhluwe-iMfolozi Park, South Africa.南非克鲁格国家公园和伊西曼格利索湿地公园中非洲水牛(非洲野水牛)的裂谷热和结节性皮肤病血清阳性率。
J S Afr Vet Assoc. 2014 Oct 16;85(1):e1-e7. doi: 10.4102/jsava.v85i1.1075.
10
Characterization of sheep pox virus vaccine for cattle against lumpy skin disease virus.用于牛预防结节性皮肤病病毒的羊痘病毒疫苗特性研究
Antiviral Res. 2014 Sep;109:1-6. doi: 10.1016/j.antiviral.2014.06.009. Epub 2014 Jun 25.

囊尾蚴病毒和牛痘病毒对抗病毒蛋白激酶 R 的种属特异性抑制作用。

Species-specific inhibition of antiviral protein kinase R by capripoxviruses and vaccinia virus.

机构信息

School of Medicine, Department of Medial Microbiology and Immunology, University of California Davis, Davis, California.

Division of Biology, Kansas State University, Manhattan, Kansas.

出版信息

Ann N Y Acad Sci. 2019 Feb;1438(1):18-29. doi: 10.1111/nyas.14000. Epub 2019 Jan 15.

DOI:10.1111/nyas.14000
PMID:30644558
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7989821/
Abstract

Double-stranded RNA-activated protein kinase R (PKR) is an important and rapidly evolving antiviral kinase. Most poxviruses contain two distinct PKR inhibitors, called E3 and K3 in vaccinia virus (VACV), the prototypic orthopoxvirus. E3 prevents PKR homodimerization by binding double-stranded RNA, while K3 acts as a pseudosubstrate inhibitor by binding directly to activated PKR and thereby inhibiting interaction with its substrate eIF2α. In our study here, we analyzed E3 and K3 orthologs from the phylogenetically distinct capripoxviruses (CaPVs), which include lumpy skin disease virus, sheeppox virus, and goatpox virus. Whereas the sheeppox virus E3 ortholog did not substantially inhibit PKR, all three CaPV K3 orthologs showed species-specific inhibition of PKR, with strong inhibition of sheep, goat, and human PKR but only weak inhibition of cow and mouse PKR. In contrast, VACV K3 strongly inhibited cow and mouse PKR but not sheep, goat, or human PKR. Infection of cell lines from the respective species with engineered VACV strains that contained different K3 orthologs showed a good correlation of PKR inhibition with virus replication and eIF2α phosphorylation. Our results show that K3 orthologs can have dramatically different effects on PKR of different species and indicate that effective PKR inhibition by K3 orthologs is crucial for virus replication.

摘要

双链 RNA 激活蛋白激酶 R(PKR)是一种重要且快速进化的抗病毒激酶。大多数痘病毒都含有两种不同的 PKR 抑制剂,在牛痘病毒(VACV)中称为 E3 和 K3,是典型的正痘病毒。E3 通过结合双链 RNA 防止 PKR 同源二聚化,而 K3 则通过直接结合激活的 PKR 作为伪底物抑制剂起作用,从而抑制与其底物 eIF2α 的相互作用。在我们的研究中,我们分析了来自系统发育上不同的山羊痘病毒(CaPVs)的 E3 和 K3 同源物,包括牛痘、绵羊痘和山羊痘病毒。尽管绵羊痘病毒 E3 同源物不能显著抑制 PKR,但三种 CaPV K3 同源物均表现出对 PKR 的种特异性抑制,对绵羊、山羊和人 PKR 具有强烈抑制作用,但对牛和鼠 PKR 仅有弱抑制作用。相比之下,VACV K3 强烈抑制牛和鼠 PKR,但不抑制绵羊、山羊或人 PKR。用含有不同 K3 同源物的工程化 VACV 株感染相应物种的细胞系表明,PKR 抑制与病毒复制和 eIF2α 磷酸化呈良好相关性。我们的结果表明,K3 同源物对不同物种的 PKR 可能具有截然不同的影响,并表明 K3 同源物对 PKR 的有效抑制对于病毒复制至关重要。