Characteristics of viral ovarian tumor domain protease from two emerging orthonairoviruses and identification of Yezo virus human infections in northeastern China as early as 2012.

IF 3.8 2区 医学 Q2 VIROLOGY Journal of Virology Pub Date : 2025-02-25 Epub Date: 2024-12-31 DOI:10.1128/jvi.01727-24
Zi-Yun Chen, Jie Zhang, Pei-Jun He, Tao Xiong, Dai-Yun Zhu, Wen-Jie Zhu, Xue-Bing Ni, Li-Feng Du, Qian Wang, Ya-Wei Zhang, Luo-Yuan Xia, Dong-Sheng Chen, Liang-Jing Li, Ming-Zhu Zhang, Xiao Ming Cui, Tian-Hong Wang, Juan Wang, Zhenfei Wang, Tian-Feng An, Wu-Chun Cao, Xiao-Hua Liu, En-Jiong Huang, Na Jia
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Abstract

Emerging tick-borne orthonairovirus infections pose a growing global concern, with limited understanding of the viral ovarian tumor-like cysteine proteases (vOTUs) encoded by novel orthonairoviruses. These vOTUs, a group of deubiquinylases (DUBs), disrupt the innate immune response. Yezo virus (YEZV), a recently discovered pathogenic orthonairovirus, was first reported in Japan in 2021. In this study, we successfully isolated and identified YEZV and a new orthonairovirus, Jiànchuān tick virus (JCTV), from Ixodes persulcatus and Haemaphysalis montgomeryi ticks, respectively, in China. We found that the vOTU domains encoded by YEZV and JCTV exhibited both DUB and deISGylase activities, though with potentially less broad deISGylation compared to that of Crimean-Congo hemorrhagic fever virus (CCHFV) during natural infection. Phylogenetic analysis of global vOTUs, including 83 new sequences, revealed a high diversity of this domain. Interestingly, retrospective screening of tick-bite patients from 2012 to 2016 in northeastern China traced YEZV infections as far back as 2012, identifying four cases. Additionally, YEZV primarily infected I. persulcatus (31.4%) and Dermacentor nuttalli (10.5%) in northern China, while JCTV exhibited high infection rates in H. montgomeryi (81.3%) in southern China. In summary, our work emphasizes the active surveillance of orthonairovirus infections and the imperative need for the development of vOTU domain-targeted anti-virals, offering potential therapeutic solutions for a broad spectrum of orthonairoviruses.IMPORTANCEThe vOTUs, a group of DUBs, mimic the functions of host DUBs to enhance viral infectivity and may serve as potential drug targets. vOTUs from different orthonairoviruses exhibit distinct preferences toward ubiquitin (Ub) and ubiquitin-like protein interferon stimulated gene 15 (ISG15). In this study, we investigated the deubiquitinase and deISGylase functions of various orthonairoviral vOTUs using both an overexpression system and natural viral infections in vitro. Our findings illustrate that the vOTUs from YEZV and JCTV can cleave both Ub and ISG15 in an overexpression system, but these viruses exhibit potentially narrower deISGylation capacity than CCHFV during natural infection. This suggests that the diversity of vOTUs may have a potential relationship with the pathogenesis.

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早在2012年中国东北地区两种新出现的正鼻空气病毒卵巢肿瘤结构域蛋白酶特征及Yezo病毒人感染的鉴定
新出现的蜱传播的正交空气病毒感染引起了越来越多的全球关注,人们对新型正交空气病毒编码的病毒性卵巢肿瘤样半胱氨酸蛋白酶(vOTUs)的了解有限。这些votu,一组去泛素化酶(dub),破坏先天免疫反应。Yezo病毒(YEZV)是最近发现的一种致病性原鼻病毒,于2021年在日本首次报告。本研究在中国成功分离鉴定了一种YEZV病毒和一种新的蜱病毒Jiànchuān蜱病毒(JCTV),分别来自过硫伊蚊和蒙哥马利血蜱。我们发现,YEZV和JCTV编码的vOTU结构域在自然感染时具有DUB和去isgylase活性,但与克里米亚-刚果出血热病毒(CCHFV)相比,去isgylase的范围可能较小。对83个新序列的系统发育分析表明,该结构域具有高度的多样性。有趣的是,对中国东北地区2012年至2016年的蜱叮咬患者进行回顾性筛查,发现早在2012年就有4例YEZV感染。此外,YEZV主要在华北地区感染过乳伊蚊(31.4%)和毛足螨(10.5%),而JCTV在华南地区感染率较高(81.3%)。综上所述,我们的工作强调了对正鼻病毒感染的主动监测和开发vOTU域靶向抗病毒药物的迫切需要,为广泛的正鼻病毒提供潜在的治疗解决方案。重要意义votu是一组dub,模仿宿主dub的功能来增强病毒的感染性,可能是潜在的药物靶点。来自不同正交空气病毒的vOTUs对泛素(Ub)和泛素样蛋白干扰素刺激基因15 (ISG15)表现出不同的偏好。在这项研究中,我们利用过表达系统和体外自然病毒感染研究了各种正交空气病毒vOTUs的去泛素酶和去isgyylase功能。我们的研究结果表明,来自YEZV和JCTV的vOTUs可以在过表达系统中切割Ub和ISG15,但这些病毒在自然感染过程中表现出比CCHFV更窄的去isg酰化能力。这提示votu的多样性可能与发病机制有潜在的关系。
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来源期刊
Journal of Virology
Journal of Virology 医学-病毒学
CiteScore
10.10
自引率
7.40%
发文量
906
审稿时长
1 months
期刊介绍: Journal of Virology (JVI) explores the nature of the viruses of animals, archaea, bacteria, fungi, plants, and protozoa. We welcome papers on virion structure and assembly, viral genome replication and regulation of gene expression, genetic diversity and evolution, virus-cell interactions, cellular responses to infection, transformation and oncogenesis, gene delivery, viral pathogenesis and immunity, and vaccines and antiviral agents.
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