Comparative transcriptome reveals EphA2 and c-Fos as key factors driving enhanced replication in high-passage porcine deltacoronavirus strain

IF 2.4 2区农林科学 Q3 MICROBIOLOGY

Veterinary microbiology Pub Date : 2024-07-31 DOI:10.1016/j.vetmic.2024.110211

Shiyu Liu , Qi Peng , Baochao Fan , Gege Zhang , Wenlong He , Chuanhong Wang , Jingyuan Xie , Xu Song , Boshui Yuan , Rongli Guo , Jizong Li , Bin Li

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引用次数: 0

Abstract

Porcine deltacoronavirus (PDCoV), a cross-species transmissible enterovirus, frequently induces severe diarrhea and vomiting symptoms in piglets, which not only pose a significant menace to the global pig industry but also a potential public safety risk. In a previous study, we isolated a vaccine candidate, PDCoV CZ2020-P100, by passaging a parental PDCoV strain in vitro, exhibiting attenuated virulence and enhanced replication. However, the factors underlying these differences between primary and passaged strains remain unknown. In this study, we present the transcriptional landscapes of porcine kidney epithelial cells (LLC-PK1) cells infected with PDCoV CZ2020-P1 strain and P100 strain using the RNA-sequencing. We identified 105 differentially expressed genes (DEGs) in P1-infected cells and 295 DEGs in P100-infected cells. Enrichment analyses indicated that many DEGs showed enrichment in immune and inflammatory responses, with a more and higher upregulation of DEGs enriched in the P100-infected group. Notably, the DEGs were concentrated in the MAPK pathway within the P100-infected group, with significant upregulation in EphA2 and c-Fos. Knockdown of EphA2 and c-Fos reduced PDCoV infection and significantly impaired P100 replication compared to P1, suggesting a novel mechanism in which EphA2 and c-Fos are highly involved in passaged virus replication. Our findings illuminate the resemblances and distinctions in the gene expression patterns of host cells infected with P1 and P100, confirming that EphA2 and c-Fos play key roles in high-passage PDCoV replication. These results enhance our understanding of the changes in virulence and replication capacity during the process of passaging.

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比较转录组显示，EphA2 和 c-Fos 是驱动高通量猪三角锥病毒株增强复制的关键因素

猪三角冠状病毒（PDCoV）是一种跨种传播的肠道病毒，经常诱发仔猪严重腹泻和呕吐症状，不仅对全球养猪业构成重大威胁，也存在潜在的公共安全风险。在之前的一项研究中，我们通过传代亲本 PDCoV 株，分离出了一种候选疫苗 PDCoV CZ2020-P100，它表现出减毒和增强的复制能力。然而，原代毒株和传代毒株之间存在这些差异的根本原因尚不清楚。在本研究中，我们利用 RNA 序列分析了感染 PDCoV CZ2020-P1 株和 P100 株的猪肾上皮细胞（LLC-PK1）的转录图谱。我们在 P1 感染细胞中发现了 105 个差异表达基因 (DEG)，在 P100 感染细胞中发现了 295 个差异表达基因 (DEG)。富集分析表明，许多 DEGs 在免疫和炎症反应中表现出富集，P100 感染组中富集的 DEGs 上调更多也更高。值得注意的是，DEGs主要集中在P100感染组的MAPK通路中，其中EphA2和c-Fos显著上调。与P1相比，EphA2和c-Fos的敲除减少了PDCoV的感染，并显著影响了P100的复制，这表明EphA2和c-Fos高度参与了传代病毒复制的新机制。我们的研究结果阐明了宿主细胞感染 P1 和 P100 后基因表达模式的相似性和差异性，证实了 EphA2 和 c-Fos 在高通量 PDCoV 复制中发挥着关键作用。这些结果加深了我们对传代过程中毒力和复制能力变化的理解。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Veterinary microbiology 农林科学-兽医学

CiteScore

5.90

自引率

6.10%

发文量

221

审稿时长

52 days

期刊介绍： Veterinary Microbiology is concerned with microbial (bacterial, fungal, viral) diseases of domesticated vertebrate animals (livestock, companion animals, fur-bearing animals, game, poultry, fish) that supply food, other useful products or companionship. In addition, Microbial diseases of wild animals living in captivity, or as members of the feral fauna will also be considered if the infections are of interest because of their interrelation with humans (zoonoses) and/or domestic animals. Studies of antimicrobial resistance are also included, provided that the results represent a substantial advance in knowledge. Authors are strongly encouraged to read - prior to submission - the Editorials (''Scope or cope'' and ''Scope or cope II'') published previously in the journal. The Editors reserve the right to suggest submission to another journal for those papers which they feel would be more appropriate for consideration by that journal. Original research papers of high quality and novelty on aspects of control, host response, molecular biology, pathogenesis, prevention, and treatment of microbial diseases of animals are published. Papers dealing primarily with immunology, epidemiology, molecular biology and antiviral or microbial agents will only be considered if they demonstrate a clear impact on a disease. Papers focusing solely on diagnostic techniques (such as another PCR protocol or ELISA) will not be published - focus should be on a microorganism and not on a particular technique. Papers only reporting microbial sequences, transcriptomics data, or proteomics data will not be considered unless the results represent a substantial advance in knowledge. Drug trial papers will be considered if they have general application or significance. Papers on the identification of microorganisms will also be considered, but detailed taxonomic studies do not fall within the scope of the journal. Case reports will not be published, unless they have general application or contain novel aspects. Papers of geographically limited interest, which repeat what had been established elsewhere will not be considered. The readership of the journal is global.