The C-Terminal Domain of Salmonid Alphavirus Nonstructural Protein 2 (nsP2) Is Essential and Sufficient To Block RIG-I Pathway Induction and Interferon-Mediated Antiviral Response

Jami, Raphaël; Mérour, Emilie; Bernard, Julie; Lamoureux, Annie; Millet, Jean K.; Biacchesi, Stéphane

doi:10.1128/jvi.01155-21

Cited by 4 publications

(1 citation statement)

References 74 publications

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“…High levels of intracellular SAV3 virus may thus possibly block or suppress expression of antiviral responses in the RTgutGC cells. Both mammalian and fish alphaviruses including SAV have been described to suppress or evade host interferon responses to escape the innate immune system of the host [46] and this could be related to protein shutdown [24]. A comparative study of SAV2 infection in TO and SHK-1 cells showed higher expression of the interferon-induced gene mx in SHK-1 cells concomitant with a lesser ability to induce CPE compared to TO cells, indicating that the ability of the virus to interfere with the cell's interferon signaling pathway is important for intracellular SAV replication and the ability to induce cytopathogenicity [43].…”

Section: Discussionmentioning

confidence: 99%

Establishment of an In Vitro Model to Study Viral Infections of the Fish Intestinal Epithelium

Løkka

Gamil

Evensen

et al. 2023

Cells

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Viral infections are still a major concern for the aquaculture industry. For salmonid fish, even though breeding strategies and vaccine development have reduced disease outbreaks, viral diseases remain among the main challenges having a negative impact on the welfare of fish and causing massive economic losses for the industry. The main entry port for viruses into the fish is through mucosal surfaces including that of the gastrointestinal tract. The contradictory functions of this surface, both creating a barrier towards the external environment and at the same time being responsible for the uptake of nutrients and ion/water regulation make it particularly vulnerable. The connection between dietary components and viral infections in fish has been poorly investigated and until now, a fish intestinal in vitro model to investigate virus–host interactions has been lacking. Here, we established the permissiveness of the rainbow trout intestinal cell line RTgutGC towards the important salmonid viruses—infectious pancreatic necrosis virus (IPNV), salmonid alphavirus (subtype 3, SAV3) and infectious salmon anemia virus (ISAV)—and explored the infection mechanisms of the three different viruses in these cells at different virus to cell ratios. Cytopathic effect (CPE), virus replication in the RTgutGC cells, antiviral cell responses and viral effects on the barrier permeability of polarized cells were investigated. We found that all virus species infected and replicated in RTgutGC cells, although with different replication kinetics and ability to induce CPE and host responses. The onset and progression of CPE was more rapid at high multiplicity of infection (MOI) for IPNV and SAV3 while the opposite was true of ISAV. A positive correlation between the MOI used and the induction of antiviral responses was observed for IPNV while a negative correlation was detected for SAV3. Viral infections compromised barrier integrity at early time points prior to observations of CPE microscopically. Further, the replication of IPNV and ISAV had a more pronounced effect on barrier function than SAV3. The in vitro infection model established herein can thus provide a novel tool to generate knowledge about the infection pathways and mechanisms used to surpass the intestinal epithelium in salmonid fish, and to study how a virus can potentially compromise gut epithelial barrier functions.

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Section: Discussionmentioning

confidence: 99%

Establishment of an In Vitro Model to Study Viral Infections of the Fish Intestinal Epithelium

Løkka

Gamil

Evensen

et al. 2023

Cells

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SAV Nsp2 regulates NF-κB signaling to induce inflammatory responses by targeting host DDX3

Gao

Han

et al. 2023

Developmental & Comparative Immunology

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Unexpected regulatory functions of cyprinid Viperin on inflammation and metabolism

Chaumont,

Jouneau,

Huetz

et al. 2024

BMC Genomics

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Background Viperin, also known as radical S-adenosyl-methionine domain containing protein 2 (RSAD2), is an interferon-inducible protein that is involved in the innate immune response against a wide array of viruses. In mammals, Viperin exerts its antiviral function through enzymatic conversion of cytidine triphosphate (CTP) into its antiviral analog ddhCTP as well as through interactions with host proteins involved in innate immune signaling and in metabolic pathways exploited by viruses during their life cycle. However, how Viperin modulates the antiviral response in fish remains largely unknown. Results For this purpose, we developed a fathead minnow (Pimephales promelas) clonal cell line in which the unique viperin gene has been knocked out by CRISPR/Cas9 genome-editing. In order to decipher the contribution of fish Viperin to the antiviral response and its regulatory role beyond the scope of the innate immune response, we performed a comparative RNA-seq analysis of viperin−/− and wildtype cell lines upon stimulation with recombinant fathead minnow type I interferon. Conclusions Our results revealed that Viperin does not exert positive feedback on the canonical type I IFN but acts as a negative regulator of the inflammatory response by downregulating specific pro-inflammatory genes and upregulating repressors of the NF-κB pathway. It also appeared to play a role in regulating metabolic processes, including one carbon metabolism, bone formation, extracellular matrix organization and cell adhesion.

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The C-Terminal Domain of Salmonid Alphavirus Nonstructural Protein 2 (nsP2) Is Essential and Sufficient To Block RIG-I Pathway Induction and Interferon-Mediated Antiviral Response

Cited by 4 publications

References 74 publications

Establishment of an In Vitro Model to Study Viral Infections of the Fish Intestinal Epithelium

Establishment of an In Vitro Model to Study Viral Infections of the Fish Intestinal Epithelium

SAV Nsp2 regulates NF-κB signaling to induce inflammatory responses by targeting host DDX3

Unexpected regulatory functions of cyprinid Viperin on inflammation and metabolism

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