Comparative effects of Novirhabdovirus genes on modulating constitutive transcription and innate antiviral responses, in different teleost host cell types

Bartolomeo Gorgoglione; Jeffery L. Ringiesn; Loc H. Pham; Brian S. Shepherd; Douglas W. Leaman

doi:10.1186/s12985-020-01372-4

Virology Journal (Jul 2020)

Comparative effects of Novirhabdovirus genes on modulating constitutive transcription and innate antiviral responses, in different teleost host cell types

Bartolomeo Gorgoglione,
Jeffery L. Ringiesn,
Loc H. Pham,
Brian S. Shepherd,
Douglas W. Leaman

Affiliations

Bartolomeo Gorgoglione: Aquatic Animal Health Laboratory, Department of Pathobiology and Diagnostic Investigation, CVM & Department of Fisheries and Wildlife, CANR - Michigan State University
Jeffery L. Ringiesn: Department of Biological Sciences, Wright State University
Loc H. Pham: Department of Biological Sciences, University of Toledo
Brian S. Shepherd: USDA/ARS/School of Freshwater Sciences, University of Wisconsin-Milwaukee
Douglas W. Leaman: Department of Biological Sciences, Wright State University

DOI: https://doi.org/10.1186/s12985-020-01372-4
Journal volume & issue: Vol. 17, no. 1
pp. 1 – 14

Abstract

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Abstract Background Infectious hematopoietic necrosis virus (IHNV) and viral hemorrhagic septicemia virus (VHSV) are highly contagious, pathogenic Novirhabdoviruses affecting fish and are thusly notifiable diseases with the World Organization for Animal Health. This study assessed the relative capacities of IHNV and VHSV genes to modulate host general transcription and explores the abilities of specific IHNV genes to interfere with the interferon pathway in heterogenous teleost cell-lines. Methods Optimized protocols allowed for efficient transient transfections in EPC, BF-2, RTG-2 and RTgill-W1 cell lines of plasmids encoding IHNV (M genogroup) and VHSV (-IVb genotype) genes, including N, P, M, G and NV. Their impact on general cellular transcription was measured 48 hours post transfection (hpt) with luciferase constructs driven by a modified β-Actin promoter (pCAG). Their modulation of the innate antiviral immune response was characterized 72 hpt, using luciferase constructs measuring rainbow trout Type I IFN or MX-1 promoter augmentation, upon MAVS co-transfection. Results M was generally confirmed as the strongest constitutive transcriptional suppressor while IHNV P, but not VHSV P, augmented constitutive transcription in fibroblastic cell types. Cell-specific effects were observed for viral G gene, with VHSV G exhibiting suppression of basal transcription in EPC and BF-2 but not in trout cells; while IHNV G was stimulatory in RTG-2, but inhibitory in RTgill-W1. NV consistently stimulated constitutive transcription, with higher augmentation patterns seen in fibroblastic compared to epithelial cells, and for IHNV NV compared to VHSV NV. The innate antiviral immune response, focusing on the IFN pathway, was silenced by IHNV M in all cell lines tested. IHNV N showed a dose-dependent suppression of type I IFN, but with minor effects on MX-1. IHNV P and G played minor IFN-inhibitory roles, consistent and dose-dependent only for G in rainbow trout cells. IHNV NV mediated a consistent stimulatory effect on either Type I IFN or MX-1, but much less pronounced in RTgill-W1. Conclusions This study extends our understanding of Novirhabdoviruses-host interaction, showing differential innate immune responses in heterogenous cell types. Viral regulators of innate immune signaling are identified, either as dose-dependent suppressors (such as M and N) or stimulators (mainly NV), indicating novel targets for the design of more efficient vaccination strategies.

Published in Virology Journal

ISSN: 1743-422X (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine: Internal medicine: Infectious and parasitic diseases
Website: http://virologyj.biomedcentral.com

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