Limited Effects of Type I Interferons on Kyasanur Forest Disease Virus in Cell Culture

Overview

Journal PLoS Negl Trop Dis

Specialties Infectious Diseases
Tropical Medicine

Date 2016 Aug 2

PMID 27479197

Citations 7

Authors

Bradley W M Cook

Charlene Ranadheera

Aidan M Nikiforuk

Todd A Cutts

Darwyn Kobasa

Deborah A Court

Steven S Theriault

Affiliations

Soon will be listed here.

Abstract

Background: The tick-borne flavivirus, Kyasanur Forest disease virus (KFDV) causes seasonal infections and periodic outbreaks in south-west India. The current vaccine offers poor protection with reported issues of coverage and immunogenicity. Since there are no approved prophylactic therapeutics for KFDV, type I IFN-α/β subtypes were assessed for antiviral potency against KFDV in cell culture.

Methodology/principal Findings: The continued passage of KFDV-infected cells with re-administered IFN-α2a treatment did not eliminate KFDV and had little effect on infectious particle production whereas the IFN-sensitive, green fluorescent protein-expressing vesicular stomatitis virus (VSV-GFP) infection was controlled. Further evaluation of the other IFN-α/β subtypes versus KFDV infection indicated that single treatments of either IFN-αWA and IFN-αΚ appeared to be more effective than IFN-α2a at reducing KFDV titres. Concentration-dependent analysis of these IFN-α/β subtypes revealed that regardless of subtype, low concentrations of IFN were able to limit cytopathic effects (CPE), while significantly higher concentrations were needed for inhibition of virion release. Furthermore, expression of the KFDV NS5 in cell culture before IFN addition enabled VSV-GFP to overcome the effects of IFN-α/β signalling, producing a robust infection.

Conclusions/significance: Treatment of cell culture with IFN does not appear to be suitable for KFDV eradication and the assay used for such studies should be carefully considered. Further, it appears that the NS5 protein is sufficient to permit KFDV to bypass the antiviral properties of IFN. We suggest that other prophylactic therapeutics should be evaluated in place of IFN for treatment of individuals with KFDV disease.

Citing Articles

Computational Exploration of Potential Pharmacological Inhibitors Targeting the Envelope Protein of the Kyasanur Forest Disease Virus.

Achappa S, Aldabaan N, Desai S, Muddapur U, Shaikh I, Mahnashi M Pharmaceuticals (Basel). 2024; 17(7).

PMID: 39065734 PMC: 11279457. DOI: 10.3390/ph17070884.

Ocular Manifestations of Flavivirus Infections.

Zina S, Hoarau G, Labetoulle M, Khairallah M, Rousseau A Pathogens. 2023; 12(12).

PMID: 38133340 PMC: 10747099. DOI: 10.3390/pathogens12121457.

Alkhurma haemorrhagic fever virus causes lethal disease in IFNAR mice.

Bhatia B, Haddock E, Shaia C, Rosenke R, Meade-White K, Griffin A Emerg Microbes Infect. 2021; 10(1):1077-1087.

PMID: 34013842 PMC: 8183530. DOI: 10.1080/22221751.2021.1932609.

Kyasanur Forest Disease and Alkhurma Hemorrhagic Fever Virus-Two Neglected Zoonotic Pathogens.

Bhatia B, Feldmann H, Marzi A Microorganisms. 2020; 8(9).

PMID: 32932653 PMC: 7564883. DOI: 10.3390/microorganisms8091406.

Immune Evasion Strategies Used by Zika Virus to Infect the Fetal Eye and Brain.

Nelson B, Roby J, Dobyns W, Rajagopal L, Gale Jr M, Adams Waldorf K Viral Immunol. 2019; 33(1):22-37.

PMID: 31687902 PMC: 6978768. DOI: 10.1089/vim.2019.0082.

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