Varicella Viruses Inhibit Interferon- Stimulated JAK-STAT Signaling through Multiple Mechanisms

Verweij, M.; Wellish, M.; Whitmer, T.; Malouli, D.; Lapel, M.; Jonjić, Stipan; Haas, J.; DeFilippis, V.; Mahalingam, R.; Früh, K.

izvor podataka: crosbi ✓

Varicella Viruses Inhibit Interferon- Stimulated JAK-STAT Signaling through Multiple Mechanisms (CROSBI ID 218307)

Prilog u časopisu | izvorni znanstveni rad | međunarodna recenzija

Verweij, M. ; Wellish, M. ; Whitmer, T. ; Malouli, D. ; Lapel, M. ; Jonjić, Stipan ; Haas, J. ; DeFilippis, V. ; Mahalingam, R. ; Früh, K. Varicella Viruses Inhibit Interferon- Stimulated JAK-STAT Signaling through Multiple Mechanisms // Plos pathogens, 11 (2015), 5-5. doi: 10.1371/journal.ppat.1004901

Podaci o odgovornosti

Autori

Verweij, M. ; Wellish, M. ; Whitmer, T. ; Malouli, D. ; Lapel, M. ; Jonjić, Stipan ; Haas, J. ; DeFilippis, V. ; Mahalingam, R. ; Früh, K.

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Osnovni podaci na ostalim jezicima

Jezik

engleski

Naslov

Varicella Viruses Inhibit Interferon- Stimulated JAK-STAT Signaling through Multiple Mechanisms

Sažetak

Varicella zoster virus (VZV) causes chickenpox in humans and, subsequently, establishes latency in the sensory ganglia from where it reactivates to cause herpes zoster. Infection of rhesus macaques with simian varicella virus (SVV) recapitulates VZV pathogenesis in humans thus representing a suitable animal model for VZV infection. While the type I interferon (IFN) response has been shown to affect VZV replication, the virus employs counter mechanisms to prevent the induction of anti-viral IFN stimulated genes (ISG). Here, we demonstrate that SVV inhibits type I IFN-activated signal transduction via the JAK-STAT pathway. SVV-infected rhesus fibroblasts were refractory to IFN stimulation displaying reduced protein levels of IRF9 and lacking STAT2 phosphorylation. Since previous work implicated involvement of the VZV immediate early gene product ORF63 in preventing ISGinduction we studied the role of SVV ORF63 in generating resistance to IFN treatment. Interestingly, SVV ORF63 did not affect STAT2 phosphorylation but caused IRF9 degradation in a proteasome-dependent manner, suggesting that SVV employs multiple mechanisms to counteract the effect of IFN. Control of SVV ORF63 protein levels via fusion to a dihydrofolate reductase (DHFR)-degradation domain additionally confirmed its requirement for viral replication. Our results also show a prominent reduction of IRF9 and inhibition of STAT2 phosphorylation in VZV-infected cells. In addition, cells expressing VZV ORF63 blocked IFN-stimulation and displayed reduced levels of the IRF9 protein. Taken together, our data suggest that varicella ORF63 prevents ISG-induction both directly via IRF9 degradation and indirectly via transcriptional control of viral proteins that interfere with STAT2 phosphorylation. SVV and VZV thus encode multiple viral gene products that tightly control IFNinduced anti-viral responses. PLOS Pathogens

Ključne riječi

Varicella zoster viruse (VZV); ORF 63; JAK-STAT signaling

Napomena

nije evidentirano

Jezik

nije evidentirano

Naslov

nije evidentirano

Sažetak

nije evidentirano

Ključne riječi

nije evidentirano

Napomena

nije evidentirano

Podaci o izdanju

Časopis

Plos pathogens

Volumen (broj)

Godina

2015.

Stranice rada

5-5

Status objave rada

objavljeno

ISSN

1553-7366

DOI

10.1371/journal.ppat.1004901

Povezanost rada

Povezane osobe

Stipan Jonjić (autor/i)

Povezane ustanove

Medicinski fakultet u Rijeci (062) (autorova ustanova)

Povezani projekti

Molekularni mehanizmi citomegalovirusnog izmicanja imunološkom nadzoru (rezultat rada na projektu)

Područje

Temeljne medicinske znanosti

Poveznice

doi.org

journals.plos.org

dx.doi.org

Indeksiranost

Scopus

Current Contents Connect (CCC)

Medline

Web of Science Core Collection, Science Citation Index Expanded (WoSCC-SCI-Exp)

Web of Science Core Collection, SCI-Exp, SSCI & A&HCI (WoSCC-SCI-Exp, SSCI, A&HCI)