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Reversible inhibition of murine cytomegalovirus replication by gamma interferon (IFN-γ) in primary macrophages involves a primed type I IFN-signaling subnetwork for full establishment of an immediate-early antiviral state (CROSBI ID 176897)

Prilog u časopisu | izvorni znanstveni rad | međunarodna recenzija

Kropp, K.A. ; Robertson, K.A. ; Sing, G. ; Rodriguez-Martin, S. ; Blanc, M. ; Lacaze, P. ; Hassim, M.F. ; Khondoker, M.R. ; Busche, A. ; Dickinson, P. et al. Reversible inhibition of murine cytomegalovirus replication by gamma interferon (IFN-γ) in primary macrophages involves a primed type I IFN-signaling subnetwork for full establishment of an immediate-early antiviral state // Journal of virology, 85 (2011), 19; 10286-10299. doi: 10.1128/JVI.00373-11

Podaci o odgovornosti

Kropp, K.A. ; Robertson, K.A. ; Sing, G. ; Rodriguez-Martin, S. ; Blanc, M. ; Lacaze, P. ; Hassim, M.F. ; Khondoker, M.R. ; Busche, A. ; Dickinson, P. ; Forster, T. ; Strobl, B. ; Mueller, M. ; Jonjić, Stipan ; Angulo, A. ; Ghazal, P.

engleski

Reversible inhibition of murine cytomegalovirus replication by gamma interferon (IFN-γ) in primary macrophages involves a primed type I IFN-signaling subnetwork for full establishment of an immediate-early antiviral state

Activated macrophages play a central role in controlling inflammatory responses to infection and are tightly regulated to rapidly mount responses to infectious challenge. Type I interferon (alpha/beta interferon [IFN-α/β]) and type II interferon (IFN-γ) play a crucial role in activating macrophages and subsequently restricting viral infections. Both types of IFNs signal through related but distinct signaling pathways, inducing a vast number of interferon-stimulated genes that are overlapping but distinguishable. The exact mechanism by which IFNs, particularly IFN-γ, inhibit DNA viruses such as cytomegalovirus (CMV) is still not fully understood. Here, we investigate the antiviral state developed in macrophages upon reversible inhibition of murine CMV by IFN-γ. On the basis of molecular profiling of the reversible inhibition, we identify a significant contribution of a restricted type I IFN subnetwork linked with IFN-γ activation. Genetic knockout of the type I-signaling pathway, in the context of IFN-γ stimulation, revealed an essential requirement for a primed type I-signaling process in developing a full refractory state in macrophages. A minimal transient induction of IFN-β upon macrophage activation with IFN-γ is also detectable. In dose and kinetic viral replication inhibition experiments with IFN-γ, the establishment of an antiviral effect is demonstrated to occur within the first hours of infection. We show that the inhibitory mechanisms at these very early times involve a blockade of the viral major immediate-early promoter activity. Altogether our results show that a primed type I IFN subnetwork contributes to an immediate-early antiviral state induced by type II IFN activation of macrophages, with a potential further amplification loop contributed by transient induction of IFN-β.

MCMV; IFN gamma; immediate-early gene

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Podaci o izdanju

85 (19)

2011.

10286-10299

objavljeno

0022-538X

10.1128/JVI.00373-11

Povezanost rada

Temeljne medicinske znanosti

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