The herpesviral antagonist m152 reveals differential activation of STING-dependent IRF and NF-κB signaling and STING's dual role during MCMV infection

Markus Stempel; Baca Chan; Vanda Juranić Lisnić; Astrid Krmpotić; Josephine Hartung; Søren R Paludan; Nadia Füllbrunn; Niels Aw Lemmermann; Melanie M Brinkmann

doi:10.15252/embj.2018100983

The herpesviral antagonist m152 reveals differential activation of STING-dependent IRF and NF-κB signaling and STING's dual role during MCMV infection

EMBO J. 2019 Mar 1;38(5):e100983. doi: 10.15252/embj.2018100983. Epub 2019 Jan 29.

Authors

Markus Stempel¹, Baca Chan¹, Vanda Juranić Lisnić², Astrid Krmpotić², Josephine Hartung¹, Søren R Paludan³, Nadia Füllbrunn¹, Niels Aw Lemmermann⁴, Melanie M Brinkmann^{5

6}

Affiliations

¹ Viral Immune Modulation Research Group, Helmholtz Centre for Infection Research, Braunschweig, Germany.
² Center for Proteomics, Faculty of Medicine, University of Rijeka, Rijeka, Croatia.
³ Department of Biomedicine, Aarhus Research Center for Innate Immunology, University of Aarhus, Aarhus, Denmark.
⁴ Institute for Virology and Research Center for Immunotherapy, University Medical Center of the Johannes Gutenberg-University Mainz, Mainz, Germany.
⁵ Viral Immune Modulation Research Group, Helmholtz Centre for Infection Research, Braunschweig, Germany m.brinkmann@tu-bs.de.
⁶ Institute of Genetics, Technische Universität Braunschweig, Braunschweig, Germany.

Abstract

Cytomegaloviruses (CMVs) are master manipulators of the host immune response. Here, we reveal that the murine CMV (MCMV) protein m152 specifically targets the type I interferon (IFN) response by binding to stimulator of interferon genes (STING), thereby delaying its trafficking to the Golgi compartment from where STING initiates type I IFN signaling. Infection with an MCMV lacking m152 induced elevated type I IFN responses and this leads to reduced viral transcript levels both in vitro and in vivo This effect is ameliorated in the absence of STING Interestingly, while m152 inhibits STING-mediated IRF signaling, it did not affect STING-mediated NF-κB signaling. Analysis of how m152 targets STING translocation reveals that STING activates NF-κB signaling already from the ER prior to its trafficking to the Golgi. Strikingly, this response is important to promote early MCMV replication. Our results show that MCMV has evolved a mechanism to specifically antagonize the STING-mediated antiviral IFN response, while preserving its pro-viral NF-κB response, providing an advantage in the establishment of an infection.

Keywords: STING; IRF3; NF‐κB; herpesvirus; innate immunity.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
Cytomegalovirus Infections / immunology*
Cytomegalovirus Infections / metabolism
Cytomegalovirus Infections / virology
Host-Pathogen Interactions / immunology*
Interferon Regulatory Factors / genetics
Interferon Regulatory Factors / metabolism*
Interferon Type I / metabolism*
Membrane Glycoproteins / genetics
Membrane Glycoproteins / metabolism*
Membrane Proteins / physiology*
Mice
Mice, Inbred BALB C
Mice, Inbred C57BL
Mice, Knockout
Muromegalovirus / genetics
Muromegalovirus / isolation & purification
Muromegalovirus / pathogenicity
NF-kappa B / genetics
NF-kappa B / metabolism*
Protein Binding
Viral Proteins / genetics
Viral Proteins / metabolism*
Virus Replication

Substances

Interferon Regulatory Factors
Interferon Type I
Membrane Glycoproteins
Membrane Proteins
NF-kappa B
Sting1 protein, mouse
Viral Proteins
m152 protein, cytomegalovirus