Herpes Simplex Virus 1 UL36USP Antagonizes Type I Interferon-Mediated Antiviral Innate Immunity

J Virol. 2018 Sep 12;92(19):e01161-18. doi: 10.1128/JVI.01161-18. Print 2018 Oct 1.

Abstract

Type I interferons (IFNs), as major components of the innate immune system, play a vital role in host resistance to a variety of pathogens. Canonical signaling mediated by type I IFNs activates the Janus kinase-signal transducer and activator of transcription (JAK-STAT) pathway through binding to the IFN-α/β receptor (IFNAR), resulting in transcription of IFN-stimulated genes (ISGs). However, viruses have evolved multiple strategies to evade this process. Here, we report that herpes simplex virus 1 (HSV-1) ubiquitin-specific protease (UL36USP) abrogates the type I IFN-mediated signaling pathway independent of its deubiquitinase (DUB) activity. In this study, ectopically expressed UL36USP inhibited IFN-β-induced activation of ISRE promoter and transcription of ISGs, and overexpression of UL36USP lacking DUB activity did not influence this effect. Furthermore, UL36USP was demonstrated to antagonize IFN-β-induced activation of JAKs and STATs via specifically binding to the IFNAR2 subunit and blocking the interaction between JAK1 and IFNAR2. More importantly, knockdown of HSV-1 UL36USP restored the formation of JAK1-IFNAR2 complex. These findings underline the roles of UL36USP-IFNAR2 interaction in counteracting the type I IFN-mediated signaling pathway and reveal a novel evasion mechanism of antiviral innate immunity by HSV-1.IMPORTANCE Type I IFNs mediate transcription of numerous antiviral genes, creating a remarkable antiviral state in the host. Viruses have evolved various mechanisms to evade this response. Our results indicated that HSV-1 encodes a ubiquitin-specific protease (UL36USP) as an antagonist to subvert type I IFN-mediated signaling. UL36USP was identified to significantly inhibit IFN-β-induced signaling independent of its deubiquitinase (DUB) activity. The underlying mechanism of UL36USP antagonizing type I IFN-mediated signaling was to specifically bind with IFNAR2 and disassociate JAK1 from IFNAR2. For the first time, we identify UL36USP as a crucial suppressor for HSV-1 to evade type I IFN-mediated signaling. Our findings also provide new insights into the innate immune evasion by HSV-1 and will facilitate our understanding of host-virus interplay.

Keywords: HSV-1; IFNAR2; UL36USP; type I IFN-mediated signaling.

MeSH terms

  • Animals
  • Chlorocebus aethiops
  • Gene Expression Regulation
  • HEK293 Cells
  • Herpesvirus 1, Human / genetics*
  • Herpesvirus 1, Human / immunology
  • Humans
  • Immune Evasion*
  • Immunity, Innate*
  • Interferon-Stimulated Gene Factor 3, gamma Subunit / genetics
  • Interferon-Stimulated Gene Factor 3, gamma Subunit / immunology
  • Interferon-alpha / genetics*
  • Interferon-alpha / immunology
  • Interferon-beta / genetics*
  • Interferon-beta / immunology
  • Janus Kinase 1 / genetics
  • Janus Kinase 1 / immunology
  • RNA, Small Interfering / genetics
  • RNA, Small Interfering / immunology
  • Receptor, Interferon alpha-beta / genetics*
  • Receptor, Interferon alpha-beta / immunology
  • STAT Transcription Factors / genetics
  • STAT Transcription Factors / immunology
  • Signal Transduction
  • Vero Cells
  • Viral Proteins / genetics*
  • Viral Proteins / immunology

Substances

  • IFNAR1 protein, human
  • IFNAR2 protein, human
  • Interferon-Stimulated Gene Factor 3, gamma Subunit
  • Interferon-alpha
  • RNA, Small Interfering
  • STAT Transcription Factors
  • UL36 protein, Human herpesvirus 1
  • Viral Proteins
  • Receptor, Interferon alpha-beta
  • Interferon-beta
  • JAK1 protein, human
  • Janus Kinase 1