MAVS Self-Association Mediates Antiviral Innate Immune Signaling

ABSTRACT The innate immune system recognizes nucleic acids during viral infection and stimulates cellular antiviral responses. Intracellular detection of RNA virus infection is mediated by the RNA helicases RIG-I (retinoic acid inducible gene I) and MDA-5, which recognize viral RNA and signal through the adaptor molecule MAVS (mitochondrial antiviral signaling) to stimulate the phosphorylation and activation of the transcription factors IRF3 (interferon regulatory factor 3) and IRF7. Once activated, IRF3 and IRF7 turn on the expression of type I interferons, such as beta interferon. Interestingly, unlike other signaling molecules identified in this pathway, MAVS contains a C-terminal transmembrane (TM) domain that is essential for both type I interferon induction and localization of MAVS to the mitochondrial outer membrane. However, the role the MAVS TM domain plays in signaling remains unclear. Here we report the identification of a function for the TM domain in mediating MAVS self-association. The activation of RIG-I/MDA-5 leads to the TM-dependent dimerization of the MAVS N-terminal caspase recruitment domain, thereby providing an interface for direct binding to and activation of the downstream effector TRAF3 (tumor necrosis factor receptor-associated factor 3). Our results reveal a role for MAVS self-association in antiviral innate immunity signaling and provide a molecular mechanism for downstream signal transduction.

Download Full-text

STING signaling and host defense against microbial infection

Experimental & Molecular Medicine ◽

10.1038/s12276-019-0333-0 ◽

2019 ◽

Vol 51 (12) ◽

pp. 1-10 ◽

Cited By ~ 12

Author(s):

Jeonghyun Ahn ◽

Glen N. Barber

Keyword(s):

Host Defense ◽

Innate Immune ◽

Type I Interferons ◽

Type I ◽

Microbial Infection ◽

Immune Signaling ◽

Pathogen Invasion ◽

Innate Immune Signaling ◽

Specific Pathogen ◽

Microbial Dna

AbstractThe first line of host defense against infectious agents involves activation of innate immune signaling pathways that recognize specific pathogen-associated molecular patterns (PAMPs). Key triggers of innate immune signaling are now known to include microbial-specific nucleic acid, which is rapidly detected in the cytosol of the cell. For example, RIG-I-like receptors (RLRs) have evolved to detect viral RNA species and to activate the production of host defense molecules and cytokines that stimulate adaptive immune responses. In addition, host defense countermeasures, including the production of type I interferons (IFNs), can also be triggered by microbial DNA from bacteria, viruses and perhaps parasites and are regulated by the cytosolic sensor, stimulator of interferon genes (STING). STING-dependent signaling is initiated by cyclic dinucleotides (CDNs) generated by intracellular bacteria following infection. CDNs can also be synthesized by a cellular synthase, cGAS, following interaction with invasive cytosolic self-DNA or microbial DNA species. The importance of STING signaling in host defense is evident since numerous pathogens have developed strategies to prevent STING function. Here, we review the relevance of STING-controlled innate immune signaling in host defense against pathogen invasion, including microbial endeavors to subvert this critical process.

Download Full-text

An Update on Innate Immune Responses during SARS-CoV-2 Infection

Viruses ◽

10.3390/v13102060 ◽

2021 ◽

Vol 13 (10) ◽

pp. 2060

Author(s):

Yu Zhang ◽

Shuaiyin Chen ◽

Yuefei Jin ◽

Wangquan Ji ◽

Weiguo Zhang ◽

...

Keyword(s):

Immune Responses ◽

Innate Immune ◽

Type I Interferons ◽

Organ Injury ◽

Type I ◽

Innate Immune Responses ◽

Innate Immune Signaling ◽

Viral Proteases ◽

Viral Components ◽

The Relationship

The severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) is a member of the Coronaviridae family, which is responsible for the COVID-19 pandemic followed by unprecedented global societal and economic disruptive impact. The innate immune system is the body’s first line of defense against invading pathogens and is induced by a variety of cellular receptors that sense viral components. However, various strategies are exploited by SARS-CoV-2 to disrupt the antiviral innate immune responses. Innate immune dysfunction is characterized by the weak generation of type I interferons (IFNs) and the hypersecretion of pro-inflammatory cytokines, leading to mortality and organ injury in patients with COVID-19. This review summarizes the existing understanding of the mutual effects between SARS-CoV-2 and the type I IFN (IFN-α/β) responses, emphasizing the relationship between host innate immune signaling and viral proteases with an insight on tackling potential therapeutic targets.

Download Full-text

ZCCHC3 modulates TLR3-mediated signaling by promoting recruitment of TRIF to TLR3

Journal of Molecular Cell Biology ◽

10.1093/jmcb/mjaa004 ◽

2020 ◽

Vol 12 (4) ◽

pp. 251-262

Author(s):

Ru Zang ◽

Huan Lian ◽

Xuan Zhong ◽

Qing Yang ◽

Hong-Bing Shu

Keyword(s):

Rna Virus ◽

Interleukin 1 ◽

Innate Immune ◽

Type I Interferons ◽

Poly I:C ◽

Type I ◽

Antiviral Genes ◽

Ligand Stimulation ◽

Tlr3 Ligand Poly ◽

Receptor Domain

Abstract Toll-like receptor 3 (TLR3)-mediated signaling is important for host defense against RNA virus. Upon viral RNA stimulation, toll and interleukin-1 receptor domain-containing adaptor inducing IFN-β (TRIF) is recruited to TLR3 and then undergoes oligomerization, which is required for the recruitment of downstream molecules to transmit signals. Here, we identified zinc finger CCHC-type containing 3 (ZCCHC3) as a positive regulator of TLR3-mediated signaling. Overexpression of ZCCHC3 promoted transcription of downstream antiviral genes stimulated by the synthetic TLR3 ligand poly(I:C). ZCCHC3-deficiency markedly inhibited TLR3- but not TLR4-mediated induction of type I interferons (IFNs) and proinflammatory cytokines. Zcchc3−/− mice were more resistant to poly(I:C)- but not lipopolysaccharide-induced inflammatory death. Mechanistically, ZCCHC3 promoted recruitment of TRIF to TLR3 after poly(I:C) stimulation. Our findings reveal that ZCCHC3 plays an important role in TLR3-mediated innate immune response by promoting the recruitment of TRIF to TLR3 after ligand stimulation.

Download Full-text

A mutation in POLR3E impairs antiviral immune response and RNA polymerase III

Proceedings of the National Academy of Sciences ◽

10.1073/pnas.2009947117 ◽

2020 ◽

Vol 117 (36) ◽

pp. 22113-22121

Author(s):

Aravind Ramanathan ◽

Michael Weintraub ◽

Natalie Orlovetskie ◽

Raphael Serruya ◽

Dhivakar Mani ◽

...

Keyword(s):

Rna Polymerase ◽

Rna Virus ◽

Rna Polymerase Iii ◽

Innate Immune ◽

Type I Interferons ◽

Homozygous Mutation ◽

Type I ◽

Protein Subunit ◽

Antiviral Immune Response ◽

Pol Iii

RNA polymerase (Pol) III has a noncanonical role of viral DNA sensing in the innate immune system. This polymerase transcribes viral genomes to produce RNAs that lead to induction of type I interferons (IFNs). However, the genetic and functional links of Pol III to innate immunity in humans remain largely unknown. Here, we describe a rare homozygous mutation (D40H) in the POLR3E gene, coding for a protein subunit of Pol III, in a child with recurrent and systemic viral infections and Langerhans cell histiocytosis. Fibroblasts derived from the patient exhibit impaired induction of type I IFN and increased susceptibility to human cytomegalovirus (HCMV) infection. Cultured cell lines infected with HCMV show induction of POLR3E expression. However, induction is not restricted to DNA virus, as sindbis virus, an RNA virus, enhances the expression of this protein. Likewise, foreign nonviral DNA elevates the steady-state level of POLR3E and elicits promoter-dependent and -independent transcription by Pol III. Remarkably, the molecular mechanism underlying the D40H mutation of POLR3E involves the assembly of defective initiation complexes of Pol III. Our study links mutated POLR3E and Pol III to an innate immune deficiency state in humans.

Download Full-text

Signaling from the RNA sensor RIG-I is regulated by ufmylation

10.1101/2021.10.26.465929 ◽

2021 ◽

Author(s):

Daltry L Snider ◽

Moonhee Park ◽

Kristen A Murphy ◽

Dia C Beachboard ◽

Stacy M Horner

Keyword(s):

Signal Transduction ◽

Translational Control ◽

Rna Binding ◽

Rna Virus ◽

Adaptor Protein ◽

Innate Immune ◽

Type I ◽

Conjugation System ◽

Contact Sites ◽

Innate Immune Signaling

The RNA binding protein RIG-I is a key initiator of the antiviral innate immune response. The signaling that mediates the antiviral response downstream of RIG-I is transduced through the adaptor protein MAVS and results in the induction of type I and III interferons (IFN). This signal transduction occurs at endoplasmic reticulum (ER)-mitochondrial contact sites, to which RIG-I and other signaling proteins are recruited following their activation. RIG-I signaling is highly regulated to prevent aberrant activation of this pathway and dysregulated induction of IFN. Previously, we identified UFL1, the E3 ligase of the ubiquitin-like modifier conjugation system called ufmylation, UFL1, as one of the proteins recruited to membranes at ER-mitochondrial contact sites in response to RIG-I activation. Here, we show that UFL1, as well as the process of ufmylation, promote IFN induction in response to RIG-I activation. We find that following RNA virus infection, UFL1 is recruited to the membrane targeting protein 14-3-3ε, and that this complex is then recruited to activated RIG-I to promote downstream innate immune signaling. Importantly, loss of ufmylation prevents 14-3-3ε interaction with RIG-I, which abrogates the interaction of RIG-I with MAVS and thus downstream signal transduction that induces IFN. Our results define ufmylation as an integral regulatory component of the RIG-I signaling pathway and as a post-translational control for IFN induction.

Download Full-text

FIP200 restricts RNA virus infection by facilitating RIG-I activation

Communications Biology ◽

10.1038/s42003-021-02450-1 ◽

2021 ◽

Vol 4 (1) ◽

Author(s):

Lingyan Wang ◽

Kun Song ◽

Wenzhuo Hao ◽

Yakun Wu ◽

Girish Patil ◽

...

Keyword(s):

Virus Infection ◽

Rna Virus ◽

Innate Immune ◽

Host Susceptibility ◽

In Vivo Studies ◽

Helicase Domain ◽

Type I ◽

Immune Signaling ◽

Innate Immune Signaling

AbstractRetinoic acid-inducible gene I (RIG-I) senses viral RNA and instigates an innate immune signaling cascade to induce type I interferon expression. Currently, the regulatory mechanisms controlling RIG-I activation remain to be fully elucidated. Here we show that the FAK family kinase-interacting protein of 200 kDa (FIP200) facilitates RIG-I activation. FIP200 deficiency impaired RIG-I signaling and increased host susceptibility to RNA virus infection. In vivo studies further demonstrated FIP200 knockout mice were more susceptible to RNA virus infection due to the reduced innate immune response. Mechanistic studies revealed that FIP200 competed with the helicase domain of RIG-I for interaction with the two tandem caspase activation and recruitment domains (2CARD), thereby facilitating the release of 2CARD from the suppression status. Furthermore, FIP200 formed a dimer and facilitated 2CARD oligomerization, thereby promoting RIG-I activation. Taken together, our study defines FIP200 as an innate immune signaling molecule that positively regulates RIG-I activation.

Download Full-text

Chicken interferon regulatory factor 7 (IRF7) can control ALV-J virus infection by triggering type I interferon production through affecting genes related with innate immune signaling pathway

Developmental & Comparative Immunology ◽

10.1016/j.dci.2021.104026 ◽

2021 ◽

Vol 119 ◽

pp. 104026

Author(s):

Yan Wang ◽

Fuling Yang ◽

Huadong Yin ◽

Qijian He ◽

Yuxiang Lu ◽

...

Keyword(s):

Type I Interferon ◽

Interferon Regulatory Factor ◽

Innate Immune ◽

Type I ◽

Interferon Production ◽

Regulatory Factor ◽

Innate Immune Signaling ◽

Immune Signaling Pathway ◽

Interferon Regulatory Factor 7 ◽

Innate Immune Signaling Pathway

Download Full-text

Bacterial Cyclic Dinucleotides and the cGAS–cGAMP–STING Pathway: A Role in Periodontitis?

Pathogens ◽

10.3390/pathogens10060675 ◽

2021 ◽

Vol 10 (6) ◽

pp. 675

Author(s):

Samira Elmanfi ◽

Mustafa Yilmaz ◽

Wilson W. S. Ong ◽

Kofi S. Yeboah ◽

Herman O. Sintim ◽

...

Keyword(s):

Immune Response ◽

Periodontal Disease ◽

Innate Immune ◽

Host Cells ◽

Type I Interferons ◽

Type I ◽

Vaccine Adjuvants ◽

Cyclic Dinucleotides ◽

Sting Pathway

Host cells can recognize cytosolic double-stranded DNAs and endogenous second messengers as cyclic dinucleotides—including c-di-GMP, c-di-AMP, and cGAMP—of invading microbes via the critical and essential innate immune signaling adaptor molecule known as STING. This recognition activates the innate immune system and leads to the production of Type I interferons and proinflammatory cytokines. In this review, we (1) focus on the possible role of bacterial cyclic dinucleotides and the STING/TBK1/IRF3 pathway in the pathogenesis of periodontal disease and the regulation of periodontal immune response, and (2) review and discuss activators and inhibitors of the STING pathway as immune response regulators and their potential utility in the treatment of periodontitis. PubMed/Medline, Scopus, and Web of Science were searched with the terms “STING”, “TBK 1”, “IRF3”, and “cGAS”—alone, or together with “periodontitis”. Current studies produced evidence for using STING-pathway-targeting molecules as part of anticancer therapy, and as vaccine adjuvants against microbial infections; however, the role of the STING/TBK1/IRF3 pathway in periodontal disease pathogenesis is still undiscovered. Understanding the stimulation of the innate immune response by cyclic dinucleotides opens a new approach to host modulation therapies in periodontology.

Download Full-text

Type I interferons and the innate immune response—more than just antiviral cytokines

Molecular Immunology ◽

10.1016/j.molimm.2004.11.008 ◽

2005 ◽

Vol 42 (8) ◽

pp. 869-877 ◽

Cited By ~ 80

Author(s):

Peter L Smith ◽

Giovanna Lombardi ◽

Graham R Foster

Keyword(s):

Immune Response ◽

Innate Immune Response ◽

Innate Immune ◽

Type I Interferons ◽

Type I

Download Full-text

DDX3 directly facilitates IKKα activation and regulates downstream signalling pathways

Biochemical Journal ◽

10.1042/bcj20180163 ◽

2018 ◽

Vol 475 (22) ◽

pp. 3595-3607 ◽

Cited By ~ 5

Author(s):

Anthony Fullam ◽

Lili Gu ◽

Yvette Höhn ◽

Martina Schröder

Keyword(s):

Nuclear Factor Κb ◽

Innate Immune ◽

Type I Interferons ◽

Signalling Pathways ◽

Type I ◽

Nuclear Factor ◽

Toll Like Receptor ◽

Disease States ◽

Dead Box ◽

Iκb Kinase

DDX3 is a DEAD-box RNA helicase that we and others have previously implicated in antiviral immune signalling pathways leading to type I interferon (IFN) induction. We previously demonstrated that it directly interacts with the kinase IKKε (IκB kinase ε), enhances it activation, and then facilitates phosphorylation of the transcription factor IRF3 by IKKε. However, the TLR7/9 (Toll-like receptor 7/9)-mediated pathway, one of the most physiologically relevant IFN induction pathways, proceeds independently of IKKε or the related kinase TBK1 (TANK-binding kinase 1). This pathway induces type I IFN production via the kinases NIK (NF-κB-inducing kinase) and IKKα and is activated when plasmacytoid dendritic cells sense viral nucleic acids. In the present study, we demonstrate that DDX3 also directly interacts with IKKα and enhances its autophosphorylation and -activation. Modulation of DDX3 expression consequently affected NIK/IKKα-mediated IRF7 phosphorylation and induction of type I interferons. In addition, alternative NF-κB (nuclear factor-κB) activation, another pathway regulated by NIK and IKKα, was also down-regulated in DDX3 knockdown cells. This substantially broadens the effects of DDX3 in innate immune signalling to pathways beyond TBK1/IKKε and IFN induction. Dysregulation of these pathways is involved in disease states, and thus, our research might implicate DDX3 as a potential target for their therapeutic manipulation.

Download Full-text