Foot-and-Mouth Disease Virus Leader Protease Cleaves G3BP1 and G3BP2 and Inhibits Stress Granule Formation

Visser, Lenneke de; Medina, Gisselle N.; Rabouw, Huib H.; Groot, Raoul J. de; Langereis, Martijn A.; Santos, Teresa de los; Kuppeveld, Frank J. M. van

doi:10.1128/jvi.00922-18

Cited by 75 publications

(79 citation statements)

References 62 publications

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“…Indeed, infection with EMCV-2A pro , but not EMCV-2Am, resulted in cleavage of eIF4G, while infection with EMCV-3C pro resulted in G3BP1 cleavage. No G3BP1 cleavage was observed in cells infected with either EMCV-L Zn , which is consistent with our previous observations (11,41,42), or EMCV-3Cm.…”

Section: Resultssupporting

confidence: 93%

“…It has been suggested that EMCV 3C pro cleaves G3BP1 and that this prevents SG assembly, although this cleavage is observed only at very late stages of infection (10 to 12 hpi) (40). In contrast, we and others did not observe G3BP1 cleavage in cells infected with either EMCV or Theiler's murine encephalomyelitis virus, and instead provided extensive evidence that the leader protein has an essential role in suppressing SG formation in cardiovirus-infected cells (11,41,42). As part of these studies, we generated EMCV-L Zn , a mutant virus in which the leader protein is inactivated by mutations that disrupt its zinc finger domain and that, as a consequence, can no longer suppress SG formation.…”

Section: Resultscontrasting

confidence: 50%

“…The oligonucleotides used for these PCRs encode flanking XhoI and NotI restriction sites that were used to ligate the PCR products into the desired plasmids. The 3C pro genes were ligated into the pcDNA-GFP vector, while the 2A pro genes were ligated into the pIRES-EGFP-MCS plasmid, both of which plasmids were described previously (42).…”

Section: Methodsmentioning

confidence: 99%

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Essential Role of Enterovirus 2A Protease in Counteracting Stress Granule Formation and the Induction of Type I Interferon

Visser

Langereis

Rabouw

et al. 2019

J Virol

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Most viruses have acquired mechanisms to suppress antiviral alpha/beta interferon (IFN-␣/␤) and stress responses. Enteroviruses (EVs) actively counteract the induction of IFN-␣/␤ gene transcription and stress granule (SG) formation, which are increasingly implicated as a platform for antiviral signaling, but the underlying mechanisms remain poorly understood. Both viral proteases (2A pro and 3C pro ) have been implicated in the suppression of these responses, but these conclusions predominantly rely on ectopic overexpression of viral proteases or addition of purified viral proteases to cell lysates. Here, we present a detailed and comprehensive comparison of the effect of individual enterovirus proteases on the formation of SGs and the induction of IFN-␣/␤ gene expression in infected cells for representative members of the enterovirus species EV-A to EV-D. First, we show that SG formation and IFN-␤ induction are suppressed in cells infected with EV-A71, coxsackie B3 virus (CV-B3), CV-A21, and EV-D68. By introducing genes encoding CV-B3 proteases in a recombinant encephalomyocarditis virus (EMCV) that was designed to efficiently activate antiviral responses, we show that CV-B3 2A pro , but not 3C pro , is the major antagonist that counters SG formation and IFN-␤ gene transcription and that 2A pro 's proteolytic activity is essential for both functions. 2A pro efficiently suppressed SG formation despite protein kinase R (PKR) activation and ␣ subunit of eukaryotic translation initiation factor 2 phosphorylation, suggesting that 2A pro antagonizes SG assembly or promotes its disassembly. Finally, we show that the ability to suppress SG formation and IFN-␤ gene transcription is conserved in the 2A pro of EV-A71, CV-A21, and EV-D68. Collectively, our results indicate that enterovirus 2A pro plays a key role in inhibiting innate antiviral cellular responses. IMPORTANCE Enteroviruses are important pathogens that can cause a variety of diseases in humans, including aseptic meningitis, myocarditis, hand-foot-and-mouth disease, conjunctivitis, and acute flaccid paralysis. Like many other viruses, enteroviruses must counteract antiviral cellular responses to establish an infection. It has been suggested that enterovirus proteases cleave cellular factors to perturb antiviral pathways, but the exact contribution of viral proteases 2A pro and 3C pro remains elusive. Here, we show that 2A pro , but not 3C pro , of all four human EV species (EV-A to EV-D) inhibits SG formation and IFN-␤ gene transcription. Our observations suggest that enterovirus 2A pro has a conserved function in counteracting antiviral host responses and thereby is the main enterovirus "security protein." Understanding the molecular mechanisms of enterovirus immune evasion strategies may help to develop countermeasures to control infections with these viruses. FIG 5 Enterovirus 2A pro suppresses the induction of type I IFN gene expression. (A)HeLa R19 cells were infected with the indicated viruses at an MOI of 10, and the cells were lysed at 8 hpi, total cell...

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Section: Resultssupporting

confidence: 93%

Section: Resultscontrasting

confidence: 50%

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Essential Role of Enterovirus 2A Protease in Counteracting Stress Granule Formation and the Induction of Type I Interferon

Visser

Langereis

Rabouw

et al. 2019

J Virol

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“…For rhinoviruses, nothing is known about their capacity to manipulate stress granule formation, however, for other picornaviruses the 2A and L proteases have recently been shown to interfere by cleaving stress granule factors such as G3BP1 and G3BP2 [106][107][108][109]. A recent report showed that binding of eiF4GI translation factor to stress granule-inducing protein G3BP1 is essential for antiviral stress granule formation, and this interaction is disrupted by the 2A or L proteases of picornaviruses [110].…”

Section: Manipulation Of Stress Granule Formationmentioning

confidence: 99%

Innate Immune Evasion by Human Respiratory RNA Viruses

2019

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The impact of respiratory virus infections on the health of children and adults can be very significant. Yet, in contrast to most other childhood infections as well as other viral and bacterial diseases, prophylactic vaccines or effective antiviral treatments against viral respiratory infections are either still not available, or provide only limited protection. Given the widespread prevalence, a general lack of natural sterilizing immunity, and/or high morbidity and lethality rates of diseases caused by influenza, respiratory syncytial virus, coronaviruses, and rhinoviruses, this difficult situation is a genuine societal challenge. A thorough understanding of the virushost interactions during these respiratory infections will most probably be pivotal to ultimately meet these challenges. This review attempts to provide a comparative overview of the knowledge about an important part of the interaction between respiratory viruses and their host: the arms race between host innate immunity and viral innate immune eva-

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“…G3BP1, also known as G3BP or HDH-VIII, is a ubiquitously expressed protein and functions as a sequence-specific, phosphorylation-dependent helicase, a cofactor, an endoribonuclease, and more (19). Recently, it has been reported that FMDV L pro and 3C pro may cleave G3BP1 to inhibit stress granule (SG) formation; however, FMDV L pro and 3C pro do not interact with G3BP1 (20,21). This finding prompted us to determine the FMDV proteins that interact with G3BP1 and the mechanism by which it regulates G3BP1 to facilitate FMDV replication and growth.…”

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confidence: 99%

Foot-and-Mouth Disease Virus 3A Protein Causes Upregulation of Autophagy-Related Protein LRRC25 To Inhibit the G3BP1-Mediated RIG-Like Helicase-Signaling Pathway

Yang

et al. 2020

J Virol

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Foot-and-mouth disease virus (FMDV) is one of the most notorious pathogens in the global livestock industry. To establish an infection, FMDV needs to counteract host antiviral responses. Several studies have shown how FMDV suppresses the type I interferon (IFN) response; however, whether FMDV modulates the integrated autophagy and innate immunity remains largely unknown. Here, the porcine Ras-GAP SH3-binding protein 1 (G3BP1) was shown to promote the retinoic acid-inducible gene I (RIG-I)-like helicase (RLH) signaling by upregulating the expression of RIG-I and melanoma differentiation-associated gene 5 (MDA5). FMDV nonstructural protein 3A interacted with G3BP1 to inhibit G3BP1 expression and G3BP1-mediated RLH signaling by upregulating the expression of autophagy-related protein LRRC25. In addition, 3A proteins of other picornaviruses, including Seneca Valley virus (SVV) 3A, enterovirus 71 (EV71) 3A, and encephalomyocarditis virus (EMCV) 3A, also showed similar actions. Taking the data together, we elucidated, for the first time, a novel mechanism by which FMDV has evolved to inhibit IFN signaling and counteract host innate antiviral responses by autophagy. IMPORTANCE We show that foot-and-mouth disease virus (FMDV) 3A inhibits retinoic acid-inducible gene I (RIG-I)-like helicase signaling by degrading G3BP1 protein. Furthermore, FMDV 3A reduces G3BP1 by upregulating the expression of autophagy-related protein LRRC25. Additionally, other picornavirus 3A proteins, such as Seneca Valley virus (SVV) 3A, enterovirus 71 (EV71) 3A, and encephalomyocarditis virus (EMCV) 3A, also degrade G3BP1 by upregulating LRRC25 expression. This study will help us improve the design of current vaccines and aid the development of novel control strategies to combat FMD.

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Foot-and-Mouth Disease Virus Leader Protease Cleaves G3BP1 and G3BP2 and Inhibits Stress Granule Formation

Cited by 75 publications

References 62 publications

Essential Role of Enterovirus 2A Protease in Counteracting Stress Granule Formation and the Induction of Type I Interferon

Essential Role of Enterovirus 2A Protease in Counteracting Stress Granule Formation and the Induction of Type I Interferon

Innate Immune Evasion by Human Respiratory RNA Viruses

Foot-and-Mouth Disease Virus 3A Protein Causes Upregulation of Autophagy-Related Protein LRRC25 To Inhibit the G3BP1-Mediated RIG-Like Helicase-Signaling Pathway

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