Rotavirus NSP1 Inhibits NFκB Activation by Inducing Proteasome-Dependent Degradation of β-TrCP: A Novel Mechanism of IFN Antagonism

Graff, Joel W.; Ettayebi, Khalil; Hardy, Michele E.

doi:10.1371/journal.ppat.1000280

Cited by 154 publications

(190 citation statements)

References 65 publications

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“…Adenovirus E1A protein inhibits TNF-a-induced NF-kB activation through suppression of IKK activity and IkBa phosphorylation (36). Rotavirus NSP1 inhibits NF-kB activation by inducing proteasomedependent degradation of b-transducin repeat-containing protein (37,38). In the current study, we report that EV71 2C protein can directly interact with IKKb by inhibiting IKKb activation and IkBa phosphorylation/degradation, and thus inhibits TNF-ainduced NF-kB activation.…”

Section: Discussionsupporting

confidence: 48%

Enterovirus 71 2C Protein Inhibits TNF-α–Mediated Activation of NF-κB by Suppressing IκB Kinase β Phosphorylation

Zheng

Zhang

et al. 2011

The Journal of Immunology

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Enterovirus 71 (EV71), a single, positive-stranded RNA virus, has been regarded as the most important neurotropic enterovirus after the eradication of the poliovirus. EV71 infection can cause hand, foot, and mouth disease or herpangina. Cytokine storm with elevated levels of proinflammatory and inflammatory cytokines, including TNF-α, has been proposed to explain the pathogenesis of EV71-induced disease. TNF-α–mediated NF-κB signaling pathway plays a key role in inflammatory response. We hypothesized that EV71 might also moderate host inflammation by interfering with this pathway. In this study, we tested this hypothesis and identified EV71 2C protein as an antagonist of TNF-α–mediated activation of NF-κB signaling pathway. Expression of 2C protein significantly reduced TNF-α–mediated NF-κB activation in 293T cells as measured by gene reporter and gel mobility shift assays. Furthermore, overexpression of TNFR-associated factor 2-, MEK kinase 1-, IκB kinase (IKK)α-, or IKKβ-induced NF-κB activation, but not constitutively active mutant of IKKβ (IKKβ SS/EE)-induced NF-κB activation, was inhibited by 2C protein. These data together suggested that the activation of IKKβ is most likely targeted by 2C; this notion was further strengthened by immunoblot detection of IKKβ phosphorylation and IκBα phosphorylation and degradation. Coimmunoprecipitation and colocalization of 2C and IKKβ expressed in mammalian cells provided compelling evidence that 2C interacts with IKKβ. Collectively, our data indicate that EV71 2C protein inhibits IKKβ activation and thus blocks NF-κB activation.

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Section: Discussionsupporting

confidence: 48%

Enterovirus 71 2C Protein Inhibits TNF-α–Mediated Activation of NF-κB by Suppressing IκB Kinase β Phosphorylation

Zheng

Zhang

et al. 2011

The Journal of Immunology

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“…The rotavirus gene segment encoding the nonstructural protein 1 (NSP1) is an important determinant of host restriction of viral replication both in vitro (17,53) and in vivo (9). Specifically, we along with others have reported a role for NSP1 in regulating the ability of rotavirus to efficiently cause diarrhea in mice (9), spread from animal to animal (9), replicate in vivo and in vitro (4,(15)(16)(17), and antagonize IFN (4,5,17,24,25,53). Thus, the host innate immune response is an important determinant of rotavirus host range restriction and depends on both the virus strain and host cell or tissue type.…”

Section: In Mouse Embryonic Fibroblasts (Mefs) the Bovine Rotavirusmentioning

confidence: 85%

“…At least two distinct mechanisms by which rotaviruses inhibit the host IFN response have been reported: (i) NSP1-mediated proteasomal degradation of host transcription factors IRF3 and IRF7, resulting in diminished IFN-␤ gene transcription and antiviral activity (4,5), and (ii) proteasomal degradation of ␤-TrCP, leading to inhibition of NF-B activity and subsequent IFN-␤ gene transcription (24). In contrast to these examples, we reported that the UK bovine rotavirus strain was unable to block IFN-␤ secretion in murine fibroblasts (17), and this correlated with the lack of murine IRF3 degradation by UK NSP1 (53).…”

mentioning

confidence: 99%

The Early Interferon Response to Rotavirus Is Regulated by PKR and Depends on MAVS/IPS-1, RIG-I, MDA-5, and IRF3

Pruijssers

Dermody

et al. 2011

J Virol

134

136

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In mouse embryonic fibroblasts (MEFs), the bovine rotavirus (UK strain) but not the simian rhesus rotavirus (RRV) robustly triggers beta interferon (IFN-␤Rotaviruses are etiological agents of severe dehydrating diarrhea in infants and young children and cause nearly 600,000 deaths globally every year (34). Rotaviruses are nonenveloped icosahedral members of the family Reoviridae and contain 11 segments of genomic double-stranded RNA (dsRNA) within a triple-layered particle. Several rotavirus vaccines have been developed to reduce rotavirus-associated mortalities (26); some are based on a modified Jennerian principle of rotavirus attenuation in the heterologous host. This phenomenon is termed host range restriction and is manifested by poor replication of rotaviruses in heterologous hosts compared to that in the homologous host (1). For example, bovine, lapine, and simian rotaviruses are all restricted for replication in humans. We are interested in understanding the mechanisms underlying host range restriction of rotaviruses in order to improve our basic knowledge of viral pathogenesis and because of the importance of these mechanisms in rational attenuation of vaccine candidates.In primary mouse embryonic fibroblasts (MEFs), several heterologous (nonmurine) rotavirus strains, including the bovine UK strain, are replication restricted by the host type I interferon (IFN) response (17, 53). In contrast, replication of homologous murine EW virus and the heterologous simian rhesus rotavirus (RRV) strain is insensitive to the presence of the interferon system. In a mouse model of rotavirus infection, RRV replication in gallbladder epithelia correlates with its ability to suppress the IFN response (N. Feng et al., submitted for publication). The rotavirus gene segment encoding the nonstructural protein 1 (NSP1) is an important determinant of host restriction of viral replication both in vitro (17,53) and in vivo (9). Specifically, we along with others have reported a role for NSP1 in regulating the ability of rotavirus to efficiently cause diarrhea in mice (9), spread from animal to animal (9), replicate in vivo and in vitro (4,(15)(16)(17), and antagonize IFN (4,5,17,24,25,53). Thus, the host innate immune response is an important determinant of rotavirus host range restriction and depends on both the virus strain and host cell or tissue type.Mammalian innate immunity to viral infection is critically dependent on a successful type I IFN response (49). The early IFN response involves initial recognition of virus within infected cells by activation of host pattern recognition receptors (PRRs) by pathogen-associated molecular patterns (PAMPs)

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“…Moreover, NSP1 seems to interact with the cellular transcription factor interferon regulatory factor 3 (IRF3) and targets it for degradation by the proteasome, thus acting to avoid the host antiviral defense by the blocking INF production [14][15][16][17][18] . However, NSP1 seems not to be necessary for rotavirus replication in vitro and its role is not fully clear 19 .…”

Section: Proteins Involved In Replication Pathogenesis and Immune Rementioning

confidence: 99%

Rotavirus Disease Mechanisms Diarrhea, Vomiting and Inflammation : How and Why

Hagbom¹

2015

Linköping University Medical Dissertations

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Rotavirus infections cause diarrhea and vomiting that can lead to severe dehydration. Despite extensive tissue damage and cell death, the inflammatory response is very limited. The focus of this thesis was to study pathophysiological mechanisms behind diarrhea and vomiting during rotavirus infection and also to investigate the mechanism behind the limited inflammatory response. An important discovery in this thesis was that rotavirus infection and the rotavirus toxin NSP4 stimulate release of the neurotransmitter serotonin from intestinal sensory enterochromaffin cells, in vitro and ex vivo. Interestingly, serotonin is known to be a mediator of both diarrhea and vomiting. Moreover, mice pups infected with rotavirus responded with central nervous system (CNS) activation in brain structures associated with vomiting, thus indicating a cross-talk between the gut and brain in rotavirus disease. Our finding that rotavirus infection activates the CNS led us to address the hypothesis that rotavirus infection not only activates the vagus nerve to stimulate vomiting, but also suppresses the inflammatory response via the cholinergic anti-inflammatory pathway, both of which are mediated by activated vagal afferent nerve signals into the brain stem. We found that mice lacking an intact vagus nerve, and mice lacking the α7 nicotine acetylcholine receptor (nAChR), being involved in cytokine suppression from macrophages, responded with a higher inflammatory response. Moreover, stimulated cytokine release from macrophages, by the rotavirus toxin NSP4, could be attenuated by nicotine, an agonist of the α7 nAChR. Thus, it seems most reasonable that the cholinergic anti-inflammatory pathway contributes to the limited inflammatory response during rotavirus infection. Moreover, rotavirus-infected mice displayed increased intestinal motility at the onset of diarrhea, which was not associated with increased intestinal permeability. The increased motility and diarrhea in infant mice could be attenuated by drugs acting on the enteric nervous system, indicating the importance and contribution of nerves in the rotavirus mediated disease. In conclusion, this thesis provides further insight into the pathophysiology of diarrhea and describe for the first time how rotavirus and host cross-talk to induce the vomiting reflex and limit inflammation. Results from these studies strongly support our hypothesis that serotonin and activation of the enteric nervous system and CNS contributes to diarrhea, vomiting and suppression of the inflammatory response in rotavirus disease

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Rotavirus NSP1 Inhibits NFκB Activation by Inducing Proteasome-Dependent Degradation of β-TrCP: A Novel Mechanism of IFN Antagonism

Cited by 154 publications

References 65 publications

Enterovirus 71 2C Protein Inhibits TNF-α–Mediated Activation of NF-κB by Suppressing IκB Kinase β Phosphorylation

Enterovirus 71 2C Protein Inhibits TNF-α–Mediated Activation of NF-κB by Suppressing IκB Kinase β Phosphorylation

The Early Interferon Response to Rotavirus Is Regulated by PKR and Depends on MAVS/IPS-1, RIG-I, MDA-5, and IRF3

Rotavirus Disease Mechanisms Diarrhea, Vomiting and Inflammation : How and Why

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