Your search keyword '"IFN antagonism"' showing total 15 results

1. Suppression of TRIM19 by arterivirus nonstructural protein 1 promotes viral replication

Author

Chia-Ming Su, Yu Fan Hung, Junyu Tang, Mingyuan Han, Roger Everett, and Dongwan Yoo

Subjects

PRRSV, TRIM19, PML, nsp1, Immune evasion, IFN antagonism, Microbiology, QR1-502, Infectious and parasitic diseases, RC109-216

Abstract

Tripartite motif (TRIM)-containing proteins are a family of regulatory proteins that can participate in the induction of antiviral cytokines and antagonize viral replication. Promyelocytic leukemia (PML) protein is known as TRIM19 and is a major scaffold protein organizing the PML nuclear bodies (NBs). PML NBs are membrane-less organelles in the nucleus and play a diverse role in maintaining cellular homeostasis including antiviral response. Porcine reproductive and respiratory syndrome virus (PRRSV), a member virus of the family Arteriviridae, inhibits type I interferon (IFN) response during infection, and nonstructural protein 1 (nsp1) of the virus has been identified as a potent IFN antagonist. We report that the numbers of PML NBs per nucleus were significantly downregulated during infection of PRRSV. The overexpression of all six isoforms of PML suppressed the PRRSV replication, and conversely, the silencing of PML gene expression enhanced the PRRSV replication. The suppression of PML NBs by the nsp1 protein was common in other member viruses of the family, represented by equine arteritis virus, lactate dehydrogenase elevating virus of mice, and simian hemorrhagic fever virus. Our study unveils a conserved viral strategy in arteriviruses for innate immune evasion.

Published

2024

2. Reprogramming viral immune evasion for a rational design of next-generation vaccines for RNA viruses

Author

Chia-Ming Su, Yijun Du, Raymond R. R. Rowland, Qiuhong Wang, and Dongwan Yoo

Subjects

type I interferons (IFNs), NF-kappa B (NF-κB), IFN antagonism, live-attenuated vaccine, veterinary vaccine, viral immune evasion, Immunologic diseases. Allergy, RC581-607

Abstract

Type I interferons (IFNs-α/β) are antiviral cytokines that constitute the innate immunity of hosts to fight against viral infections. Recent studies, however, have revealed the pleiotropic functions of IFNs, in addition to their antiviral activities, for the priming of activation and maturation of adaptive immunity. In turn, many viruses have developed various strategies to counteract the IFN response and to evade the host immune system for their benefits. The inefficient innate immunity and delayed adaptive response fail to clear of invading viruses and negatively affect the efficacy of vaccines. A better understanding of evasion strategies will provide opportunities to revert the viral IFN antagonism. Furthermore, IFN antagonism-deficient viruses can be generated by reverse genetics technology. Such viruses can potentially serve as next-generation vaccines that can induce effective and broad-spectrum responses for both innate and adaptive immunities for various pathogens. This review describes the recent advances in developing IFN antagonism-deficient viruses, their immune evasion and attenuated phenotypes in natural host animal species, and future potential as veterinary vaccines.

Published

2023

3. SARS-CoV-2 Disrupts Proximal Elements in the JAK-STAT Pathway.

Author

Da-Yuan Chen, Khan, Nazimuddin, Close, Brianna J., Goel, Raghuveera K., Blum, Benjamin, Tavares, Alexander H., Kenney, Devin, Conway, Hasahn L., Ewoldt, Jourdan K., Chitalia, Vipul C., Crossland, Nicholas A., Chen, Christopher S., Kotton, Darrell N., Baker, Susan C., Fuchs, Serge Y., Connor, John H., Douam, Florian, Emili, Andrew, and Saeed, Mohsan

Subjects

*JAK-STAT pathway, *SARS-CoV-2, *JANUS kinases, *PROTEIN-tyrosine kinases, *INTERFERON receptors, *VIRAL replication, *LUNGS

Abstract

SARS-CoV-2 can infect multiple organs, including lung, intestine, kidney, heart, liver, and brain. The molecular details of how the virus navigates through diverse cellular environments and establishes replication are poorly defined. Here, we generated a panel of phenotypically diverse, SARS-CoV-2-infectible human cell lines representing different body organs and performed longitudinal survey of cellular proteins and pathways broadly affected by the virus. This revealed universal inhibition of interferon signaling across cell types following SARS-CoV-2 infection. We performed systematic analyses of the JAK-STAT pathway in a broad range of cellular systems, including immortalized cells and primary-like cardiomyocytes, and found that SARS-CoV-2 targeted the proximal pathway components, including Janus kinase 1 (JAK1), tyrosine kinase 2 (Tyk2), and the interferon receptor subunit 1 (IFNAR1), resulting in cellular desensitization to type I IFN. Detailed mechanistic investigation of IFNAR1 showed that the protein underwent ubiquitination upon SARS-CoV-2 infection. Furthermore, chemical inhibition of JAK kinases enhanced infection of stem cell-derived cultures, indicating that the virus benefits from inhibiting the JAKSTAT pathway. These findings suggest that the suppression of interferon signaling is a mechanism widely used by the virus to evade antiviral innate immunity, and that targeting the viral mediators of immune evasion may help block virus replication in patients with COVID-19. [ABSTRACT FROM AUTHOR]

Published

2021

4. Suppression of TRIM19 by arterivirus nonstructural protein 1 promotes viral replication.

Author

Su, Chia-Ming, Hung, Yu Fan, Tang, Junyu, Han, Mingyuan, Everett, Roger, and Yoo, Dongwan

Subjects

*VIRAL nonstructural proteins, *PORCINE reproductive & respiratory syndrome, *VIRAL replication, *TYPE I interferons, *SCAFFOLD proteins, *GENE silencing

Abstract

• PRRSV reduces the formation of PML nuclear bodies in which PML protein is a major component. • PML NBs were significantly downregulated by PRRSV nsp1β. • Viral suppression of PML NBs was common in the family Arteriviridae. Tripartite motif (TRIM)-containing proteins are a family of regulatory proteins that can participate in the induction of antiviral cytokines and antagonize viral replication. Promyelocytic leukemia (PML) protein is known as TRIM19 and is a major scaffold protein organizing the PML nuclear bodies (NBs). PML NBs are membrane-less organelles in the nucleus and play a diverse role in maintaining cellular homeostasis including antiviral response. Porcine reproductive and respiratory syndrome virus (PRRSV), a member virus of the family Arteriviridae, inhibits type I interferon (IFN) response during infection, and nonstructural protein 1 (nsp1) of the virus has been identified as a potent IFN antagonist. We report that the numbers of PML NBs per nucleus were significantly downregulated during infection of PRRSV. The overexpression of all six isoforms of PML suppressed the PRRSV replication, and conversely, the silencing of PML gene expression enhanced the PRRSV replication. The suppression of PML NBs by the nsp1 protein was common in other member viruses of the family, represented by equine arteritis virus, lactate dehydrogenase elevating virus of mice, and simian hemorrhagic fever virus. Our study unveils a conserved viral strategy in arteriviruses for innate immune evasion. [ABSTRACT FROM AUTHOR]

Published

2024

5. Phage display technique identifies the interaction of severe acute respiratory syndrome coronavirus open reading frame 6 protein with nuclear pore complex interacting protein NPIPB3 in modulating Type I interferon antagonism

Author

Su-Hua Huang, Tzu-Ying Lee, Ying-Ju Lin, Lei Wan, Chih-Ho Lai, and Cheng-Wen Lin

Subjects

IFN antagonism, NPIPB3, ORF6, phage display, SARS-CoV, Microbiology, QR1-502

Abstract

Background/Purpose: Severe acute respiratory syndrome coronavirus (SARS-CoV) proteins including ORF6 inhibit Type I interferon (IFN) signaling. Methods: This study identified SARS-CoV ORF6-interacting proteins using the phage displayed human lung cDNA libraries, and examined the association of ORF6–host factor interaction with Type I IFN antagonism. After the fifth round of biopanning with Escherichia coli-synthesized ORF6-His tagged protein, the relative binding affinity of phage clones to ORF6 was determined using direct enzyme-linked immunosorbent assay. Results: The highest affinity clone to ORF6 displayed the C-terminal domain of NPIPB3 (nuclear pore complex interacting protein family, member B3; also named as phosphatidylinositol-3-kinase-related kinase SMG-1 isoform 1 homolog). The coimmunoprecipitation assay demonstrated the direct binding of ORF6 to the C-terminal domain of NPIPB3 in vitro. Confocal imaging revealed a close colocalization of SARS-CoV ORF6 protein with NPIPB3 in human promonocytes. The dual luciferase reporter assay showed that the C-terminal domain of NPIPB3 attenuated the antagonistic activity of SARS-CoV ORF6 on IFN-β-induced ISRE (IFN stimulated response element)-responsive firefly luciferase activity. In addition, confocal imaging and Western blotting assays revealed that the increases in STAT-1 nuclear translocation and phosphorylation occurred in the transfected cells expressing both genes of ORF6 and NPIPB3, but not in the ORF6-expressing cells in response to IFN-β. Conclusion: The overexpression of NPIPB3 restored the IFN-β responses in SARS-CoV ORF6 expressing cells, indicating that the interaction of SARS CoV ORF6 and NPIPB3 reduced Type I IFN antagonism by SARS-CoV ORF6.

Published

2017

6. Mechanisms of Non-segmented Negative Sense RNA Viral Antagonism of Host RIG-I-Like Receptors.

Author

Leung, Daisy W.

Subjects

*PATTERN perception receptors, *TYPE I interferons, *RNA viruses, *INTERFERON receptors, *RNA

Abstract

The pattern recognition receptors RIG-I-like receptors (RLRs) are critical molecules for cytosolic viral recognition and for subsequent activation of type I interferon production. The interferon signaling pathway plays a key role in viral detection and generating antiviral responses. Among the many pathogens, the non-segmented negative sense RNA viruses target the RLR pathway using a variety of mechanisms. Here, I review the current state of knowledge on the molecular mechanisms that allow non-segmented negative sense RNA virus recognition and antagonism of RLRs. Unlabelled Image • Type I IFN signaling is important for pathogen recognition and activation of antiviral responses. • RIG-I-like receptors are highly regulated cytosolic pattern recognition receptors that stimulate IFN signaling. • Non-segmented negative strand RNA viruses have developed different strategies and multipronged approaches to inhibit RLR signaling. [ABSTRACT FROM AUTHOR]

Published

2019

7. Reprogramming viral immune evasion for a rational design of next-generation vaccines for RNA viruses.

Author

Su CM, Du Y, Rowland RRR, Wang Q, and Yoo D

Subjects

Animals, Immune Evasion, Antiviral Agents pharmacology, Interferon Type I, Vaccines, RNA Viruses

Abstract

Type I interferons (IFNs-α/β) are antiviral cytokines that constitute the innate immunity of hosts to fight against viral infections. Recent studies, however, have revealed the pleiotropic functions of IFNs, in addition to their antiviral activities, for the priming of activation and maturation of adaptive immunity. In turn, many viruses have developed various strategies to counteract the IFN response and to evade the host immune system for their benefits. The inefficient innate immunity and delayed adaptive response fail to clear of invading viruses and negatively affect the efficacy of vaccines. A better understanding of evasion strategies will provide opportunities to revert the viral IFN antagonism. Furthermore, IFN antagonism-deficient viruses can be generated by reverse genetics technology. Such viruses can potentially serve as next-generation vaccines that can induce effective and broad-spectrum responses for both innate and adaptive immunities for various pathogens. This review describes the recent advances in developing IFN antagonism-deficient viruses, their immune evasion and attenuated phenotypes in natural host animal species, and future potential as veterinary vaccines., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2023 Su, Du, Rowland, Wang and Yoo.)

Published

2023

8. SARS-CoV-2 Disrupts Proximal Elements in the JAK-STAT Pathway

Author

Benjamin C. Blum, Mohsan Saeed, Raghuveera Kumar Goel, Brianna J. Close, Jourdan K. Ewoldt, Susan C. Baker, Alexander H Tavares, Devin Kenney, Hasahn L. Conway, Florian Douam, Darrell N. Kotton, Nazimuddin Khan, Andrew Emili, Da-Yuan Chen, Serge Y. Fuchs, Vipul C. Chitalia, Christopher S. Chen, John H Connor, and Nicholas A. Crossland

Subjects

0301 basic medicine, Cell type, Immunology, IFN signaling, Receptor, Interferon alpha-beta, Biology, Virus Replication, Microbiology, Virus, Cell Line, JAK-STAT pathway, 03 medical and health sciences, 0302 clinical medicine, proteomics, Interferon, Virology, medicine, Humans, Myocytes, Cardiac, Janus Kinases, virus-host interactions, immune evasion, TYK2 Kinase, IFN antagonism, Innate immune system, Janus kinase 1, Host Microbial Interactions, SARS-CoV-2, JAK-STAT signaling pathway, COVID-19, Janus Kinase 1, Immunity, Innate, Cell biology, 030104 developmental biology, STAT1 Transcription Factor, Viral replication, Gene Expression Regulation, Tyrosine kinase 2, 030220 oncology & carcinogenesis, Insect Science, Interferon Type I, Pathogenesis and Immunity, human cell lines, medicine.drug, Signal Transduction

Abstract

SARS-CoV-2 can infect multiple organs, including lung, intestine, kidney, heart, liver, and brain. The molecular details of how the virus navigates through diverse cellular environments and establishes replication are poorly defined. Here, we generated a panel of phenotypically diverse, SARS-CoV-2-infectible human cell lines representing different body organs and performed longitudinal survey of cellular proteins and pathways broadly affected by the virus. This revealed universal inhibition of interferon signaling across cell types following SARS-CoV-2 infection. We performed systematic analyses of the JAK-STAT pathway in a broad range of cellular systems, including immortalized cells and primary-like cardiomyocytes, and found that SARS-CoV-2 targeted the proximal pathway components, including Janus kinase 1 (JAK1), tyrosine kinase 2 (Tyk2), and the interferon receptor subunit 1 (IFNAR1), resulting in cellular desensitization to type I IFN. Detailed mechanistic investigation of IFNAR1 showed that the protein underwent ubiquitination upon SARS-CoV-2 infection. Furthermore, chemical inhibition of JAK kinases enhanced infection of stem cell-derived cultures, indicating that the virus benefits from inhibiting the JAK-STAT pathway. These findings suggest that the suppression of interferon signaling is a mechanism widely used by the virus to evade antiviral innate immunity, and that targeting the viral mediators of immune evasion may help block virus replication in patients with COVID-19. IMPORTANCE SARS-CoV-2 can infect various organs in the human body, but the molecular interface between the virus and these organs remains unexplored. In this study, we generated a panel of highly infectible human cell lines originating from various body organs and employed these cells to identify cellular processes commonly or distinctly disrupted by SARS-CoV-2 in different cell types. One among the universally impaired processes was interferon signaling. Systematic analysis of this pathway in diverse culture systems showed that SARS-CoV-2 targets the proximal JAK-STAT pathway components, destabilizes the type I interferon receptor though ubiquitination, and consequently renders the infected cells resistant to type I interferon. These findings illuminate how SARS-CoV-2 can continue to propagate in different tissues even in the presence of a disseminated innate immune response.

Published

2021

9. Biogenesis of non-structural protein 1 (nsp1) and nsp1-mediated type I interferon modulation in arteriviruses.

Author

Han, Mingyuan, Kim, Chi Yong, Rowland, Raymond R.R., Fang, Ying, Kim, Daewoo, and Yoo, Dongwan

Subjects

*VIRAL nonstructural proteins, *INTERFERONS, *ANTIVIRAL agents, *PORCINE reproductive & respiratory syndrome, *CREB-binding protein, *ARTERIVIRIDAE

Abstract

Abstract: Type I interferons (IFNs-α/β) play a key role for the antiviral state of host, and the porcine arterivirus; porcine reproductive and respiratory syndrome virus (PRRSV), has been shown to down-regulate the production of IFNs during infection. Non-structural protein (nsp) 1 of PRRSV has been identified as a viral IFN antagonist, and the nsp1α subunit of nsp1 has been shown to degrade the CREB-binding protein (CBP) and to inhibit the formation of enhanceosome thus resulting in the suppression of IFN production. The study was expanded to other member viruses in the family Arteriviridae: equine arteritis virus (EAV), murine lactate dehydrogenase-elevating virus (LDV), and simian hemorrhagic fever virus (SHFV). While PRRSV–nsp1 and LDV–nsp1 were auto-cleaved to produce the nsp1α and nsp1β subunits, EAV–nsp1 remained uncleaved. SHFV–nsp1 was initially predicted to be cleaved to generate three subunits (nsp1α, nsp1β, and nsp1γ), but only two subunits were generated as SHFV–nsp1αβ and SHFV–nsp1γ. The papain-like cysteine protease (PLP) 1α motif in nsp1α remained inactive for SHFV, and only the PLP1β motif of nsp1β was functional to generate SHFV–nsp1γ subunit. All subunits of arterivirus nsp1 were localized in the both nucleus and cytoplasm, but PRRSV–nsp1β, LDV–nsp1β, EAV–nsp1, and SHFV–nsp1γ were predominantly found in the nucleus. All subunits of arterivirus nsp1 contained the IFN suppressive activity and inhibited both interferon regulatory factor 3 (IRF3) and NF-κB mediated IFN promoter activities. Similar to PRRSV–nsp1α, CBP degradation was evident in cells expressing LDV–nsp1α and SHFV–nsp1γ, but no such degradation was observed for EAV–nsp1. Regardless of CBP degradation, all subunits of arterivirus nsp1 suppressed the IFN-sensitive response element (ISRE)-promoter activities. Our data show that the nsp1-mediated IFN modulation is a common strategy for all arteriviruses but their mechanism of action may differ from each other. [Copyright &y& Elsevier]

Published

2014

10. The non-structural 5A protein of hepatitis C virus exhibits genotypic differences in interferon antagonism

Author

Tsai, Ya-Hui, Kuang, Wan-Fen, Lu, Tsai-Yi, Kao, Jia-Horng, Lai, Ming-Yang, Liu, Chun-Jen, Chen, Pei-Jer, and Hwang, Lih-Hwa

Subjects

*HEPATITIS C virus, *INTERFERONS, *DRUG antagonism, *HEPATITIS viruses, *VIRAL disease treatment, *DNA replication, *PROTEIN kinases, *PROTEIN binding

Abstract

Background/Aims: Patients infected with hepatitis C virus (HCV) genotype 2 or 3 usually respond better to interferon (IFN) treatment than those infected with genotype 1. In this study, we investigated whether the non-structural 5A protein (NS5A) of HCV genotypes 1 and 2 (1b-NS5A and 2a-NS5A, respectively) exerted differential counteractivities against IFN treatment. Methods: We compared the inhibitory effects of 1b-NS5As and 2a-NS5As on IFN activity. We also investigated the replication inhibition of HCV subgenomic replicons containing 1b-NS5A or 2a-NS5A in response to IFN treatment. Results: 1b-NS5As exerted more profound inhibitory effects on IFN activity than 2a-NS5As. The replication of the 2a-NS5A-containing replicons was more sensitive to IFN treatment than that of the 1b-NS5A-containing replicons. Deletion of the interferon sensitivity-determining region/protein kinase R-binding domain (PKR-BD), the V3 domain, or the C-terminus region of NS5A significantly abrogated its anti-IFN activity. Domain swapping between 1b-NS5A and 2a-NS5A in the V3 domain and/or the C-terminus region resulted in a transfer of their anti-IFN activity. Conclusions: 1b-NS5As exert higher magnitudes of IFN antagonism than do 2a-NS5As. The V3 and the C-terminus regions are responsible for the differential anti-IFN effects. This phenomenon may partly explain the genotype-linked differences in the response of HCV to IFN treatment. [Copyright &y& Elsevier]

Published

2008

11. SARS-CoV-2 Disrupts Proximal Elements in the JAK-STAT Pathway.

Author

Chen DY, Khan N, Close BJ, Goel RK, Blum B, Tavares AH, Kenney D, Conway HL, Ewoldt JK, Chitalia VC, Crossland NA, Chen CS, Kotton DN, Baker SC, Fuchs SY, Connor JH, Douam F, Emili A, and Saeed M

Subjects

Cell Line, Gene Expression Regulation, Humans, Immune Evasion, Immunity, Innate, Interferon Type I metabolism, Janus Kinase 1 metabolism, Myocytes, Cardiac, Receptor, Interferon alpha-beta metabolism, STAT1 Transcription Factor metabolism, Signal Transduction, TYK2 Kinase metabolism, Virus Replication, COVID-19 metabolism, Host Microbial Interactions physiology, Janus Kinases metabolism, SARS-CoV-2 metabolism

Abstract

SARS-CoV-2 can infect multiple organs, including lung, intestine, kidney, heart, liver, and brain. The molecular details of how the virus navigates through diverse cellular environments and establishes replication are poorly defined. Here, we generated a panel of phenotypically diverse, SARS-CoV-2-infectible human cell lines representing different body organs and performed longitudinal survey of cellular proteins and pathways broadly affected by the virus. This revealed universal inhibition of interferon signaling across cell types following SARS-CoV-2 infection. We performed systematic analyses of the JAK-STAT pathway in a broad range of cellular systems, including immortalized cells and primary-like cardiomyocytes, and found that SARS-CoV-2 targeted the proximal pathway components, including Janus kinase 1 (JAK1), tyrosine kinase 2 (Tyk2), and the interferon receptor subunit 1 (IFNAR1), resulting in cellular desensitization to type I IFN. Detailed mechanistic investigation of IFNAR1 showed that the protein underwent ubiquitination upon SARS-CoV-2 infection. Furthermore, chemical inhibition of JAK kinases enhanced infection of stem cell-derived cultures, indicating that the virus benefits from inhibiting the JAK-STAT pathway. These findings suggest that the suppression of interferon signaling is a mechanism widely used by the virus to evade antiviral innate immunity, and that targeting the viral mediators of immune evasion may help block virus replication in patients with COVID-19. IMPORTANCE SARS-CoV-2 can infect various organs in the human body, but the molecular interface between the virus and these organs remains unexplored. In this study, we generated a panel of highly infectible human cell lines originating from various body organs and employed these cells to identify cellular processes commonly or distinctly disrupted by SARS-CoV-2 in different cell types. One among the universally impaired processes was interferon signaling. Systematic analysis of this pathway in diverse culture systems showed that SARS-CoV-2 targets the proximal JAK-STAT pathway components, destabilizes the type I interferon receptor though ubiquitination, and consequently renders the infected cells resistant to type I interferon. These findings illuminate how SARS-CoV-2 can continue to propagate in different tissues even in the presence of a disseminated innate immune response.

Published

2021

12. Biogenesis of non-structural protein 1 (nsp1) and nsp1-mediated type I interferon modulation in arteriviruses

Author

Mingyuan Han, Dongwan Yoo, Ying Fang, Daewoo Kim, Raymond R. R. Rowland, and Chi Yong Kim

Subjects

Gene Expression Regulation, Viral, Simian hemorrhagic fever virus, Protein subunit, viruses, nsp1, Viral Nonstructural Proteins, Virus Replication, Virus, Arteriviridae, Cell Line, Arterivirus, LDV, Interferon, Virology, SHFV, medicine, Animals, Humans, Cloning, Molecular, IFN antagonism, biology, virus diseases, biology.organism_classification, Porcine reproductive and respiratory syndrome virus, Molecular biology, CBP degradation, EAV, Interferon Type I, PRRSV, IRF3, medicine.drug, Interferon regulatory factors

Abstract

Type I interferons (IFNs-α/β) play a key role for the antiviral state of host, and the porcine arterivirus; porcine reproductive and respiratory syndrome virus (PRRSV), has been shown to down-regulate the production of IFNs during infection. Non-structural protein (nsp) 1 of PRRSV has been identified as a viral IFN antagonist, and the nsp1α subunit of nsp1 has been shown to degrade the CREB-binding protein (CBP) and to inhibit the formation of enhanceosome thus resulting in the suppression of IFN production. The study was expanded to other member viruses in the family Arteriviridae: equine arteritis virus (EAV), murine lactate dehydrogenase-elevating virus (LDV), and simian hemorrhagic fever virus (SHFV). While PRRSV–nsp1 and LDV–nsp1 were auto-cleaved to produce the nsp1α and nsp1β subunits, EAV–nsp1 remained uncleaved. SHFV–nsp1 was initially predicted to be cleaved to generate three subunits (nsp1α, nsp1β, and nsp1γ), but only two subunits were generated as SHFV–nsp1αβ and SHFV–nsp1γ. The papain-like cysteine protease (PLP) 1α motif in nsp1α remained inactive for SHFV, and only the PLP1β motif of nsp1β was functional to generate SHFV–nsp1γ subunit. All subunits of arterivirus nsp1 were localized in the both nucleus and cytoplasm, but PRRSV–nsp1β, LDV–nsp1β, EAV–nsp1, and SHFV–nsp1γ were predominantly found in the nucleus. All subunits of arterivirus nsp1 contained the IFN suppressive activity and inhibited both interferon regulatory factor 3 (IRF3) and NF-κB mediated IFN promoter activities. Similar to PRRSV–nsp1α, CBP degradation was evident in cells expressing LDV–nsp1α and SHFV–nsp1γ, but no such degradation was observed for EAV–nsp1. Regardless of CBP degradation, all subunits of arterivirus nsp1 suppressed the IFN-sensitive response element (ISRE)-promoter activities. Our data show that the nsp1-mediated IFN modulation is a common strategy for all arteriviruses but their mechanism of action may differ from each other.

Published

2014

13. Phage display technique identifies the interaction of severe acute respiratory syndrome coronavirus open reading frame 6 protein with nuclear pore complex interacting protein NPIPB3 in modulating Type I interferon antagonism

Author

Ying Ju Lin, Lei Wan, Chih Ho Lai, Cheng Wen Lin, Tzu Ying Lee, and Su Hua Huang

Subjects

0301 basic medicine, Microbiology (medical), Phage display, Protein family, Immunoprecipitation, lcsh:QR1-502, Enzyme-Linked Immunosorbent Assay, Biopanning, Protein Serine-Threonine Kinases, Biology, lcsh:Microbiology, Article, Phosphatidylinositol 3-Kinases, Viral Proteins, 03 medical and health sciences, Interferon, Immunology and Microbiology(all), medicine, Humans, NPIPB3, Immunology and Allergy, Nuclear pore, Cells, Cultured, IFN antagonism, Microscopy, Confocal, 030102 biochemistry & molecular biology, General Immunology and Microbiology, SARS-CoV, General Medicine, Transfection, ORF6, Molecular biology, 030104 developmental biology, Infectious Diseases, Severe acute respiratory syndrome-related coronavirus, Host-Pathogen Interactions, Interferon Type I, Phosphorylation, phage display, Cell Surface Display Techniques, Protein Binding, medicine.drug

Abstract

Background/Purpose Severe acute respiratory syndrome coronavirus (SARS-CoV) proteins including ORF6 inhibit Type I interferon (IFN) signaling. Methods This study identified SARS-CoV ORF6-interacting proteins using the phage displayed human lung cDNA libraries, and examined the association of ORF6–host factor interaction with Type I IFN antagonism. After the fifth round of biopanning with Escherichia coli -synthesized ORF6-His tagged protein, the relative binding affinity of phage clones to ORF6 was determined using direct enzyme-linked immunosorbent assay. Results The highest affinity clone to ORF6 displayed the C-terminal domain of NPIPB3 (nuclear pore complex interacting protein family, member B3; also named as phosphatidylinositol-3-kinase-related kinase SMG-1 isoform 1 homolog). The coimmunoprecipitation assay demonstrated the direct binding of ORF6 to the C-terminal domain of NPIPB3 in vitro . Confocal imaging revealed a close colocalization of SARS-CoV ORF6 protein with NPIPB3 in human promonocytes. The dual luciferase reporter assay showed that the C-terminal domain of NPIPB3 attenuated the antagonistic activity of SARS-CoV ORF6 on IFN-β-induced ISRE (IFN stimulated response element)-responsive firefly luciferase activity. In addition, confocal imaging and Western blotting assays revealed that the increases in STAT-1 nuclear translocation and phosphorylation occurred in the transfected cells expressing both genes of ORF6 and NPIPB3, but not in the ORF6-expressing cells in response to IFN-β. Conclusion The overexpression of NPIPB3 restored the IFN-β responses in SARS-CoV ORF6 expressing cells, indicating that the interaction of SARS CoV ORF6 and NPIPB3 reduced Type I IFN antagonism by SARS-CoV ORF6.

Published

2015

14. Dengue virus co-opts UBR4 to degrade STAT2 and antagonize type I IFN signaling

Author

JULIET MORRISON, MAUDRY LAURENT ROLLE, ANA MAESTRE, LUBBERTUS C. F. MULDER, VIVIANA SIMON, ANA FERNANDEZ SESMA, ADOLFO GARCÍA SASTRE, PISANELLI, GIUSEPPE, Virus and Cells - Gordon research Conference, Juliet, Morrison, MAUDRY LAURENT, Rolle, Ana, Maestre, Pisanelli, Giuseppe, LUBBERTUS C. F., Mulder, Viviana, Simon, ANA FERNANDEZ, Sesma, and ADOLFO GARCÍA, Sastre

Subjects

dengue viru, UBR4, IFN antagonism, STAT2

Abstract

An estimated 50 million dengue virus (DENV) infections occur annually and more than forty percent of the human population is currently at risk of developing dengue fever (DF) or dengue hemorrhagic fever (DHF). Despite the prevalence and potential severity of DF and DHF, there are no approved vaccines or antiviral therapeutics available. An improved understanding of DENV immune evasion is pivotal for the rational development of anti-DENV therapeutics. Antagonism of type I interferon (IFN-I) signaling is a crucial mechanism of DENV immune evasion. DENV NS5 protein inhibits IFN-I signaling by mediating proteasome-dependent STAT2 degradation. Only proteolytically-processed NS5 can efficiently mediate STAT2 degradation, though both unprocessed and processed NS5 bind STAT2. Here we identify UBR4, a 600-kDa member of the N-recognin family, as an interacting partner of DENV NS5 that preferentially binds to processed NS5. Our results also demonstrate that DENV NS5 bridges STAT2 and UBR4. Furthermore, we show that UBR4 promotes DENV-mediated STAT2 degradation, and most importantly, that UBR4 is necessary for efficient viral replication in IFN-I competent cells. Our data underscore the importance of NS5-mediated STAT2 degradation in DENV replication and identify UBR4 as a host protein that is specifically exploited by DENV to inhibit IFN-I signaling via STAT2 degradation.

Published

2013

15. Phage display technique identifies the interaction of severe acute respiratory syndrome coronavirus open reading frame 6 protein with nuclear pore complex interacting protein NPIPB3 in modulating Type I interferon antagonism.

Author

Huang SH, Lee TY, Lin YJ, Wan L, Lai CH, and Lin CW

Subjects

Cell Surface Display Techniques, Cells, Cultured, Enzyme-Linked Immunosorbent Assay, Humans, Immunoprecipitation, Microscopy, Confocal, Protein Binding, Protein Serine-Threonine Kinases, Host-Pathogen Interactions, Interferon Type I antagonists & inhibitors, Phosphatidylinositol 3-Kinases metabolism, Severe acute respiratory syndrome-related coronavirus physiology, Viral Proteins metabolism

Abstract

Background/purpose: Severe acute respiratory syndrome coronavirus (SARS-CoV) proteins including ORF6 inhibit Type I interferon (IFN) signaling., Methods: This study identified SARS-CoV ORF6-interacting proteins using the phage displayed human lung cDNA libraries, and examined the association of ORF6-host factor interaction with Type I IFN antagonism. After the fifth round of biopanning with Escherichia coli-synthesized ORF6-His tagged protein, the relative binding affinity of phage clones to ORF6 was determined using direct enzyme-linked immunosorbent assay., Results: The highest affinity clone to ORF6 displayed the C-terminal domain of NPIPB3 (nuclear pore complex interacting protein family, member B3; also named as phosphatidylinositol-3-kinase-related kinase SMG-1 isoform 1 homolog). The coimmunoprecipitation assay demonstrated the direct binding of ORF6 to the C-terminal domain of NPIPB3 in vitro. Confocal imaging revealed a close colocalization of SARS-CoV ORF6 protein with NPIPB3 in human promonocytes. The dual luciferase reporter assay showed that the C-terminal domain of NPIPB3 attenuated the antagonistic activity of SARS-CoV ORF6 on IFN-β-induced ISRE (IFN stimulated response element)-responsive firefly luciferase activity. In addition, confocal imaging and Western blotting assays revealed that the increases in STAT-1 nuclear translocation and phosphorylation occurred in the transfected cells expressing both genes of ORF6 and NPIPB3, but not in the ORF6-expressing cells in response to IFN-β., Conclusion: The overexpression of NPIPB3 restored the IFN-β responses in SARS-CoV ORF6 expressing cells, indicating that the interaction of SARS CoV ORF6 and NPIPB3 reduced Type I IFN antagonism by SARS-CoV ORF6., (Copyright © 2015. Published by Elsevier B.V.)

Published

2017