Your search keyword '"viral glycoproteins"' showing total 110 results

1. Guanylate-binding protein 5 antagonizes viral glycoproteins independently of furin processing

Author

Hana Veler, Cheng Man Lun, Abdul A. Waheed, and Eric O. Freed

Subjects

GBP5, viral glycoproteins, HIV-1 Env, MLV Env, SARS-CoV-2 S, SARS-CoV S, Microbiology, QR1-502

Abstract

ABSTRACT Guanylate-binding protein (GBP) 5 is an interferon-inducible cellular factor with broad anti-viral activity. Recently, GBP5 has been shown to antagonize the glycoproteins of a number of enveloped viruses, in part by disrupting the host enzyme furin. Here we show that GBP5 strongly impairs the infectivity of virus particles bearing not only viral glycoproteins that depend on furin cleavage for infectivity—the envelope (Env) glycoproteins of HIV-1 and murine leukemia virus and the spike (S) glycoprotein of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2)—but also viral glycoproteins that do not depend on furin cleavage: vesicular stomatitis virus glycoprotein and SARS-CoV S. We observe that GBP5 disrupts proper N-linked protein glycosylation and reduces the incorporation of viral glycoproteins into virus particles. The glycosylation of the cellular protein CD4 is also altered by GBP5 expression. Flow cytometry analysis shows that GBP5 expression reduces the cell-surface levels of HIV-1 Env and the S glycoproteins of SARS-CoV and SARS-CoV-2. Our data demonstrate that, under the experimental conditions used, inhibition of furin-mediated glycoprotein cleavage is not the primary anti-viral mechanism of action of GBP5. Rather, the antagonism appears to be related to impaired trafficking of glycoproteins to the plasma membrane. These results provide novel insights into the broad antagonism of viral glycoprotein function by the cellular host innate immune response.IMPORTANCEThe surface of enveloped viruses contains viral envelope glycoproteins, an important structural component facilitating virus attachment and entry while also acting as targets for the host adaptive immune system. In this study, we show that expression of GBP5 in virus-producer cells alters the glycosylation, cell-surface expression, and virion incorporation of viral glycoproteins across several virus families. This research provides novel insights into the broad impact of the host cell anti-viral factor GBP5 on protein glycosylation and trafficking.

Published

2024

2. The Antiviral Activity of Interferon-Induced Transmembrane Proteins and Virus Evasion Strategies.

Author

Wang, Jingjing, Luo, Yuhang, Katiyar, Harshita, Liang, Chen, and Liu, Qian

Subjects

*MEMBRANE proteins, *VIRAL proteins, *MEMBRANE fusion, *GLYCOPROTEINS, *VIRUS diseases, *TYPE I interferons

Abstract

Interferons (IFNs) are antiviral cytokines that defend against viral infections by inducing the expression of interferon-stimulated genes (ISGs). Interferon-inducible transmembrane proteins (IFITMs) 1, 2, and 3 are crucial ISG products and members of the CD225 protein family. Compelling evidence shows that IFITMs restrict the infection of many unrelated viruses by inhibiting the virus–cell membrane fusion at the virus entry step via the modulation of lipid composition and membrane properties. Meanwhile, viruses can evade IFITMs' restrictions by either directly interacting with IFITMs via viral glycoproteins or by altering the native entry pathway. At the same time, cumulative evidence suggests context-dependent and multifaceted roles of IFITMs in modulating virus infections and cell signaling. Here, we review the diverse antiviral mechanisms of IFITMs, the viral antagonizing strategies, and the regulation of IFITM activity in host cells. The mechanisms behind the antiviral activity of IFITMs could aid the development of broad-spectrum antivirals and enhance preparedness for future pandemics. [ABSTRACT FROM AUTHOR]

Published

2024

3. Herpes Simplex Virus 1 Glycoprotein B from a Hyperfusogenic Virus Mediates Enhanced Cell–Cell Fusion.

Author

Gianopulos, Katrina A., Makio, Albina O., Pritchard, Suzanne M., Cunha, Cristina W., Hull, McKenna A., and Nicola, Anthony V.

Subjects

*CELL fusion, *MEMBRANE fusion, *NUCLEAR fusion, *GLYCOPROTEINS

Abstract

Herpes simplex virus 1 (HSV-1) causes significant morbidity and death in humans worldwide. Herpes simplex virus 1 has a complex fusion mechanism that is incompletely understood. The HSV-1 strain ANG has notable fusion and entry activities that distinguish it from wild type. HSV-1 ANG virions fused with the Vero cell surface at 4 °C and also entered cells more efficiently at 15 °C, relative to wild type HSV-1 strain KOS virions, consistent with a hyperfusogenic phenotype. Understanding the molecular basis for the unique entry and fusion activities of HSV-1 strain ANG will help decipher the HSV fusion reaction and entry process. Sequencing of HSV-1 ANG genes revealed multiple changes in gB, gC, gD, gH, and gL proteins relative to wild type HSV-1 strains. The ANG UL45 gene sequence, which codes for a non-essential envelope protein, was identical to wild type KOS. HSV-1 ANG gB, gD, and gH/gL were necessary and sufficient to mediate cell–cell fusion in a virus-free reporter assay. ANG gB, when expressed with wild type KOS gD and gH/gL, increased membrane fusion, suggesting that ANG gB has hyperfusogenic cell–cell fusion activity. Replacing the KOS gD, gH, or gL with the corresponding ANG alleles did not enhance cell–cell fusion. The novel mutations in the ANG fusion and entry glycoproteins provide a platform for dissecting the cascade of interactions that culminate in HSV fusion and entry. [ABSTRACT FROM AUTHOR]

Published

2024

4. The Antiviral Activity of Interferon-Induced Transmembrane Proteins and Virus Evasion Strategies

Author

Jingjing Wang, Yuhang Luo, Harshita Katiyar, Chen Liang, and Qian Liu

Subjects

IFITMs, antiviral activity, virus and cell membrane fusion, viral glycoproteins, virus evasion, immune modulation, Microbiology, QR1-502

Abstract

Interferons (IFNs) are antiviral cytokines that defend against viral infections by inducing the expression of interferon-stimulated genes (ISGs). Interferon-inducible transmembrane proteins (IFITMs) 1, 2, and 3 are crucial ISG products and members of the CD225 protein family. Compelling evidence shows that IFITMs restrict the infection of many unrelated viruses by inhibiting the virus–cell membrane fusion at the virus entry step via the modulation of lipid composition and membrane properties. Meanwhile, viruses can evade IFITMs’ restrictions by either directly interacting with IFITMs via viral glycoproteins or by altering the native entry pathway. At the same time, cumulative evidence suggests context-dependent and multifaceted roles of IFITMs in modulating virus infections and cell signaling. Here, we review the diverse antiviral mechanisms of IFITMs, the viral antagonizing strategies, and the regulation of IFITM activity in host cells. The mechanisms behind the antiviral activity of IFITMs could aid the development of broad-spectrum antivirals and enhance preparedness for future pandemics.

Published

2024

5. MicroRNA-25/93 induction by Vpu as a mechanism for counteracting MARCH1-restriction on HIV-1 infectivity in macrophages

Author

Robert Lodge, Zaikun Xu, Mckenna Eklund, Christina Stürzel, Frank Kirchhoff, Michel J. Tremblay, Tom C. Hobman, and Éric A. Cohen

Subjects

human immunodeficiency virus, microRNA, restriction factor, viral glycoproteins, MARCH proteins, HIV-1 countermeasures, Microbiology, QR1-502

Abstract

ABSTRACT The type 1 interferon-regulated E3 ubiquitin ligase MARCH1 reduces surface expression of HIV-1 envelope glycoproteins (Env) and their packaging into nascent virions, a condition that restricts viral infectivity. However, how HIV-1 counters this restriction, notably during infection of macrophages, remains unclear. Here, we show that the HIV-1 accessory protein Vpu increases the levels of microRNAs-25 and -93 to target MARCH1 mRNA. By recruiting β-TRCP, a component of the SCFβ-TRCP E3 ligase complex that targets phosphorylated β-catenin for degradation, Vpu increases β-catenin levels, which, in concert with TCF4/LEF, drives transcription of the MARCH1-targeting microRNAs. This potentiates HIV-1 infectivity as a result of increased Env incorporation into nascent virions. Pharmacological targeting of the β-catenin pathway inhibits Vpu-mediated upregulation of microRNAs-25 and -93 and restores MARCH1 restriction on HIV-1 infectivity. Overall, our findings highlight a novel mechanism by which HIV-1 counteracts MARCH1 by downregulating its expression via Vpu-mediated induction of microRNAs-25 and -93. IMPORTANCE In order to efficiently produce infectious viral particles, HIV must counter several restrictions exerted by host cell antiviral proteins. MARCH1 is a member of the MARCH protein family that restricts HIV infection by limiting the incorporation of viral envelope glycoproteins into nascent virions. Here, we identified two regulatory RNAs, microRNAs-25 and -93, induced by the HIV-1 accessory protein Vpu, that downregulate MARCH1 mRNA. We also show that Vpu induces these cellular microRNAs in macrophages by hijacking the cellular β-catenin pathway. The notion that HIV-1 has evolved a mechanism to counteract MARCH1 restriction on viral infectivity underlines the importance of MARCH1 in the host antiviral response.

Published

2023

6. Herpes Simplex Virus 1 Glycoprotein B from a Hyperfusogenic Virus Mediates Enhanced Cell–Cell Fusion

Author

Katrina A. Gianopulos, Albina O. Makio, Suzanne M. Pritchard, Cristina W. Cunha, McKenna A. Hull, and Anthony V. Nicola

Subjects

herpesviruses, viral glycoproteins, membrane fusion, virus entry, Microbiology, QR1-502

Abstract

Herpes simplex virus 1 (HSV-1) causes significant morbidity and death in humans worldwide. Herpes simplex virus 1 has a complex fusion mechanism that is incompletely understood. The HSV-1 strain ANG has notable fusion and entry activities that distinguish it from wild type. HSV-1 ANG virions fused with the Vero cell surface at 4 °C and also entered cells more efficiently at 15 °C, relative to wild type HSV-1 strain KOS virions, consistent with a hyperfusogenic phenotype. Understanding the molecular basis for the unique entry and fusion activities of HSV-1 strain ANG will help decipher the HSV fusion reaction and entry process. Sequencing of HSV-1 ANG genes revealed multiple changes in gB, gC, gD, gH, and gL proteins relative to wild type HSV-1 strains. The ANG UL45 gene sequence, which codes for a non-essential envelope protein, was identical to wild type KOS. HSV-1 ANG gB, gD, and gH/gL were necessary and sufficient to mediate cell–cell fusion in a virus-free reporter assay. ANG gB, when expressed with wild type KOS gD and gH/gL, increased membrane fusion, suggesting that ANG gB has hyperfusogenic cell–cell fusion activity. Replacing the KOS gD, gH, or gL with the corresponding ANG alleles did not enhance cell–cell fusion. The novel mutations in the ANG fusion and entry glycoproteins provide a platform for dissecting the cascade of interactions that culminate in HSV fusion and entry.

Published

2024

7. Activation of TLR4 by viral glycoproteins: A double-edged sword?

Author

Halajian, Emily A., LeBlanc, Emmanuelle V., Gee, Katrina, and Colpitts, Che C.

Subjects

RESPIRATORY syncytial virus, EBOLA virus, GLYCOPROTEINS, TOLL-like receptors, PATTERN perception receptors, DENGUE viruses, THERAPEUTICS, VIRUS diseases

Abstract

Recognition of viral infection by pattern recognition receptors is paramount for a successful immune response to viral infection. However, an unbalanced proinflammatory response can be detrimental to the host. Recently, multiple studies have identified that the SARS-CoV-2 spike protein activates Toll-like receptor 4 (TLR4), resulting in the induction of proinflammatory cytokine expression. Activation of TLR4 by viral glycoproteins has also been observed in the context of other viral infection models, including respiratory syncytial virus (RSV), dengue virus (DENV) and Ebola virus (EBOV). However, the mechanisms involved in virus-TLR4 interactions have remained unclear. Here, we review viral glycoproteins that act as pathogen-associated molecular patterns to induce an immune response via TLR4. We explore the current understanding of the mechanisms underlying how viral glycoproteins are recognized by TLR4 and discuss the contribution of TLR4 activation to viral pathogenesis. We identify contentious findings and research gaps that highlight the importance of understanding viral glycoprotein-mediated TLR4 activation for potential therapeutic approaches. [ABSTRACT FROM AUTHOR]

Published

2022

8. Guanylate-binding protein 5 antagonizes viral glycoproteins independently of furin processing.

Author

Veler H, Lun CM, Waheed AA, and Freed EO

Subjects

Humans, Cell Line, env Gene Products, Human Immunodeficiency Virus metabolism, env Gene Products, Human Immunodeficiency Virus genetics, Glycosylation, GTP-Binding Proteins metabolism, GTP-Binding Proteins genetics, HEK293 Cells, Leukemia Virus, Murine genetics, Leukemia Virus, Murine physiology, SARS-CoV-2 metabolism, Spike Glycoprotein, Coronavirus metabolism, Spike Glycoprotein, Coronavirus genetics, Viral Envelope Proteins metabolism, Viral Envelope Proteins genetics, Furin metabolism, Furin genetics, HIV-1 genetics, HIV-1 physiology

Abstract

Guanylate-binding protein (GBP) 5 is an interferon-inducible cellular factor with broad anti-viral activity. Recently, GBP5 has been shown to antagonize the glycoproteins of a number of enveloped viruses, in part by disrupting the host enzyme furin. Here we show that GBP5 strongly impairs the infectivity of virus particles bearing not only viral glycoproteins that depend on furin cleavage for infectivity-the envelope (Env) glycoproteins of HIV-1 and murine leukemia virus and the spike (S) glycoprotein of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2)-but also viral glycoproteins that do not depend on furin cleavage: vesicular stomatitis virus glycoprotein and SARS-CoV S. We observe that GBP5 disrupts proper N -linked protein glycosylation and reduces the incorporation of viral glycoproteins into virus particles. The glycosylation of the cellular protein CD4 is also altered by GBP5 expression. Flow cytometry analysis shows that GBP5 expression reduces the cell-surface levels of HIV-1 Env and the S glycoproteins of SARS-CoV and SARS-CoV-2. Our data demonstrate that, under the experimental conditions used, inhibition of furin-mediated glycoprotein cleavage is not the primary anti-viral mechanism of action of GBP5. Rather, the antagonism appears to be related to impaired trafficking of glycoproteins to the plasma membrane. These results provide novel insights into the broad antagonism of viral glycoprotein function by the cellular host innate immune response., Importance: The surface of enveloped viruses contains viral envelope glycoproteins, an important structural component facilitating virus attachment and entry while also acting as targets for the host adaptive immune system. In this study, we show that expression of GBP5 in virus-producer cells alters the glycosylation, cell-surface expression, and virion incorporation of viral glycoproteins across several virus families. This research provides novel insights into the broad impact of the host cell anti-viral factor GBP5 on protein glycosylation and trafficking., Competing Interests: The authors declare no conflict of interest.

Published

2024

9. Activation of TLR4 by viral glycoproteins: A double-edged sword?

Author

Emily A. Halajian, Emmanuelle V. LeBlanc, Katrina Gee, and Che C. Colpitts

Subjects

Toll-like receptor 4, viral glycoproteins, cytokine storm, SARS-CoV-2, dengue, Microbiology, QR1-502

Abstract

Recognition of viral infection by pattern recognition receptors is paramount for a successful immune response to viral infection. However, an unbalanced proinflammatory response can be detrimental to the host. Recently, multiple studies have identified that the SARS-CoV-2 spike protein activates Toll-like receptor 4 (TLR4), resulting in the induction of proinflammatory cytokine expression. Activation of TLR4 by viral glycoproteins has also been observed in the context of other viral infection models, including respiratory syncytial virus (RSV), dengue virus (DENV) and Ebola virus (EBOV). However, the mechanisms involved in virus-TLR4 interactions have remained unclear. Here, we review viral glycoproteins that act as pathogen-associated molecular patterns to induce an immune response via TLR4. We explore the current understanding of the mechanisms underlying how viral glycoproteins are recognized by TLR4 and discuss the contribution of TLR4 activation to viral pathogenesis. We identify contentious findings and research gaps that highlight the importance of understanding viral glycoprotein-mediated TLR4 activation for potential therapeutic approaches.

Published

2022

10. Anti-influenza activity of elderberry (Sambucus nigra)

Author

Golnoosh Torabian, Peter Valtchev, Qayyum Adil, and Fariba Dehghani

Subjects

Elderberry, Anti-influenza activity, Cyanidin 3-glucoside, Viral glycoproteins, Immune system, Nutrition. Foods and food supply, TX341-641

Abstract

Elderberry extract is effective in treatment of flu. This study aimed to determine the mechanism of action of elderberry and its primary active compound, cyanidin 3-glucoside (cyn 3-glu), against influenza virus. The direct effect was studied via hemagglutination inhibition assay, plaque reduction assay, and flow cytometry analysis. In addition, to assess the indirect immunomodulatory effect, the modulation of pro-inflammatory cytokines was evaluated. Elderberry showed mild inhibitory effect at the early stages of the influenza virus cycle, with considerably stronger effect (therapeutic index of 12 ± 1.3) in the post-infection phase. Our data further support both direct effects of elderberry extract by blocking viral glycoproteins as well as indirect effects by increased expression of IL-6, IL-8, and TNF. Cyn 3-glu despite demonstrating a similar direct mechanism of action (IC50 of 0.069 mg/ml) compared to the elderberry juice, did not affect the expression of pro-inflammatory cytokines. In conclusion, elderberry exhibits multiple modes of therapeutic action against influenza infection.

Published

2019

11. Exploring lectin–glycan interactions to combat COVID-19: Lessons acquired from other enveloped viruses.

Author

Silva, Luís Cláudio Nascimento da, Mendonça, Juliana Silva Pereira, Oliveira, Weslley Felix de, Batista, Karla Lílian Rodrigues, Zagmignan, Adrielle, Viana, Isabelle Freire Tabosa, and Correia, Maria Tereza dos Santos

Subjects

*LECTINS, *COVID-19, *PLANT lectins, *SARS-CoV-2, *VIRUS diseases, *PROTEIN engineering, *VIRAL envelopes

Abstract

The emergence of a new human coronavirus severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) has imposed great pressure on the health system worldwide. The presence of glycoproteins on the viral envelope opens a wide range of possibilities for the application of lectins to address some urgent problems involved in this pandemic. In this work, we discuss the potential contributions of lectins from nonmammalian sources in the development of several fields associated with viral infections, most notably COVID-19. We review the literature on the use of nonmammalian lectins as a therapeutic approach against members of the Coronaviridae family, including recent advances in strategies of protein engineering to improve their efficacy. The applications of lectins as adjuvants for antiviral vaccines are also discussed. Finally, we present some emerging strategies employing lectins for the development of biosensors, microarrays, immunoassays and tools for purification of viruses from whole blood. Altogether, the data compiled in this review highlight the importance of structural studies aiming to improve our knowledge about the basis of glycan recognition by lectins and its repercussions in several fields, providing potential solutions for complex aspects that are emerging from different health challenges. [ABSTRACT FROM AUTHOR]

Published

2021

12. Herpes Simplex Virus Glycoprotein C Regulates Low-pH Entry

Author

Tri Komala Sari, Katrina A. Gianopulos, Darin J. Weed, Seth M. Schneider, Suzanne M. Pritchard, and Anthony V. Nicola

Subjects

herpesviruses, herpes simplex virus, viral entry, viral glycoproteins, Microbiology, QR1-502

Abstract

ABSTRACT Herpes simplex viruses (HSVs) cause significant morbidity and mortality in humans worldwide. Herpesviruses mediate entry by a multicomponent virus-encoded machinery. Herpesviruses enter cells by endosomal low-pH and pH-neutral mechanisms in a cell-specific manner. HSV mediates cell entry via the envelope glycoproteins gB and gD and the heterodimer gH/gL regardless of pH or endocytosis requirements. Specifics concerning HSV envelope proteins that function selectively in a given entry pathway have been elusive. Here, we demonstrate that gC regulates cell entry and infection by a low-pH pathway. Conformational changes in the core herpesviral fusogen gB are critical for membrane fusion. The presence of gC conferred a higher pH threshold for acid-induced antigenic changes in gB. Thus, gC may selectively facilitate low-pH entry by regulating conformational changes in the fusion protein gB. We propose that gC modulates the HSV fusion machinery during entry into pathophysiologically relevant cells, such as human epidermal keratinocytes. IMPORTANCE Herpesviruses are ubiquitous pathogens that cause lifelong latent infections and that are characterized by multiple entry pathways. We propose that herpes simplex virus (HSV) gC plays a selective role in modulating HSV entry, such as entry into epithelial cells, by a low-pH pathway. gC facilitates a conformational change of the main fusogen gB, a class III fusion protein. We propose a model whereby gC functions with gB, gD, and gH/gL to allow low-pH entry. In the absence of gC, HSV entry occurs at a lower pH, coincident with trafficking to a lower pH compartment where gB changes occur at more acidic pHs. This report identifies a new function for gC and provides novel insight into the complex mechanism of HSV entry and fusion.

Published

2020

13. Backbone Free Energy Estimator Applied to Viral Glycoproteins.

Author

Penner, Robert C.

Subjects

*GLYCOPROTEINS, *HYDROGEN, *DATABASES, *HYDROGEN bonding, *SPINE, *VIRAL antibodies

Abstract

Earlier analysis of the Protein Data Bank derived the distribution of rotations from the plane of a protein hydrogen bond donor peptide group to the plane of its acceptor peptide group. The quasi Boltzmann formalism of Pohl–Finkelstein is employed to estimate free energies of protein elements with these hydrogen bonds, pinpointing residues with a high propensity for conformational change. This is applied to viral glycoproteins as well as capsids, where the 90th+ percentiles of free energies determine residues that correlate well with viral fusion peptides and other functional domains in known cases and thus provide a novel method for predicting these sites of importance as antiviral drug or vaccine targets in general. The method is implemented at https://bion-server.au.dk/hbonds/ from an uploaded Protein Data Bank file. [ABSTRACT FROM AUTHOR]

Published

2020

14. Viral Glycoproteins Induce NLRP3 Inflammasome Activation and Pyroptosis in Macrophages

Author

Hannah S. Eisfeld, Alexander Simonis, Sandra Winter, Jason Chhen, Luisa J. Ströh, Thomas Krey, Manuel Koch, Sebastian J. Theobald, and Jan Rybniker

Subjects

NLRP3, IL-1β, pyroptosis, viral glycoproteins, innate immunity, macrophages, Microbiology, QR1-502

Abstract

Infections with viral pathogens are widespread and can cause a variety of different diseases. In-depth knowledge about viral triggers initiating an immune response is necessary to decipher viral pathogenesis. Inflammasomes, as part of the innate immune system, can be activated by viral pathogens. However, viral structural components responsible for inflammasome activation remain largely unknown. Here we analyzed glycoproteins derived from SARS-CoV-1/2, HCMV and HCV, required for viral entry and fusion, as potential triggers of NLRP3 inflammasome activation and pyroptosis in THP-1 macrophages. All tested glycoproteins were able to potently induce NLRP3 inflammasome activation, indicated by ASC-SPECK formation and secretion of cleaved IL-1β. Lytic cell death via gasdermin D (GSDMD), pore formation, and pyroptosis are required for IL-1β release. As a hallmark of pyroptosis, we were able to detect cleavage of GSDMD and, correspondingly, cell death in THP-1 macrophages. CRISPR-Cas9 knockout of NLRP3 and GSDMD in THP-1 macrophages confirmed and strongly support the evidence that viral glycoproteins can act as innate immunity triggers. With our study, we decipher key mechanisms of viral pathogenesis by showing that viral glycoproteins potently induce innate immune responses. These insights could be beneficial in vaccine development and provide new impulses for the investigation of vaccine-induced innate immunity.

Published

2021

15. Strategies to induce broadly protective antibody responses to viral glycoproteins

Author

F Krammer

Subjects

influenza, universal vaccine, viral glycoproteins, filovirus, arenavirus, hcv, hiv, conserved epitope, heterosubtypic immunity, hemagglutinin, Internal medicine, RC31-1245

Abstract

Introduction: Currently, several universal/broadly protective influenza virus vaccine candidates are under development. Many of these vaccines are based on strategies to induce protective antibody responses against the surface glycoproteins of antigenically and genetically diverse influenza viruses. These strategies might also be applicable to surface glycoproteins of a broad range of other important viral pathogens. Areas covered: Common strategies include sequential vaccination with divergent antigens, multivalent approaches, vaccination with glycan-modified antigens, vaccination with minimal antigens and vaccination with antigens that have centralized/optimized sequences. Here we review these strategies and the underlying concepts. Furthermore, challenges, feasibility and applicability to other viral pathogens are discussed. Expert commentary: Several broadly protective/universal influenza virus vaccine strategies will be tested in humans in the coming years. If successful in terms of safety and immunological readouts, they will move forward into efficacy trials. In the meantime, successful vaccine strategies might also be applied to other antigenically diverse viruses of concern.

Published

2017

16. Two Point Mutations in Old World Hantavirus Glycoproteins Afford the Generation of Highly Infectious Recombinant Vesicular Stomatitis Virus Vectors

Author

Megan M. Slough, Kartik Chandran, and Rohit K. Jangra

Subjects

Dobrava-Belgrade virus, Hantaan virus, hantavirus, recombinant vesicular stomatitis, viral entry, viral glycoproteins, Microbiology, QR1-502

Abstract

ABSTRACT Rodent-to-human transmission of hantaviruses is associated with severe disease. Currently, no FDA-approved, specific antivirals or vaccines are available, and the requirement for high biocontainment (biosafety level 3 [BSL-3]) laboratories limits hantavirus research. To study hantavirus entry in a BSL-2 laboratory, we set out to generate replication-competent, recombinant vesicular stomatitis viruses (rVSVs) bearing the Gn and Gc (Gn/Gc) entry glycoproteins. As previously reported, rVSVs bearing New World hantavirus Gn/Gc were readily rescued from cDNAs, but their counterparts bearing Gn/Gc from the Old World hantaviruses, Hantaan virus (HTNV) or Dobrava-Belgrade virus (DOBV), were refractory to rescue. However, serial passage of the rescued rVSV-HTNV Gn/Gc virus markedly increased its infectivity and capacity for cell-to-cell spread. This gain in viral fitness was associated with the acquisition of two point mutations: I532K in the cytoplasmic tail of Gn and S1094L in the membrane-proximal stem of Gc. Follow-up experiments with rVSVs and single-cycle VSV pseudotypes confirmed these results. Mechanistic studies revealed that both mutations were determinative and contributed to viral infectivity in a synergistic manner. Our findings indicate that the primary mode of action of these mutations is to relocalize HTNV Gn/Gc from the Golgi complex to the cell surface, thereby affording significantly enhanced Gn/Gc incorporation into budding VSV particles. Finally, I532K/S1094L mutations in DOBV Gn/Gc permitted the rescue of rVSV-DOBV Gn/Gc, demonstrating that incorporation of cognate mutations into other hantaviral Gn/Gc proteins could afford the generation of rVSVs that are otherwise challenging to rescue. The robust replication-competent rVSVs, bearing HTNV and DOBV Gn/Gc, reported herein may also have utility as vaccines. IMPORTANCE Human hantavirus infections cause hantavirus pulmonary syndrome in the Americas and hemorrhagic fever with renal syndrome (HFRS) in Eurasia. No FDA-approved vaccines and therapeutics exist for these deadly viruses, and their development is limited by the requirement for high biocontainment. In this study, we identified and characterized key amino acid changes in the surface glycoproteins of HFRS-causing Hantaan virus that enhance their incorporation into recombinant vesicular stomatitis virus (rVSV) particles. The replication-competent rVSVs encoding Hantaan virus and Dobrava-Belgrade virus glycoproteins described in this work provide a powerful and facile system to study hantavirus entry under lower biocontainment and may have utility as hantavirus vaccines.

Published

2019

17. Furin‐mediated protein processing in infectious diseases and cancer

Author

Elisabeth Braun and Daniel Sauter

Subjects

bacterial toxins, cancer, furin, guanylate‐binding proteins, proprotein convertases, viral glycoproteins, Immunologic diseases. Allergy, RC581-607

Abstract

Abstract Proteolytic cleavage regulates numerous processes in health and disease. One key player is the ubiquitously expressed serine protease furin, which cleaves a plethora of proteins at polybasic recognition motifs. Mammalian substrates of furin include cytokines, hormones, growth factors and receptors. Thus, it is not surprising that aberrant furin activity is associated with a variety of disorders including cancer. Furthermore, the enzymatic activity of furin is exploited by numerous viral and bacterial pathogens, thereby enhancing their virulence and spread. In this review, we describe the physiological and pathophysiological substrates of furin and discuss how dysregulation of a simple proteolytic cleavage event may promote infectious diseases and cancer. One major focus is the role of furin in viral glycoprotein maturation and pathogenicity. We also outline cellular mechanisms regulating the expression and activation of furin and summarise current approaches that target this protease for therapeutic intervention.

Published

2019

18. Production of Influenza Virus Glycoproteins Using Insect Cells.

Author

Loganathan M, Francis B, and Krammer F

Subjects

Animals, Baculoviridae genetics, Baculoviridae metabolism, Glycoproteins genetics, Glycoproteins metabolism, Hemagglutinin Glycoproteins, Influenza Virus, Recombinant Proteins, Insecta metabolism, Influenza A Virus, H5N1 Subtype, Influenza Vaccines

Abstract

The baculovirus/insect cell expression system is a very useful tool for reagent and antigen generation in vaccinology, virology, and immunology. It allows for the production of recombinant glycoproteins, which are used as antigens in vaccination studies and as reagents in immunological assays. Here, we describe the process of recombinant glycoprotein production using the baculovirus/insect cell expression system., (© 2024. The Author(s), under exclusive license to Springer Science+Business Media, LLC, part of Springer Nature.)

Published

2024

19. Anti-influenza activity of elderberry (Sambucus nigra).

Author

Torabian, Golnoosh, Valtchev, Peter, Adil, Qayyum, and Dehghani, Fariba

Abstract

Graphical abstract Highlights • Elderberry exhibits multiple modes of therapeutic action against influenza infection. • Elderberry showed a mild inhibitory effect at early stages of the influenza cycle. • Its impact on the post-infection phase is considerably stronger than the early stages. • Elderberry possesses immunomodulatory property through stimulation of cytokines. • Cyn 3-glu had direct effects on influenza but did not stimulate the immune system. Abstract Elderberry extract is effective in treatment of flu. This study aimed to determine the mechanism of action of elderberry and its primary active compound, cyanidin 3-glucoside (cyn 3-glu), against influenza virus. The direct effect was studied via hemagglutination inhibition assay, plaque reduction assay, and flow cytometry analysis. In addition, to assess the indirect immunomodulatory effect, the modulation of pro-inflammatory cytokines was evaluated. Elderberry showed mild inhibitory effect at the early stages of the influenza virus cycle, with considerably stronger effect (therapeutic index of 12 ± 1.3) in the post-infection phase. Our data further support both direct effects of elderberry extract by blocking viral glycoproteins as well as indirect effects by increased expression of IL-6, IL-8, and TNF. Cyn 3-glu despite demonstrating a similar direct mechanism of action (IC50 of 0.069 mg/ml) compared to the elderberry juice, did not affect the expression of pro-inflammatory cytokines. In conclusion, elderberry exhibits multiple modes of therapeutic action against influenza infection. [ABSTRACT FROM AUTHOR]

Published

2019

20. BanLec-eGFP Chimera as a Tool for Evaluation of Lectin Binding to High-Mannose Glycans on Microorganisms

Author

Zorana Lopandić, Luka Dragačević, Dragan Popović, Uros Andjelković, Rajna Minić, and Marija Gavrović-Jankulović

Subjects

banana lectin, eGFP, fluorescence, viral glycoproteins, influenza vaccine, florescence-linked lectin sorbent assay, Microbiology, QR1-502

Abstract

Fluorescently labeled lectins are useful tools for in vivo and in vitro studies of the structure and function of tissues and various pathogens such as viruses, bacteria, and fungi. For the evaluation of high-mannose glycans present on various glycoproteins, a three-dimensional (3D) model of the chimera was designed from the crystal structures of recombinant banana lectin (BanLec, Protein Data Bank entry (PDB): 5EXG) and an enhanced green fluorescent protein (eGFP, PDB 4EUL) by applying molecular modeling and molecular mechanics and expressed in Escherichia coli. BanLec-eGFP, produced as a soluble cytosolic protein of about 42 kDa, revealed β-sheets (41%) as the predominant secondary structures, with the emission peak maximum detected at 509 nm (excitation wavelength 488 nm). More than 65% of the primary structure was confirmed by mass spectrometry. Competitive BanLec-eGFP binding to high mannose glycans of the influenza vaccine (Vaxigrip®) was shown in a fluorescence-linked lectin sorbent assay (FLLSA) with monosaccharides (mannose and glucose) and wild type BanLec and H84T BanLec mutant. BanLec-eGFP exhibited binding to mannose residues on different strains of Salmonella in flow cytometry, with especially pronounced binding to a Salmonella Typhi clinical isolate. BanLec-eGFP can be a useful tool for screening high-mannose glycosylation sites on different microorganisms.

Published

2021

21. Analysis of dispensable glycoproteins of herpes simplex virus type 1

Author

Preetha Balan, K. V.

Subjects

579, Recombinant viruses, Viral glycoproteins

Published

1993

22. Genital Herpes: Insights into Sexually Transmitted Infectious Disease

Author

Dinesh Jaishankar and Deepak Shukla

Subjects

herpes simplex virus, virus entry, viral glycoproteins, viral latency, antivirals, Biology (General), QH301-705.5

Abstract

Etiology, transmission and protection: Herpes simplex virus-2 (HSV-2) is a leading cause of sexually transmitted infections with recurring manifestations throughout the lifetime of infected hosts. Currently no effective vaccines or prophylactics exist that provide complete protection or immunity from the virus, which is endemic throughout the world. Pathology/Symptomatology: Primary and recurrent infections result in lesions and inflammation around the genital area and the latter accounts for majority of genital herpes instances. Immunocompromised patients including neonates are susceptible to additional systemic infections including debilitating consequences of nervous system inflammation. Epidemiology, incidence and prevalence: More than 500 million people are infected worldwide and most reported cases involve the age groups between 16-40 years, which coincides with an increase in sexual activity among this age group. While these numbers are an estimate, the actual numbers may be underestimated as many people are asymptomatic or do not report the symptoms. Treatment and curability: Currently prescribed medications, mostly nucleoside analogs, only reduce the symptoms caused by an active infection, but do not eliminate the virus or reduce latency. Therefore, no cure exists against genital herpes and infected patients suffer from periodic recurrences of disease symptoms for their entire lives. Molecular mechanisms of infection: The last few decades have generated many new advances in our understanding of the mechanisms that drive HSV infection. The viral entry receptors such as nectin-1 and HVEM have been identified, cytoskeletal signaling and membrane structures such as filopodia have been directly implicated in viral entry, host motor proteins and their viral ligands have been shown to facilitate capsid transport and many host and HSV proteins have been identified that help with viral replication and pathogenesis. New understanding has emerged on the role of autophagy and other innate immune mechanisms that are subverted to enhance HSV pathogenesis. This review summarizes our current understanding of HSV-2 and associated diseases and available or upcoming new treatments.

Published

2016

23. Does the Cytoplasmic Tail Matter? Mechanism of Viral Envelope Glycoprotein Targeting by Membrane-Associated-RING-CH (MARCH) Proteins

Author

Cheng man Lun, Abdul A. Waheed, and Eric O. Freed

Subjects

MARCH proteins, E3 ubiquitin ligase, viral glycoproteins, cytoplasmic tail, antiviral factor, General Works

Abstract

The MARCH family of RING-finger E3 ubiquitin ligases comprise 11 members that have been reported to play a variety of roles in the downregulation of cell-surface proteins involved in adaptive immunity. The RING-CH domain of MARCH proteins is thought to ubiquitinate the cytoplasmic tails (CTs) of target proteins, leading to protein degradation through either lysosomal or proteasomal pathways. Three MARCH proteins (MARCH1, 2, and 8) have recently been reported to target the HIV-1 envelope glycoprotein (Env) and vesicular stomatitis virus G glycoprotein (VSV-G), thereby impairing the infectivity of HIV-1 virions bearing HIV-1 Env or VSV-G. However, the mechanism of antiviral activity remains poorly defined. Our data show that MARCH proteins antagonize the full-length forms of HIV-1 Env, VSV-G, and Ebola glycoprotein (GP), and impair the infectivity of HIV-1 virions bearing these viral glycoproteins. This Env-targeting activity of the MARCH proteins requires the E3 ubiquitin ligase activity of the RING-CH domain. We observe that the MARCH protein targeting of VSV-G is, to a large extent, CT-dependent. In striking contrast, the MARCH-protein targeting of HIV-1 Env and Ebola GP does not require the CT. Confocal microscopy data demonstrate that MARCH proteins are able to trap the viral glycoproteins in an intracellular compartment. We observe that the endogenous expression of MARCH8 in T-cell lines and PBMCs is inducible by type I interferons (a and b) and is also upregulated by HIV-1 infection. Current studies are aimed at identifying the cellular target for MARCH-mediated ubiquitination in the context of their antiviral activity. These results will clarify the mechanism by which MARCH proteins antagonize viral glycoproteins and provide insights into the antiviral role of cellular inhibitory factors in Env biogenesis, trafficking, and virion incorporation.

Published

2020

24. MicroRNA-25/93 induction by Vpu as a mechanism for counteracting MARCH1-restriction on HIV-1 infectivity in macrophages.

Author

Lodge R, Xu Z, Eklund M, Stürzel C, Kirchhoff F, Tremblay MJ, Hobman TC, and Cohen ÉA

Subjects

Humans, Viral Regulatory and Accessory Proteins genetics, Viral Regulatory and Accessory Proteins metabolism, Human Immunodeficiency Virus Proteins genetics, Antiviral Agents metabolism, Macrophages metabolism, GPI-Linked Proteins metabolism, HIV Infections metabolism, HIV-1 physiology, HIV Seropositivity, MicroRNAs genetics, MicroRNAs metabolism

Abstract

Importance: In order to efficiently produce infectious viral particles, HIV must counter several restrictions exerted by host cell antiviral proteins. MARCH1 is a member of the MARCH protein family that restricts HIV infection by limiting the incorporation of viral envelope glycoproteins into nascent virions. Here, we identified two regulatory RNAs, microRNAs-25 and -93, induced by the HIV-1 accessory protein Vpu, that downregulate MARCH1 mRNA. We also show that Vpu induces these cellular microRNAs in macrophages by hijacking the cellular β-catenin pathway. The notion that HIV-1 has evolved a mechanism to counteract MARCH1 restriction on viral infectivity underlines the importance of MARCH1 in the host antiviral response., Competing Interests: The authors declare no conflict of interest.

Published

2023

25. Evaluation of Anti-Proprotein Convertase Activity of Diterpene Andrographolid Derived Products

Author

Basak, Ajoy, Banik, Upendra K., Basak, Sarmistha, Seidah, Nabil G., Li, Suiyang, and Khatib, A-Majid, editor

Published

2006

26. Strategies to induce broadly protective antibody responses to viral glycoproteins.

Author

Krammer, F

Abstract

Introduction: Currently, several universal/broadly protective influenza virus vaccine candidates are under development. Many of these vaccines are based on strategies to induce protective antibody responses against the surface glycoproteins of antigenically and genetically diverse influenza viruses. These strategies might also be applicable to surface glycoproteins of a broad range of other important viral pathogens. Areas covered: Common strategies include sequential vaccination with divergent antigens, multivalent approaches, vaccination with glycan-modified antigens, vaccination with minimal antigens and vaccination with antigens that have centralized/optimized sequences. Here we review these strategies and the underlying concepts. Furthermore, challenges, feasibility and applicability to other viral pathogens are discussed. Expert commentary: Several broadly protective/universal influenza virus vaccine strategies will be tested in humans in the coming years. If successful in terms of safety and immunological readouts, they will move forward into efficacy trials. In the meantime, successful vaccine strategies might also be applied to other antigenically diverse viruses of concern. [ABSTRACT FROM PUBLISHER]

Published

2017

27. Exploiting Herpes Simplex Virus Entry for Novel Therapeutics

Author

Deepak Shukla and Satvik Hadigal

Subjects

herpes, HSV-1, HSV-2, therapeutics, peptides, entry, G1 and G2, aptamers, dendrimers, AC-8, dermaseptins, PI3K inhibitor, K-5 compounds, nanoparticles, compound SP-510-50, apolipoprotein E, viral glycoproteins, gB, gD, gH/gL, viral surfing, hemifusion, fusion, endocytosis, Microbiology, QR1-502

Abstract

Herpes Simplex virus (HSV) is associated with a variety of diseases such as genital herpes and numerous ocular diseases. At the global level, high prevalence of individuals who are seropositive for HSV, combined with its inconspicuous infection, remains a cause for major concern. At the molecular level, HSV entry into a host cell involves multiple steps, primarily the interaction of viral glycoproteins with various cell surface receptors, many of which have alternate substitutes. The molecular complexity of the virus to enter a cell is also enhanced by the existence of different modes of viral entry. The availability of many entry receptors, along with a variety of entry mechanisms, has resulted in a virus that is capable of infecting virtually all cell types. While HSV uses a wide repertoire of viral and host factors in establishing infection, current therapeutics aimed against the virus are not as diversified. In this particular review, we will focus on the initial entry of the virus into the cell, while highlighting potential novel therapeutics that can control this process. Virus entry is a decisive step and effective therapeutics can translate to less virus replication, reduced cell death, and detrimental symptoms.

Published

2013

28. Backbone Free Energy Estimator Applied to Viral Glycoproteins

Author

Robert C. Penner

Subjects

Models, Molecular, Protein Conformation, Peptide, Hemagglutinin Glycoproteins, Influenza Virus, Encephalitis Viruses, Tick-Borne, 03 medical and health sciences, antiviral drugs, Viral Proteins, 0302 clinical medicine, Viral Envelope Proteins, Group (periodic table), Genetics, Humans, Databases, Protein, Molecular Biology, Research Articles, 030304 developmental biology, Glycoproteins, chemistry.chemical_classification, 0303 health sciences, vaccine targets, Membrane Glycoproteins, Models, Statistical, Plane (geometry), Hydrogen bond, Protein Stability, Estimator, Computational Biology, Hydrogen Bonding, computer.file_format, Protein Data Bank, Acceptor, Computational Mathematics, Crystallography, Computational Theory and Mathematics, chemistry, Influenza A virus, 030220 oncology & carcinogenesis, Modeling and Simulation, Paramyxovirinae, Thermodynamics, Glycoprotein, viral glycoproteins, computer, Viral Fusion Proteins

Abstract

Earlier analysis of the Protein Data Bank derived the distribution of rotations from the plane of a protein hydrogen bond donor peptide group to the plane of its acceptor peptide group. The quasi Boltzmann formalism of Pohl-Finkelstein is employed to estimate free energies of protein elements with these hydrogen bonds, pinpointing residues with a high propensity for conformational change. This is applied to viral glycoproteins as well as capsids, where the 90th+ percentiles of free energies determine residues that correlate well with viral fusion peptides and other functional domains in known cases and thus provide a novel method for predicting these sites of importance as antiviral drug or vaccine targets in general. The method is implemented at https://bion-server.au.dk/hbonds/ from an uploaded Protein Data Bank file.

Published

2020

29. BanLec-eGFP Chimera as a Tool for Evaluation of Lectin Binding to High-Mannose Glycans on Microorganisms

Author

Lopandić, Zorana, Dragačević, Luka, Popović, Dragan M., Anđelković, Uroš, Minić, Rajna, Gavrović-Jankulović, Marija, Lopandić, Zorana, Dragačević, Luka, Popović, Dragan M., Anđelković, Uroš, Minić, Rajna, and Gavrović-Jankulović, Marija

Abstract

Fluorescently labeled lectins are useful tools for in vivo and in vitro studies of the structure and function of tissues and various pathogens such as viruses, bacteria, and fungi. For the evaluation of high-mannose glycans present on various glycoproteins, a three-dimensional (3D) model of the chimera was designed from the crystal structures of recombinant banana lectin (BanLec, Protein Data Bank entry (PDB): 5EXG) and an enhanced green fluorescent protein (eGFP, PDB 4EUL) by applying molecular modeling and molecular mechanics and expressed in Escherichia coli. BanLec-eGFP, produced as a soluble cytosolic protein of about 42 kDa, revealed β-sheets (41%) as the predominant secondary structures, with the emission peak maximum detected at 509 nm (excitation wavelength 488 nm). More than 65% of the primary structure was confirmed by mass spectrometry. Competitive BanLec-eGFP binding to high mannose glycans of the influenza vaccine (Vaxigrip®) was shown in a fluorescence-linked lectin sorbent assay (FLLSA) with monosaccharides (mannose and glucose) and wild type BanLec and H84T BanLec mutant. BanLec-eGFP exhibited binding to mannose residues on different strains of Salmonella in flow cytometry, with especially pronounced binding to a Salmonella Typhi clinical isolate. BanLec-eGFP can be a useful tool for screening high-mannose glycosylation sites on different microorganisms.

Published

2021

30. Anti-influenza activity of elderberry (Sambucus nigra)

Author

Peter Valtchev, Qayyum Adil, Fariba Dehghani, and Golnoosh Torabian

Subjects

0301 basic medicine, Cyanidin 3-glucoside, Cyanidin, Medicine (miscellaneous), Pharmacology, Sambucus nigra, Virus, Anti-influenza activity, Viral glycoproteins, 03 medical and health sciences, chemistry.chemical_compound, 0404 agricultural biotechnology, Therapeutic index, medicine, TX341-641, IC50, 030109 nutrition & dietetics, Nutrition and Dietetics, Hemagglutination assay, biology, Nutrition. Foods and food supply, 04 agricultural and veterinary sciences, biology.organism_classification, 040401 food science, Immune system, chemistry, Mechanism of action, Elderberry, Tumor necrosis factor alpha, medicine.symptom, Food Science

Abstract

Elderberry extract is effective in treatment of flu. This study aimed to determine the mechanism of action of elderberry and its primary active compound, cyanidin 3-glucoside (cyn 3-glu), against influenza virus. The direct effect was studied via hemagglutination inhibition assay, plaque reduction assay, and flow cytometry analysis. In addition, to assess the indirect immunomodulatory effect, the modulation of pro-inflammatory cytokines was evaluated. Elderberry showed mild inhibitory effect at the early stages of the influenza virus cycle, with considerably stronger effect (therapeutic index of 12 ± 1.3) in the post-infection phase. Our data further support both direct effects of elderberry extract by blocking viral glycoproteins as well as indirect effects by increased expression of IL-6, IL-8, and TNF. Cyn 3-glu despite demonstrating a similar direct mechanism of action (IC50 of 0.069 mg/ml) compared to the elderberry juice, did not affect the expression of pro-inflammatory cytokines. In conclusion, elderberry exhibits multiple modes of therapeutic action against influenza infection.

Published

2019

31. Mechanism of Viral Glycoprotein Targeting by Membrane-Associated RING-CH Proteins

Author

Ahlam Majadly, Abdul Waheed, Eric O. Freed, Nicole Powell, and Cheng Man Lun

Subjects

viruses, Ubiquitin-Protein Ligases, Intracellular Space, cellular inhibitory factors, medicine.disease_cause, Virus Replication, spike protein, Microbiology, Article, 03 medical and health sciences, HIV-1 Env, Ubiquitin, Viral envelope, Species Specificity, Viral Envelope Proteins, Interferon, Virology, medicine, Humans, RNA Viruses, Amino Acid Sequence, VSV-G, Cells, Cultured, 030304 developmental biology, chemistry.chemical_classification, 0303 health sciences, Ebola virus, Ebola virus GP, biology, SARS-CoV-2, 030302 biochemistry & molecular biology, Virion, Membrane Proteins, biology.organism_classification, QR1-502, Ubiquitin ligase, Cell biology, HEK293 Cells, chemistry, Viral replication, Gene Expression Regulation, E3 ubiquitin ligase, Vesicular stomatitis virus, Mutation, biology.protein, Interferons, Glycoprotein, viral glycoproteins, medicine.drug

Abstract

An emerging class of cellular inhibitory proteins has been identified that targets viral glycoproteins. These include the membrane-associated RING-CH (MARCH) family of E3 ubiquitin ligases that, among other functions, downregulate cell surface proteins involved in adaptive immunity. The RING-CH domain of MARCH proteins is thought to function by catalyzing the ubiquitination of the cytoplasmic tails (CTs) of target proteins, leading to their degradation. MARCH proteins have recently been reported to target retroviral envelope glycoproteins (Env) and vesicular stomatitis virus G glycoprotein (VSV-G). However, the mechanism of antiviral activity remains poorly defined. Here we show that MARCH8 antagonizes the full-length forms of HIV-1 Env, VSV-G, Ebola virus glycoprotein (EboV-GP), and the spike (S) protein of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), thereby impairing the infectivity of virions pseudotyped with these viral glycoproteins. This MARCH8-mediated targeting of viral glycoproteins requires the E3 ubiquitin ligase activity of the RING-CH domain. We observe that MARCH8 protein antagonism of VSV-G is CT dependent. In contrast, MARCH8-mediated targeting of HIV-1 Env, EboV-GP, and SARS-CoV-2 S protein by MARCH8 does not require the CT, suggesting a novel mechanism of MARCH-mediated antagonism of these viral glycoproteins. Confocal microscopy data demonstrate that MARCH8 traps the viral glycoproteins in an intracellular compartment. We observe that the endogenous expression of MARCH8 in several relevant human cell types is rapidly inducible by type I interferon. These results help to inform the mechanism by which MARCH proteins exert their antiviral activity and provide insights into the role of cellular inhibitory factors in antagonizing the biogenesis, trafficking, and virion incorporation of viral glycoproteins.IMPORTANCE Viral envelope glycoproteins are an important structural component on the surfaces of enveloped viruses that direct virus binding and entry and also serve as targets for the host adaptive immune response. In this study, we investigate the mechanism of action of the MARCH family of cellular proteins that disrupt the trafficking and virion incorporation of viral glycoproteins across several virus families. This research provides novel insights into how host cell factors antagonize viral replication, perhaps opening new avenues for therapeutic intervention in the replication of a diverse group of highly pathogenic enveloped viruses.

Published

2021

32. Mechanism of Viral Glycoprotein Targeting by Membrane-associated-RING-CH Proteins

Author

Eric O. Freed, Cheng Man Lun, Nicole Powell, Abdul Waheed, and Ahlam Majadly

Subjects

viruses, cellular inhibitory factors, medicine.disease_cause, HIV-1 Env, Ubiquitin, Interferon, medicine, VSV-G, chemistry.chemical_classification, Ebola virus, Ebola virus GP, biology, Chemistry, Acquired immune system, biology.organism_classification, Ubiquitin ligase, Cell biology, SARS-CoV-2 spike protein, E3 ubiquitin ligase, Vesicular stomatitis virus, biology.protein, Glycoprotein, viral glycoproteins, Biogenesis, medicine.drug, Research Article

Abstract

Viral envelope glycoproteins are an important structural component on the surfaces of enveloped viruses that direct virus binding and entry and also serve as targets for the host adaptive immune response. In this study, we investigate the mechanism of action of the MARCH family of cellular proteins that disrupt the trafficking and virion incorporation of viral glycoproteins across several virus families., An emerging class of cellular inhibitory proteins has been identified that targets viral glycoproteins. These include the membrane-associated RING-CH (MARCH) family of E3 ubiquitin ligases that, among other functions, downregulate cell surface proteins involved in adaptive immunity. The RING-CH domain of MARCH proteins is thought to function by catalyzing the ubiquitination of the cytoplasmic tails (CTs) of target proteins, leading to their degradation. MARCH proteins have recently been reported to target retroviral envelope glycoproteins (Env) and vesicular stomatitis virus G glycoprotein (VSV-G). However, the mechanism of antiviral activity remains poorly defined. Here we show that MARCH8 antagonizes the full-length forms of HIV-1 Env, VSV-G, Ebola virus glycoprotein (EboV-GP), and the spike (S) protein of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), thereby impairing the infectivity of virions pseudotyped with these viral glycoproteins. This MARCH8-mediated targeting of viral glycoproteins requires the E3 ubiquitin ligase activity of the RING-CH domain. We observe that MARCH8 protein antagonism of VSV-G is CT dependent. In contrast, MARCH8-mediated targeting of HIV-1 Env, EboV-GP, and SARS-CoV-2 S protein by MARCH8 does not require the CT, suggesting a novel mechanism of MARCH-mediated antagonism of these viral glycoproteins. Confocal microscopy data demonstrate that MARCH8 traps the viral glycoproteins in an intracellular compartment. We observe that the endogenous expression of MARCH8 in several relevant human cell types is rapidly inducible by type I interferon. These results help to inform the mechanism by which MARCH proteins exert their antiviral activity and provide insights into the role of cellular inhibitory factors in antagonizing the biogenesis, trafficking, and virion incorporation of viral glycoproteins.

Published

2021

33. BanLec-eGFP Chimera as a Tool for Evaluation of Lectin Binding to High-Mannose Glycans on Microorganisms

Author

Luka Dragačević, Dragan Popovic, Rajna Minić, Zorana Lopandić, Uroš Andjelković, and Marija Gavrović-Jankulović

Subjects

0301 basic medicine, glycoprotein, fluorescence linked lectin sorbent assay, Protein Conformation, Protein Data Bank (RCSB PDB), lcsh:QR1-502, Mannose, enhanced green fluorescent protein, IC50, Crystallography, X-Ray, Biochemistry, Protein Structure, Secondary, lcsh:Microbiology, Green fluorescent protein, chemistry.chemical_compound, Lectins, protein purification, eGFP, Protein purification, binding affinity, antigen binding, biotinylation, lectin binding, mass spectrometry, biology, ion exchange chromatography, Flow Cytometry, hemagglutin, molecular mechanics, structure analysis, 3. Good health, protein protein interaction, Salmonella enterica serovar Typhi, fluorescence, Plant Lectins, viral glycoproteins, immunoblotting, surface plasmon resonance, Protein Binding, Glycan, crystal structure, Glycosylation, in vitro study, glycosylation, Green Fluorescent Proteins, low cytometry, BanLec, Article, florescence-linked lectin sorbent assay, 03 medical and health sciences, Polysaccharides, Escherichia coli, banana lectin, controlled study, human, protein structure, Molecular Biology, structure activity relation, Salmonella strains, 030102 biochemistry & molecular biology, binding site, human cell, Lectin, Musa, nucleotide sequence, X ray crystallography, amino acid sequence, circular dichroism, epitope mapping, 030104 developmental biology, chemistry, biology.protein, enzymatic assay, molecular model, influenza vaccine, Peptides

Abstract

Fluorescently labeled lectins are useful tools for in vivo and in vitro studies of the structure and function of tissues and various pathogens such as viruses, bacteria, and fungi. For the evaluation of high-mannose glycans present on various glycoproteins, a three-dimensional (3D) model of the chimera was designed from the crystal structures of recombinant banana lectin (BanLec, Protein Data Bank entry (PDB): 5EXG) and an enhanced green fluorescent protein (eGFP, PDB 4EUL) by applying molecular modeling and molecular mechanics and expressed in Escherichia coli. BanLec-eGFP, produced as a soluble cytosolic protein of about 42 kDa, revealed &beta, sheets (41%) as the predominant secondary structures, with the emission peak maximum detected at 509 nm (excitation wavelength 488 nm). More than 65% of the primary structure was confirmed by mass spectrometry. Competitive BanLec-eGFP binding to high mannose glycans of the influenza vaccine (Vaxigrip&reg, ) was shown in a fluorescence-linked lectin sorbent assay (FLLSA) with monosaccharides (mannose and glucose) and wild type BanLec and H84T BanLec mutant. BanLec-eGFP exhibited binding to mannose residues on different strains of Salmonella in flow cytometry, with especially pronounced binding to a Salmonella Typhi clinical isolate. BanLec-eGFP can be a useful tool for screening high-mannose glycosylation sites on different microorganisms.

Published

2021

34. Arms Race between Enveloped Viruses and the Host ERAD Machinery

Author

Dylan A. Frabutt and Yong-Hui Zheng

Subjects

enveloped viruses, viral glycoproteins, endoplasmic reticulum-associated degradation, ERAD, unfolded protein response, UPR, ER stress, Microbiology, QR1-502

Abstract

Enveloped viruses represent a significant category of pathogens that cause serious diseases in animals. These viruses express envelope glycoproteins that are singularly important during the infection of host cells by mediating fusion between the viral envelope and host cell membranes. Despite low homology at protein levels, three classes of viral fusion proteins have, as of yet, been identified based on structural similarities. Their incorporation into viral particles is dependent upon their proper sub-cellular localization after being expressed and folded properly in the endoplasmic reticulum (ER). However, viral protein expression can cause stress in the ER, and host cells respond to alleviate the ER stress in the form of the unfolded protein response (UPR); the effects of which have been observed to potentiate or inhibit viral infection. One important arm of UPR is to elevate the capacity of the ER-associated protein degradation (ERAD) pathway, which is comprised of host quality control machinery that ensures proper protein folding. In this review, we provide relevant details regarding viral envelope glycoproteins, UPR, ERAD, and their interactions in host cells.

Published

2016

35. Does the Cytoplasmic Tail Matter? Mechanism of Viral Envelope Glycoprotein Targeting by Membrane-Associated-RING-CH (MARCH) Proteins

Author

Abdul A. Waheed, Cheng Man Lun, and Eric O. Freed

Subjects

chemistry.chemical_classification, biology, Chemistry, viruses, virus diseases, lcsh:A, Protein degradation, medicine.disease_cause, biology.organism_classification, Ubiquitin ligase, Cell biology, cytoplasmic tail, Ubiquitin, Viral envelope, E3 ubiquitin ligase, Cytoplasm, Vesicular stomatitis virus, Protein targeting, biology.protein, medicine, lcsh:General Works, Glycoprotein, viral glycoproteins, antiviral factor, MARCH proteins

Abstract

The MARCH family of RING-finger E3 ubiquitin ligases comprise 11 members that have been reported to play a variety of roles in the downregulation of cell-surface proteins involved in adaptive immunity. The RING-CH domain of MARCH proteins is thought to ubiquitinate the cytoplasmic tails (CTs) of target proteins, leading to protein degradation through either lysosomal or proteasomal pathways. Three MARCH proteins (MARCH1, 2, and 8) have recently been reported to target the HIV-1 envelope glycoprotein (Env) and vesicular stomatitis virus G glycoprotein (VSV-G), thereby impairing the infectivity of HIV-1 virions bearing HIV-1 Env or VSV-G. However, the mechanism of antiviral activity remains poorly defined. Our data show that MARCH proteins antagonize the full-length forms of HIV-1 Env, VSV-G, and Ebola glycoprotein (GP), and impair the infectivity of HIV-1 virions bearing these viral glycoproteins. This Env-targeting activity of the MARCH proteins requires the E3 ubiquitin ligase activity of the RING-CH domain. We observe that the MARCH protein targeting of VSV-G is, to a large extent, CT-dependent. In striking contrast, the MARCH-protein targeting of HIV-1 Env and Ebola GP does not require the CT. Confocal microscopy data demonstrate that MARCH proteins are able to trap the viral glycoproteins in an intracellular compartment. We observe that the endogenous expression of MARCH8 in T-cell lines and PBMCs is inducible by type I interferons (a and b) and is also upregulated by HIV-1 infection. Current studies are aimed at identifying the cellular target for MARCH-mediated ubiquitination in the context of their antiviral activity. These results will clarify the mechanism by which MARCH proteins antagonize viral glycoproteins and provide insights into the antiviral role of cellular inhibitory factors in Env biogenesis, trafficking, and virion incorporation.

Published

2020

36. Exploring lectin-glycan interactions to combat COVID-19: Lessons acquired from other enveloped viruses

Author

Luís Cláudio Nascimento da Silva, Juliana Silva Pereira Mendonça, Karla Lílian Rodrigues Batista, Isabelle F. T. Viana, Maria Tereza dos Santos Correia, Weslley Felix de Oliveira, and Adrielle Zagmignan

Subjects

0301 basic medicine, 2019-20 coronavirus outbreak, Glycan, Coronavirus disease 2019 (COVID-19), Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), AcademicSubjects/SCI01000, Computational biology, Review, immunization, Biochemistry, Antiviral Agents, 03 medical and health sciences, 0302 clinical medicine, Viral envelope, Polysaccharides, Lectins, antiviral therapy, Coronaviridae, Humans, biology, SARS-CoV-2, Lectin, COVID-19, blood purification, biology.organism_classification, biosensors, Human coronavirus, 3. Good health, COVID-19 Drug Treatment, 030104 developmental biology, 030220 oncology & carcinogenesis, biology.protein, Carbohydrate Metabolism, viral glycoproteins

Abstract

The emergence of a new human coronavirus severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) has imposed great pressure on the health system worldwide. The presence of glycoproteins on the viral envelope opens a wide range of possibilities for the application of lectins to address some urgent problems involved in this pandemic. In this work, we discuss the potential contributions of lectins from nonmammalian sources in the development of several fields associated with viral infections, most notably COVID-19. We review the literature on the use of nonmammalian lectins as a therapeutic approach against members of the Coronaviridae family, including recent advances in strategies of protein engineering to improve their efficacy. The applications of lectins as adjuvants for antiviral vaccines are also discussed. Finally, we present some emerging strategies employing lectins for the development of biosensors, microarrays, immunoassays and tools for purification of viruses from whole blood. Altogether, the data compiled in this review highlight the importance of structural studies aiming to improve our knowledge about the basis of glycan recognition by lectins and its repercussions in several fields, providing potential solutions for complex aspects that are emerging from different health challenges.

Published

2020

37. Herpes Simplex Virus Glycoprotein C Regulates Low-pH Entry

Author

Seth M. Schneider, Darin J. Weed, Suzanne M. Pritchard, Anthony V. Nicola, Tri Komala Sari, and Katrina A. Gianopulos

Subjects

Conformational change, herpesviruses, Endosome, viruses, lcsh:QR1-502, Herpesvirus 1, Human, medicine.disease_cause, Endocytosis, Microbiology, lcsh:Microbiology, Host-Microbe Biology, 03 medical and health sciences, Protein Domains, Viral Envelope Proteins, Viral entry, Chlorocebus aethiops, medicine, Animals, Humans, Molecular Biology, Vero Cells, 030304 developmental biology, chemistry.chemical_classification, 0303 health sciences, 030306 microbiology, Lipid bilayer fusion, Herpes Simplex, Hydrogen-Ion Concentration, Virus Internalization, herpes simplex virus, Fusion protein, QR1-502, 3. Good health, Cell biology, Herpes simplex virus, chemistry, viral entry, Glycoprotein, viral glycoproteins, Research Article

Abstract

Herpesviruses are ubiquitous pathogens that cause lifelong latent infections and that are characterized by multiple entry pathways. We propose that herpes simplex virus (HSV) gC plays a selective role in modulating HSV entry, such as entry into epithelial cells, by a low-pH pathway. gC facilitates a conformational change of the main fusogen gB, a class III fusion protein. We propose a model whereby gC functions with gB, gD, and gH/gL to allow low-pH entry. In the absence of gC, HSV entry occurs at a lower pH, coincident with trafficking to a lower pH compartment where gB changes occur at more acidic pHs. This report identifies a new function for gC and provides novel insight into the complex mechanism of HSV entry and fusion., Herpes simplex viruses (HSVs) cause significant morbidity and mortality in humans worldwide. Herpesviruses mediate entry by a multicomponent virus-encoded machinery. Herpesviruses enter cells by endosomal low-pH and pH-neutral mechanisms in a cell-specific manner. HSV mediates cell entry via the envelope glycoproteins gB and gD and the heterodimer gH/gL regardless of pH or endocytosis requirements. Specifics concerning HSV envelope proteins that function selectively in a given entry pathway have been elusive. Here, we demonstrate that gC regulates cell entry and infection by a low-pH pathway. Conformational changes in the core herpesviral fusogen gB are critical for membrane fusion. The presence of gC conferred a higher pH threshold for acid-induced antigenic changes in gB. Thus, gC may selectively facilitate low-pH entry by regulating conformational changes in the fusion protein gB. We propose that gC modulates the HSV fusion machinery during entry into pathophysiologically relevant cells, such as human epidermal keratinocytes. IMPORTANCE Herpesviruses are ubiquitous pathogens that cause lifelong latent infections and that are characterized by multiple entry pathways. We propose that herpes simplex virus (HSV) gC plays a selective role in modulating HSV entry, such as entry into epithelial cells, by a low-pH pathway. gC facilitates a conformational change of the main fusogen gB, a class III fusion protein. We propose a model whereby gC functions with gB, gD, and gH/gL to allow low-pH entry. In the absence of gC, HSV entry occurs at a lower pH, coincident with trafficking to a lower pH compartment where gB changes occur at more acidic pHs. This report identifies a new function for gC and provides novel insight into the complex mechanism of HSV entry and fusion.

Published

2020

38. Additional Glycosylation Within a Specific Hypervariable Region of Subtype 3a of Hepatitis C Virus Protects Against Virus Neutralization.

Author

Anjum, Sadia, Wahid, Ahmed, Afzal, Muhammad Sohail, Albecka, Anna, Alsaleh, Khaled, Ahmad, Tahir, Baumert, Thomas F., Wychowski, Czeslaw, Qadri, Ishtiaq, Penin, François, and Dubuisson, Jean

Subjects

*HEPATITIS C risk factors, *GLYCOPROTEINS, *GLYCOSYLATION, *MOLECULAR structure of amino acids, *LIVER diseases

Abstract

Background. The envelope glycoprotein E2 of hepatitis C virus (HCV) contains several hypervariable regions. Interestingly, 2 regions of intragenotypic hypervariability within E2 have been described as being specific to HCV subtype 3a. Based on their amino acid position in E2, they were named HVR495 and HVR575. Here, we further investigated these regions in order to better understand their role in HCV infection.Methods. Sequences of HCV envelope glycoproteins from Pakistani patients infected with subtype 3a were cloned and compared with other subtype 3a sequences. The entry functions and the sensitivity to antibody neutralization of selected HCV glycoprotein sequences were tested in the HCV pseudotyped particles (HCVpp) system. In addition, the cell-cultured HCV system (HCVcc) was also used to confirm some of the data obtained with the HCVpp system.Results. We observed interesting new features within HVR495 and HVR575 for several subtype 3a isolates. Indeed, changes in glycosylation sites were observed with the appearance of a new glycosylation site within HVR495. Importantly, HCVpp and HCVcc that contained this new HVR495 glycosylation site were less sensitive to antibody neutralization.Conclusions. We identified a new glycosylation site within the HVR495 region of HCV subtype 3a that has a protective effect against antibody neutralization. [ABSTRACT FROM AUTHOR]

Published

2013

39. Identification and Functional Analysis of Membrane Proteins gD, gE, gI, and pUS9 of Infectious Laryngotracheitis Virus.

Author

Pavlova, Sophia, Veits, Jutta, Mettenleiter, Thomas C., and Fuchs, Walter

Subjects

VIRUS diseases in poultry, WESTERN immunoblotting, GLYCOPROTEINS, MAREK'S disease, AVIAN leukosis, HERPESVIRUS diseases in animals

Abstract

The article offers information on a study that prepared monospecific rabbit antisera against infectious laryngotracheitis virus (ILTV) gD, gE, and gI, and the ILTV type II membrane protein pUS9. The study detected proteins of approximately 65 and 70 kDa (gD), 62 kDa (gI), 75 kDa (gE), or 37 kDa(pUS9) in western blot analyses of infected chicken cells. Identified as abundant virion proteins are gD, gI, and gE, but not pUS9 while gE and gI were shown to be N-glycosylated. d gE-, gI-, and pUS9-deleted ILTV recombinants were isolated.

Published

2013

40. Exploiting Herpes Simplex Virus Entry for Novel Therapeutics.

Author

Hadigal, Satvik and Shukla, Deepak

Subjects

*HERPES simplex virus, *HERPES genitalis, *GLYCOPROTEINS, *CELL receptors, *HERPESVIRUSES, *HERPES simplex, *SEXUALLY transmitted diseases

Abstract

Herpes Simplex virus (HSV) is associated with a variety of diseases such as genital herpes and numerous ocular diseases. At the global level, high prevalence of individuals who are seropositive for HSV, combined with its inconspicuous infection, remains a cause for major concern. At the molecular level, HSV entry into a host cell involves multiple steps, primarily the interaction of viral glycoproteins with various cell surface receptors, many of which have alternate substitutes. The molecular complexity of the virus to enter a cell is also enhanced by the existence of different modes of viral entry. The availability of many entry receptors, along with a variety of entry mechanisms, has resulted in a virus that is capable of infecting virtually all cell types. While HSV uses a wide repertoire of viral and host factors in establishing infection, current therapeutics aimed against the virus are not as diversified. In this particular review, we will focus on the initial entry of the virus into the cell, while highlighting potential novel therapeutics that can control this process. Virus entry is a decisive step and effective therapeutics can translate to less virus replication, reduced cell death, and detrimental symptoms. [ABSTRACT FROM AUTHOR]

Published

2013

41. Computational separation of conformational heterogeneity using cryo-electron tomography and 3D sub-volume averaging

Author

Frank, Gabriel A., Bartesaghi, Alberto, Kuybeda, Oleg, Borgnia, Mario J., White, Tommi A., Sapiro, Guillermo, and Subramaniam, Sriram

Subjects

*TOMOGRAPHY, *HIV-1 glycoprotein 120, *GLYCOPROTEINS, *IMAGE registration, *MACROMOLECULES, *MOLECULAR structure

Abstract

Abstract: We have previously used cryo-electron tomography combined with sub-volume averaging and classification to obtain 3D structures of macromolecular assemblies in cases where a single dominant species was present, and applied these methods to the analysis of a variety of trimeric HIV-1 and SIV envelope glycoproteins (Env). Here, we extend these studies by demonstrating automated, iterative, missing wedge-corrected 3D image alignment and classification methods to distinguish multiple conformations that are present simultaneously. We present a method for measuring the spatial distribution of the vector elements representing distinct conformational states of Env. We identify data processing strategies that allow clear separation of the previously characterized closed and open conformations, as well as unliganded and antibody-liganded states of Env when they are present in mixtures. We show that identifying and removing spikes with the lowest signal-to-noise ratios improves the overall accuracy of alignment between individual Env sub-volumes, and that alignment accuracy, in turn, determines the success of image classification in assessing conformational heterogeneity in heterogeneous mixtures. We validate these procedures for computational separation by successfully separating and reconstructing distinct 3D structures for unliganded and antibody-liganded as well as open and closed conformations of Env present simultaneously in mixtures. [Copyright &y& Elsevier]

Published

2012

42. In vitro analysis of the factors contributing to the antiviral state induced by a plasmid encoding the viral haemorrhagic septicaemia virus glycoprotein G in transfected trout cells

Author

Ortega-Villaizan, M., Chico, V., Martinez-Lopez, A., Falco, A., Perez, L., Coll, J.M., and Estepa, A.

Subjects

*VIRAL hemorrhagic septicemia, *GLYCOPROTEINS, *GENE transfection, *CELL lines, *PLASMIDS, *DNA vaccines, *NATURAL immunity, *RHABDOVIRUSES, *RAINBOW trout, *CELL receptors

Abstract

Abstract: We have found out that transfection of the RTG-2 cell line with the viral haemorrhagic septicaemia virus (VHSV) glycoprotein G (GVHSV)-coding plasmid induces an anti-VHSV state, similar to that induced by poly I:C. Taking the advantage of the constitutive expression of toll-like receptor 9 gene (tlr9) in RTG-2 cells, we have investigated whether this antiviral state was induced by the cytosine-phosphodiester-guanine (CpG) motifs present in the plasmid DNA, by the endogenous expression of GVHSV protein or by both elements. For that, we have analysed the expression profile of the rainbow trout tlr9 and several genes related to TLR9-mediated immune response in the absence or presence of a lysosomotropic drug that specifically blocks TLR9–CpG DNA interaction. The results suggested that the high levels of cell protection conferred by a plasmid encoding GVHSV gene are due to GVHSV rather than to the CpG motifs within plasmid DNA. Therefore, plasmid DNA might not play a key role in the immune response elicited by DNA vaccines or perhaps other receptors instead TLR9 could be implicated in CpG motifs recognition and signalling. In addition, since RTG-2 cells express tlr9 gene, this cell line could be a good tool for screening TLR9 agonists, such as the immunomodulatory oligonucleotides (IMOs), as fish DNA vaccine adjuvants. [ABSTRACT FROM AUTHOR]

Published

2011

43. Requirements for cell rounding and surface protein down-regulation by Ebola virus glycoprotein

Author

Francica, Joseph R., Matukonis, Meghan K., and Bates, Paul

Subjects

*EBOLA virus, *GLYCOPROTEINS, *HEMORRHAGIC fever, *INTEGRINS, *CELLULAR pathology, *VIRUS diseases, *PROTEINS

Abstract

Abstract: Ebola virus causes an acute hemorrhagic fever that is associated with high morbidity and mortality. The viral glycoprotein is thought to contribute to pathogenesis, though precise mechanisms are unknown. Cellular pathogenesis can be modeled in vitro by expression of the Ebola viral glycoprotein (GP) in cells, which causes dramatic morphological changes, including cell rounding and surface protein down-regulation. These effects are known to be dependent on the presence of a highly glycosylated region of the glycoprotein, the mucin domain. Here we show that the mucin domain from the highly pathogenic Zaire subtype of Ebola virus is sufficient to cause characteristic cytopathology when expressed in the context of a foreign glycoprotein. Similarly to full length Ebola GP, expression of the mucin domain causes rounding, detachment from the extracellular matrix, and the down-regulation of cell surface levels of β1 integrin and major histocompatibility complex class 1. These effects were not seen when the mucin domain was expressed in the context of a glycophosphatidylinositol-anchored isoform of the foreign glycoprotein. In contrast to earlier analysis of full length Ebola glycoproteins, chimeras carrying the mucin domains from the Zaire and Reston strains appear to cause similar levels of down-modulation and cell detachment. Cytopathology associated with Ebola glycoprotein expression does not occur when GP expression is restricted to the endoplasmic reticulum. In contrast to a previously published report, our results demonstrate that GP-induced surface protein down-regulation is not mediated through a dynamin-dependent pathway. Overall, these results support a model in which the mucin domain of Ebola GP acts at the cell surface to induce protein down modulation and cytopathic effects. [Copyright &y& Elsevier]

Published

2009

44. Molecular Characteristics of the Nipah Virus Glycoproteins.

Author

DIEDERICH, SANDRA and MAISNER, ANDREA

Subjects

*NIPAH virus, *PARAMYXOVIRUSES, *RESPIRATORY diseases, *ENCEPHALITIS, *BATS

Abstract

Nipah virus (NiV) is a highly pathogenic paramyxovirus, which emerged in 1998 from fruit bats in Malaysia and caused an outbreak of severe respiratory disease in pigs and fatal encephalitis in humans with high mortality rates. In contrast to most paramyxoviruses, NiV can infect a large variety of mammalian species. Due to this broad host range, its zoonotic potential, its high pathogenicity for humans, and the lack of effective vaccines or therapeutics, NiV was classified as a biosafety level 4 pathogen. This article provides an overview of the molecular characteristics of NiV focusing on the structure, functions, and unique biological properties of the two NiV surface glycoproteins, the receptor-binding G protein, and the fusion protein F. Since viral glycoproteins are major determinants for cell tropism and virus spread, a detailed knowledge of these proteins can help to understand the molecular basis of viral pathogenicity. [ABSTRACT FROM AUTHOR]

Published

2007

45. Effects of newcastle disease virus glycoproteins on the structural and thermal behaviour of 1,2-dihexadecyl-sn-glycero-3-phosphatidylcholine lipid membranes under osmotic stress conditions

Author

Pravchanska, Rita, Borissova, Petrana, Doumanova, Lyubka, Neitchev, Vassil, and Laggner, Peter

Subjects

*NEWCASTLE disease virus, *GLYCOPROTEINS, *PARAMYXOVIRUSES, *BILAYER lipid membranes

Abstract

Abstract: The interaction of hem agglutininneuraminidase (HN) and fusion (F) glycoproteins with swollen vesicles of 1,2-dihexadecyl-sn-glycero-3-phosphatidylcholine (DHPC) was investigated under transition from gel to fluid phase. X-ray studies of the structure of lipid/HN-F mixtures in normal and swollen vesicles have shown that the lamellar bilayer structure predominate in the gel and liquid crystalline phases. A swollen lipid phase, in which the mean repeat distance of lipid bilayers is larger than in the other phases was found. The nature of this phase is similar to the anomalous bilayer swelling reported in literature. The presence of HN and F in the vesicles led to the coexistence of structures with low and high lamellar order, showing larger repeat distance in comparison with the pure lipid. This finding was attributed to the increase in the lipid bilayer thickness due to the HN-F included in the free water layer. The thermal behaviour of the system was not affected by the vesicle swelling. The data showed the existence of gel and liquid crystalline lamellar phases and changes in lipid/HN-F specific heats, mainly due to the concentration effect of the HN-F and its location in the free water layer. [Copyright &y& Elsevier]

Published

2006

46. Immunotherapeutic activity of a recombinant combined gB–gD–gE vaccine against recurrent HSV-2 infections in a guinea pig model

Author

Manservigi, Roberto, Boero, Anna, Argnani, Rafaela, Caselli, Elisabetta, Zucchini, Silvia, Miriagou, Vivì, Mavromara, Penelope, Cilli, Michele, Grossi, Maria Pia, Balboni, Pier Giorgio, and Cassai, Enzo

Subjects

*HERPESVIRUS diseases, *HERPES simplex virus, *GUINEA pigs, *HERPES genitalis

Abstract

Abstract: The guinea pig model of recurrent genital herpes simplex virus type 2 (HSV-2) infection was used to test the immunotherapeutic activity of a glycoprotein subunit vaccine. Vaccine formulation consisted of three recombinant herpes simplex virus (HSV) glycoproteins, namely gB1s, gD2t and gE1t, plus aluminium hydroxide [Al(OH)3)] adjuvant. One month after viral challenge, infected animals were therapeutically immunised by seven subcutaneous injections of a low dose of antigens with a weekly interval for the first five and a fortnightly interval for the last two administrations. Results showed that the treatment was highly effective in ameliorating the recidivist pathology of animals, suggesting that this kind of vaccine formulation and administration may be helpful for therapeutic intervention in humans affected by recurrent herpes infections. [Copyright &y& Elsevier]

Published

2005

47. The two envelope membrane glycoproteins of Tomato spotted wilt virus show differences in lectin-binding properties and sensitivities to glycosidases

Author

Naidu, Rayapati A., Ingle, Caroline J., Deom, Carl M., and Sherwood, John L.

Subjects

*GLYCOPROTEINS, *LECTINS, *BUNYAVIRUSES, *OLIGOSACCHARIDES

Abstract

Tomato spotted wilt virus (TSWV, Genus: Tospovirus, Family: Bunyaviridae) is a major constraint to the production of several different crops of agronomic and horticultural importance worldwide. The amino acid sequence of the two envelope membrane glycoproteins, designated as GN (N-terminal) and GC (C-terminal), of TSWV contain several tripeptide sequences, Asn-Xaa-Ser/Thr, suggesting that the proteins are N-glycosylated. In this study, the lectin-binding properties of the viral glycoproteins and their sensitivities to glycosidases were examined to obtain information on the nature of potential oligosaccharide moieties present on GN and GC. The viral proteins were separated by sodium dodecyl sulphate-polyacrylamide gel electrophoresis (SDS-PAGE) and probed by affinoblotting using a battery of biotinylated lectins with specificity to different oligosaccharide structures. GC showed strong binding with five mannose-binding lectins, four N-acetyllactosamine-binding lectins and one fucose-binding lectin. GN was resolved into two molecular masses and only the slow migrating form showed binding, albeit to a lesser extent than GC, with three of the five mannose-binding lectins. The N-acetyllactosamine- and fucose-specific lectins did not bind to either molecular mass form of GN. None of the galactose-, N-acetylgalactosamine-, or sialic acid-binding lectins tested showed binding specificity to GC or GN. Treatment of the denatured virions with endoglycosidase H and peptide:N-glycosidase F (PNGase F) resulted in a significant decrease in the binding of GC to high mannose- and N-acetyllactosamine-specific lectins. However, no such differences in lectin binding were apparent with GN. These results indicate the presence of N-linked oligosaccharides of high mannose- and complex-type on GC and possibly high mannose-type on GN. Differences in the extent of binding of the two envelope glycoproteins to different lectins suggest that GC is likely to be more heavily N-glycosylated than GN. No evidence was observed for the presence of O-linked oligosaccharides on GN or GC. [Copyright &y& Elsevier]

Published

2004

48. Individual Expression of Sindbis Virus Glycoproteins. E1 Alone Promotes Cell Fusion

Author

Sanz, Miguel Angel, Rejas, Marıa Teresa, and Carrasco, Luis

Subjects

*GLYCOPROTEINS, *CELL fusion

Abstract

The envelope of alphavirus particles contains two major glycoproteins, E1 and E2, that participate in virus entry and assembly of new virus particles. Interactions between these glycoproteins determine their correct functioning. The expression of each glycoprotein in the absence of the other counterpart was achieved by means of electroporation of modified Sindbis virus (SV) genomes. In addition, in trans coexpression of both glycoproteins was also tested in BHK cells. Synthesis of the E1 glycoprotein alone gave rise to cell fusion after incubation in low-pH medium. In addition, expression of E1 in the absence of the E2 precursor, PE2 (E3+E2), induced the formation of cytoplasmic vacuoles in the transfected cells. The normal phenotype was recovered when PE2 was coexpressed in trans with E1. Moreover, this coexpression modified the processing of the PE2 glycoprotein. PE2 synthesized in the absence of E1 gave rise to a product, E2′, whose migration was slower in SDS–polyacrylamide gel than that of genuine E2 from SV-infected cells. This alteration was corrected upon in trans coexpression of E1 and PE2. These results suggest that the two glycoproteins, E1 and PE2, interact after their expression from two separate SV genomes. Notably, BHK cells cotransfected with the two modified genomes produced SV particles. Our findings suggest that SV E1 and E2 synthesized in trans can interact with each other and participate together with capsid protein in the assembly of new virus particles. [Copyright &y& Elsevier]

Published

2003

49. Folding of viral glycoproteins in the endoplasmic reticulum

Author

Molinari, Maurizio

Subjects

*GLYCOPROTEINS, *ENDOPLASMIC reticulum, *PROTEIN folding

Abstract

The endoplasmic reticulum (ER) is a subcellular compartment specialized in folding and assembly of newly synthesized polypeptides. The polypeptides expressed in the ER include all secretory proteins produced in the cell, lumenal or membrane-bound proteins of the endocytic/vacuolar and secretory compartments and transmembrane proteins that operate at the plasma membrane. In the lumen of the ER, molecular chaperones and folding factors facilitate the maturation of newly synthesized proteins. In a process defined as ER-quality control, they also warrant that only properly structured and assembled products leave the ER and are transported to their target organelles and compartments. If proper maturation fails, the aberrant products are degraded. Quality control in the ER is essential to prevent exit of improperly regulated or not-functional products that could lead to harmful effects. The mechanisms of protein folding and quality control in the ER are far from being fully understood. They are fundamental for the life of cells and organisms, but they are also linked to important human hereditary diseases in which mutated gene products are retained in the ER and degraded (e.g., cystic fibrosis and hereditary lung emphysema). [Copyright &y& Elsevier]

Published

2002

50. Novel Epstein-Barr virus-like particles incorporating gH/gL-EBNA1 or gB-LMP2 induce high neutralizing antibody titers and EBV-specific T-cell responses in immunized mice

Author

Elizabeth M. Perez, Joslyn Foley, Rute Silva, Timelia Tison, and Javier Gordon Ogembo

Subjects

0301 basic medicine, Epstein-Barr Virus Infections, Herpesvirus 4, Human, Immunogen, T-Lymphocytes, viruses, CHO Cells, virus-like particles, medicine.disease_cause, Viral Matrix Proteins, Mice, 03 medical and health sciences, Cricetulus, Antigen, Viral envelope, Stomach Neoplasms, Cricetinae, vaccine, hemic and lymphatic diseases, Tumor Cells, Cultured, medicine, Animals, Humans, Epstein-Barr virus, Neutralizing antibody, viral latency proteins, B cell, Immunity, Cellular, Mice, Inbred BALB C, Viral matrix protein, biology, Antibodies, Neutralizing, Virology, Epstein–Barr virus, 3. Good health, 030104 developmental biology, medicine.anatomical_structure, Epstein-Barr Virus Nuclear Antigens, Oncology, Immunology, biology.protein, Female, Immunization, Antibody, viral glycoproteins, Research Paper

Abstract

Previous Epstein-Barr virus (EBV) prophylactic vaccines based on the major surface glycoprotein gp350/220 as an immunogen have failed to block viral infection in humans, suggesting a need to target other viral envelope glycoproteins. In this study, we reasoned that incorporating gH/gL or gB, critical glycoproteins for viral fusion and entry, on the surface of a virus-like particle (VLP) would be more immunogenic than gp350/220 for generating effective neutralizing antibodies to prevent viral infection of both epithelial and B cell lines. To boost the humoral response and trigger cell-mediated immunity, EBV nuclear antigen 1 (EBNA1) and latent membrane protein 2 (LMP2), intracellular latency proteins expressed in all EBV-infected cells, were also included as critical components of the polyvalent EBV VLP. gH/gL-EBNA1 and gB-LMP2 VLPs were efficiently produced in Chinese hamster ovary cells, an FDA-approved vehicle for mass-production of biologics. Immunization with gH/gL-EBNA1 and gB-LMP2 VLPs without adjuvant generated both high neutralizing antibody titers in vitro and EBV-specific T-cell responses in BALB/c mice. These data demonstrate that EBV glycoprotein(s)-based VLPs have excellent immunogenicity, and represent a potentially safe vaccine that will be invaluable not only in preventing EBV infection, but importantly, in preventing and treating the 200,000 cases of EBV-associated cancers that occur globally every year.

Published

2016