Your search keyword '"Viral Envelope Proteins physiology"' showing total 1,261 results

1. Feline Leukemia Virus-B Envelope Together With its GlycoGag and Human Immunodeficiency Virus-1 Nef Mediate Resistance to Feline SERINC5.

Author

Cano-Ortiz L, Gu Q, de Sousa-Pereira P, Zhang Z, Chiapella C, Twizerimana AP, Lin C, Franco AC, VandeWoude S, Luedde T, Baldauf HM, and Münk C

Subjects

Animals, Cats, Glycosylation, Humans, HIV-1 physiology, Immunodeficiency Virus, Feline physiology, Leukemia Virus, Feline physiology, Membrane Proteins physiology, Viral Envelope Proteins physiology, nef Gene Products, Human Immunodeficiency Virus physiology

Abstract

Human SERINC5 (SER5) protein is a recently described restriction factor against human immunodeficiency virus-1 (HIV-1), which is antagonized by HIV-1 Nef protein. Other retroviral accessory proteins such as the glycosylated Gag (glycoGag) from the murine leukemia virus (MLV) can also antagonize SER5. In addition, some viruses escape SER5 restriction by expressing a SER5-insensitive envelope (Env) glycoprotein. Here, we studied the activity of human and feline SER5 on HIV-1 and on the two pathogenic retroviruses in cats, feline immunodeficiency virus (FIV) and feline leukemia virus (FeLV). HIV-1 in absence of Nef is restricted by SER5 from domestic cats and protected by its Nef protein. The sensitivity of feline retroviruses FIV and FeLV to human and feline SER5 is considerably different: FIV is sensitive to feline and human SER5 and lacks an obvious mechanism to counteract SER5 activity, while FeLV is relatively resistant to SER5 inhibition. We speculated that similar to MLV, FeLV-A or FeLV-B express glycoGag proteins and investigated their function against human and feline SER5 in wild type and envelope deficient virus variants. We found that the endogenous FeLV recombinant virus, FeLV-B but not wild type exogenous FeLV-A envelope mediates a strong resistance against human and feline SER5. GlycoGag has an additional but moderate role to enhance viral infectivity in the presence of SER5 that seems to be dependent on the FeLV envelope. These findings may explain, why in vivo FeLV-B has a selective advantage and causes higher FeLV levels in infected cats compared to infections of FeLV-A only., Competing Interests: Declaration of interests The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2021 Elsevier Ltd. All rights reserved.)

Published

2022

2. Zika virus baculovirus-expressed envelope protein elicited humoral and cellular immunity in immunocompetent mice.

Author

Shin M, Kim K, Lee HJ, Lee R, Jung YJ, Park J, and Hahn TW

Subjects

Animals, Male, Mice, Inbred C57BL, Mice, Baculoviridae immunology, Immunity, Cellular, Immunity, Humoral, Immunocompetence immunology, Vaccines, Synthetic, Viral Envelope Proteins immunology, Viral Envelope Proteins physiology, Viral Vaccines immunology, Zika Virus immunology, Zika Virus Infection immunology, Zika Virus Infection virology

Abstract

Zika virus (ZIKV) is a mosquito-borne virus that has a high risk of inducing Guillain-Barré syndrome and microcephaly in newborns. Because vaccination is considered the most effective strategy against ZIKV infection, we designed a recombinant vaccine utilizing the baculovirus expression system with two strains of ZIKV envelope protein (MR766, Env_M; ZBRX6, Env_Z). Animals inoculated with Env_M and Env_Z produced ZIKV-specific antibodies and secreted effector cytokines such as interferon-γ, tumor necrosis factor-α, and interleukin-12. Moreover, the progeny of immunized females had detectable maternal antibodies that protected them against two ZIKV strains (MR766 and PRVABC59) and a Dengue virus strain. We propose that the baculovirus expression system ZIKV envelope protein recombinant provides a safe and effective vaccine strategy., (© 2022. The Author(s).)

Published

2022

3. Receptors and ligands for herpes simplex viruses: Novel insights for drug targeting.

Author

Huang Y, Song Y, Li J, Lv C, Chen ZS, and Liu Z

Subjects

Drug Development, Drug Discovery methods, Humans, Membrane Glycoproteins classification, Antiviral Agents pharmacology, Herpes Simplex drug therapy, Herpes Simplex prevention & control, Herpes Simplex virology, Herpesvirus 1, Human drug effects, Herpesvirus 1, Human physiology, Ligands, Viral Envelope Proteins classification, Viral Envelope Proteins physiology, Virus Internalization drug effects

Abstract

Human herpes simplex viruses (HSVs) belong to the Herpesviridae family. At present, no vaccine or curative treatment is available for the prevention of HSV infections. Here, we review the cell surface receptors that are recognized by HSV's glycoprotein B, glycoprotein C, glycoprotein D, and the glycoprotein H - glycoprotein L complex to facilitate entry into host cells. These receptors include heparan sulfate (HS), herpesvirus entry mediator (HVEM), and nectin-1/-2, 3-O-sulfated heparan sulfate (3-OS HS)., Competing Interests: Declaration of Competing Interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2021 Elsevier Ltd. All rights reserved.)

Published

2022

4. The host range restriction of bat-associated no-known-vector flaviviruses occurs post-entry.

Author

Charles J, Tangudu CS, Nunez-Avellaneda D, Brault AC, and Blitvich BJ

Subjects

Animals, Cell Line, Chiroptera virology, Flavivirus genetics, Gene Transfer Techniques, Genes, Viral, Genes, env, Genome, Viral, Viral Envelope Proteins genetics, Viral Envelope Proteins physiology, Viral Load, Viral Plaque Assay, Virus Attachment, Virus Replication, Yellow fever virus genetics, Yellow fever virus physiology, Zika Virus genetics, Zika Virus physiology, Flavivirus physiology, Host Specificity, Virus Internalization

Abstract

Most flaviviruses are transmitted horizontally between vertebrate hosts by haematophagous arthropods. Others exhibit host ranges restricted to vertebrates or arthropods. Vertebrate-specific flaviviruses are commonly referred to as no-known-vector (NKV) flaviviruses and can be separated into bat- and rodent-associated NKV flaviviruses. Rio Bravo virus (RBV) is one of eight recognized bat-associated NKV (B-NKV) flaviviruses. Studies designed to identify the genetic determinants that condition the host range restriction of B-NKV flaviviruses have never been performed. To investigate whether the host range restriction occurs at the level of attachment or entry, chimeric flaviviruses were created by inserting the pre-membrane and envelope protein genes of RBV into the genetic backbones of yellow fever virus (YFV) and Zika virus (ZIKV), two mosquito-borne flaviviruses associated with human disease. The chimeric viruses infected both vertebrate and mosquito cells. In vertebrate cells, all viruses produced similar mean peak titres, but the chimeric viruses grew more slowly than their parental viruses during early infection. In mosquito cells, the chimeric virus of YFV and RBV grew more slowly than YFV at early post-inoculation time points, but reached a similar mean peak titre. In contrast, the chimeric virus of ZIKV and RBV produced a mean peak titre that was approximately 10-fold lower than ZIKV. The chimeric virus of YFV and RBV produced an intermediate plaque phenotype, while the chimeric virus of ZIKV and RBV produced smaller plaques than both parental viruses. To conclude, we provide evidence that the structural glycoproteins of RBV permit entry into both mosquito and vertebrate cells, indicating that the host range restriction of B-NKV flaviviruses is mediated by a post-attachment/entry event.

Published

2021

5. In vitro adaptation and characterization of attenuated hypervariable region 1 swap chimeras of hepatitis C virus.

Author

Olesen CH, Augestad EH, Troise F, Bukh J, and Prentoe J

Subjects

Cell Line, Chimera, HEK293 Cells, Hepacivirus pathogenicity, Humans, Virus Internalization, Adaptation, Physiological physiology, Hepacivirus physiology, Immune Evasion physiology, Viral Envelope Proteins physiology

Abstract

Hepatitis C virus (HCV) chronically infects 70 million people worldwide with an estimated annual disease-related mortality of 400,000. A vaccine could prevent spread of this pervasive human pathogen, but has proven difficult to develop, partly due to neutralizing antibody evasion mechanisms that are inherent features of the virus envelope glycoproteins, E1 and E2. A central actor is the E2 motif, hypervariable region 1 (HVR1), which protects several non-overlapping neutralization epitopes through an incompletely understood mechanism. Here, we show that introducing different HVR1-isolate sequences into cell-culture infectious JFH1-based H77 (genotype 1a) and J4 (genotype 1b) Core-NS2 recombinants can lead to severe viral attenuation. Culture adaptation of attenuated HVR1-swapped recombinants permitted us to identify E1/E2 substitutions at conserved positions both within and outside HVR1 that increased the infectivity of attenuated HVR1-swapped recombinants but were not adaptive for original recombinants. H77 recombinants with HVR1 from multiple other isolates consistently acquired substitutions at position 348 in E1 and position 385 in HVR1 of E2. Interestingly, HVR1-swapped J4 recombinants primarily acquired other substitutions: F291I (E1), F438V (E2), F447L/V/I (E2) and V710L (E2), indicating a different adaptation pathway. For H77 recombinants, the adaptive E1/E2 substitutions increased sensitivity to the neutralizing monoclonal antibodies AR3A and AR4A, whereas for J4 recombinants, they increased sensitivity to AR3A, while having no effect on sensitivity to AR4A. To evaluate effects of the substitutions on AR3A and AR4A binding, we performed ELISAs on extracted E1/E2 protein and performed immunoprecipitation of relevant viruses. However, extracted E1/E2 protein and immunoprecipitation of HCV particles only reproduced the neutralization phenotypes of the J4 recombinants. Finally, we found that the HVR1-swap E1/E2 substitutions decrease virus entry dependency on co-receptor SR-BI. Our study identifies E1/E2 positions that could be critical for intra-complex HVR1 interactions while emphasizing the need for developing novel tools for molecular studies of E1/E2 interactions., Competing Interests: The authors have declared that no competing interests exist.

Published

2021

6. The requirement of glycoprotein C (gC) for interindividual spread is a conserved function of gC for avian herpesviruses.

Author

Vega-Rodriguez W, Xu H, Ponnuraj N, Akbar H, Kim T, and Jarosinski KW

Subjects

Amino Acid Sequence, Animals, Herpesvirus 2, Gallid metabolism, Herpesvirus 2, Gallid physiology, Marek Disease transmission, Marek Disease virology, Sequence Homology, Amino Acid, Viral Envelope Proteins chemistry, Virus Replication, Chickens virology, Herpesvirus 2, Gallid pathogenicity, Viral Envelope Proteins physiology

Abstract

We have formerly shown that glycoprotein C (gC) of Gallid alphaherpesvirus 2, better known as Marek's disease (MD) alphaherpesvirus (MDV), is required for interindividual spread in chickens. Since gC is conserved within the Alphaherpesvirinae subfamily, we hypothesized gC was important for interindividual spread of other alphaherpesviruses. To test this hypothesis, we first generated a fluorescent protein tagged clone of Gallid alphaherpesvirus 3 MD vaccine strain 301B/1 to track virus replication in cell culture and chickens using fluorescent microscopy. Following validation of this system, we removed the open reading frame of 301B/1 gC from the genome and determined whether it was required for interindividual spread using experimental and natural infection studies. Interindividual spread of MD vaccine 301B/1 was abrogated by removal of 301B/1 gC. Rescuent virus in which 301B/1 gC was inserted back into the genome efficiently spread among chickens. To further study the conserved function of gC, we replaced 301B/1 gC with MDV gC and this virus also efficiently spread in chickens. These data suggest the essential function of alphaherpesvirus gC proteins is conserved and can be exploited during the generation of future vaccines against MD that affects the poultry industry worldwide.

Published

2021

7. Bombyx mori nucleopolyhedrovirus F-like protein Bm14 is a factor for viral-induced cytopathic effects via regulating oxidative phosphorylation and cellular ROS levels.

Author

Kong X, Xu W, Chen N, Li Y, Shen Y, and Wu X

Subjects

Animals, Cell Line, Gene Expression Profiling, Host Microbial Interactions, Mutation, RNA-Seq, Up-Regulation, Bombyx virology, Cytopathogenic Effect, Viral, Nucleopolyhedroviruses metabolism, Oxidative Phosphorylation, Reactive Oxygen Species metabolism, Viral Envelope Proteins physiology, Virus Diseases metabolism

Abstract

Bombyx mori nucleopolyhedrovirus (BmNPV) is highly pathogenic to Bombyx mori, silkworm, which causes serious cytopathic effects (CPEs) during infection. However, the role of viral protein in the virus-induced CPEs remains unclear. Here, we discovered that BmNPV infection induced severe CPEs including titer-dependent cell floating and changes in cellular surface morphology. Further explorations revealed the involvement of F-like protein (Bm14), a viral envelope protein, in inducing cytotoxicity and detachment of adherent BmN cells, and its disruption significantly impaired the virus infection-mediated CPEs. Intriguingly, transcriptomic analysis identified the tight association of Bm14 deletion with the activation of cellular oxidative phosphorylation pathway, consistent with the elevated mitochondrial membrane potential (MMP) levels and ATP concentrations as well as reduced ROS levels. Collectively, our results characterized for the first time the novel role of Bm14 in accelerating viral-induced cytopathogenicity via suppressing the cellular oxidative phosphorylation levels and upregulating the ROS levels., (Copyright © 2020 Elsevier Inc. All rights reserved.)

Published

2021

8. The crystal structure of the emerging human-infecting hepatitis E virus E2s protein.

Author

Bai C, Cai J, Han P, Qi J, Yuen KY, and Wang Q

Subjects

Antibodies, Viral, Antigens, Viral chemistry, Antigens, Viral genetics, Crystallography, X-Ray, Epitopes chemistry, Epitopes genetics, Hepatitis E immunology, Hepatitis E virology, Hepatitis E virus genetics, Hepatitis E virus physiology, Humans, Hydrophobic and Hydrophilic Interactions, Models, Molecular, Protein Conformation, Protein Structure, Quaternary, Protein Subunits, Sequence Homology, Amino Acid, Static Electricity, Viral Envelope Proteins genetics, Viral Envelope Proteins physiology, Hepatitis E virus chemistry, Viral Envelope Proteins chemistry

Abstract

Hepatitis E virus (HEV) is a non-enveloped, globular particle that is responsible for acute hepatitis. HEV is classified into the Hepeviridae family and can be divided into four species (A-D). All HEV variants that infect humans are reported to belong to species A (HEV-A), except species C (HEV-C), which was reported to infect humans in December 2018. We determined the crystal structure of the HEV-C E2s domain at 1.8 Å resolution. It contains a classical 12-stranded β-sandwich motif and forms dimers by hydrogen bonding, though the amino acid residues that form hydrogen bonds are quite different from the residues of HEV-A. The HEV-C E2s domain shares the common groove region with other structurally related viruses, and some subtle differences in this region may be related to host adoption or antibody binding. Antibody binding experiments and structural analysis revealed that HEV-C E2s is able to bind to the previously reported broad-spectrum antibody 8G12 but not bind to the antibody 8C11. Meanwhile, the structure analysis shows that HEV-C E2s does not have the key sites for binding to host cells as displayed by HEV-A (Genotype 1) E2s. These structural and biological findings present important implications for understanding the molecular mechanisms of host recognition and entry of HEV-C, as well as provide clues to the development of therapeutic antibodies and vaccines against HEV-C infection., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2020 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2020

9. MARCH8 Inhibits Ebola Virus Glycoprotein, Human Immunodeficiency Virus Type 1 Envelope Glycoprotein, and Avian Influenza Virus H5N1 Hemagglutinin Maturation.

Author

Yu C, Li S, Zhang X, Khan I, Ahmad I, Zhou Y, Li S, Shi J, Wang Y, and Zheng YH

Subjects

Animals, Cell Line, Chlorocebus aethiops, Ebolavirus physiology, Glycosylation, HEK293 Cells, HIV-1 physiology, HeLa Cells, Hep G2 Cells, Humans, Influenza A Virus, H5N1 Subtype physiology, Protein Binding, THP-1 Cells, Ubiquitin-Protein Ligases metabolism, Vero Cells, Viral Fusion Proteins antagonists & inhibitors, Viral Fusion Proteins metabolism, Ebolavirus chemistry, Glycoproteins antagonists & inhibitors, HIV-1 chemistry, Hemagglutinins, Viral metabolism, Influenza A Virus, H5N1 Subtype chemistry, Ubiquitin-Protein Ligases genetics, Viral Envelope Proteins antagonists & inhibitors, Viral Envelope Proteins physiology

Abstract

Membrane-associated RING-CH-type 8 (MARCH8) strongly blocks human immunodeficiency virus type 1 (HIV-1) envelope glycoprotein (Env) incorporation into virions by downregulating its cell surface expression, but the mechanism is still unclear. We now report that MARCH8 also blocks the Ebola virus (EBOV) glycoprotein (GP) incorporation via surface downregulation. To understand how these viral fusion proteins are downregulated, we investigated the effects of MARCH8 on EBOV GP maturation and externalization via the conventional secretion pathway. MARCH8 interacted with EBOV GP and furin when detected by immunoprecipitation and retained the GP/furin complex in the Golgi when their location was tracked by a bimolecular fluorescence complementation (BiFC) assay. MARCH8 did not reduce the GP expression or affect the GP modification by high-mannose N -glycans in the endoplasmic reticulum (ER), but it inhibited the formation of complex N -glycans on the GP in the Golgi. Additionally, the GP O -glycosylation and furin-mediated proteolytic cleavage were also inhibited. Moreover, we identified a novel furin cleavage site on EBOV GP and found that only those fully glycosylated GPs were processed by furin and incorporated into virions. Furthermore, the GP shedding and secretion were all blocked by MARCH8. MARCH8 also blocked the furin-mediated cleavage of HIV-1 Env (gp160) and the highly pathogenic avian influenza virus H5N1 hemagglutinin (HA). We conclude that MARCH8 has a very broad antiviral activity by prohibiting different viral fusion proteins from glycosylation and proteolytic cleavage in the Golgi, which inhibits their transport from the Golgi to the plasma membrane and incorporation into virions. IMPORTANCE Enveloped viruses express three classes of fusion proteins that are required for their entry into host cells via mediating virus and cell membrane fusion. Class I fusion proteins are produced from influenza viruses, retroviruses, Ebola viruses, and coronaviruses. They are first synthesized as a type I transmembrane polypeptide precursor that is subsequently glycosylated and oligomerized. Most of these precursors are cleaved en route to the plasma membrane by a cellular protease furin in the late secretory pathway, generating the trimeric N-terminal receptor-binding and C-terminal fusion subunits. Here, we show that a cellular protein, MARCH8, specifically inhibits the furin-mediated cleavage of EBOV GP, HIV-1 Env, and H5N1 HA. Further analyses uncovered that MARCH8 blocked the EBOV GP glycosylation in the Golgi and inhibited its transport from the Golgi to the plasma membrane. Thus, MARCH8 has a very broad antiviral activity by specifically inactivating different viral fusion proteins., (Copyright © 2020 Yu et al.)

Published

2020

10. Restoring Herpesvirus Entry Mediator (HVEM) Immune Function in HVEM -/- Mice Rescues Herpes Simplex Virus 1 Latency and Reactivation Independently of Binding to Glycoprotein D.

Author

Tormanen K, Wang S, Jaggi U, and Ghiasi H

Subjects

Animals, Female, Glycoproteins metabolism, Herpes Simplex virology, Herpesvirus 1, Human pathogenicity, Humans, Male, Mice, Mice, Inbred C57BL, Mice, Transgenic, Receptors, Tumor Necrosis Factor, Member 14 immunology, Viral Envelope Proteins genetics, Viral Envelope Proteins physiology, Virus Internalization, Virus Latency physiology, Herpesvirus 1, Human physiology, Receptors, Tumor Necrosis Factor, Member 14 metabolism, Viral Envelope Proteins metabolism

Abstract

The immune modulatory protein herpes virus entry mediator (HVEM) is one of several cellular receptors used by herpes simplex virus 1 (HSV-1) for cell entry. HVEM binds to HSV-1 glycoprotein D (gD) but is not necessary for HSV-1 replication in vitro or in vivo Previously, we showed that although HSV-1 replication was similar in wild-type (WT) control and HVEM -/- mice, HSV-1 does not establish latency or reactivate effectively in mice lacking HVEM, suggesting that HVEM is important for these functions. It is not known whether HVEM immunomodulatory functions contribute to latency and reactivation or whether its binding to gD is necessary. We used HVEM -/- mice to establish three transgenic mouse lines that express either human WT HVEM or human or mouse HVEM with a point mutation that ablates its ability to bind to gD. Here, we show that HVEM immune function, not its ability to bind gD, is required for WT levels of latency and reactivation. We further show that HVEM binding to gD does not affect expression of the HVEM ligands BTLA, CD160, or LIGHT. Interestingly, our results suggest that binding of HVEM to gD may contribute to efficient upregulation of CD8α but not PD1, TIM-3, CTLA4, or interleukin 2 (IL-2). Together, our results establish that HVEM immune function, not binding to gD, mediates establishment of latency and reactivation. IMPORTANCE HSV-1 is a common cause of ocular infections worldwide and a significant cause of preventable blindness. Corneal scarring and blindness are consequences of the immune response induced by repeated reactivation events. Therefore, HSV-1 therapeutic approaches should focus on preventing latency and reactivation. Our data suggest that the immune function of HVEM plays an important role in the HSV-1 latency and reactivation cycle that is independent of HVEM binding to gD., (Copyright © 2020 American Society for Microbiology.)

Published

2020

11. Human Cytomegalovirus Glycoprotein-Initiated Signaling Mediates the Aberrant Activation of Akt.

Author

Mahmud J, Miller MJ, Altman AM, and Chan GC

Subjects

Cell Line, Cells, Cultured, Cytomegalovirus pathogenicity, Cytomegalovirus physiology, Cytomegalovirus Infections metabolism, ErbB Receptors metabolism, Host-Pathogen Interactions, Humans, Macrophages metabolism, Monocytes metabolism, Phosphatidylinositol 3-Kinase metabolism, Phosphatidylinositol 3-Kinases metabolism, Signal Transduction, Transcriptional Activation, Viral Envelope Proteins physiology, Viral Fusion Proteins metabolism, Virus Internalization, Proto-Oncogene Proteins c-akt metabolism, Viral Envelope Proteins metabolism

Abstract

Human cytomegalovirus (HCMV) is a major cause of morbidity and mortality among immunocompromised and immunonaive individuals. HCMV-induced signaling initiated during viral entry stimulates a rapid noncanonical activation of Akt to drive the differentiation of short-lived monocytes into long-lived macrophages, which is essential for viral dissemination and persistence. We found that HCMV glycoproteins gB and gH directly bind and activate cellular epidermal growth factor receptor (EGFR) and integrin β1, respectively, to reshape canonical Akt signaling within monocytes. The remodeling of the Akt signaling network was due to the recruitment of nontraditional Akt activators to either the gB- or gH-generated receptor signaling complexes. Phosphoinositide 3-kinase (PI3K) comprised of the p110β catalytic subunit was recruited to the gB/EGFR complex despite p110δ being the primary PI3K isoform found within monocytes. Concomitantly, SH2 domain-containing inositol 5-phosphatase 1 (SHIP1) was recruited to the gH/integrin β1 complex, which is critical to aberrant Akt activation, as SHIP1 diverts PI3K signaling toward a noncanonical pathway. Although integrin β1 was required for SHIP1 recruitment, gB-activated EGFR mediated SHIP1 activation, underscoring the importance of the interplay between gB- and gH-mediated signaling to the unique activation of Akt during HCMV infection. Indeed, SHIP1 activation mediated the increased expression of Mcl-1 and HSP27, two Akt-dependent antiapoptotic proteins specifically upregulated during HCMV infection but not during growth factor treatment. Overall, our data indicate that HCMV glycoproteins gB and gH work in concert to initiate an HCMV-specific signalosome responsible for the atypical activation of Akt required for infected monocyte survival and ultimately viral persistence. IMPORTANCE Human cytomegalovirus (HCMV) infection is endemic throughout the world regardless of socioeconomic conditions and geographic locations with a seroprevalence reaching up to 100% in some developing countries. Although asymptomatic in healthy individuals, HCMV can cause severe multiorgan disease in immunocompromised or immunonaive patients. HCMV disease is a direct consequence of monocyte-mediated systematic spread of the virus following infection. Because monocytes are short-lived cells, HCMV must subvert the natural short life-span of these blood cells by inducing a distinct activation of Akt, a serine/theonine protein kinase. In this work, we demonstrate that HCMV glycoproteins gB and gH work in tandem to reroute classical host cellular receptor signaling to aberrantly activate Akt and drive survival of infected monocytes. Deciphering how HCMV modulates the cellular pathway to induce monocyte survival is important to develop a new class of anti-HCMV drugs that could target and prevent spread of the virus by eliminating infected monocytes., (Copyright © 2020 American Society for Microbiology.)

Published

2020

12. Herpesvirus membrane fusion - a team effort.

Author

Vollmer B and Grünewald K

Subjects

Humans, Virus Internalization, Glycoproteins physiology, Herpes Simplex virology, Herpesvirus 1, Human physiology, Viral Envelope Proteins physiology

Abstract

One of the essential steps in every viral 'life' cycle is entry into the host cell. Membrane-enveloped viruses carry dedicated proteins to catalyse the fusion of the viral and cellular membrane. Herpesviruses feature a set of essential, structurally diverse glycoproteins on the viral surface that form a multicomponent fusion machinery, necessary for the entry mechanism. For Herpes simplex virus 1, these essential glycoproteins are gD, gH, gL and gB. In this review we describe the functions of the individual components, the potential interactions between them as well as the influence of post-translational modifications on the fusion mechanism., (Copyright © 2019. Published by Elsevier Ltd.)

Published

2020

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

Author

Komala Sari T, Gianopulos KA, Weed DJ, Schneider SM, Pritchard SM, and Nicola AV

Subjects

Animals, Chlorocebus aethiops, Humans, Protein Domains, Vero Cells, Viral Envelope Proteins physiology, Herpes Simplex virology, Herpesvirus 1, Human physiology, Hydrogen-Ion Concentration, Viral Envelope Proteins chemistry, Virus Internalization

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., (Copyright © 2020 Komala Sari et al.)

Published

2020

14. [Extracellular maturation of hepatitis C virus: a plasma cloak of invisibility].

Author

Chanut M, Granier C, Cosset FL, and Denolly S

Subjects

Antibodies, Neutralizing metabolism, Hepacivirus genetics, Hepacivirus immunology, Hepacivirus ultrastructure, Hepatitis C blood, Hepatitis C immunology, Hepatitis C virology, Hepatitis C Antibodies metabolism, Hepatitis C Antigens metabolism, Host-Pathogen Interactions, Humans, Surface Properties, Viral Envelope Proteins genetics, Viral Envelope Proteins physiology, Viremia blood, Viremia immunology, Viremia virology, Virion physiology, Virion ultrastructure, Antibodies, Neutralizing immunology, Hepacivirus physiology, Hepatitis C Antibodies immunology, Hepatitis C Antigens immunology, Lipoproteins blood, Viral Envelope Proteins immunology

Published

2019

15. Nipah and Hendra Virus Glycoproteins Induce Comparable Homologous but Distinct Heterologous Fusion Phenotypes.

Author

Bradel-Tretheway BG, Zamora JLR, Stone JA, Liu Q, Li J, and Aguilar HC

Subjects

Giant Cells metabolism, Glycoproteins genetics, HEK293 Cells, Hendra Virus genetics, Humans, Membrane Fusion, Nipah Virus genetics, Viral Envelope Proteins genetics, Viral Envelope Proteins physiology, Viral Fusion Proteins genetics, Virus Attachment, Virus Internalization, Glycoproteins metabolism, Hendra Virus physiology, Henipavirus Infections virology, Nipah Virus physiology, Phenotype, Viral Fusion Proteins physiology

Abstract

Nipah and Hendra viruses (NiV and HeV) exhibit high lethality in humans and are biosafety level 4 (BSL-4) paramyxoviruses in the growing genus Henipavirus The attachment (G) and fusion (F) envelope glycoproteins are both required for viral entry into cells and for cell-cell fusion, which is pathognomonic of henipaviral infections. Here, we compared the fusogenic capacities between homologous and heterologous pairs of NiV and HeV glycoproteins. Importantly, to accurately measure their fusogenic capacities, as these depend on glycoprotein cell surface expression (CSE) levels, we inserted identical extracellular tags to both fusion (FLAG tags) or both attachment (hemagglutinin [HA] tags) glycoproteins. Importantly, these tags were placed in extracellular sites where they did not affect glycoprotein expression or function. NiV and HeV glycoproteins induced comparable levels of homologous HEK293T cell-cell fusion. Surprisingly, however, while the heterologous NiV F/HeV G (NF/HG) combination yielded a hypofusogenic phenotype, the heterologous HeV F/NiV G (HF/NG) combination yielded a hyperfusogenic phenotype. Pseudotyped viral entry levels primarily corroborated the fusogenic phenotypes of the glycoprotein pairs analyzed. Furthermore, we constructed G and F chimeras that allowed us to map the overall regions in G and F that contributed to these hyperfusogenic or hypofusogenic phenotypes. Importantly, the fusogenic phenotypes of the glycoprotein combinations negatively correlated with the avidities of F-G interactions, supporting the F/G dissociation model of henipavirus-induced membrane fusion, even in the context of heterologous glycoprotein pairs. IMPORTANCE The NiV and HeV henipaviruses are BSL-4 pathogens transmitted from bats. NiV and HeV often lead to human death and animal diseases. The formation of multinucleated cells (syncytia) is a hallmark of henipaviral infections and is caused by fusion of cells coordinated by interactions of the viral attachment (G) and fusion (F) glycoproteins. We found via various assays that viral entry and syncytium formation depend on the viral origin of the glycoproteins, with HeV F and NiV G promoting higher membrane fusion levels than their counterparts. This is important knowledge, since both viruses use the same bat vector species and potential coinfections of these or subsequent hosts may alter the outcome of disease., (Copyright © 2019 American Society for Microbiology.)

Published

2019

16. Interferon Gamma Inhibits Varicella-Zoster Virus Replication in a Cell Line-Dependent Manner.

Author

Shakya AK, O'Callaghan DJ, and Kim SK

Subjects

A549 Cells, Antiviral Agents metabolism, Cell Line, Humans, Immediate-Early Proteins genetics, Immediate-Early Proteins metabolism, Immediate-Early Proteins physiology, Interferon-beta genetics, Interferon-gamma pharmacology, Janus Kinase 1 metabolism, Open Reading Frames, Protein Binding, STAT Transcription Factors metabolism, Signal Transduction, Trans-Activators metabolism, Trans-Activators physiology, Viral Envelope Proteins genetics, Viral Envelope Proteins metabolism, Viral Envelope Proteins physiology, Herpesvirus 3, Human metabolism, Interferon-gamma metabolism, Virus Replication drug effects

Abstract

The major immediate early 62 (IE62) protein of varicella-zoster virus (VZV) is delivered to newly infected cell nuclei, where it initiates VZV replication by transactivating viral immediate early (IE), early (E), and late (L) genes. Interferon gamma (IFN-γ) is a potent cytokine produced following primary VZV infection. Furthermore, VZV reactivation correlates with a decline in IFN-γ-producing immune cells. Our results showed that treatment with 20 ng/ml of IFN-γ completely reduced intracellular VZV yield in A549 lung epithelial cells, MRC-5 lung fibroblasts, and ARPE-19 retinal epithelial cells at 4 days post-VZV infection. However, IFN-γ reduced virus yield only 2-fold in MeWo melanoma cells compared to that of untreated cells. IFN-β significantly inhibited VZV replication in both ARPE-19 and MeWo cells. In luciferase assays with VZV open reading frame 61 (ORF61) promoter reporter plasmid, IFN-γ abrogated the transactivation activity of IE62 by 95%, 97%, and 89% in A549, ARPE-19, and MRC-5 cells, respectively. However, IFN-γ abrogated IE62's transactivation activity by 16% in MeWo cells, indicating that IFN-γ inhibits VZV replication as well as IE62-mediated transactivation in a cell line-dependent manner. The expression of VZV IE62 and ORF63 suppressed by IFN-γ was restored by JAK1 inhibitor treatment, indicating that the inhibition of VZV replication is mediated by JAK/STAT1 signaling. In the presence of IFN-γ, knockdown of interferon response factor 1 (IRF1) increased VZV replication. Ectopic expression of IRF1 reduced VZV yields 4,000-fold in MRC-5 and ARPE-19 cells but 3-fold in MeWo cells. These results suggest that IFN-γ blocks VZV replication by inhibiting IE62 function in a cell line-dependent manner. IMPORTANCE Our results showed that IFN-γ significantly inhibited VZV replication in a cell line-dependent manner. IFN-γ inhibited VZV gene expression after the immediate early stage of infection and abrogated IE62-mediated transactivation. These results suggest that IFN-γ blocks VZV replication by inhibiting IE62 function in a cell line-dependent manner. Understanding the mechanisms by which IFN-γ plays a role in VZV gene programming may be important in determining the tissue restriction of VZV., (Copyright © 2019 American Society for Microbiology.)

Published

2019

17. The Infectious Bronchitis Coronavirus Envelope Protein Alters Golgi pH To Protect the Spike Protein and Promote the Release of Infectious Virus.

Author

Westerbeck JW and Machamer CE

Subjects

Animals, Bronchitis immunology, Bronchitis virology, Cell Membrane metabolism, Chlorocebus aethiops, Coronavirus pathogenicity, Coronavirus Envelope Proteins, Coronavirus Infections virology, Golgi Apparatus physiology, HeLa Cells, Humans, Hydrogen-Ion Concentration, Infectious bronchitis virus immunology, Secretory Pathway, Vero Cells, Viral Envelope Proteins physiology, Virion metabolism, Virus Assembly, Virus Diseases metabolism, Coronavirus metabolism, Spike Glycoprotein, Coronavirus metabolism, Viral Envelope Proteins metabolism

Abstract

Coronaviruses (CoVs) assemble by budding into the lumen of the early Golgi complex prior to exocytosis. The small CoV envelope (E) protein plays roles in assembly, virion release, and pathogenesis. CoV E has a single hydrophobic domain (HD), is targeted to Golgi membranes, and has cation channel activity in vitro The E protein from avian infectious bronchitis virus (IBV) has dramatic effects on the secretory system, which require residues in the HD. Mutation of the HD of IBV E in a recombinant virus background results in impaired growth kinetics, impaired release of infectious virions, accumulation of IBV spike (S) protein on the plasma membrane compared to wild-type (WT) IBV-infected cells, and aberrant cleavage of IBV S on virions. We previously reported the formation of two distinct oligomeric pools of IBV E in transfected and infected cells. Disruption of the secretory pathway by IBV E correlates with a form that is likely monomeric, suggesting that the effects on the secretory pathway are independent of E ion channel activity. Here, we present evidence suggesting that the monomeric form of IBV E correlates with an increased Golgi luminal pH. Infection with IBV or expression of IBV E induces neutralization of Golgi pH, promoting a model in which IBV E alters the secretory pathway through interaction with host cell factors, protecting IBV S from premature cleavage and leading to the efficient release of infectious virus from the cells. This is the first demonstration of a coronavirus-induced alteration in the microenvironment of the secretory pathway. IMPORTANCE Coronaviruses are important human pathogens with significant zoonotic potential. Progress has been made toward identifying potential vaccine candidates for highly pathogenic human CoVs, including the use of attenuated viruses that lack the CoV E protein or express E mutants. However, no approved vaccines or antiviral therapeutics exist. Understanding the role of the CoV E protein in virus assembly and release is thus an important prerequisite for potential vaccines as well as in identifying novel antiviral therapeutics., (Copyright © 2019 American Society for Microbiology.)

Published

2019

18. The N Terminus of Human Cytomegalovirus Glycoprotein O Is Important for Binding to the Cellular Receptor PDGFRα.

Author

Stegmann C, Rothemund F, Laib Sampaio K, Adler B, and Sinzger C

Subjects

Alanine, Cell Line, Cells, Cultured, Cytomegalovirus metabolism, Cytomegalovirus Infections immunology, Cytomegalovirus Infections metabolism, Cytomegalovirus Infections virology, Endocytosis, Endothelial Cells virology, Epithelial Cells virology, Fibroblasts virology, Humans, Membrane Glycoproteins genetics, Membrane Glycoproteins physiology, Mutation, Viral Envelope Proteins genetics, Viral Envelope Proteins physiology, Virion metabolism, Virus Internalization, Membrane Glycoproteins metabolism, Receptor, Platelet-Derived Growth Factor alpha metabolism, Viral Envelope Proteins metabolism, Virus Replication genetics

Abstract

The human cytomegalovirus (HCMV) glycoprotein complex gH/gL/gO is required for the infection of cells by cell-free virions. It was recently shown that entry into fibroblasts depends on the interaction of gO with the platelet-derived growth factor receptor alpha (PDGFRα). This interaction can be blocked with soluble PDGFRα-Fc, which binds to HCMV virions and inhibits entry. The aim of this study was to identify parts of gO that contribute to PDGFRα binding. In a systematic mutational approach, we targeted potential interaction sites by exchanging conserved clusters of charged amino acids of gO with alanines. To screen for impaired interaction with PDGFRα, virus mutants were tested for sensitivity to inhibition by soluble PDGFRα-Fc. Two mutants with mutations within the N terminus of gO (amino acids 56 to 61 and 117 to 121) were partially resistant to neutralization. To validate whether these mutations impair interaction with PDGFRα-Fc, we compared binding of PDGFRα-Fc to mutant and wild-type virions via quantitative immunofluorescence analysis. PDGFRα-Fc staining intensities were reduced by 30% to 60% with mutant virus particles compared to wild-type particles. In concordance with the reduced binding to the soluble receptor, virus penetration into fibroblasts, which relies on binding to the cellular PDGFRα, was also reduced. In contrast, PDGFRα-independent penetration into endothelial cells was unaltered, demonstrating that the phenotypes of the gO mutant viruses were specific for the interaction with PDGFRα. In conclusion, the mutational screening of gO revealed that the N terminus of gO contributes to efficient spread in fibroblasts by promoting the interaction of virions with its cellular receptor. IMPORTANCE The human cytomegalovirus is a highly prevalent pathogen that can cause severe disease in immunocompromised hosts. Currently used drugs successfully target the viral replication within the host cell, but their use is restricted due to side effects and the development of resistance. An alternative approach is the inhibition of virus entry, for which understanding the details of the initial virus-cell interaction is desirable. As binding of the viral gH/gL/gO complex to the cellular PDGFRα drives infection of fibroblasts, this is a potential target for inhibition of infection. Our mutational mapping approach suggests the N terminus as the receptor binding portion of the protein. The respective mutants were partially resistant to inhibition by PDGFRα-Fc but also attenuated for infection of fibroblasts, indicating that such mutations have little if any benefit for the virus. These findings highlight the potential of targeting the interaction of gH/gL/gO with PDGFRα for therapeutic inhibition of HCMV., (Copyright © 2019 American Society for Microbiology.)

Published

2019

19. Hepatitis C Virus E2 Envelope Glycoprotein Induces an Immunoregulatory Phenotype in Macrophages.

Author

Kwon YC, Meyer K, Peng G, Chatterjee S, Hoft DF, and Ray R

Subjects

Antigens, CD metabolism, Antigens, Differentiation, Myelomonocytic metabolism, Complement C3 metabolism, Dendritic Cells metabolism, ErbB Receptors metabolism, Humans, Interleukin-10 metabolism, Phenotype, Proto-Oncogene Proteins c-akt metabolism, Receptors, Cell Surface metabolism, Tetraspanin 28 metabolism, Host-Pathogen Interactions immunology, Macrophages metabolism, Viral Envelope Proteins physiology

Abstract

A comprehensive strategy to control hepatitis C virus (HCV) infection needs a vaccine. Our phase I study with recombinant HCV E1/E2 envelope glycoprotein (EnvGPs) as a candidate vaccine did not induce a strong immune response in volunteers. We analyzed the interactions of HCV EnvGPs with human monocyte-derived macrophages as antigen-presenting cells. HCV E2 induced immune regulatory cytokine interleukin (IL)-10 and soluble CD163 (sCD163) protein expression in macrophages from 7 of 9 blood donors tested. Furthermore, HCV E2 enhanced Stat3 and suppressed Stat1 activation, reflecting macrophage polarization toward M2 phenotype. E2-associated macrophage polarization appeared to be dependent of its interaction with CD81 leading endothelial growth factor receptor (EGFR) activation. Additionally, E2 suppressed the expression of C3 complement, similar to HCV-exposed dendritic cells (DCs), implying potential impairment of immune cell priming. Conclusion: Our results suggest that E2 EnvGP may not be an ideal candidate for HCV vaccine development, and discrete domains within E2 may prove to be more capable of elliciting a protective immune response. (Hepatology 2018)., (© 2018 by the American Association for the Study of Liver Diseases.)

Published

2019

20. Role of heparan sulfate in entry and exit of Ross River virus glycoprotein-pseudotyped retroviral vectors.

Author

Kesari AS, Sharkey CM, and Sanders DA

Subjects

Animals, Cell Line, Cricetinae, Mice, Mutation, Protein Binding, Virus Internalization, Heparitin Sulfate physiology, Moloney murine leukemia virus physiology, Ross River virus physiology, Viral Envelope Proteins physiology, Virus Release physiology

Abstract

Variants of Ross River virus (RRV) that bind to heparan sulfate (HS) were previously selected by serial passaging in cell culture. To explore the effects of mutations that convey HS utilization, we pseudotyped Moloney murine leukemia virus (MoMLV), with the RRV envelope. We substituted amino-acid residues 216 and 218 on RRV-E2-envelope glycoprotein with basic amino-acid residues, because these mutations confer affinity for HS upon RRV. However, T216R-RRV- and N218R-RRV-pseudotyped viruses possessed lower transduction titers, and we demonstrated that HS-affinity impeded release of pseudotyped virus from producer cells. Addition of heparinase to HS-expressing target cells reduces the transduction efficiency of the T216R-RRV- and N218R-RRV-pseudotyped viruses, whereas no such effect is seen in cells lacking HS. Under appropriate conditions, these T216R-RRV- and N218R-RRV-pseudotyped viruses have enhanced capacities for transducing HS-expressing cells. General principles concerning viral adaptation to the use of attachment factors and design of pseudotyped viral vectors are discussed., (Copyright © 2019 Elsevier Inc. All rights reserved.)

Published

2019

21. Overexpression of the Interferon-Inducible Isoform 4 of NCOA7 Dissects the Entry Route of Enveloped Viruses and Demonstrates that HIV Enters Cells via Fusion at the Plasma Membrane.

Author

Herold N

Subjects

Cell Membrane virology, Humans, Protein Isoforms, Viral Envelope Proteins physiology, Endocytosis, HIV-1 physiology, Nuclear Receptor Coactivators genetics, Virus Internalization

Abstract

The HIV-1 entry-route is a matter of ongoing controversy, and there is evidence for fusion either at the cell surface or from within endosomes. A recent report demonstrated that isoform 4 of nuclear receptor coactivator 7 (NCOA7 iso4 ) interacts with endolysosomal vacuolar-type H⁺-ATPase (V-ATPase), increasing lytic activity and thereby severely affecting the entry of vesicular stomatitis virus glycoprotein (VSV-G)-mediated, but not HIV-Env-mediated, entry and infection. As basal expression of NCOA7 iso4 is low in the absence of type-1 interferons, its overexpression is a novel tool to study viral entry.

Published

2019

22. Critical role for cholesterol in Lassa fever virus entry identified by a novel small molecule inhibitor targeting the viral receptor LAMP1.

Author

Wang MK, Ren T, Liu H, Lim SY, Lee K, Honko A, Zhou H, Dyall J, Hensley L, Gartin AK, and Cunningham JM

Subjects

Adamantane analogs & derivatives, Adamantane chemistry, Adamantane pharmacology, Animals, Antiviral Agents chemistry, Antiviral Agents pharmacology, Cell Line, Chlorocebus aethiops, HEK293 Cells, Host-Pathogen Interactions genetics, Host-Pathogen Interactions physiology, Humans, Lassa Fever etiology, Lassa virus drug effects, Lysosomal Membrane Proteins antagonists & inhibitors, Lysosomal Membrane Proteins genetics, Models, Molecular, Mutation, Protein Stability, Protein Structure, Tertiary, Receptors, Virus antagonists & inhibitors, Receptors, Virus genetics, Vero Cells, Viral Envelope Proteins chemistry, Viral Envelope Proteins genetics, Viral Envelope Proteins physiology, Virus Internalization drug effects, Cholesterol metabolism, Lassa virus pathogenicity, Lassa virus physiology, Lysosomal Membrane Proteins physiology, Receptors, Virus physiology

Abstract

Lassa fever virus (LASV) is endemic in West Africa and causes severe hemorrhagic fever and sensorineural hearing loss. We identified a small molecule inhibitor of LASV and used it to analyze the mechanism of entry. Using a photo-reactive analog that retains antiviral activity as a probe, we identified the inhibitor target as lysosome-associated membrane protein 1 (LAMP1), a host factor that binds to the LASV glycoprotein (GP) during infection. We found that LAMP1 binding to LASV GP is cholesterol-dependent, and that the inhibitor blocks infection by competing with cholesterol in LAMP1. Mutational analysis of a docking-based model identified a putative inhibitor binding site in the cholesterol-binding pocket within the LAMP1 domain that binds GP. These findings identify a critical role for cholesterol in LASV entry and a potential target for therapeutic intervention., Competing Interests: Authors Tao Ren, Kyungae Lee and James Cunningham hold patent 9676763, June 13, 2017, "Methods of Treating Ebola" that discloses the structure and function of compound 3.3.

Published

2018

23. Structural basis of antiviral activity of peptides from MPER of FIV gp36.

Author

Grimaldi M, Stillitano I, Amodio G, Santoro A, Buonocore M, Moltedo O, Remondelli P, and D'Ursi AM

Subjects

Amino Acid Sequence, Animals, Cats, Circular Dichroism, Disease Models, Animal, Feline Acquired Immunodeficiency Syndrome virology, Glycoproteins genetics, HIV Infections virology, Humans, Immunodeficiency Virus, Feline genetics, Immunodeficiency Virus, Feline pathogenicity, Nuclear Magnetic Resonance, Biomolecular, Peptide Fragments chemistry, Peptide Fragments pharmacology, Protein Conformation, Viral Envelope Proteins genetics, Virus Internalization drug effects, Antiviral Agents chemistry, Antiviral Agents pharmacology, Glycoproteins chemistry, Glycoproteins physiology, Immunodeficiency Virus, Feline physiology, Viral Envelope Proteins chemistry, Viral Envelope Proteins physiology

Abstract

Feline immunodeficiency virus (FIV) is a naturally occurring Lentivirus causing acquired immunodeficiency syndrome in felines. It is considered a useful non-primate model to study HIV infection, and to test anti-HIV vaccine. Similarly to HIV, FIV enters cells via a mechanism involving a surface glycoprotein named gp36. C8 is a short synthetic peptide corresponding to the residues 770WEDWVGWI777 of gp36 membrane proximal external region (MPER). It elicits antiviral activity by inhibiting the fusion of the FIV and host cell membrane. C8 is endowed with evident membrane binding property, inducing alteration of the phospholipid bilayer and membrane fusion. The presence and the position of tryptophan residues in C8 are important for antiviral activity: the C8 derivative C6a, obtained by truncating the N-terminal 770WE771 residues, exhibits conserved antiviral activity, while the C8 derivative C6b, derived from the truncation of the C-terminal 776WI777, is nearly inactive. To elucidate the structural factors that induce the different activity profiles of C6a and C6b, in spite of their similarity, we investigated the structural behaviour of the two peptides in membrane mimicking environments. Conformational data on the short peptides C6a and C6b, matched to those of their parent peptide C8, allow describing a pharmacophore model of antiviral fusion inhibitors. This includes the essential structural motifs to design new simplified molecules overcoming the pharmacokinetic and high cost limitations affecting the antiviral entry inhibitors that currently are in therapy., Competing Interests: The authors have declared that no competing interests exist.

Published

2018

24. Zika Virus Envelope Protein induces G2/M Cell Cycle Arrest and Apoptosis via an Intrinsic Cell Death Signaling Pathway in Neuroendocrine PC12 Cells.

Author

Liu J, Li Q, Li X, Qiu Z, Li A, Liang W, Chen H, Cai X, Chen X, Duan X, Li J, Wu W, Xu M, Mao Y, Chen H, Li J, Gu W, and Li H

Subjects

Animals, Apoptosis physiology, Caspase 3 genetics, Caspase 3 metabolism, Caspase 9 genetics, Caspase 9 metabolism, Cell Cycle Checkpoints physiology, Cyclin-Dependent Kinase Inhibitor p21 genetics, Cyclin-Dependent Kinase Inhibitor p21 metabolism, Genetic Vectors genetics, Lentivirus genetics, PC12 Cells, Proto-Oncogene Proteins c-bcl-2 genetics, Proto-Oncogene Proteins c-bcl-2 metabolism, Rats, Signal Transduction genetics, Signal Transduction physiology, Tumor Suppressor Protein p53 genetics, Tumor Suppressor Protein p53 metabolism, Viral Envelope Proteins genetics, bcl-2-Associated X Protein genetics, bcl-2-Associated X Protein metabolism, Apoptosis genetics, Cell Cycle Checkpoints genetics, Viral Envelope Proteins metabolism, Viral Envelope Proteins physiology, Zika Virus metabolism

Abstract

Clinical evidence suggests that there exists a strong correlation between Zika virus (ZIKV) infection and abnormal development of the nervous system. However, the underlying mechanisms remain to be elusive. In this study, recombinant lentiviral vectors coding for ZIKV structural proteins and truncations (prM-Env, M-Env and Env) were transduced into PC12 cells. Envelope (Env) overexpression induced significant inhibition of proliferation and triggered G2/M cell cycle arrest and apoptosis in PC12 cells. Flow cytometry and western blot analysis showed that the apoptosis was associated with up-regulation of both p53 and p21 Cip1/Waf1 and down-regulation of cyclin B1. Presence of aberrant nuclei clusters were confirmed by immunofluorescence staining analysis. The data indicate that overexpression of prM-Env, M-Env or Env led to apoptosis via an intrinsic cell death signaling pathway that is dependent on the activation of caspase-9 and caspase-3 and accompanied by an increased ratio of Bax to Bcl-2 in transduced PC12 cells. In summary, our results suggest that ZIKV Env protein causes apoptosis in PC12 cells via an intrinsic cell death signaling pathway, which may contribute to ZIKV-induced abnormal development of the nervous system., Competing Interests: Competing Interests: The authors have declared that no competing interest exists.

Published

2018

25. The E2 glycoprotein is necessary but not sufficient for the adaptation of classical swine fever virus lapinized vaccine C-strain to the rabbit.

Author

Li Y, Xie L, Zhang L, Wang X, Li C, Han Y, Hu S, Sun Y, Li S, Luo Y, Liu L, Munir M, and Qiu HJ

Subjects

Amino Acid Substitution, Animals, Cell Line, Classical Swine Fever virology, Classical Swine Fever Virus chemistry, Classical Swine Fever Virus genetics, Classical Swine Fever Virus pathogenicity, Mutation, Rabbits, Swine, Viral Envelope Proteins chemistry, Viral Envelope Proteins genetics, Viral Vaccines, Adaptation, Biological, Classical Swine Fever Virus physiology, Viral Envelope Proteins physiology

Abstract

Classical swine fever virus (CSFV) C-strain was developed through hundreds of passages of a highly virulent CSFV in rabbits. To investigate the molecular basis for the adaptation of C-strain to the rabbit (ACR), a panel of chimeric viruses with the exchange of glycoproteins E rns , E1, and/or E2 between C-strain and the highly virulent Shimen strain and a number of mutant viruses with different amino acid substitutions in E2 protein were generated and evaluated in rabbits. Our results demonstrate that Shimen-based chimeras expressing E rns -E1-E2, E rns -E2 or E1-E2 but not E rns -E1, E rns , E1, or E2 of C-strain can replicate in rabbits, indicating that E2 in combination with either E rns or E1 confers the ACR. Notably, E2 and the amino acids P108 and T109 in Domain I of E2 are critical in ACR. Collectively, our data indicate that E2 is crucial in mediating the ACR, which requires synergistic contribution of E rns or E1., (Copyright © 2018 Elsevier Inc. All rights reserved.)

Published

2018

26. Role of Rab GTPases in HSV-1 infection: Molecular understanding of viral maturation and egress.

Author

Raza S, Alvisi G, Shahin F, Husain U, Rabbani M, Yaqub T, Anjum AA, Sheikh AA, Nawaz M, and Ali MA

Subjects

Glycoproteins metabolism, Herpesvirus 1, Human pathogenicity, Humans, Protein Transport physiology, Viral Envelope Proteins physiology, Viral Proteins genetics, Virus Assembly physiology, rab1 GTP-Binding Proteins physiology, rab27 GTP-Binding Proteins physiology, rab5 GTP-Binding Proteins physiology, Herpes Simplex metabolism, Herpesvirus 1, Human physiology, Virus Physiological Phenomena, Virus Release physiology, rab GTP-Binding Proteins physiology

Abstract

Most enveloped viruses exploit complex cellular pathways for assembly and egress from the host cell, and the large DNA virus Herpes simplex virus 1 (HSV-1) makes no exception, hijacking several cellular transport pathways for its glycoprotein trafficking and maturation, as well as for viral morphogenesis and egress according to the envelopment, de-envelopment and re-envelopment model. Importantly Rab GTPases, widely distributed master regulators of intracellular membrane trafficking pathways, have recently being tightly implicated in such process. Indeed, siRNA-mediated genetic ablation of specific Rab proteins differently affected HSV-1 production, suggesting a complex role of different Rab proteins in HSV-1 life cycle. In this review, we discuss how different Rabs can regulate HSV-1 assembly/egress and the potential therapeutic applications of such findings for the management of HSV-1 infections., (Copyright © 2018 Elsevier Ltd. All rights reserved.)

Published

2018

27. Fusogenic properties of the Ectodomain of HCV E2 envelope protein.

Author

Rodríguez-Rodríguez M, Tello D, Gómez-Gutiérrez J, Peterson DL, Gavilanes F, and Yélamos B

Subjects

Cholesterol chemistry, Endocytosis, Genes, env, Hydrogen-Ion Concentration, Liposomes, Membrane Lipids chemistry, Membrane Lipids metabolism, Peptide Fragments chemistry, Peptide Fragments genetics, Peptide Fragments physiology, Phospholipids metabolism, Protein Domains, Recombinant Proteins metabolism, Spectrometry, Fluorescence, Temperature, Viral Envelope Proteins genetics, Viral Envelope Proteins physiology, Hepacivirus physiology, Viral Envelope Proteins chemistry, Virus Internalization

Abstract

The steps leading from hepatitis C virus (HCV) attachment to the hepatocytes to the fusion of viral and cellular membranes remain uncharacterized. In this regard, we have studied the mechanism underlying the HCV fusion process using liposomes and a truncated form of E2 protein lacking the transmembrane region, E2 661 (amino acids 384-661). E2 661 has been previously obtained by using the baculovirus expression system and shown to behave as an independent folding domain (M. Rodriguez-Rodriguez, D. Tello, B. Yelamos, J. Gomez-Gutierrez, B. Pacheco, S. Ortega, A.G. Serrano, D.L. Peterson, F. Gavilanes, Structural properties of the ectodomain of hepatitis C virus E2 envelope protein, Virus Res. 139 (2009) 91-99). This form has been used in lipid-protein interaction studies with different model vesicles, at different pHs and by employing a variety of fluorescent assays. The obtained results indicate that E2 661 induces vesicle aggregation, lipid mixing and liposome leakage, reaching higher values in the presence of negatively charged phospholipids and cholesterol at acidic pH. Therefore, the results of these studies would be indicative of an HCV infection process through receptor mediated endocytosis. Accordingly, E2 might be important in the HCV initial infective steps, interacting with the target membranes and giving rise to their subsequent destabilization., (Copyright © 2017 Elsevier B.V. All rights reserved.)

Published

2018

28. Pseudotyped baculovirus is an effective gene expression tool for studying molecular function during axolotl limb regeneration.

Author

Oliveira CR, Lemaitre R, Murawala P, Tazaki A, Drechsel DN, and Tanaka EM

Subjects

Ambystoma mexicanum genetics, Amputation, Surgical, Animals, Gene Expression Profiling, Genes, Reporter, Genes, Synthetic, Hedgehog Proteins genetics, Hedgehog Proteins physiology, Homeodomain Proteins physiology, Humans, Membrane Glycoproteins physiology, Mesoderm cytology, Recombinant Proteins metabolism, Regeneration genetics, Transgenes, Viral Envelope Proteins physiology, Wound Healing genetics, Wound Healing physiology, Ambystoma mexicanum physiology, Forelimb physiology, Gene Expression Regulation, Genetic Vectors genetics, Nucleopolyhedroviruses genetics, Regeneration physiology, Transduction, Genetic

Abstract

Axolotls can regenerate complex structures through recruitment and remodeling of cells within mature tissues. Accessing the underlying mechanisms at a molecular resolution is crucial to understand how injury triggers regeneration and how it proceeds. However, gene transformation in adult tissues can be challenging. Here we characterize the use of pseudotyped baculovirus (BV) as an effective gene transfer method both for cells within mature limb tissue and within the blastema. These cells remain competent to participate in regeneration after transduction. We further characterize the effectiveness of BV for gene overexpression studies by overexpressing Shh in the blastema, which yields a high penetrance of classic polydactyly phenotypes. Overall, our work establishes BV as a powerful tool to access gene function in axolotl limb regeneration., (Copyright © 2017 Elsevier Inc. All rights reserved.)

Published

2018

29. The amino-terminus of the hepatitis C virus (HCV) p7 viroporin and its cleavage from glycoprotein E2-p7 precursor determine specific infectivity and secretion levels of HCV particle types.

Author

Denolly S, Mialon C, Bourlet T, Amirache F, Penin F, Lindenbach B, Boson B, and Cosset FL

Subjects

Amino Acid Sequence, Cell Line, HEK293 Cells, Hepacivirus genetics, Hepatitis C etiology, Hepatitis C virology, Host-Pathogen Interactions genetics, Host-Pathogen Interactions physiology, Humans, Models, Biological, Mutation, Protein Processing, Post-Translational, Viral Envelope Proteins chemistry, Viral Envelope Proteins genetics, Viral Nonstructural Proteins physiology, Viral Proteins chemistry, Viral Proteins genetics, Virulence genetics, Virulence physiology, Virus Assembly genetics, Virus Assembly physiology, Hepacivirus pathogenicity, Hepacivirus physiology, Viral Envelope Proteins physiology, Viral Proteins physiology

Abstract

Viroporins are small transmembrane proteins with ion channel activities modulating properties of intracellular membranes that have diverse proviral functions. Hepatitis C virus (HCV) encodes a viroporin, p7, acting during assembly, envelopment and secretion of viral particles (VP). HCV p7 is released from the viral polyprotein through cleavage at E2-p7 and p7-NS2 junctions by signal peptidase, but also exists as an E2p7 precursor, of poorly defined properties. Here, we found that ectopic p7 expression in HCVcc-infected cells reduced secretion of particle-associated E2 glycoproteins. Using biochemical assays, we show that p7 dose-dependently slows down the ER-to-Golgi traffic, leading to intracellular retention of E2, which suggested that timely E2p7 cleavage and p7 liberation are critical events to control E2 levels. By studying HCV mutants with accelerated E2p7 processing, we demonstrate that E2p7 cleavage controls E2 intracellular expression and secretion levels of nucleocapsid-free subviral particles and infectious virions. In addition, our imaging data reveal that, following p7 liberation, the amino-terminus of p7 is exposed towards the cytosol and coordinates the encounter between NS5A and NS2-based assembly sites loaded with E1E2 glycoproteins, which subsequently leads to nucleocapsid envelopment. We identify punctual mutants at p7 membrane interface that, by abrogating NS2/NS5A interaction, are defective for transmission of infectivity owing to decreased secretion of core and RNA and to increased secretion of non/partially-enveloped particles. Altogether, our results indicate that the retarded E2p7 precursor cleavage is essential to regulate the intracellular and secreted levels of E2 through p7-mediated modulation of the cell secretory pathway and to unmask critical novel assembly functions located at p7 amino-terminus.

Published

2017

30. An ancestral retroviral protein identified as a therapeutic target in type-1 diabetes.

Author

Levet S, Medina J, Joanou J, Demolder A, Queruel N, Réant K, Normand M, Seffals M, Dimier J, Germi R, Piofczyk T, Portoukalian J, Touraine JL, and Perron H

Subjects

Animals, Antiviral Agents therapeutic use, Cohort Studies, Diabetes Mellitus, Type 1 complications, Endogenous Retroviruses genetics, Endogenous Retroviruses pathogenicity, Female, Humans, Hyperglycemia complications, Insulin metabolism, Insulin Antagonists pharmacology, Islets of Langerhans metabolism, Male, Mice, Mice, Transgenic, RNA, Viral blood, Viral Envelope Proteins drug effects, Diabetes Mellitus, Type 1 drug therapy, Diabetes Mellitus, Type 1 virology, Endogenous Retroviruses drug effects, Viral Envelope Proteins physiology

Abstract

Human endogenous retroviruses (HERVs), remnants of ancestral viral genomic insertions, are known to represent 8% of the human genome and are associated with several pathologies. In particular, the envelope protein of HERV-W family (HERV-W-Env) has been involved in multiple sclerosis pathogenesis. Investigations to detect HERV-W-Env in a few other autoimmune diseases were negative, except in type-1 diabetes (T1D). In patients suffering from T1D, HERV-W-Env protein was detected in 70% of sera, and its corresponding RNA was detected in 57% of peripheral blood mononuclear cells. While studies on human Langerhans islets evidenced the inhibition of insulin secretion by HERV-W-Env, this endogenous protein was found to be expressed by acinar cells in 75% of human T1D pancreata. An extensive immunohistological analysis further revealed a significant correlation between HERV-W-Env expression and macrophage infiltrates in the exocrine part of human pancreata. Such findings were corroborated by in vivo studies on transgenic mice expressing HERV-W-env gene, which displayed hyperglycemia and decreased levels of insulin, along with immune cell infiltrates in their pancreas. Altogether, these results strongly suggest an involvement of HERV-W-Env in T1D pathogenesis. They also provide potentially novel therapeutic perspectives, since unveiling a pathogenic target in T1D.

Published

2017

31. Identification of two mutation sites in spike and envelope proteins mediating optimal cellular infection of porcine epidemic diarrhea virus from different pathways.

Author

Sun M, Ma J, Yu Z, Pan Z, Lu C, and Yao H

Subjects

Animals, Chlorocebus aethiops, Coronavirus Infections virology, Mutation genetics, Porcine epidemic diarrhea virus genetics, Porcine epidemic diarrhea virus physiology, Spike Glycoprotein, Coronavirus physiology, Swine, Vero Cells, Viral Envelope Proteins physiology, Coronavirus Infections veterinary, Porcine epidemic diarrhea virus pathogenicity, Spike Glycoprotein, Coronavirus genetics, Swine Diseases virology, Viral Envelope Proteins genetics

Abstract

Entry of the α-coronavirus porcine epidemic diarrhea virus (PEDV) requires specific proteases to activate spike (S) protein for the membrane fusion of the virion to the host cell following receptor binding. Herein, PEDV isolate 85-7 could proliferate and induce cell-cell fusion in a trypsin independent manner on Vero cells, and eight homologous mutation strains were screened by continuous proliferation in the absence of trypsin on Vero cells. According to the whole genome sequence comparative analysis, we identified four major variations located in nonstructural protein 2, S, open reading frame 3, and envelope (E) genes, respectively. Comparative analyses of their genomic variations and proliferation characteristics identified a single mutation within the S2' cleavage site between C30 and C40 mutants: the substitution of conserved arginine (R) by a glycine (G) (R895G). This change resulted in weaker cell-cell fusion, smaller plaque morphology, higher virus titer and serious microfilament condensation. Further analysis confirmed that this mutation was responsible for optimal cell-adaptation, but not the determinant for trypsin-dependent entry of PEDV. Otherwise, a novel variation (16-20 aa deletion and an L25P mutation) in the transmembrane domain of the E protein affected multiple infection processes, including up-regulation of the production of the ER stress indicator GRP78, improving the expression of pro-inflammatory cytokines IL-6 and IL-8, and promoting apoptosis. The results of this study provide a better understanding of the potential mechanisms of viral functional proteins in PEDV replication, infection, and fitness.

Published

2017

32. Scavenger receptor class B member 1 (SCARB1) variants modulate hepatitis C virus replication cycle and viral load.

Author

Westhaus S, Deest M, Nguyen ATX, Stanke F, Heckl D, Costa R, Schambach A, Manns MP, Berg T, Vondran FWR, Sarrazin C, Ciesek S, and von Hahn T

Subjects

Cell Line, Genetic Variation, Humans, Polymorphism, Single Nucleotide, Viral Envelope Proteins physiology, Viral Load, Virus Internalization, Virus Replication, Hepacivirus physiology, Hepatitis C genetics, Hepatitis C virology, Host-Pathogen Interactions genetics, Host-Pathogen Interactions physiology, Scavenger Receptors, Class B genetics, Scavenger Receptors, Class B physiology

Abstract

Background & Aims: There are numerous coding and non-coding variants in the SCARB1 gene that encodes scavenger receptor class B member 1 (SR-BI), a key receptor for both high density lipoproteins and hepatitis C virus (HCV). Many have been linked to clinical phenotypes, yet their impact on the HCV replication cycle is incompletely understood. The aim of this study was to analyze the impact of these variants on the molecular biology and clinical course of HCV., Methods: We analyzed key coding non-synonymous as well as non-coding SCARB1 variants using virological in vitro and human genetics approaches., Results: Non-synonymous variants: S112F and T175A have greatly reduced HCV receptor function. When present on the cell surface, these variants are impaired in their ability to interact with HCV E2. Non-coding variants: The G allele in rs3782287 is associated with decreased viral load. Haplotype analysis confirmed these findings and identified haplotype rs3782287 A/rs5888 C as a risk allele associated with increased viral load. We also detected a trend towards lower hepatic SR-BI expression in individuals with the rs3782287 GG genotype associated with low viral load suggesting a potential underlying mechanism., Conclusion: Coding and non-coding genetic SCARB1 variants modulate the HCV replication cycle and possibly clinical features of hepatitis C. These findings underscore the relevance of SR-BI as an HCV receptor and contribute to our understanding of inter-individual variation in HCV infection., Lay Summary: The cell surface receptor SR-BI (scavenger receptor class B member 1), is essential for hepatitis C virus (HCV) entry into hepatocytes. Variations in the gene coding this receptor influence infectivity and viral load. We analyzed these variations to gain a better understanding of inter-individual differences over the course of HCV infection., (Copyright © 2017 European Association for the Study of the Liver. Published by Elsevier B.V. All rights reserved.)

Published

2017

33. ORF7 of Varicella-Zoster Virus Is Required for Viral Cytoplasmic Envelopment in Differentiated Neuronal Cells.

Author

Jiang HF, Wang W, Jiang X, Zeng WB, Shen ZZ, Song YG, Yang H, Liu XJ, Dong X, Zhou J, Sun JY, Yu FL, Guo L, Cheng T, Rayner S, Zhao F, Zhu H, and Luo MH

Subjects

Capsid metabolism, Cell Differentiation, Cell Line, Cytoplasm virology, Gene Deletion, Genome, Viral, Herpes Zoster virology, Herpesvirus 3, Human genetics, Humans, Neuroblastoma, Viral Envelope Proteins genetics, Virion, Virus Internalization, Virus Replication, Herpesvirus 3, Human physiology, Neurons physiology, Neurons virology, Viral Envelope Proteins physiology, Viral Proteins genetics, Viral Proteins metabolism

Abstract

Although a varicella-zoster virus (VZV) vaccine has been used for many years, the neuropathy caused by VZV infection is still a major health concern. Open reading frame 7 (ORF7) of VZV has been recognized as a neurotropic gene in vivo , but its neurovirulent role remains unclear. In the present study, we investigated the effect of ORF7 deletion on VZV replication cycle at virus entry, genome replication, gene expression, capsid assembly and cytoplasmic envelopment, and transcellular transmission in differentiated neural progenitor cells (dNPCs) and neuroblastoma SH-SY5Y (dSY5Y) cells. Our results demonstrate that the ORF7 protein is a component of the tegument layer of VZV virions. Deleting ORF7 did not affect viral entry, viral genome replication, or the expression of typical viral genes but clearly impacted cytoplasmic envelopment of VZV capsids, resulting in a dramatic increase of envelope-defective particles and a decrease in intact virions. The defect was more severe in differentiated neuronal cells of dNPCs and dSY5Y. ORF7 deletion also impaired transmission of ORF7-deficient virus among the neuronal cells. These results indicate that ORF7 is required for cytoplasmic envelopment of VZV capsids, virus transmission among neuronal cells, and probably the neuropathy induced by VZV infection. IMPORTANCE The neurological damage caused by varicella-zoster virus (VZV) reactivation is commonly manifested as clinical problems. Thus, identifying viral neurovirulent genes and characterizing their functions are important for relieving VZV related neurological complications. ORF7 has been previously identified as a potential neurotropic gene, but its involvement in VZV replication is unclear. In this study, we found that ORF7 is required for VZV cytoplasmic envelopment in differentiated neuronal cells, and the envelopment deficiency caused by ORF7 deletion results in poor dissemination of VZV among neuronal cells. These findings imply that ORF7 plays a role in neuropathy, highlighting a potential strategy to develop a neurovirulence-attenuated vaccine against chickenpox and herpes zoster and providing a new target for intervention of neuropathy induced by VZV., (Copyright © 2017 American Society for Microbiology.)

Published

2017

34. [Endogenous retroviral sequences in the human genome can play a physiological or pathological role].

Author

Medina J, Charvet B, Leblanc P, Germi R, Horvat B, Marche PN, and Perron H

Subjects

Animals, Cytomegalovirus physiology, DNA Methylation, Endogenous Retroviruses genetics, Gene Expression Regulation, Viral, Herpesviridae pathogenicity, Herpesviridae physiology, Herpesviridae Infections genetics, Herpesviridae Infections pathology, Herpesviridae Infections virology, Herpesvirus 4, Human physiology, Humans, Viral Envelope Proteins genetics, Viral Envelope Proteins physiology, Endogenous Retroviruses pathogenicity, Endogenous Retroviruses physiology, Genome, Human genetics

Abstract

Human endogenous retroviruses (HERV) represent a large part of our genome and the few elements that have retained a potential of expression still remain "dormant" in physiological conditions. In some instances, they can be awakened by environmental factors activating their expression. The best studied conditions of HERV activation are infections caused by microorganisms such as viruses of the Herpesvirus family. This activation can thus lead to the expression of pathogenic proteins such as envelope proteins belonging to the HERV-W and HERV-K families, respectively involved in Multiple Sclerosis (MS) and amyotrophic lateral sclerosis (ALS). Endogenous retroviral proteins can also acquire a physiological function beneficial for humans. This is the case of Syncytin-1 from the HERV-W family, that is involved in placenta formation., (© 2017 médecine/sciences – Inserm.)

Published

2017

35. The Pseudorabies Virus Glycoprotein gE/gI Complex Suppresses Type I Interferon Production by Plasmacytoid Dendritic Cells.

Author

Lamote JAS, Kestens M, Van Waesberghe C, Delva J, De Pelsmaeker S, Devriendt B, and Favoreel HW

Subjects

Animals, Cells, Cultured, Dendritic Cells immunology, Dendritic Cells virology, Immune Evasion, Immunity, Innate, Immunomodulation, MAP Kinase Signaling System, Pseudorabies virology, Sus scrofa, Dendritic Cells metabolism, Interferon Type I biosynthesis, Pseudorabies immunology, Viral Envelope Proteins physiology

Abstract

Plasmacytoid dendritic cells (pDC) play a central role in the antiviral immune response, both in the innate response and in shaping the adaptive response, mainly because of their ability to produce massive amounts of type I interferon (TI-IFN). Here, we report that cells infected with the live attenuated Bartha vaccine strain of porcine alphaherpesvirus pseudorabies virus (PRV) trigger a dramatically increased TI-IFN response by porcine primary pDC compared to cells infected with wild-type PRV strains (Becker and Kaplan). Since Bartha is one of the relatively few examples of a highly successful alphaherpesvirus vaccine, identification of factors that may contribute to its efficacy may provide insights for the rational design of other alphaherpesvirus vaccines. The Bartha vaccine genome displays several mutations compared to the genome of wild-type PRV strains, including a large deletion in the unique short (US) region, encompassing the glycoprotein E (gE), gI, US9, and US2 genes. Using recombinant PRV Becker strains harboring the entire Bartha US deletion or single mutations in the four affected US genes, we demonstrate that the absence of the viral gE/gI complex contributes to the observed increased IFN-α response. Furthermore, we show that the absence of gE leads to an enhanced extracellular signal-regulated kinase 1/2 (ERK1/2) phosphorylation in pDC, which correlates with a higher TI-IFN production by pDC. In conclusion, the PRV Bartha vaccine strain triggers strongly increased TI-IFN production by porcine pDC. Our data further indicate that the gE/gI glycoprotein complex suppresses TI-IFN production by pDC, which represents the first alphaherpesvirus factor that suppresses pDC activity. IMPORTANCE Several alphaherpesviruses, including herpes simpex virus, still lack effective vaccines. However, the highly successful Bartha vaccine has contributed substantially to eradication of the porcine alphaherpesvirus pseudorabies virus (PRV) in several countries. The impact of Bartha on the immune response is still poorly understood. Type I interferon (TI-IFN)-producing plasmacytoid dendritic cells (pDC) may play an important role in vaccine development. Here, we show that Bartha elicits a dramatically increased type I interferon (TI-IFN) response in primary porcine pDC compared to wild-type strains. In addition, we found that the gE/gI complex, which is absent in Bartha, inhibits the pDC TI-IFN response. This is the first description of an immune cell type that is differentially affected by Bartha versus wild-type PRV and is the first report describing an alphaherpesvirus protein that inhibits the TI-IFN response by pDC. These data may therefore contribute to the rational design of other alphaherpesvirus vaccines., (Copyright © 2017 American Society for Microbiology.)

Published

2017

36. Functional Analysis of Hepatitis C Virus (HCV) Envelope Protein E1 Using a trans -Complementation System Reveals a Dual Role of a Putative Fusion Peptide of E1 in both HCV Entry and Morphogenesis.

Author

Tong Y, Chi X, Yang W, and Zhong J

Subjects

Cell Line, Tumor, Coculture Techniques, HEK293 Cells, Humans, Membrane Fusion, Protein Binding, Protein Interaction Domains and Motifs, Protein Multimerization, Virus Replication, Hepacivirus physiology, Viral Envelope Proteins physiology, Virus Internalization

Abstract

Hepatitis C virus (HCV) is an enveloped RNA virus belonging to the Flaviviridae family. It infects mainly human hepatocytes and causes chronic liver diseases, including cirrhosis and cancer. HCV encodes two envelope proteins, E1 and E2, that form a heterodimer and mediate virus entry. While E2 has been extensively studied, less has been done so for E1, and its role in the HCV life cycle still needs to be elucidated. Here we developed a new cell culture model for HCV infection based on the trans -complementation of E1. Virus production of the HCV genome lacking the E1-encoding sequence can be efficiently rescued by the ectopic expression of E1 in trans The resulting virus, designated HCVΔE1, can propagate in packaging cells expressing E1 but results in only single-cycle infection in naive cells. By using the HCVΔE1 system, we explored the role of a putative fusion peptide (FP) of E1 in HCV infection. Interestingly, we found that the FP not only contributes to HCV entry, as previously reported, but also may be involved in virus morphogenesis. Finally, we identified amino acid residues in FP that are critical for biological functions of E1. In summary, our work not only provides a new cell culture model for studying HCV but also provides some insights into understanding the role of E1 in the HCV life cycle. IMPORTANCE Hepatitis C virus (HCV), an enveloped RNA virus, encodes two envelope proteins, E1 and E2, that form a heterodimeric complex to mediate virus entry. Compared to E2, the biological functions of E1 in the virus life cycle are not adequately investigated. Here we developed a new cell culture model for single-cycle HCV infection based on the trans -complementation of E1. The HCV genome lacking the E1-encoding sequence can be efficiently rescued for virus production by the ectopic expression of E1 in trans This new model renders a unique system to dissect functional domains and motifs in E1. Using this system, we found that a putative fusion peptide in E1 is a multifunctional structural element contributing to both HCV entry and morphogenesis. Our work has provided a new cell culture model to study HCV and provides insights into understanding the biological roles of E1 in the HCV life cycle., (Copyright © 2017 American Society for Microbiology.)

Published

2017

37. Mildly Acidic pH Triggers an Irreversible Conformational Change in the Fusion Domain of Herpes Simplex Virus 1 Glycoprotein B and Inactivation of Viral Entry.

Author

Weed DJ, Pritchard SM, Gonzalez F, Aguilar HC, and Nicola AV

Subjects

Animals, Chlorocebus aethiops, Hydrogen-Ion Concentration, Protein Domains, Vero Cells, Viral Envelope Proteins physiology, Virus Attachment, Virus Internalization, Herpes Simplex virology, Herpesvirus 1, Human physiology, Viral Envelope Proteins chemistry

Abstract

Herpes simplex virus (HSV) entry into a subset of cells requires endocytosis and endosomal low pH. Preexposure of isolated virions to mildly acidic pH of 5 to 6 partially inactivates HSV infectivity in an irreversible manner. Acid inactivation is a hallmark of viruses that enter via low-pH pathways; this occurs by pretriggering conformational changes essential for fusion. The target and mechanism(s) of low-pH inactivation of HSV are unclear. Here, low-pH-treated HSV-1 was defective in fusion activity and yet retained normal levels of attachment to cell surface heparan sulfate and binding to nectin-1 receptor. Low-pH-triggered conformational changes in gB reported to date are reversible, despite irreversible low-pH inactivation. gB conformational changes and their reversibility were measured by antigenic analysis with a panel of monoclonal antibodies and by detecting changes in oligomeric conformation. Three-hour treatment of HSV-1 virions with pH 5 or multiple sequential treatments at pH 5 followed by neutral pH caused an irreversible >2.5 log infectivity reduction. While changes in several gB antigenic sites were reversible, alteration of the H126 epitope was irreversible. gB oligomeric conformational change remained reversible under all conditions tested. Altogether, our results reveal that oligomeric alterations and fusion domain changes represent distinct conformational changes in gB, and the latter correlates with irreversible low-pH inactivation of HSV. We propose that conformational change in the gB fusion domain is important for activation of membrane fusion during viral entry and that in the absence of a host target membrane, this change results in irreversible inactivation of virions. IMPORTANCE HSV-1 is an important pathogen with a high seroprevalence throughout the human population. HSV infects cells via multiple pathways, including a low-pH route into epithelial cells, the primary portal into the host. HSV is inactivated by low-pH preexposure, and gB, a class III fusion protein, undergoes reversible conformational changes in response to low-pH exposure. Here, we show that low-pH inactivation of HSV is irreversible and due to a defect in virion fusion activity. We identified an irreversible change in the fusion domain of gB following multiple sequential low-pH exposures or following prolonged low-pH treatment. This change appears to be separable from the alteration in gB quaternary structure. Together, the results are consistent with a model by which low pH can have an activating or inactivating effect on HSV depending on the presence of a target membrane., (Copyright © 2017 American Society for Microbiology.)

Published

2017

38. An Optimized Hepatitis C Virus E2 Glycoprotein Core Adopts a Functional Homodimer That Efficiently Blocks Virus Entry.

Author

McCaffrey K, Boo I, Owczarek CM, Hardy MP, Perugini MA, Fabri L, Scotney P, Poumbourios P, and Drummer HE

Subjects

Allosteric Regulation, Antibodies, Neutralizing chemistry, Antibodies, Viral chemistry, Cell Line, Tumor, Epitopes chemistry, Epitopes immunology, HEK293 Cells, Hepatocytes virology, Humans, Kinetics, Protein Binding, Protein Folding, Protein Interaction Domains and Motifs, Protein Structure, Quaternary, Tetraspanin 28 chemistry, Viral Envelope Proteins physiology, Hepacivirus physiology, Viral Envelope Proteins chemistry, Virus Internalization

Abstract

The hepatitis C virus (HCV) envelope glycoprotein E2 is the major target of broadly neutralizing antibodies in vivo and is the focus of efforts in the rational design of a universal B cell vaccine against HCV. The E2 glycoprotein exhibits a high degree of amino acid variability which localizes to three discrete regions: hypervariable region 1 (HVR1), hypervariable region 2 (HVR2), and the intergenotypic variable region (igVR). All three variable regions contribute to immune evasion and/or isolate-specific structural variations, both important considerations for vaccine design. A high-resolution structural definition of the intact HCV envelope glycoprotein complex containing E1 and E2 remains to be elucidated, while crystallographic structures of a recombinant E2 ectodomain failed to resolve HVR1, HVR2, and a major neutralization determinant adjacent to HVR1. To obtain further information on E2, we characterized the role of all three variable regions in E2 ectodomain folding and function in the context of a recombinant ectodomain fragment (rE2). We report that removal of the variable regions accelerates binding to the major host cell receptor CD81 and that simultaneous deletion of HVR2 and the igVR is required to maintain wild-type CD81-binding characteristics. The removal of the variable regions also rescued the ability of rE2 to form a functional homodimer. We propose that the rE2 core provides novel insights into the role of the variable motifs in the higher-order assembly of the E2 ectodomain and may have implications for E1E2 structure on the virion surface. IMPORTANCE Hepatitis C virus (HCV) infection affects ∼2% of the population globally, and no vaccine is available. HCV is a highly variable virus, and understanding the presentation of key antigenic sites at the virion surface is important for the design of a universal vaccine. This study investigates the role of three surface-exposed variable regions in E2 glycoprotein folding and function in the context of a recombinant soluble ectodomain. Our data demonstrate the variable motifs modulate binding of the E2 ectodomain to the major host cell receptor CD81 and have an impact on the formation of an E2 homodimer with high-affinity binding to CD81., (Copyright © 2017 American Society for Microbiology.)

Published

2017

39. Epidemiological and etiological investigation of dengue fever in the Fujian province of China during 2004-2014.

Author

Wang J, Chen H, Huang M, Zhang Y, Xie J, Yan Y, Zheng K, and Weng Y

Subjects

Asia, Southeastern ethnology, Asian People, China epidemiology, DNA, Complementary chemistry, DNA, Complementary genetics, Dengue ethnology, Dengue virology, Dengue Virus classification, Dengue Virus physiology, Genotype, Host-Pathogen Interactions, Humans, Phylogeny, RNA, Viral genetics, RNA, Viral isolation & purification, Reverse Transcriptase Polymerase Chain Reaction, Seasons, Sequence Analysis, DNA, Viral Envelope Proteins classification, Viral Envelope Proteins genetics, Viral Envelope Proteins physiology, Dengue epidemiology, Dengue Virus genetics, Disease Outbreaks, Genetic Variation

Abstract

Dengue fever (DF) is a vector-borne disease and a tremendous socioeconomic burden on tropical and subtropical countries worldwide. To explore the characteristics of DF epidemic in the Fujian province, information of DF cases in Fujian during 2004-2014 was collected and analyzed. The complete E genes of 48 viral isolates were amplified and sequenced for phylogenetic analysis. A total of 733 cases was reported, of which 612 (83.5%) occurred during the peak period from August to October. Additionally, 76% (190/250) of imported cases originated from Southeast Asia countries, by the epidemiological investigation. Phylogenetic analysis of the 48 viral isolates revealed that three genotypes (I, IV, V) of DENV1, and one genotype each of DENV2 (cosmopolitan) and DENV3 (I) circulated in Fujian during 2004-2014. Similar to the results of the epidemiological investigations, the source of most of the viral isolates, including imported and indigenous cases, may be Southeast Asia countries; however, importation from adjacent provinces was also observed in recent years. Overall, DF is considered an imported epidemic disease in Fujian. Increasing diversity of the viral source and geographic expansion of the area affected by DF in recent years highlights the necessity for strengthening surveillance of the DF epidemic and developing strategies for DF prevention and control in Fujian.

Published

2017

40. Structural basis for Epstein-Barr virus host cell tropism mediated by gp42 and gHgL entry glycoproteins.

Author

Sathiyamoorthy K, Hu YX, Möhl BS, Chen J, Longnecker R, and Jardetzky TS

Subjects

Animals, CHO Cells, Cricetulus, Epithelial Cells virology, Herpesvirus 4, Human chemistry, Mutation, Protein Conformation, Viral Envelope Proteins chemistry, Herpesvirus 4, Human physiology, Viral Envelope Proteins physiology, Viral Tropism

Abstract

Herpesvirus entry into host cells is mediated by multiple virally encoded receptor binding and membrane fusion glycoproteins. Despite their importance in host cell tropism and associated disease pathology, the underlying and essential interactions between these viral glycoproteins remain poorly understood. For Epstein-Barr virus (EBV), gHgL/gp42 complexes bind HLA class II to activate membrane fusion with B cells, but gp42 inhibits fusion and entry into epithelial cells. To clarify the mechanism by which gp42 controls the cell specificity of EBV infection, here we determined the structure of gHgL/gp42 complex bound to an anti-gHgL antibody (E1D1). The critical regulator of EBV tropism is the gp42 N-terminal domain, which tethers the HLA-binding domain to gHgL by wrapping around the exterior of three gH domains. Both the gp42 N-terminal domain and E1D1 selectively inhibit epithelial-cell fusion; however, they engage distinct surfaces of gHgL. These observations clarify key determinants of EBV host cell tropism.

Published

2016

41. Generation and characterization of a monoclonal antibody against duck Tembusu virus envelope protein.

Author

Han K, Zhao D, Liu Y, Liu Q, Huang X, Yang J, Bi K, Xu T, and Li Y

Subjects

Animals, Cell Line, Tumor, Cricetinae, Female, Flaviviridae metabolism, Gene Expression Regulation, Viral, Mice, Mice, Inbred BALB C, Neutralization Tests, Antibodies, Monoclonal, Ducks, Flaviviridae immunology, Viral Envelope Proteins physiology

Abstract

Duck Tembusu virus (DTMUV) is a newly emerging pathogenic flavivirus that has caused massive economic losses to the duck industry in China. Envelope (E) protein of DTMUV is an important structural protein, which is able to induce protective immune response in target animals and can be used as specific serological diagnosis tool. In this study, a novel monoclonal antibody, designated mAb 3E9, was generated against DTMUV E protein. It is positive in indirect ELISA against both His-E protein and the purified whole viral antigen. Also, this mAb showed positive reaction with DTMUV in Western blot and indirect immunofluorescence assay, and the isotype was IgG1. End-point neutralizing assay performed in BHK-21 cells revealed that the neutralization titer of 3E9 against DTMUV JS804 strain reached 1:50. Furthermore, functional studies revealed that 3E9 blocks infection of DTMUV at a step on viral attachment. The anti-E mAbs produced in the present work may be valuable in developing an antigen-capture ELISA test for antigen detection or a competitive ELISA test for antibody detection or therapeutic medicine for DTMUV in poultry.

Published

2016

42. Multiple Strategies Reveal a Bidentate Interaction between the Nipah Virus Attachment and Fusion Glycoproteins.

Author

Stone JA, Vemulapati BM, Bradel-Tretheway B, and Aguilar HC

Subjects

Animals, Cell Line, Flow Cytometry methods, HEK293 Cells, Humans, Immunoprecipitation, Models, Biological, Nipah Virus genetics, Nipah Virus pathogenicity, Peptide Fragments chemistry, Peptide Fragments genetics, Peptide Fragments physiology, Protein Interaction Domains and Motifs, Solubility, Viral Envelope Proteins chemistry, Viral Envelope Proteins genetics, Viral Fusion Proteins chemistry, Viral Fusion Proteins genetics, Viral Fusion Proteins physiology, Virus Attachment, Virus Internalization, Nipah Virus physiology, Viral Envelope Proteins physiology

Abstract

The paramyxoviral family contains many medically important viruses, including measles virus, mumps virus, parainfluenza viruses, respiratory syncytial virus, human metapneumovirus, and the deadly zoonotic henipaviruses Hendra and Nipah virus (NiV). To both enter host cells and spread from cell to cell within infected hosts, the vast majority of paramyxoviruses utilize two viral envelope glycoproteins: the attachment glycoprotein (G, H, or hemagglutinin-neuraminidase [HN]) and the fusion glycoprotein (F). Binding of G/H/HN to a host cell receptor triggers structural changes in G/H/HN that in turn trigger F to undergo a series of conformational changes that result in virus-cell (viral entry) or cell-cell (syncytium formation) membrane fusion. The actual regions of G/H/HN and F that interact during the membrane fusion process remain relatively unknown though it is generally thought that the paramyxoviral G/H/HN stalk region interacts with the F head region. Studies to determine such interactive regions have relied heavily on coimmunoprecipitation approaches, whose limitations include the use of detergents and the micelle-mediated association of proteins. Here, we developed a flow-cytometric strategy capable of detecting membrane protein-protein interactions by interchangeably using the full-length form of G and a soluble form of F, or vice versa. Using both coimmunoprecipitation and flow-cytometric strategies, we found a bidentate interaction between NiV G and F, where both the stalk and head regions of NiV G interact with F. This is a new structural-biological finding for the paramyxoviruses. Additionally, our studies disclosed regions of the NiV G and F glycoproteins dispensable for the G and F interactions., Importance: Nipah virus (NiV) is a zoonotic paramyxovirus that causes high mortality rates in humans, with no approved treatment or vaccine available for human use. Viral entry into host cells relies on two viral envelope glycoproteins: the attachment (G) and fusion (F) glycoproteins. Binding of G to the ephrinB2 or ephrinB3 cell receptors triggers conformational changes in G that in turn cause F to undergo conformational changes that result in virus-host cell membrane fusion and viral entry. It is currently unknown, however, which specific regions of G and F interact during membrane fusion. Past efforts to determine the interacting regions have relied mainly on coimmunoprecipitation, a technique with some pitfalls. We developed a flow-cytometric assay to study membrane protein-protein interactions, and using this assay we report a bidentate interaction whereby both the head and stalk regions of NiV G interact with NiV F, a new finding for the paramyxovirus family., (Copyright © 2016, American Society for Microbiology. All Rights Reserved.)

Published

2016

43. Reaction-diffusion basis of retroviral infectivity.

Author

Sadiq SK

Subjects

Binding Sites, Computer Simulation, Diffusion, Gene Products, gag ultrastructure, Models, Biological, Protein Binding, Retroviridae physiology, Retroviridae ultrastructure, Viral Envelope Proteins physiology, Viral Envelope Proteins ultrastructure, Virion physiology, Virion ultrastructure, Virulence physiology, Gene Products, gag chemistry, Gene Products, gag physiology, Models, Chemical, Retroviridae chemistry, Viral Envelope Proteins chemistry, Virion chemistry

Abstract

Retrovirus particle (virion) infectivity requires diffusion and clustering of multiple transmembrane envelope proteins (Env 3 ) on the virion exterior, yet is triggered by protease-dependent degradation of a partially occluding, membrane-bound Gag polyprotein lattice on the virion interior. The physical mechanism underlying such coupling is unclear and only indirectly accessible via experiment. Modelling stands to provide insight but the required spatio-temporal range far exceeds current accessibility by all-atom or even coarse-grained molecular dynamics simulations. Nor do such approaches account for chemical reactions, while conversely, reaction kinetics approaches handle neither diffusion nor clustering. Here, a recently developed multiscale approach is considered that applies an ultra-coarse-graining scheme to treat entire proteins at near-single particle resolution, but which also couples chemical reactions with diffusion and interactions. A model is developed of Env 3 molecules embedded in a truncated Gag lattice composed of membrane-bound matrix proteins linked to capsid subunits, with freely diffusing protease molecules. Simulations suggest that in the presence of Gag but in the absence of lateral lattice-forming interactions, Env 3 diffuses comparably to Gag-absent Env 3 Initial immobility of Env 3 is conferred through lateral caging by matrix trimers vertically coupled to the underlying hexameric capsid layer. Gag cleavage by protease vertically decouples the matrix and capsid layers, induces both matrix and Env 3 diffusion, and permits Env 3 clustering. Spreading across the entire membrane surface reduces crowding, in turn, enhancing the effect and promoting infectivity.This article is part of the themed issue 'Multiscale modelling at the physics-chemistry-biology interface'., (© 2016 The Author(s).)

Published

2016

44. Aqueous solutions of didecyldimethylammonium chloride and octaethylene glycol monododecyl ether: Toward synergistic formulations against enveloped viruses.

Author

Nardello-Rataj V and Leclercq L

Subjects

Animals, Chlorocebus aethiops, Dose-Response Relationship, Drug, Drug Synergism, Hep G2 Cells, Herpesvirus 1, Human drug effects, Herpesvirus 1, Human physiology, Humans, Pharmaceutical Solutions chemistry, Pharmaceutical Solutions pharmacology, Polyethylene Glycols pharmacology, Quaternary Ammonium Compounds pharmacology, Vero Cells, Viral Envelope Proteins physiology, Water pharmacology, Drug Compounding methods, Polyethylene Glycols chemistry, Quaternary Ammonium Compounds chemistry, Viral Envelope Proteins antagonists & inhibitors, Water chemistry

Abstract

Micellization of di-n-decyldimethylammonium chloride, [DiC10][Cl], and octaethylene glycol monododecyl ether, C12E8, mixtures have been investigated by surface tension and conductivity measurements. From these results, various physicochemical and thermodynamic key parameters (e.g. micellar mole fraction of [DiC10][Cl], interaction parameter, free energy of micellization, etc.) have been evaluated and discussed in detail. The results prove high synergistic effect between the two surfactants. Based on these results, the virucidal activity of an equimolar mixture of [DiC10][Cl] and C12E8 has been investigated. A marked synergism was observed on lipid-containing deoxyribonucleic and ribonucleic acid viruses, such as herpes virus, respiratory syncytial virus, and vaccinia viruses. In contrast, Coxsackievirus (non-enveloped virus) was not inactivated. These results support that the mechanism is based on the extraction of lipids and/or proteins from the envelope inside the mixed micelles. This extraction creates "holes" the size of which increases with concentration up to a specific value which triggers the virus inactivation. Such a mixture could be used to extend the spectrum of virucidal activity of the amphiphiles virucides commonly employed in numerous disinfectant solutions., (Copyright © 2016 Elsevier B.V. All rights reserved.)

Published

2016

45. Exocytosis of Alphaherpesvirus Virions, Light Particles, and Glycoproteins Uses Constitutive Secretory Mechanisms.

Author

Hogue IB, Scherer J, and Enquist LW

Subjects

Animals, Biological Transport, Cell Line, Cell Membrane metabolism, Fluorescent Dyes, Herpesvirus 1, Human physiology, Herpesvirus 1, Suid chemistry, Herpesvirus 1, Suid pathogenicity, Herpesvirus 1, Suid physiology, Herpesvirus 1, Suid ultrastructure, Herpesvirus 2, Human physiology, Humans, Hydrogen-Ion Concentration, Immune Evasion, Microscopy, Fluorescence methods, Protein Transport, Sus scrofa, Viral Envelope Proteins physiology, Virion ultrastructure, Virus Assembly, rab GTP-Binding Proteins metabolism, Exocytosis, Glycoproteins metabolism, Virion physiology

Abstract

Unlabelled: Many molecular and cell biological details of the alphaherpesvirus assembly and egress pathway remain unclear. Recently we developed a live-cell fluorescence microscopy assay of pseudorabies virus (PRV) exocytosis, based on total internal reflection fluorescence (TIRF) microscopy and a virus-encoded pH-sensitive fluorescent probe. Here, we use this assay to distinguish three classes of viral exocytosis in a nonpolarized cell type: (i) trafficking of viral glycoproteins to the plasma membrane, (ii) exocytosis of viral light particles, and (iii) exocytosis of virions. We find that viral glycoproteins traffic to the cell surface in association with constitutive secretory Rab GTPases and exhibit free diffusion into the plasma membrane after exocytosis. Similarly, both virions and light particles use these same constitutive secretory mechanisms for egress from infected cells. Furthermore, we show that viral light particles are distinct from cellular exosomes. Together, these observations shed light on viral glycoprotein trafficking steps that precede virus particle assembly and reinforce the idea that virions and light particles share a biogenesis and trafficking pathway., Importance: The alphaherpesviruses, including the important human pathogens herpes simplex virus 1 (HSV-1), HSV-2, and varicella-zoster virus (VZV), are among the few viruses that have evolved to exploit the mammalian nervous system. These viruses typically cause mild recurrent herpetic or zosteriform lesions but can also cause debilitating herpes encephalitis, more frequently in very young, old, immunocompromised, or nonnatural hosts. Importantly, many of the molecular and cellular mechanisms of viral assembly and egress remain unclear. This study addresses the trafficking of viral glycoproteins to the plasma membrane, exocytosis of light particles, and exocytosis of virions. Trafficking of glycoproteins affects immune evasion and pathogenesis and may precede virus particle assembly. The release of light particles may also contribute to immune evasion and pathogenesis. Finally, exocytosis of virions is important to understand, as this final step in the virus replication cycle produces infectious extracellular particles capable of spreading to the next round of host cells., (Copyright © 2016 Hogue et al.)

Published

2016

46. The deletion of residues 268-292 of E1 impairs the ability of HCV envelope proteins to induce pore formation.

Author

Lombana L, Ortega-Atienza S, Gómez-Gutiérrez J, Yélamos B, Peterson DL, and Gavilanes F

Subjects

Amino Acid Sequence, HEK293 Cells, Hepacivirus genetics, Humans, Liposomes, Mutagenesis, Sequence Deletion, Viral Envelope Proteins genetics, Virus Internalization, Hepacivirus physiology, Viral Envelope Proteins physiology

Abstract

We have obtained a chimeric protein containing the ectodomains of hepatitis C virus (HCV) envelope proteins but lacking the region 268-292 of E1. All its structural properties are coincident with those of the corresponding full length chimera. The deleted and entire chimeras were compared in terms of their membrane destabilizing properties. No differences were found in their ability to induce vesicle aggregation and lipid mixing but the deleted chimera showed a reduced capacity to promote leakage. The role of the deletion was also studied by obtaining HCV pseudoparticles (HCVpp). Both E1 and E2, and also the E1 deleted mutant, were incorporated into HCVpp to a similar level. However, HCVpp containing the E1 deleted protein are almost unable to infect Huh7 cells. These results point to the involvement of the region 268-292 in the formation of pores in the membrane necessary for the complete fusion of the membranes., (Copyright © 2016 Elsevier B.V. All rights reserved.)

Published

2016

47. Analysis of the entry mechanism of Crimean-Congo hemorrhagic fever virus, using a vesicular stomatitis virus pseudotyping system.

Author

Suda Y, Fukushi S, Tani H, Murakami S, Saijo M, Horimoto T, and Shimojima M

Subjects

Animals, Cell Adhesion Molecules physiology, Chlorocebus aethiops, HEK293 Cells, Hemorrhagic Fever Virus, Crimean-Congo genetics, Hemorrhagic Fever Virus, Crimean-Congo pathogenicity, Hemorrhagic Fever, Crimean etiology, Hemorrhagic Fever, Crimean virology, Humans, Jurkat Cells, Lectins, C-Type physiology, Receptors, Cell Surface physiology, Vero Cells, Vesicular stomatitis Indiana virus genetics, Vesicular stomatitis Indiana virus physiology, Viral Envelope Proteins genetics, Viral Envelope Proteins physiology, Hemorrhagic Fever Virus, Crimean-Congo physiology, Virus Internalization

Abstract

Crimean-Congo hemorrhagic fever (CCHF) is a tick-borne disease causing severe hemorrhagic symptoms with a nearly 30 % case-fatality rate in humans. The experimental use of CCHF virus (CCHFV), which causes CCHF, requires high-biosafety-level (BSL) containment. In contrast, pseudotyping of various viral glycoproteins (GPs) onto vesicular stomatitis virus (VSV) can be used in facilities with lower BSL containment, and this has facilitated studies on the viral entry mechanism and the measurement of neutralizing activity, especially for highly pathogenic viruses. In the present study, we generated high titers of pseudotyped VSV bearing the CCHFV envelope GP and analyzed the mechanisms involved in CCHFV infection. A partial deletion of the CCHFV GP cytoplasmic domain increased the titer of the pseudotyped VSV, the entry mechanism of which was dependent on the CCHFV envelope GP. Using the pseudotype virus, DC-SIGN (a calcium-dependent [C-type] lectin cell-surface molecule) was revealed to enhance viral infection and act as an entry factor for CCHFV.

Published

2016

48. Editorial overview: Virus structure and assembly: Virions - from structure and physics to design principles.

Author

Zlotnick A and Huiskonen JT

Subjects

Capsid physiology, Models, Biological, Viral Envelope Proteins physiology, Viral Structures, Virion physiology, Virus Assembly

Published

2016

49. The V1 region of gp120 is preferentially selected during SIV/HIV transmission and is indispensable for envelope function and virus infection.

Author

Li Y, Dittmer U, Wang Y, Song J, Sun B, and Yang R

Subjects

Animals, HEK293 Cells, HIV Envelope Protein gp120 chemistry, HIV Envelope Protein gp120 genetics, HIV Envelope Protein gp120 metabolism, HIV Envelope Protein gp41 chemistry, HIV Envelope Protein gp41 genetics, HIV Envelope Protein gp41 metabolism, HIV Envelope Protein gp41 physiology, HIV Infections virology, HIV-1 genetics, HIV-2 genetics, HIV-2 physiology, Humans, Membrane Fusion physiology, Membrane Glycoproteins chemistry, Membrane Glycoproteins genetics, Membrane Glycoproteins metabolism, Peptide Fragments chemistry, Peptide Fragments genetics, Peptide Fragments metabolism, Recombinant Proteins chemistry, Recombinant Proteins metabolism, Simian Acquired Immunodeficiency Syndrome virology, Simian Immunodeficiency Virus genetics, Viral Envelope Proteins chemistry, Viral Envelope Proteins genetics, Viral Envelope Proteins metabolism, HIV Envelope Protein gp120 physiology, HIV Infections transmission, HIV-1 physiology, Membrane Glycoproteins physiology, Peptide Fragments physiology, Simian Acquired Immunodeficiency Syndrome transmission, Simian Immunodeficiency Virus physiology, Viral Envelope Proteins physiology

Abstract

A transmission bottleneck occurs during each human immunodeficiency virus (HIV) transmission event, which allows only a few viruses to establish new infection. However, the genetic characteristics of the transmitted viruses that are preferentially selected have not been fully elucidated. Here, we analyzed amino acids changes in the envelope protein during simian immunodeficiency virus (SIV)/HIV deep transmission history and current HIV evolution within the last 15-20 years. Our results confirmed that the V1V2 region of gp120 protein, particularly V1, was preferentially selected. A shorter V1 region was preferred during transmission history, while during epidemic, HIV may evolve to an expanded V1 region gradually and thus escape immune recognition. We then constructed different HIV-1 V1 mutants using different HIV-1 subtypes to elucidate the role of the V1 region in envelope function. We found that the V1 region, although highly variable, was indispensable for virus entry and infection, probably because V1 deletion mutants exhibited impaired processing of gp160 into mature gp120 and gp41. Additionally, the V1 region affected Env incorporation. These results indicated that the V1 region played a critical role in HIV transmission and infection.

Published

2016

50. gD-Independent Superinfection Exclusion of Alphaherpesviruses.

Author

Criddle A, Thornburg T, Kochetkova I, DePartee M, and Taylor MP

Subjects

Animals, Cell Line, Cells, Cultured, Chlorocebus aethiops, Rats, Reassortant Viruses, Vero Cells, Viral Envelope Proteins physiology, Herpesvirus 1, Human physiology, Herpesvirus 1, Suid physiology, Superinfection virology

Abstract

Unlabelled: Many viruses have the capacity to prevent a cell from being infected by a second virus, often termed superinfection exclusion. Alphaherpesviruses, including the human pathogen herpes simplex virus 1 (HSV-1) and the animal herpesvirus pseudorabies virus (PRV), encode a membrane-bound glycoprotein, gD, that can interfere with subsequent virion entry. We sought to characterize the timing and mechanism of superinfection exclusion during HSV-1 and PRV infection. To this end, we utilized recombinant viruses expressing fluorescent protein (FP) markers of infection that allowed the visualization of viral infections by microscopy and flow cytometry as well as the differentiation of viral progeny. Our results demonstrated the majority of HSV-1- and PRV-infected cells establish superinfection exclusion by 2 h postinfection. The modification of viral infections by virion inactivation and phosphonoacetic acid, cycloheximide, and actinomycin D treatments indicated new protein synthesis is needed to establish superinfection exclusion. Primary infection with gene deletion PRV recombinants identified that new gD expression is not required to establish superinfection exclusion of a secondary viral inoculum. We also identified the timing of coinfection events during axon-to-cell spread, with most occurring within a 2-h window, suggesting a role for cellular superinfection exclusion during neuroinvasive spread of infection. In summary, we have characterized a gD-independent mechanism of superinfection exclusion established by two members of the alphaherpesvirus family and identified a potential role of exclusion during the pathogenic spread of infection., Importance: Superinfection exclusion is a widely observed phenomenon initiated by a primary viral infection to prevent further viruses from infecting the same cell. The capacity for alphaherpesviruses to infect the same cell impacts rates of interviral recombination and disease. Interviral recombination allows genome diversification, facilitating the development of resistance to antiviral therapeutics and evasion of vaccine-mediated immune responses. Our results demonstrate superinfection exclusion occurs early, through a gD-independent process, and is important in the directed spread of infection. Identifying when and where in an infected host viral genomes are more likely to coinfect the same cell and generate viral recombinants will enhance the development of effective antiviral therapies and interventions., (Copyright © 2016 Criddle et al.)

Published

2016