Your search keyword '"Nathalie Callens"' showing total 15 results

1. Hepatitis C virus alters the morphology and function of peroxisomes

Author

Esther Martin de Fourchambault, Nathalie Callens, Jean-Michel Saliou, Marie Fourcot, Oceane Delos, Nicolas Barois, Quentin Thorel, Santseharay Ramirez, Jens Bukh, Laurence Cocquerel, Justine Bertrand-Michel, Guillemette Marot, Yasmine Sebti, Jean Dubuisson, and Yves Rouillé

Subjects

hepatitis C virus, HCV genotype, peroxisome, proximity biotinylation, APEX2, CRISPR-Cas9, Microbiology, QR1-502

Abstract

Despite the introduction of effective treatments for hepatitis C in clinics, issues remain regarding the liver disease induced by chronic hepatitis C virus (HCV) infection. HCV is known to disturb the metabolism of infected cells, especially lipid metabolism and redox balance, but the mechanisms leading to HCV-induced pathogenesis are still poorly understood. In an APEX2-based proximity biotinylation screen, we identified ACBD5, a peroxisome membrane protein, as located in the vicinity of HCV replication complexes. Confocal microscopy confirmed the relocation of peroxisomes near HCV replication complexes and indicated that their morphology and number are altered in approximately 30% of infected Huh-7 cells. Peroxisomes are small versatile organelles involved among other functions in lipid metabolism and ROS regulation. To determine their importance in the HCV life cycle, we generated Huh-7 cells devoid of peroxisomes by inactivating the PEX5 and PEX3 genes using CRISPR/Cas9 and found that the absence of peroxisomes had no impact on replication kinetics or infectious titers of HCV strains JFH1 and DBN3a. The impact of HCV on peroxisomal functions was assessed using sub-genomic replicons. An increase of ROS was measured in peroxisomes of replicon-containing cells, correlated with a significant decrease of catalase activity with the DBN3a strain. In contrast, HCV replication had little to no impact on cytoplasmic and mitochondrial ROS, suggesting that the redox balance of peroxisomes is specifically impaired in cells replicating HCV. Our study provides evidence that peroxisome function and morphology are altered in HCV-infected cells.

Published

2023

2. A reporter cell line for the automated quantification of SARS-CoV-2 infection in living cells

Author

Lowiese Desmarets, Nathalie Callens, Eik Hoffmann, Adeline Danneels, Muriel Lavie, Cyril Couturier, Jean Dubuisson, Sandrine Belouzard, and Yves Rouillé

Subjects

coronavirus, SARS-CoV-2, antivirals, high content imaging, screening, 3CLpro, Microbiology, QR1-502

Abstract

The SARS-CoV-2 pandemic and the urgent need for massive antiviral testing highlighted the lack of a good cell-based assay that allowed for a fast, automated screening of antivirals in high-throughput content with minimal handling requirements in a BSL-3 environment. The present paper describes the construction of a green fluorescent substrate that, upon cleavage by the SARS-CoV-2 main protease, re-localizes from the cytoplasm in non-infected cells to the nucleus in infected cells. The construction was stably expressed, together with a red fluorescent nuclear marker, in a highly susceptible clone derived from Vero-81 cells. With this fluorescent reporter cell line, named F1G-red, SARS-CoV-2 infection can be scored automatically in living cells by comparing the patterns of green and red fluorescence signals acquired by automated confocal microscopy in a 384-well plate format. We show the F1G-red system is sensitive to several SARS-CoV-2 variants of concern and that it can be used to assess antiviral activities of compounds in dose–response experiments. This high-throughput system will provide a reliable tool for antiviral screening against SARS-CoV-2.

Published

2022

3. Morphology and Molecular Composition of Purified Bovine Viral Diarrhea Virus Envelope.

Author

Nathalie Callens, Britta Brügger, Pierre Bonnafous, Hervé Drobecq, Mathias J Gerl, Thomas Krey, Gleyder Roman-Sosa, Till Rümenapf, Olivier Lambert, Jean Dubuisson, and Yves Rouillé

Subjects

Immunologic diseases. Allergy, RC581-607, Biology (General), QH301-705.5

Abstract

The family Flaviviridae includes viruses that have different virion structures and morphogenesis mechanisms. Most cellular and molecular studies have been so far performed with viruses of the Hepacivirus and Flavivirus genera. Here, we studied bovine viral diarrhea virus (BVDV), a member of the Pestivirus genus. We set up a method to purify BVDV virions and analyzed their morphology by electron microscopy and their protein and lipid composition by mass spectrometry. Cryo-electron microscopy showed near spherical viral particles displaying an electron-dense capsid surrounded by a phospholipid bilayer with no visible spikes. Most particles had a diameter of 50 nm and about 2% were larger with a diameter of up to 65 nm, suggesting some size flexibility during BVDV morphogenesis. Morphological and biochemical data suggested a low envelope glycoprotein content of BVDV particles, E1 and E2 being apparently less abundant than Erns. Lipid content of BVDV particles displayed a ~2.3 to 3.5-fold enrichment in cholesterol, sphingomyelin and hexosyl-ceramide, concomitant with a 1.5 to 5-fold reduction of all glycerophospholipid classes, as compared to lipid content of MDBK cells. Although BVDV buds in the endoplasmic reticulum, its lipid content differs from a typical endoplasmic reticulum membrane composition. This suggests that BVDV morphogenesis includes a mechanism of lipid sorting. Functional analyses confirmed the importance of cholesterol and sphingomyelin for BVDV entry. Surprisingly, despite a high cholesterol and sphingolipid content of BVDV envelope, E2 was not found in detergent-resistant membranes. Our results indicate that there are differences between the structure and molecular composition of viral particles of Flaviviruses, Pestiviruses and Hepaciviruses within the Flaviviridae family.

Published

2016

4. NS2 protein of hepatitis C virus interacts with structural and non-structural proteins towards virus assembly.

Author

Costin-Ioan Popescu, Nathalie Callens, Dave Trinel, Philippe Roingeard, Darius Moradpour, Véronique Descamps, Gilles Duverlie, François Penin, Laurent Héliot, Yves Rouillé, and Jean Dubuisson

Subjects

Immunologic diseases. Allergy, RC581-607, Biology (General), QH301-705.5

Abstract

Growing experimental evidence indicates that, in addition to the physical virion components, the non-structural proteins of hepatitis C virus (HCV) are intimately involved in orchestrating morphogenesis. Since it is dispensable for HCV RNA replication, the non-structural viral protein NS2 is suggested to play a central role in HCV particle assembly. However, despite genetic evidences, we have almost no understanding about NS2 protein-protein interactions and their role in the production of infectious particles. Here, we used co-immunoprecipitation and/or fluorescence resonance energy transfer with fluorescence lifetime imaging microscopy analyses to study the interactions between NS2 and the viroporin p7 and the HCV glycoprotein E2. In addition, we used alanine scanning insertion mutagenesis as well as other mutations in the context of an infectious virus to investigate the functional role of NS2 in HCV assembly. Finally, the subcellular localization of NS2 and several mutants was analyzed by confocal microscopy. Our data demonstrate molecular interactions between NS2 and p7 and E2. Furthermore, we show that, in the context of an infectious virus, NS2 accumulates over time in endoplasmic reticulum-derived dotted structures and colocalizes with both the envelope glycoproteins and components of the replication complex in close proximity to the HCV core protein and lipid droplets, a location that has been shown to be essential for virus assembly. We show that NS2 transmembrane region is crucial for both E2 interaction and subcellular localization. Moreover, specific mutations in core, envelope proteins, p7 and NS5A reported to abolish viral assembly changed the subcellular localization of NS2 protein. Together, these observations indicate that NS2 protein attracts the envelope proteins at the assembly site and it crosstalks with non-structural proteins for virus assembly.

Published

2011

5. Functional and Physical Interaction between the Arf Activator GBF1 and Hepatitis C Virus NS3 Protein

Author

Lucie Goueslain, Yves Rouillé, Rayan Farhat, Nadjet Lebsir, Catherine L. Jackson, Jean Dubuisson, Nathalie Callens, Centre d’Infection et d’Immunité de Lille - INSERM U 1019 - UMR 9017 - UMR 8204 (CIIL), Institut Pasteur de Lille, Réseau International des Instituts Pasteur (RIIP)-Réseau International des Instituts Pasteur (RIIP)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Université de Lille-Centre Hospitalier Régional Universitaire [Lille] (CHRU Lille)-Centre National de la Recherche Scientifique (CNRS), Institut Jacques Monod (IJM (UMR_7592)), Université Paris Diderot - Paris 7 (UPD7)-Centre National de la Recherche Scientifique (CNRS), Centre National de la Recherche Scientifique (CNRS)-Centre Hospitalier Régional Universitaire [Lille] (CHRU Lille)-Université de Lille-Institut National de la Santé et de la Recherche Médicale (INSERM)-Institut Pasteur de Lille, Réseau International des Instituts Pasteur (RIIP)-Réseau International des Instituts Pasteur (RIIP), Centre d’Infection et d’Immunité de Lille (CIIL) - U1019 - UMR 8204 (CIIL), and Réseau International des Instituts Pasteur (RIIP)-Réseau International des Instituts Pasteur (RIIP)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Université de Lille-Centre National de la Recherche Scientifique (CNRS)

Subjects

hepatitis C virus, NS3, Hepatitis C virus, viruses, Immunology, Mutant, Hepacivirus, [SDV.BC.BC]Life Sciences [q-bio]/Cellular Biology/Subcellular Processes [q-bio.SC], Viral Nonstructural Proteins, Biology, Virus Replication, medicine.disease_cause, Microbiology, Genome, Virus, Cell Line, 03 medical and health sciences, Virology, medicine, Guanine Nucleotide Exchange Factors, Humans, 030304 developmental biology, Host factor, 0303 health sciences, 030302 biochemistry & molecular biology, RNA, virus diseases, ADP ribosylation factor, Hepatitis C, digestive system diseases, Virus-Cell Interactions, 3. Good health, Viral replication, Insect Science, [SDV.MP.VIR]Life Sciences [q-bio]/Microbiology and Parasitology/Virology, RNA, Viral, viral replication, GBF1

Abstract

International audience; GBF1 has emerged as a host factor required for the genome replication of RNA viruses of different families. During the hepatitis C virus (HCV) life cycle, GBF1 performs a critical function at the onset of genome replication but is dispensable when the replication is established. To better understand how GBF1 regulates HCV infection, we have looked for interactions between GBF1 and HCV proteins. NS3 was found to interact with GBF1 in yeast two-hybrid, coimmunoprecipitation, and proximity ligation assays and to interfere with GBF1 function and alter GBF1 intracellular localization in cells expressing NS3. The interaction was mapped to the Sec7 domain of GBF1 and the protease domain of NS3. A reverse yeast two-hybrid screen to identify mutations altering NS3-GBF1 interaction yielded an NS3 mutant (N77D, Con1 strain) that is nonreplicative despite conserved protease activity and does not interact with GBF1. The mutated residue is exposed at the surface of NS3, suggesting it is part of the domain of NS3 that interacts with GBF1. The corresponding mutation in strain JFH-1 (S77D) produces a similar phenotype. Our results provide evidence for an interaction between NS3 and GBF1 and suggest that an alteration of this interaction is detrimental to HCV genome replication.IMPORTANCE: Single-stranded, positive-sense RNA viruses rely to a significant extent on host factors to achieve the replication of their genome. GBF1 is such a cellular protein that is required for the replication of several RNA viruses, but its mechanism of action during viral infections is not yet defined. In this study, we investigated potential interactions that GBF1 might engage in with proteins of HCV, a GBF1-dependent virus. We found that GBF1 interacts with NS3, a nonstructural protein involved in HCV genome replication, and our results suggest that this interaction is important for GBF1 function during HCV replication. Interestingly, GBF1 interaction with HCV appears different from its interaction with enteroviruses, another group of GBF1-dependent RNA viruses, in keeping with the fact that HCV and enteroviruses use different functions of GBF1.

Published

2019

6. Identification of a dominant endoplasmic reticulum-retention signal in yellow fever virus pre-membrane protein

Author

Karin Séron, Nathalie Callens, Jean Dubuisson, Yves Rouillé, and Yann Ciczora

Subjects

Endoplasmic reticulum, C-terminus, Molecular Sequence Data, ER retention, Protein Sorting Signals, Biology, Endoplasmic Reticulum, Fusion protein, Virology, Protein Structure, Secondary, Transmembrane protein, Transport protein, Protein Transport, Transmembrane domain, Viral Envelope Proteins, Membrane protein, Yellow Fever, Humans, Amino Acid Sequence, Yellow fever virus, Dimerization, HeLa Cells

Abstract

Yellow fever virus (YFV) encodes two envelope proteins, pre-membrane (prM) and envelope (E), that accumulate in the endoplasmic reticulum (ER). The C termini of prM and E form two antiparallel transmembrane alpha-helices that contain ER-retention signals. To understand further the ER retention of the prME heterodimer, we characterized the subcellular localization of chimeric proteins made of a reporter protein fused to the transmembrane segments of YFV envelope proteins. We showed that at least three of the transmembrane segments of the prME heterodimer are ER-retention signals. Interestingly, increasing the length of these alpha-helices led to the export of the chimeric proteins out of the ER. Furthermore, adding a diacidic export signal at the C terminus of the first transmembrane segment of the E protein also induced export to the cell surface. However, adding this export signal at the C terminus of the first transmembrane segment of E in the context of prME did not change the subcellular localization of the prME heterodimer, suggesting the presence of a stronger ER-retention signal outside the first transmembrane segment of E. Importantly, the diacidic export motif added to the C terminus of the first transmembrane segment of the prM protein was not sufficient to export a chimeric protein out of the ER, indicating that this sequence is a dominant ER-retention signal. Together, these data indicate that a combination of several signals of different strengths contributes to the ER retention of the YFV envelope protein heterodimer.

Published

2009

7. Contribution of the charged residues of hepatitis C virus glycoprotein E2 transmembrane domain to the functions of the E1E2 heterodimer

Author

Claire Montpellier, Anne Op De Beeck, Birke Bartosch, François-Loïc Cosset, Jean Dubuisson, Yann Ciczora, and Nathalie Callens

Subjects

Protein Folding, Hepacivirus, Biology, Endoplasmic Reticulum, medicine.disease_cause, Cell Line, Cell membrane, Structure-Activity Relationship, Viral Envelope Proteins, Virology, medicine, Humans, Glycoproteins, chemistry.chemical_classification, Mutation, Endoplasmic reticulum, Cell Membrane, ER retention, Transmembrane protein, Protein Structure, Tertiary, Transmembrane domain, medicine.anatomical_structure, chemistry, Biochemistry, Glycoprotein, Biogenesis

Abstract

The envelope glycoproteins of Hepatitis C virus (HCV), E1 and E2, form a heterodimer that is retained in the endoplasmic reticulum (ER). The transmembrane (TM) domains play a major role in E1E2 heterodimerization and in ER retention. Two fully conserved charged residues in the middle of the TM domain of E2 (Asp and Arg) are crucial for these functions. Replacement of the Asp residue by a Leu impaired E1E2 heterodimerization, whereas the Arg-to-Leu mutation had a milder effect. Both Asp and Arg residues were shown to contribute to the ER retention function of E2. In addition, the entry function of HCV envelope glycoproteins was affected by these mutations. Together, these data indicate that the charged residues present in the TM domain of E2 play a major role in the biogenesis and the entry function of the E1E2 heterodimer. However, the Asp and Arg residues do not contribute equally to these functions.

Published

2005

8. High Density Lipoproteins Facilitate Hepatitis C Virus Entry through the Scavenger Receptor Class B Type I

Author

Emmanuelle Blanchard, Anne Op De Beeck, Nathalie Callens, Cécile Voisset, Jean Dubuisson, Ngoc Vu-Dac, Assemblage et réplication du virus de l'hépatite C (ARVHC), and Centre National de la Recherche Scientifique (CNRS)

Subjects

CD36 Antigens, Sucrose, Hepatitis C virus, Down-Regulation, Hepacivirus, Biology, Ligands, medicine.disease_cause, Biochemistry, Cell Line, 03 medical and health sciences, 0302 clinical medicine, Viral Envelope Proteins, RNA interference, Centrifugation, Density Gradient, medicine, Humans, Immunoprecipitation, Gene silencing, Gene Silencing, RNA, Small Interfering, Receptors, Immunologic, Scavenger receptor, Receptor, Molecular Biology, Glycoproteins, 030304 developmental biology, Receptors, Scavenger, chemistry.chemical_classification, 0303 health sciences, Dose-Response Relationship, Drug, Cell Biology, Scavenger Receptors, Class B, Entry into host, Ligand (biochemistry), Lipids, Virology, 3. Good health, chemistry, [SDV.MP.VIR]Life Sciences [q-bio]/Microbiology and Parasitology/Virology, RNA Interference, lipids (amino acids, peptides, and proteins), 030211 gastroenterology & hepatology, Lipoproteins, HDL, Glycoprotein, Protein Binding

Abstract

The scavenger receptor class B type I (SR-BI) has recently been shown to interact with hepatitis C virus (HCV) envelope glycoprotein E2, suggesting that it might be involved at some step of HCV entry into host cells. However, due to the absence of a cell culture system to efficiently amplify HCV, it is not clear how SR-BI contributes to HCV entry. Here, we sought to determine how high density lipoproteins (HDLs), the natural ligand of SR-BI, affect HCV entry. By using the recently described infectious HCV pseudotyped particles (HCVpps) that display functional E1E2 glycoprotein complexes, we showed that HDLs are able to markedly enhance HCVpp entry. We did not find any evidence of HDL association with HCVpps, suggesting that HCVpps do not enter into target cells using HDL as a carrier to bind to its receptor. Interestingly, lipid-free apoA-I and apoA-II, the major HDL apolipoproteins, were unable to enhance HCVpp infectivity. In addition, drugs inhibiting HDL cholesteryl transfer (block lipid transport (BLT)-2 and BLT-4) reduced HDL enhancement of HCVpp entry, suggesting a role for lipid transfer in facilitating HCVpp entry. Importantly, silencing of SR-BI expression in target cells by RNA interference markedly reduced HDL-mediated enhancement of HCVpp entry. Finally, enhancement of HCVpp entry was also suppressed when the SR-BI binding region on HCV glycoprotein E2 was deleted. Altogether, these data indicate that HDL-mediated enhancement of HCVpp entry involves a complex interplay between SR-BI, HDL, and HCV envelope glycoproteins, and they highlight the active role of HDLs in HCV entry.

Published

2005

9. FEV acts as a transcriptional repressor through its DNA-binding ETS domain and alanine-rich domain

Author

Philippe Maurer, Carmen Brenner, Yvan de Launoit, Carine Van Lint, Nathalie Callens, Laurent Coutte, and Jean-Luc Baert

Subjects

Cancer Research, Transcription, Genetic, medicine.drug_class, Repressor, Biology, Response Elements, Transfection, Cell Line, Transcription (biology), Proto-Oncogene Proteins, Tumor Cells, Cultured, Genetics, medicine, Animals, Humans, Gene Silencing, Nuclear protein, Molecular Biology, Psychological repression, Transcription factor, Cell Nucleus, Alanine, Proto-Oncogene Proteins c-ets, General transcription factor, Histone deacetylase inhibitor, Nuclear Proteins, Molecular biology, Protein Structure, Tertiary, respiratory tract diseases, DNA-Binding Proteins, Repressor Proteins, COS Cells, Rabbits, Repressor lexA, Transcription Factors, circulatory and respiratory physiology

Abstract

Although most Ets transcription factors have been characterized as transcriptional activators, some of them display repressor activity. Here we characterize an Ets-family member, the very specifically expressed human Fifth Ewing Variant (FEV), as a transcriptional repressor. We show that among a broad range of human cell lines, only Dami megakaryocytic cells express FEV. This nuclear protein binds to Ets-binding sites, such as that of the human ICAM-1 promoter. We used this promoter to demonstrate that FEV can repress both basal transcription and, even more strongly, ectopically Ets-activated transcription. We identified two domains responsible for FEV-mediated repression: the ETS domain, responsible for passive repression, and the carboxy-terminal alanine-rich domain, involved in active repression. In the Ets-independent LEXA system also, FEV acts as a transcriptional repressor via its alanine-rich carboxy-terminal domain. The mechanism by which FEV actively represses transcription is currently unknown, since FEV-triggered repression is not reversed by the histone deacetylase inhibitor trichostatin A. We also showed that long-term overexpression of FEV proteins containing the alanine-rich domain prevents cell clones from growing, whereas clones expressing a truncated FEV protein lacking this domain develop like control cells. This confirms the importance of this domain in FEV-triggered repression.

Published

2003

10. Genomic organization and expression of the mouse Brca2 gene

Author

Nathalie Callens, Agnès Begue, Yvan de Launoit, Carine Van Lint, Jacques Simard, Martine Dumont, and Jean-Luc Baert

Subjects

Gene isoform, Therapeutic gene modulation, Molecular Sequence Data, Pair-rule gene, Biology, Gene product, Mice, Sequence Homology, Nucleic Acid, Gene cluster, Genetics, Animals, Humans, RNA, Messenger, Promoter Regions, Genetic, Enhancer, Sequence Deletion, BRCA2 Protein, Base Sequence, Gene Expression Profiling, Chromosome Mapping, Promoter, 3T3 Cells, Exons, Molecular biology, Introns, Gene Expression Regulation, Organ Specificity, PAX6, Transcription Initiation Site

Abstract

A mutation of the Brca2 gene product is responsible for a large proportion of the inherited breast cancers. Here, we have demonstrated that the mouse Brca2 gene is composed of 27 exons and 26 introns, spanning approximately 48 kbp, almost all intron-exon junctions being classical. The overall mouse Brca2 gene structure is highly similar in the coding sequences to that of the human gene. The predicted 11-kb transcript is predominantly present in testis, spleen, thymus, epididymis, and seminal vesicles. A smaller-size, strong positive hybridization signal, which was obtained by using 5' end exons as probes, is ubiquitously observed in mouse tissues. The exact origin and function of this small transcript is currently unknown. The transcription start site of this gene has been identified at approximately 300 bp upstream from the translation initiation codon, and the first 148 bp proximal TATA-less promoter region is sufficient to activate maximal transcription of this gene in mammary cells.

Published

2002

11. NS2 Protein of Hepatitis C Virus Interacts with Structural and Non-Structural Proteins towards Virus Assembly

Author

François Penin, Darius Moradpour, Philippe Roingeard, Yves Rouillé, Nathalie Callens, Gilles Duverlie, Costin-Ioan Popescu, Véronique Descamps, Jean Dubuisson, Dave Trinel, and Laurent Héliot

Subjects

Models, Molecular, Viral protein, QH301-705.5, viruses, Molecular Sequence Data, Immunology, Hepacivirus, Plasma protein binding, Viral Nonstructural Proteins, Biology, medicine.disease_cause, Models, Biological, Microbiology, Virus, Protein–protein interaction, Viral Proteins, Protein structure, Viral Envelope Proteins, Virology, Genetics, medicine, Humans, Protein Interaction Domains and Motifs, Tissue Distribution, Amino Acid Sequence, Biology (General), Virology/Virion Structure, Assembly, and Egress, NS5A, Molecular Biology, Cells, Cultured, Viral Core Proteins, Virus Assembly, virus diseases, biochemical phenomena, metabolism, and nutrition, RC581-607, Cell biology, NS2-3 protease, Viral replication, Parasitology, Hepacivirus/genetics, Hepacivirus/metabolism, Protein Binding, Protein Interaction Domains and Motifs/genetics, Protein Interaction Domains and Motifs/physiology, Viral Core Proteins/metabolism, Viral Envelope Proteins/chemistry, Viral Envelope Proteins/metabolism, Viral Nonstructural Proteins/chemistry, Viral Nonstructural Proteins/genetics, Viral Proteins/genetics, Viral Proteins/metabolism, Virus Assembly/genetics, Virus Assembly/physiology, Immunologic diseases. Allergy, Research Article

Abstract

Growing experimental evidence indicates that, in addition to the physical virion components, the non-structural proteins of hepatitis C virus (HCV) are intimately involved in orchestrating morphogenesis. Since it is dispensable for HCV RNA replication, the non-structural viral protein NS2 is suggested to play a central role in HCV particle assembly. However, despite genetic evidences, we have almost no understanding about NS2 protein-protein interactions and their role in the production of infectious particles. Here, we used co-immunoprecipitation and/or fluorescence resonance energy transfer with fluorescence lifetime imaging microscopy analyses to study the interactions between NS2 and the viroporin p7 and the HCV glycoprotein E2. In addition, we used alanine scanning insertion mutagenesis as well as other mutations in the context of an infectious virus to investigate the functional role of NS2 in HCV assembly. Finally, the subcellular localization of NS2 and several mutants was analyzed by confocal microscopy. Our data demonstrate molecular interactions between NS2 and p7 and E2. Furthermore, we show that, in the context of an infectious virus, NS2 accumulates over time in endoplasmic reticulum-derived dotted structures and colocalizes with both the envelope glycoproteins and components of the replication complex in close proximity to the HCV core protein and lipid droplets, a location that has been shown to be essential for virus assembly. We show that NS2 transmembrane region is crucial for both E2 interaction and subcellular localization. Moreover, specific mutations in core, envelope proteins, p7 and NS5A reported to abolish viral assembly changed the subcellular localization of NS2 protein. Together, these observations indicate that NS2 protein attracts the envelope proteins at the assembly site and it crosstalks with non-structural proteins for virus assembly., Author Summary Hepatitis C virus (HCV) causes major health problems worldwide. Understanding the major steps of the life cycle of this virus is essential to developing new and more efficient antiviral molecules. Virus assembly is the least understood step of the HCV life cycle. Growing experimental evidence indicates that, in addition to the physical virion components, the HCV non-structural proteins are intimately involved in orchestrating morphogenesis. Since it is dispensable for HCV RNA replication, the non-structural viral protein NS2 is suggested to play a central role in HCV particle assembly. Molecular interactions between NS2 and other HCV proteins were demonstrated. Furthermore, NS2 was shown to accumulate over time in endoplasmic reticulum-derived structures and to colocalize with the viral envelope glycoproteins and viral components of the replication complex in close proximity to the HCV core protein and lipid droplets. Importantly, specific mutations within NS2 that affected HCV infectivity could also alter the subcellular localization of NS2 protein and its interactions, suggesting that this subcellular localization and its interactions are essential for HCV particle assembly. Altogether, these observations indicate that NS2 protein plays an important role in connecting different viral components that are essential for virus assembly.

Published

2011

12. Transmembrane domains of hepatitis C virus envelope glycoproteins: residues involved in E1E2 heterodimerization and involvement of these domains in virus entry

Author

Jean Dubuisson, Nathalie Callens, François Penin, Eve-Isabelle Pécheur, Yann Ciczora, Institut de biologie et chimie des protéines [Lyon] (IBCP), Université Claude Bernard Lyon 1 (UCBL), Université de Lyon-Université de Lyon-Centre National de la Recherche Scientifique (CNRS), and Deleage, Gilbert

Subjects

Immunology, Mutant, Molecular Sequence Data, Hepacivirus, Biology, Microbiology, Cell Line, 03 medical and health sciences, Viral Envelope Proteins, Viral entry, Virology, [SDV.BBM] Life Sciences [q-bio]/Biochemistry, Molecular Biology, Humans, [SDV.BBM]Life Sciences [q-bio]/Biochemistry, Molecular Biology, Amino Acid Sequence, Protein Structure, Quaternary, Peptide sequence, 030304 developmental biology, chemistry.chemical_classification, 0303 health sciences, Virulence, Structure and Assembly, 030302 biochemistry & molecular biology, Wild type, Tryptophan, Alanine scanning, Virus Internalization, Transmembrane protein, 3. Good health, Protein Structure, Tertiary, Transmembrane domain, chemistry, Biochemistry, Amino Acid Substitution, Insect Science, Mutagenesis, Site-Directed, Glycoprotein, Dimerization

Abstract

International audience; The transmembrane (TM) domains of hepatitis C virus (HCV) envelope glycoproteins E1 and E2 have been shown to play multiple roles during the biogenesis of the E1E2 heterodimer. By using alanine scanning insertion mutagenesis within the TM domains of HCV envelope glycoproteins, we have previously shown that the central regions of these domains as well as the N-terminal part of the TM domain of E1 are involved in heterodimerization. Here, we used a tryptophan replacement scan of these regions to identify individual residues that participate in those interactions. Our mutagenesis study identified at least four residues involved in heterodimerization: Gly 354, Gly 358, Lys 370, and Asp 728. Interestingly, Gly 354 and Gly 358 belong to a GXXXG oligomerization motif. Our tryptophan mutants were also used to generate retrovirus-based, HCV-pseudotyped particles (HCVpp) in order to analyze the effects of these mutations on virus entry. Surprisingly, two mutants consistently displayed higher infectivity compared to that of the wild type. In contrast, HCVpp infectivity was strongly affected for many mutants, despite normal E1E2 heterodimerization and normal levels of incorporation of HCV glycoproteins into HCVpp. The characterization of some of these HCVpp mutants in the recently developed in vitro fusion assay using fluorescent-labeled liposomes indicated that mutations reducing HCVpp infectivity without altering E1E2 heterodimerization affected the fusion properties of HCV envelope glycoproteins. In conclusion, this mutational analysis identified residues involved in E1E2 heterodimerization and revealed that the TM domains of HCV envelope glycoproteins play a major role in the fusion properties of these proteins.The transmembrane (TM) domains of hepatitis C virus (HCV) envelope glycoproteins E1 and E2 have been shown to play multiple roles during the biogenesis of the E1E2 heterodimer. By using alanine scanning insertion mutagenesis within the TM domains of HCV envelope glycoproteins, we have previously shown that the central regions of these domains as well as the N-terminal part of the TM domain of E1 are involved in heterodimerization. Here, we used a tryptophan replacement scan of these regions to identify individual residues that participate in those interactions. Our mutagenesis study identified at least four residues involved in heterodimerization: Gly 354, Gly 358, Lys 370, and Asp 728. Interestingly, Gly 354 and Gly 358 belong to a GXXXG oligomerization motif. Our tryptophan mutants were also used to generate retrovirus-based, HCV-pseudotyped particles (HCVpp) in order to analyze the effects of these mutations on virus entry. Surprisingly, two mutants consistently displayed higher infectivity compared to that of the wild type. In contrast, HCVpp infectivity was strongly affected for many mutants, despite normal E1E2 heterodimerization and normal levels of incorporation of HCV glycoproteins into HCVpp. The characterization of some of these HCVpp mutants in the recently developed in vitro fusion assay using fluorescent-labeled liposomes indicated that mutations reducing HCVpp infectivity without altering E1E2 heterodimerization affected the fusion properties of HCV envelope glycoproteins. In conclusion, this mutational analysis identified residues involved in E1E2 heterodimerization and revealed that the TM domains of HCV envelope glycoproteins play a major role in the fusion properties of these proteins.

Published

2007

13. Basic Residues in Hypervariable Region 1 of Hepatitis C Virus Envelope Glycoprotein E2 Contribute to Virus Entry

Author

Birke Bartosch, François Penin, Yann Ciczora, Jean Dubuisson, Nathalie Callens, Ngoc Vu-Dac, François-Loïc Cosset, Jean-Michel Pawlotsky, Institut de biologie et chimie des protéines [Lyon] (IBCP), Université Claude Bernard Lyon 1 (UCBL), Université de Lyon-Université de Lyon-Centre National de la Recherche Scientifique (CNRS), and Deleage, Gilbert

Subjects

viruses, Immunology, Mutant, Hepacivirus, Biology, Microbiology, Virus, 03 medical and health sciences, Viral Proteins, 0302 clinical medicine, Viral envelope, Viral Envelope Proteins, Viral entry, Virology, [SDV.BBM] Life Sciences [q-bio]/Biochemistry, Molecular Biology, Tumor Cells, Cultured, Humans, [SDV.BBM]Life Sciences [q-bio]/Biochemistry, Molecular Biology, 030304 developmental biology, Infectivity, chemistry.chemical_classification, 0303 health sciences, virus diseases, digestive system diseases, 3. Good health, Hypervariable region, Virus-Cell Interactions, chemistry, Insect Science, 030211 gastroenterology & hepatology, Glycoprotein, CD81

Abstract

International audience; The N terminus of hepatitis C virus (HCV) envelope glycoprotein E2 contains a hypervariable region (HVR1) which has been proposed to play a role in viral entry. Despite strong amino acid variability, HVR1 is globally basic, with basic residues located at specific sequence positions. Here we show by analyzing a large number of HVR1 sequences that the frequency of basic residues at each position is genotype dependent. We also used retroviral pseudotyped particles (HCVpp) harboring genotype 1a envelope glycoproteins to study the role of HVR1 basic residues in entry. Interestingly, HCVpp infectivity globally increased with the number of basic residues in HVR1. However, a shift in position of some charged residues also modulated HCVpp infectivity. In the absence of basic residues, infectivity was reduced to the same level as that of a mutant deleted of HVR1. We also analyzed the effect of these mutations on interactions with some potential HCV receptors. Recognition of CD81 was not affected by changes in the number of charged residues, and we did not find a role for heparan sulfates in HCVpp entry. The involvement of the scavenger receptor class B type I (SR-BI) was indirectly analyzed by measuring the enhancement of infectivity of the mutants in the presence of the natural ligand of SR-BI, high-density lipoproteins (HDL). However, no correlation between the number of basic residues within HVR1 and HDL enhancement effect was observed. Despite the lack of evidence of the involvement of known potential receptors, our results demonstrate that the presence of basic residues in HVR1 facilitates virus entry.The N terminus of hepatitis C virus (HCV) envelope glycoprotein E2 contains a hypervariable region (HVR1) which has been proposed to play a role in viral entry. Despite strong amino acid variability, HVR1 is globally basic, with basic residues located at specific sequence positions. Here we show by analyzing a large number of HVR1 sequences that the frequency of basic residues at each position is genotype dependent. We also used retroviral pseudotyped particles (HCVpp) harboring genotype 1a envelope glycoproteins to study the role of HVR1 basic residues in entry. Interestingly, HCVpp infectivity globally increased with the number of basic residues in HVR1. However, a shift in position of some charged residues also modulated HCVpp infectivity. In the absence of basic residues, infectivity was reduced to the same level as that of a mutant deleted of HVR1. We also analyzed the effect of these mutations on interactions with some potential HCV receptors. Recognition of CD81 was not affected by changes in the number of charged residues, and we did not find a role for heparan sulfates in HCVpp entry. The involvement of the scavenger receptor class B type I (SR-BI) was indirectly analyzed by measuring the enhancement of infectivity of the mutants in the presence of the natural ligand of SR-BI, high-density lipoproteins (HDL). However, no correlation between the number of basic residues within HVR1 and HDL enhancement effect was observed. Despite the lack of evidence of the involvement of known potential receptors, our results demonstrate that the presence of basic residues in HVR1 facilitates virus entry.

Published

2005

14. Role of N-linked glycans in the functions of hepatitis C virus envelope glycoproteins

Author

Claire Montpellier, Anne Goffard, Nathalie Callens, Jean Dubuisson, François-Loïc Cosset, Czeslaw Wychowski, Birke Bartosch, Dubuisson, Jean, Assemblage et réplication du virus de l'hépatite C (ARVHC), and Centre National de la Recherche Scientifique (CNRS)

Subjects

Glycan, Carcinoma, Hepatocellular, Glycosylation, Hepacivirus, Hepatitis C virus, Immunology, medicine.disease_cause, Microbiology, 03 medical and health sciences, chemistry.chemical_compound, Viral envelope, Polysaccharides, Cell Line, Tumor, Virology, medicine, Humans, 030304 developmental biology, chemistry.chemical_classification, [SDV.MP.VIR] Life Sciences [q-bio]/Microbiology and Parasitology/Virology, 0303 health sciences, Signal peptidase, biology, Structure and Assembly, Endoplasmic reticulum, Liver Neoplasms, 030302 biochemistry & molecular biology, Gene Products, env, biology.organism_classification, 3. Good health, chemistry, Biochemistry, Mutagenesis, Insect Science, [SDV.MP.VIR]Life Sciences [q-bio]/Microbiology and Parasitology/Virology, biology.protein, Glycoprotein, Plasmids

Abstract

Hepatitis C virus (HCV) encodes two viral envelope glycoproteins. E1 contains 4 or 5 N-linked glycosylation sites and E2 contains up to 11, with most of the sites being well conserved, suggesting that they play an essential role in some functions of these proteins. For this study, we used retroviral pseudotyped particles harboring mutated HCV envelope glycoproteins to study these glycans. The mutants were named with an N followed by a number related to the relative position of the potential glycosylation site in each glycoprotein (E1N1 to E1N4 for E1 mutants and E2N1 to E2N11 for E2 mutants). The characterization of these mutants allowed us to define three phenotypes. For the first group (E1N3, E2N3, E2N5, E2N6, E2N7, and E2N9), the infectivities of the mutants were close to that of the wild type. The second group (E1N1, E1N2, E1N4, E2N1, and E2N11) contained mutants that were still infectious but whose infectivities were reduced to

Published

2005

15. Transcriptional regulation of the murine brca2 gene by CREB/ATF transcription factors

Author

Jean-Luc Baert, Yvan de Launoit, Nathalie Callens, Carine Van Lint, Didier Monté, and Morten Sunesen

Subjects

Teratocarcinoma, Transcriptional Activation, endocrine system diseases, Response element, Genes, BRCA2, Biophysics, Activating transcription factor, E-box, Biology, CREB, Biochemistry, Cell Line, ATF/CREB, Cyclic AMP Response Element Modulator, Mice, Structure-Activity Relationship, Cell Line, Tumor, Animals, skin and connective tissue diseases, Enhancer, Cyclic AMP Response Element-Binding Protein, Promoter Regions, Genetic, Molecular Biology, BRCA2 Protein, General transcription factor, Promoter, Epithelial Cells, Cell Biology, Blood Proteins, Molecular biology, Activating Transcription Factors, DNA-Binding Proteins, Repressor Proteins, Gene Expression Regulation, biology.protein, NIH 3T3 Cells, Transcription Factors

Abstract

The brca2 gene encodes a nuclear protein which is mainly involved in DNA repair and, when mutated, is responsible for some of the hereditary breast cancers. However, brca2 expression is also deregulated in sporadic breast tumors. In the mouse brca2 gene we had earlier identified a region of 148bp upstream of the transcription start site sufficient to activate its expression. In the present report, we show that the -92 to -40bp region is essential for the transcription of brca2 in murine mammary cells and that this nucleotide sequence contains one putative CREB/ATF consensus site (cAMP responsive element: CRE). We demonstrated that the mutation of this binding site led to a highly significant reduction of the mouse brca2 transcription, and that CREB, CREM, and/or ATF-1 functionally bound to and regulated this promoter. Therefore, the regulation of the promoter of the mouse brca2 gene is driven by this family of transcription factors.

Published

2003