Your search keyword '"CD81 antigen"' showing total 20 results

1. Hepatitis C virus enters liver cells using the CD81 receptor complex proteins calpain-5 and CBLB.

Author

Bruening, Janina, Lasswitz, Lisa, Banse, Pia, Kahl, Sina, Marinach, Carine, Vondran, Florian W., Kaderali, Lars, Silvie, Olivier, Pietschmann, Thomas, Meissner, Felix, and Gerold, Gisa

Subjects

*HEPATITIS C virus, *MALARIA, *PLASMODIUM, *CD81 antigen, *LIVER cells

Abstract

Hepatitis C virus (HCV) and the malaria parasite Plasmodium use the membrane protein CD81 to invade human liver cells. Here we mapped 33 host protein interactions of CD81 in primary human liver and hepatoma cells using high-resolution quantitative proteomics. In the CD81 protein network, we identified five proteins which are HCV entry factors or facilitators including epidermal growth factor receptor (EGFR). Notably, we discovered calpain-5 (CAPN5) and the ubiquitin ligase Casitas B-lineage lymphoma proto-oncogene B (CBLB) to form a complex with CD81 and support HCV entry. CAPN5 and CBLB were required for a post-binding and pre-replication step in the HCV life cycle. Knockout of CAPN5 and CBLB reduced susceptibility to all tested HCV genotypes, but not to other enveloped viruses such as vesicular stomatitis virus and human coronavirus. Furthermore, Plasmodium sporozoites relied on a distinct set of CD81 interaction partners for liver cell entry. Our findings reveal a comprehensive CD81 network in human liver cells and show that HCV and Plasmodium highjack selective CD81 interactions, including CAPN5 and CBLB for HCV, to invade cells. [ABSTRACT FROM AUTHOR]

Published

2018

2. Structure-Guided Combinatorial Engineering Facilitates Affinity and Specificity Optimization of Anti-CD81 Antibodies.

Author

Nelson, Bryce, Adams, Jarrett, Kuglstatter, Andreas, Li, Zhijian, Harris, Seth F., Liu, Yang, Bohini, Sandya, Ma, Han, Klumpp, Klaus, Gao, Junjun, and Sidhu, Sachdev S.

Subjects

*IMMUNOGLOBULINS, *HEPATITIS C virus, *SURFACE plasmon resonance, *CD81 antigen, *KRA

Abstract

Hepatitis C viral infection is the major cause of chronic hepatitis that affects as many as 71 million people worldwide. Rather than target the rapidly shifting viruses and their numerous serotypes, four independent antibodies were made to target the host antigen CD81 and were shown to block hepatitis C viral entry. The single-chain variable fragment of each antibody was crystallized in complex with the CD81 large extracellular loop in order to guide affinity maturation of two distinct antibodies by phage display. Affinity maturation of antibodies using phage display has proven to be critical to therapeutic antibody development and typically involves modification of the paratope for increased affinity, improved specificity, enhanced stability or a combination of these traits. One antibody was engineered for increased affinity for human CD81 large extracellular loop that equated to increased efficacy, while the second antibody was engineered for cross-reactivity with cynomolgus CD81 to facilitate animal model testing. The use of structures to guide affinity maturation library design demonstrates the utility of combining structural analysis with phage display technologies. [ABSTRACT FROM AUTHOR]

Published

2018

3. A Sequence in the loop domain of hepatitis C virus E2 protein identified in silico as crucial for the selective binding to human CD81.

Author

Chang, Chun-Chun, Hsu, Hao-Jen, Yen, Jui-Hung, Lo, Shih-Yen, and Liou, Je-Wen

Subjects

*HEPATITIS C virus, *CD81 antigen, *CHIMPANZEES, *MOLECULAR docking, *SURFACE plasmon resonance

Abstract

Hepatitis C virus (HCV) is a species-specific pathogenic virus that infects only humans and chimpanzees. Previous studies have indicated that interactions between the HCV E2 protein and CD81 on host cells are required for HCV infection. To determine the crucial factors for species-specific interactions at the molecular level, this study employed in silico molecular docking involving molecular dynamic simulations of the binding of HCV E2 onto human and rat CD81s. In vitro experiments including surface plasmon resonance measurements and cellular binding assays were applied for simple validations of the in silico results. The in silico studies identified two binding regions on the HCV E2 loop domain, namely E2-site1 and E2-site2, as being crucial for the interactions with CD81s, with the E2-site2 as the determinant factor for human-specific binding. Free energy calculations indicated that the E2/CD81 binding process might follow a two-step model involving (i) the electrostatic interaction-driven initial binding of human-specific E2-site2, followed by (ii) changes in the E2 orientation to facilitate the hydrophobic and van der Waals interaction-driven binding of E2-site1. The sequence of the human-specific, stronger-binding E2-site2 could serve as a candidate template for the future development of HCV-inhibiting peptide drugs. [ABSTRACT FROM AUTHOR]

Published

2017

4. Mice Expressing Minimally Humanized CD81 and Occludin Genes Support Hepatitis C Virus Uptake In Vivo.

Author

Qiang Ding, von Schaewen, Markus, Hrebikova, Gabriela, Heller, Brigitte, Sandmann, Lisa, Plaas, Mario, and Ploss, Alexander

Subjects

*CD81 antigen, *OCCLUDINS, *HEPATITIS C virus, *AMINO acid sequence, *LABORATORY mice

Abstract

Hepatitis C virus (HCV) causes chronic infections in at least 150 million individuals worldwide. HCV has a narrow host range and robustly infects only humans and chimpanzees. The underlying mechanisms for this narrow host range are incompletely understood. At the level of entry, differences in the amino acid sequences between the human and mouse orthologues of two essential host factors, the tetraspanin CD81 and the tight junction protein occludin (OCLN), explain, at least in part, HCV's limited ability to enter mouse hepatocytes. We have previously shown that adenoviral or transgenic overexpression of human CD81 and OCLN facilitates HCV uptake into mouse hepatocytes in vitro and in vivo. In efforts to refine these models, we constructed knock-in mice in which the second extracellular loops of CD81 and OCLN were replaced with the respective human sequences, which contain the determinants that are critical for HCV uptake. We demonstrate that the humanized CD81 and OCLN were expressed at physiological levels in a tissue-appropriate fashion. Mice bearing the humanized alleles formed normal tight junctions and did not exhibit any immunologic abnormalities, indicating that interactions with their physiological ligands were intact. HCV entry factor knock-in mice take up HCV with an efficiency similar to that in mice expressing HCV entry factors transgenically or adenovirally, demonstrating the utility of this model for studying HCV infection in vivo. [ABSTRACT FROM AUTHOR]

Published

2017

5. Mechanism of Structural Tuning of the Hepatitis C Virus Human Cellular Receptor CD81 Large Extracellular Loop.

Author

Cunha, Eva S., Sfriso, Pedro, Rojas, Adriana L., Hospital, Adam, Orozco, Modesto, and Abrescia, Nicola G.A.

Subjects

*HEPATITIS C virus, *BIOCHEMICAL mechanism of action, *CD81 antigen, *EXTRACELLULAR fluid, *TETRASPANIN, *LIVER cells

Abstract

Summary Hepatitis C virus (HCV) enters into human hepatocytes via tetraspanin hCD81. HCV glycoprotein E2 recognizes the “head” subdomain of the large extracellular loop (LEL) of CD81 (hCD81 LEL ), but the precise mechanism of virus cell attachment and entry remains elusive. Here, by combining the structural analysis of a conspicuous number of crystallized CD81 LEL molecules with molecular dynamics simulations, we show that the conformational plasticity of the hCD81 LEL head subdomain is a molecular property of the receptor. The observed closed, intermediate, and open conformations of the head subdomain provide distinct binding platforms. Simulations at pH 7.4 and 4.0 indicate that this dynamism is pH modulated. The crystallized double conformation of the disulfide bridge C157-C175 at the base of the head subdomain identifies this bond as the molecular zipper of the plasticity of hCD81 LEL . We propose that this conformational dependence of hCD81 LEL , which is finely tuned by pH and redox conditions, enables the virus-receptor interactions to diversely re-engage at endosomal conditions. [ABSTRACT FROM AUTHOR]

Published

2017

6. Alirocumab, a Therapeutic Human Antibody to PCSK9, Does Not Affect CD81 Levels or Hepatitis C Virus Entry and Replication into Hepatocytes.

Author

Ramanathan, Aarti, Gusarova, Viktoria, Stahl, Neil, Gurnett-Bander, Anne, and Kyratsous, Christos A.

Subjects

*THERAPEUTIC use of immunoglobulins, *CD81 antigen, *HEPATITIS C virus, *VIRAL replication, *LIVER cells, *PROPROTEIN convertases, *LOW density lipoproteins

Abstract

Background: Proprotein convertase subtilisin/kexin type 9 (PSCK9) is secreted mainly from the liver and binds to the low-density lipoprotein receptor (LDLR), reducing LDLR availability and thus resulting in an increase in LDL-cholesterol. While the LDLR has been implicated in the cell entry process of the hepatitis C virus (HCV), overexpression of an artificial non-secreted, cell membrane-bound form of PCSK9 has also been shown to reduce surface expression of CD81, a major component of the HCV entry complex, leading to concerns that pharmacological inhibition of PCSK9 may increase susceptibility to HCV infection by increasing either CD81 or LDLR availability. Here, we evaluated effects of PCSK9 and PCSK9 blockade on CD81 levels and HCV entry with a physiologically relevant model using native secreted PCSK9 and a monoclonal antibody to PCSK9, alirocumab. Methods and Results: Flow cytometry and Western blotting of human hepatocyte Huh-7 cells showed that, although LDLR levels were reduced when cells were exposed to increasing PCSK9 concentrations, there was no correlation between total or surface CD81 levels and the presence and amount of soluble PCSK9. Moreover, inhibiting PCSK9 with the monoclonal antibody alirocumab did not affect expression levels of CD81. In an in vitro model of HCV entry, addition of soluble PCSK9 or treatment with alirocumab had no effect on the ability of either lentiviral particles bearing the HCV glycoproteins or JFH-1 based cell culture virus to enter hepatocytes. Consistent with these in vitro findings, no differences were observed in hepatic CD81 levels using in vivo mouse models, including Pcsk9-/- mice compared with wild-type controls and hyperlipidemic mice homozygous for human Pcsk9 and heterozygous for Ldlr deletion, treated with either alirocumab or isotype control antibody. Conclusion: These results suggest that inhibition of PCSK9 with alirocumab has no effect on CD81 and does not result in increased susceptibility to HCV entry. [ABSTRACT FROM AUTHOR]

Published

2016

7. CD81 and CLDN1 polymorphisms and hepatitis C virus infection susceptibility: A case–control study.

Author

Sun, Shuang, Jin, Guojiang, and Kang, Hui

Subjects

*HEPATITIS C, *CD81 antigen, *HEPATITIS C virus, *SINGLE nucleotide polymorphisms, *DISEASE susceptibility, *CLAUDINS, *GENETICS

Abstract

CD81 and CLDN1 interact to form a CD81–CLDN1 co-receptor complex that is crucial in hepatitis C virus (HCV) entry. Variations in the two genes were shown to influence immunological functions; therefore, we hypothesized that polymorphisms in these genes may contribute to HCV susceptibility. A case–control study consisting of 461 patients and 461 controls was conducted to explore the associations between CD81 rs708564 and CLDN1 rs893051 and HCV susceptibility in a Chinese population. We found a decreased HCV risk associated with the CD81 rs708564 TT (odds ratio (OR) = 0.66, 95% CI = 0.44–0.98) genotype. The gene–gene interaction between CD81 and CLDN1 polymorphisms also decreased HCV risk in a joint multiplicative manner (OR for the presence of both CD81 rs708564 TT and CLDN1 rs893051 GG genotypes = 0.59, 95% CI = 0.36–0.97). Furthermore, the CD81 rs708564 TT genotype conferred a more pronounced decrease in HCV susceptibility in combination with lower levels of high-density lipoprotein cholesterol (HDL-C; OR = 0.71, 95% CI = 0.52–0.96), and higher levels of low-density lipoprotein cholesterol (OR = 0.24, 95% CI = 0.09–0.65). We also observed a decreased HCV susceptibility in individuals with higher HDL-C levels who carried the CLDN1 rs893051 G/C genotype. These findings suggest that homozygous CD81 rs708564 TT may be a genetic modifier for avoiding HCV infection whether as a sole single nucleotide polymorphism or combined with the CLDN1 rs893051 GG genotype, and this effect is associated with serum levels of lipoprotein. [ABSTRACT FROM AUTHOR]

Published

2015

8. A View of the E2-CD81 Interface at the Binding Site of a Neutralizing Antibody against Hepatitis C Virus.

Author

Harman, Christine, Lilin Zhong, Li Ma, Liu, Peter, Lu Deng, Zhong Zhao, Hailing Yan, Struble, Evi, Virata-Theimer, Maria Luisa, and Pei Zhang

Subjects

*HEPATITIS C virus, *HEPATITIS C treatment, *CD81 antigen, *BINDING sites, *THERAPEUTIC use of immunoglobulins, *CELL membranes

Abstract

Hepatitis C virus (HCV) glycoprotein E2 is considered a major target for generating neutralizing antibodies against HCV, primarily due to its role of engaging host entry factors, such as CD81, a key cell surface protein associated with HCV entry. Based on a series of biochemical analyses in combination with molecular docking, we present a description of a potential binding interface formed between the E2 protein and CD81. The virus side of this interface includes a hydrophobic helix motif comprised of residuesW437LAGLF442, which encompasses the binding site of a neutralizing monoclonal antibody, mAb41. The helical conformation of this motif provides a structural framework for the positioning of residues F442 and Y443, serving as contact points for the interaction with CD81. The cell side of this interface likewise involves a surface-exposed hydrophobic helix, namely, the D-helix of CD81, which coincides with the binding site of 1D6, a monoclonal anti-CD81 antibody known to block HCV entry. Our illustration of this virus-host interface suggests an important role played by theW437LAGLF442 helix of the E2 protein in the hydrophobic interaction with the D-helix of CD81, thereby facilitating our understanding of the mechanism for antibody-mediated neutralization of HCV. [ABSTRACT FROM AUTHOR]

Published

2015

9. Impact of single nucleotide polymorphisms in the essential HCV entry factor CD81 on HCV infectivity and neutralization.

Author

Deest, Maximilian, Westhaus, Sandra, Steinmann, Eike, Manns, Michael P., von Hahn, Thomas, and Ciesek, Sandra

Subjects

*HEPATITIS C treatment, *SINGLE nucleotide polymorphisms, *HEPATITIS C virus, *NEUTRALIZATION (Chemistry), *CD81 antigen, *RNA

Abstract

Highlights: [•] CD81 variants that exist in the human population are fully functional as HCV receptors. [•] RNA replication and release of new particles were not affected by the CD81 variants. [•] Neutralizing CD81 antibodies retained their ability to inhibit HCV infection on target cells with any of the CD81 variants. [•] Presence of CD81 variants would not diminish the efficacy of therapeutic regimens that include CD81-antibodies. [Copyright &y& Elsevier]

Published

2014

10. Cross-linking of CD81 by HCV-E2 protein inhibits human intrahepatic plasmacytoid dendritic cells response to CpG-ODN.

Author

Tu, Zhengkun, Zhang, Ping, Li, Haijun, Niu, Junqi, Jin, Xia, and Su, Lishan

Subjects

*DENDRITIC cells, *PROTEIN crosslinking, *CPG nucleotides, *CD81 antigen, *HEPATITIS C virus, *IMMUNOGLOBULINS, *CELL proliferation, *CELLULAR immunity

Abstract

Highlights: [•] Cross-linking CD81 by HCV-E2 and anti-CD81 antibody inhibit CpG-induced pDCs IFN-α secretion. [•] Cross-linking CD81 by HCV-E2 and anti-CD81 antibody down-regulate HLA-DR, CD80 and CD86 expression on pDCs. [•] Cross-linking CD81 by HCV-E2 and anti-CD81 antibody suppressed pDC proliferation and survival induced by CpG ODN. [•] The blockade of CD81 by soluble anti-CD81 antibody restores pDC response to CpG-ODN. [ABSTRACT FROM AUTHOR]

Published

2013

11. EWI-2wint promotes CD81 clustering that abrogates Hepatitis C Virus entry.

Author

Potel, Julie, Rassam, Patrice, Montpellier, Claire, Kaestner, Laura, Werkmeister, Elisabeth, Tews, Birke A., Couturier, Cyril, Popescu, Costin‐Ioan, Baumert, Thomas F., Rubinstein, Eric, Dubuisson, Jean, Milhiet, Pierre‐Emmanuel, and Cocquerel, Laurence

Subjects

*HEPATITIS C virus, *CD81 antigen, *CLUSTERING of particles, *TETRASPANIN, *MICROSCOPY, *CHEMICAL inhibitors, *GENE expression

Abstract

CD81 is a major receptor for Hepatitis C Virus ( HCV). It belongs to the tetraspanin family whose members form dynamic clusters with numerous partner proteins and with one another, forming tetraspanin-enriched areas in the plasma membrane. In our study, we combined single-molecule microscopy and biochemistry experiments to investigate the clustering and membrane behaviour of CD81 in the context of cells expressing EWI-2wint, a natural inhibitor of HCV entry. Interestingly, we found that EWI-2wint reduces the global diffusion of CD81 molecules due to a decrease of the diffusion rate of mobile CD81molecules and an increase in the proportion of confined molecules. Indeed, we demonstrated that EWI-2wint promotes CD81 clustering and confinement in CD81-enriched areas. In addition, we showed that EWI-2wint influences the colocalization of CD81 with Claudin-1 - a co-receptor required for HCV entry. Together, our results indicate that a change in membrane partitioning of CD81 occurs in the presence of EWI-2wint. This study gives new insights on the mechanism by which HCV enters into its target cells, namely by exploiting the dynamic properties of CD81. [ABSTRACT FROM AUTHOR]

Published

2013

12. Identification of ligands that target the HCV-E2 binding site on CD81.

Author

Olaby, Reem, Azzazy, Hassan, Harris, Rodney, Chromy, Brett, Vielmetter, Jost, and Balhorn, Rod

Subjects

*HEPATITIS C virus, *LIGANDS (Biochemistry), *CELL receptors, *CD81 antigen, *INTERFEROMETRY, *SURFACE plasmon resonance, *GLYCOPROTEINS, *LIVER cells

Abstract

Hepatitis C is a global health problem. While many drug companies have active R&D efforts to develop new drugs for treating Hepatitis C virus (HCV), most target the viral enzymes. The HCV glycoprotein E2 has been shown to play an essential role in hepatocyte invasion by binding to CD81 and other cell surface receptors. This paper describes the use of AutoDock to identify ligand binding sites on the large extracellular loop of the open conformation of CD81 and to perform virtual screening runs to identify sets of small molecule ligands predicted to bind to two of these sites. The best sites selected by AutoLigand were located in regions identified by mutational studies to be the site of E2 binding. Thirty-six ligands predicted by AutoDock to bind to these sites were subsequently tested experimentally to determine if they bound to CD81-LEL. Binding assays conducted using surface Plasmon resonance revealed that 26 out of 36 (72 %) of the ligands bound in vitro to the recombinant CD81-LEL protein. Competition experiments performed using dual polarization interferometry showed that one of the ligands predicted to bind to the large cleft between the C and D helices was also effective in blocking E2 binding to CD81-LEL. [ABSTRACT FROM AUTHOR]

Published

2013

13. Hepatoma polarization limits CD81 and hepatitis C virus dynamics.

Author

Harris, H. J., Clerte, C., Farquhar, M. J., Goodall, M., Hu, K., Rassam, P., Dosset, P., Wilson, G. K., Balfe, P., IJzendoorn, S. C., Milhiet, P. E., and McKeating, J. A.

Subjects

*HEPATOCELLULAR carcinoma, *CD81 antigen, *HEPATITIS C virus, *HEPATOCYTE growth factor, *CYTOSKELETON, *COMPARATIVE studies

Abstract

Many viruses target the polarized epithelial apex during host invasion. In contrast, hepatitis C virus ( HCV) engages receptors at the basal surface of hepatocytes in the polarized liver parenchyma. Hepatocyte polarization limits HCV entry by undefined mechanism(s). Given the recent reports highlighting a role for receptor mobility in pathogen entry, we studied the effect(s) of hepatocyte polarization on viral receptor and HCV pseudoparticle ( HCVpp) dynamics using real-time fluorescence recovery after photobleaching and single particle tracking. Hepatoma polarization reduced CD81 and HCVpp dynamics at the basal membrane. Since cell polarization is accompanied by changes in the actin cytoskeleton and CD81 links to actin via its C-terminus, we studied the dynamics of a mutant CD81 lacking a C-terminal tail ( CD81ΔC) and its effect(s) on HCVpp mobility and infection. CD81ΔC showed an increased frequency of confined trajectories and a reduction of Brownian diffusing molecules compared to wild-type protein in non-polarized cells. However, these changes were notobserved in polarized cells. HCVpp showed a significant reduction in Brownian diffusion and infection of CD81ΔC expressing non-polarized cells. In summary, these data highlight the dynamic nature of CD81 and demonstrate a role for CD81 lateral diffusion to regulate HCV infection in a polarization-dependent manner. [ABSTRACT FROM AUTHOR]

Published

2013

14. Active RNA Replication of Hepatitis C Virus Downregulates CD81 Expression.

Author

Po-Yuan Ke and Chen, Steve S. -L.

Subjects

*HEPATITIS C virus, *RNA, *GENOMES, *CELLS, *REPLICATION factors (Biochemistry), *CD81 antigen

Abstract

So far how hepatitis C virus (HCV) replication modulates subsequent virus growth and propagation still remains largely unknown. Here we determine the impact of HCV replication status on the consequential virus growth by comparing normal and high levels of HCV RNA expression. We first engineered a full-length, HCV genotype 2a JFH1 genome containing a blasticidin-resistant cassette inserted at amino acid residue of 420 in nonstructural (NS) protein 5A, which allowed selection of human hepatoma Huh7 cells stably-expressing HCV. Short-term establishment of HCV stable cells attained a highly- replicating status, judged by higher expressions of viral RNA and protein as well as higher titer of viral infectivity as opposed to cells harboring the same genome without selection. Interestingly, maintenance of highly-replicating HCV stable cells led to decreased susceptibility to HCV pseudotyped particle (HCVpp) infection and downregulated cell surface level of CD81, a critical HCV entry (co)receptor. The decreased CD81 cell surface expression occurred through reduced total expression and cytoplasmic retention of CD81 within an endoplasmic reticulum -associated compartment. Moreover, productive viral RNA replication in cells harboring a JFH1 subgenomic replicon containing a similar blasticidin resistance gene cassette in NS5A and in cells robustly replicating full-length infectious genome also reduced permissiveness to HCVpp infection through decreasing the surface expression of CD81. The downregulation of CD81 surface level in HCV RNA highly-replicating cells thus interfered with reinfection and led to attenuated viral amplification. These findings together indicate that the HCV RNA replication status plays a crucial determinant in HCV growth by modulating the expression and intracellular localization of CD81. [ABSTRACT FROM AUTHOR]

Published

2013

15. Cd81 Interacts with the T Cell Receptor to Suppress Signaling.

Author

Cevik, Safak Isil, Keskin, Nazli, Belkaya, Serkan, Ozlu, Meral Ilcim, Deniz, Emre, Tazebay, Uygar Halis, and Erman, Batu

Subjects

*CD81 antigen, *T cell receptors, *B cells, *HEPATITIS C virus, *MEMBRANE proteins, *YEAST

Abstract

CD81 (TAPA-1) is a ubiquitously expressed tetraspanin protein identified as a component of the B lymphocyte receptor (BCR) and as a receptor for the Hepatitis C Virus. In an effort to identify trans-membrane proteins that interact with the T-cell antigen receptor (TCR), we performed a membrane yeast two hybrid screen and identified CD81 as an interactor of the CD3delta subunit of the TCR. We found that in the absence of CD81, in thymocytes from knockout mice, TCR engagement resulted in stronger signals. These results were recapitulated in T cell lines that express low levels of CD81 through shRNA mediated silencing. Increased signaling did not result from alterations in the levels of TCR on the surface of T lymphocytes. Although CD81 is not essential for normal T lymphocyte development, it plays an important role in regulating TCR and possibly pre-TCR signal transduction by controlling the strength of signaling. CD81 dependent alterations in thymocyte signaling are evident in increased CD5 expression on CD81 deficient double positive (DP) thymocytes. We conclude that CD81 interacts with the T cell receptor to suppress signaling. [ABSTRACT FROM AUTHOR]

Published

2012

16. Anti-hepatitis C virus E2 (HCV/E2) glycoprotein monoclonal antibodies and neutralization interference

Author

Sautto, Giuseppe, Mancini, Nicasio, Diotti, Roberta A., Solforosi, Laura, Clementi, Massimo, and Burioni, Roberto

Subjects

*HEPATITIS C virus, *MONOCLONAL antibodies, *GLYCOPROTEINS, *EPITOPES, *CD81 antigen, *AMINO acids, *MOLECULAR biology, *ANTIVIRAL agents, *THERAPEUTICS

Abstract

Abstract: The suggested HCV escape mechanism consisting in the elicitation of antibody (Ab) subpopulations interfering with the neutralizing activity of other Abs has recently been questioned. In particular, it was originally reported that Abs directed against the 436–447 region (epitope II) of HCV/E2 glycoprotein may interfere with the neutralizing Abs directed against the 412–423 region (epitope I) involved in the binding to CD81. In this paper, we investigate on the molecular features of this phenomenon describing an anti-HCV/E2 monoclonal Ab (mAb) (e509) endowed with a weak neutralizing activity, and whose epitope is centered on epitope II. Interestingly, e509 influenced the potent neutralizing activity of AP33, one of the best characterized anti-HCV/E2 mAb, whereas it did not show any interfering activity against two other broadly neutralizing mAbs (e20 and e137), whose epitopes partially overlap with that of e509 and which possibly displace it from the antigen. These data may give a possible clue to interpret the conflicting studies published to date on the mechanism of interference, suggesting the existence of at least two groups of broadly neutralizing anti-HCV/E2 Abs: (i) those whose epitope is focused on the 412–423 CD81-binding region and whose activity may be hampered by other Abs directed against the 436–447 region, and (ii) those directed against CD81-binding regions but whose epitope contains also residues within the 436–447 region recognized by interfering mAbs, thus competing with them for binding. The conflicting results of previous studies may therefore depend on the relative amount of each of these two populations in the polyclonal preparations used. Overall, a better comprehension of this phenomenon may be of importance in the set up of novel mAb-based anti-HCV therapeutic strategies. [Copyright &y& Elsevier]

Published

2012

17. Cd81 Interacts with the T Cell Receptor to Suppress Signaling

Author

Safak Isil Cevik, Nazli Keskin, Meral Ilcim Ozlu, Serkan Belkaya, Uygar H. Tazebay, Batu Erman, and Emre Deniz

Subjects

Proteomics, Mouse, cell maturation, Lymphocyte proliferation, Cell Communication, Signal transduction, Lymphocyte Activation, Biochemistry, gene silencing, Mice, 0302 clinical medicine, Signal Initiation, CD81 antigen, Cytotoxic T cell, Lymphoid Organs, Membrane Receptor Signaling, lcsh:Science, 0303 health sciences, Thymocytes, TCR signaling cascade, Mus, Mechanisms of Signal Transduction, Signaling cascades, Flow Cytometry, 3. Good health, Thymocyte, Immunologic Receptor Signaling, Cell signaling, immunoregulation, lymphocyte differentiation, T cell, Immune Cells, Immunology, lymphocyte proliferation, CD5 Antigens, Transfection, Tetraspanin 28, 03 medical and health sciences, T lymphocyte receptor delta chain, short hairpin RNA, Humans, human, protein expression, Biology, human cell, intracellular signaling, lcsh:R, thymocyte, Proteins, biochemical phenomena, metabolism, and nutrition, Molecular Development, Signaling, CD3 antigen, lcsh:Q, Cytometry, Developmental Biology, Anatomy and Physiology, viruses, lcsh:Medicine, Gene Expression, Antigens, CD5, Antigens, CD81, Molecular cell biology, Immune Physiology, RNA, Small Interfering, Mice, Knockout, Multidisciplinary, Hepatitis C virus, T Cells, article, Receptors, Antigen, T-Cell, gamma-delta, Animal Models, Signaling in Selected Disciplines, medicine.anatomical_structure, protein protein interaction, two hybrid system, Membranes and Sorting, Signal Transduction, Research Article, Plasmids, Protein Binding, CD3, gene rearrangement, chemical and pharmacologic phenomena, Immunological Signaling, Model Organisms, Two-Hybrid System Techniques, medicine, Animals, controlled study, Protein Interactions, 030304 developmental biology, T-cell receptor, nucleotide sequence, T lymphocyte, antigen function, Molecular biology, biological factors, CD5 antigen, HEK293 Cells, Immune System, biology.protein, T lymphocyte receptor, protein determination, 030215 immunology

Abstract

CD81 (TAPA-1) is a ubiquitously expressed tetraspanin protein identified as a component of the B lymphocyte receptor (BCR) and as a receptor for the Hepatitis C Virus. In an effort to identify trans-membrane proteins that interact with the T-cell antigen receptor (TCR), we performed a membrane yeast two hybrid screen and identified CD81 as an interactor of the CD3delta subunit of the TCR. We found that in the absence of CD81, in thymocytes from knockout mice, TCR engagement resulted in stronger signals. These results were recapitulated in T cell lines that express low levels of CD81 through shRNA mediated silencing. Increased signaling did not result from alterations in the levels of TCR on the surface of T lymphocytes. Although CD81 is not essential for normal T lymphocyte development, it plays an important role in regulating TCR and possibly pre-TCR signal transduction by controlling the strength of signaling. CD81 dependent alterations in thymocyte signaling are evident in increased CD5 expression on CD81 deficient double positive (DP) thymocytes. We conclude that CD81 interacts with the T cell receptor to suppress signaling. © 2012 Cevik et al.

Published

2012

18. P199 SYNDECAN-1 AS A COFACTOR OF CD81 IN HEPATITIS C VIRUS INFECTION OF HEPATOCYTES.

Author

Grigorov, B., Gentil-dit-Maurin, A., Varbanov, M., Blaising, J., Michelet, M., Ruggiero, F., and Pécheur, E.-I.

Subjects

*HEPATITIS C virus, *SYNDECANS, *COFACTORS (Biochemistry), *CD81 antigen, *HEPATITIS C treatment

Published

2014

19. P207 mir-194 IS A HEPATOCYTE GATE KEEPER HINDERING HCV ENTRY THROUGH TARGETING CD81 RECEPTOR.

Author

Mekky, R.Y., El-Ekiaby, N.M., Hamza, M.T., El-Sayed, M., Esmat, G., and Abdelaziz, A.I.

Subjects

*LIVER cells, *HEPATITIS C virus, *CD81 antigen, *TARGETED drug delivery, *MICRORNA

Published

2014

20. Hepatitis C Virus Infects the Endothelial Cells of the Blood-Brain Barrier.

Author

Fletcher, Nicola F., Wilson, Garrick K., Murray, Jacinta, Hu, Ke, Lewis, Andrew, Reynolds, Gary M., Stamataki, Zania, Meredith, Luke W., Rowe, Ian A., Luo, Guangxiang, Lopez–Ramirez, Miguel A., Baumert, Thomas F., Weksler, Babette, Couraud, Pierre–Olivier, Kim, Kwang Sik, Romero, Ignacio A., Jopling, Catherine, Morgello, Susan, Balfe, Peter, and McKeating, Jane A.

Subjects

CENTRAL nervous system abnormalities, HEPATITIS C virus, BLOOD-brain barrier, LIVER diseases, APOPTOSIS, CD81 antigen, CLAUDINS, ENDOTHELIUM, APOLIPOPROTEIN E

Abstract

Background & Aims: Hepatitis C virus (HCV) infection leads to progressive liver disease and is associated with a variety of extrahepatic syndromes, including central nervous system (CNS) abnormalities. However, it is unclear whether such cognitive abnormalities are a function of systemic disease, impaired hepatic function, or virus infection of the CNS. Methods: We measured levels of HCV RNA and expression of the viral entry receptor in brain tissue samples from 10 infected individuals (and 3 uninfected individuals, as controls) and human brain microvascular endothelial cells by using quantitative polymerase chain reaction and immunochemical and confocal imaging analyses. HCV pseudoparticles and cell culture–derived HCV were used to study the ability of endothelial cells to support viral entry and replication. Results: Using quantitative polymerase chain reaction, we detected HCV RNA in brain tissue of infected individuals at significantly lower levels than in liver samples. Brain microvascular endothelia and brain endothelial cells expressed all of the recognized HCV entry receptors. Two independently derived brain endothelial cell lines, hCMEC/D3 and HBMEC, supported HCV entry and replication. These processes were inhibited by antibodies against the entry factors CD81, scavenger receptor BI, and claudin-1; by interferon; and by reagents that inhibit NS3 protease and NS5B polymerase. HCV infection promotes endothelial permeability and cellular apoptosis. Conclusions: Human brain endothelial cells express functional receptors that support HCV entry and replication. Virus infection of the CNS might lead to HCV-associated neuropathologies. [Copyright &y& Elsevier]

Published

2012