Monoclonal Antibodies Directed toward the Hepatitis C Virus Glycoprotein E2 Detect Antigenic Differences Modulated by the N-Terminal Hypervariable Region 1 (HVR1), HVR2, and Intergenotypic Variable Region

Hepatitis C virus (HCV) envelope glycoproteins E1 and E2 form a heterodimer and mediate receptor interactions and viral fusion. Both E1 and E2 are targets of the neutralizing antibody (NAb) response and are candidates for the production of vaccines that generate humoral immunity. Previous studies de...

Descripción completa

Detalles Bibliográficos
Autores principales: Alhammad, Yousef, Gu, Jun, Boo, Irene, Harrison, David, McCaffrey, Kathleen, Vietheer, Patricia T., Edwards, Stirling, Quinn, Charles, Coulibaly, Fásseli, Poumbourios, Pantelis, Drummer, Heidi E.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Society for Microbiology 2015
Materias:
Structure and Assembly
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4665232/
https://www.ncbi.nlm.nih.gov/pubmed/26378182
http://dx.doi.org/10.1128/JVI.02070-15
_version_ 1782403550921359360
author Alhammad, Yousef
Gu, Jun
Boo, Irene
Harrison, David
McCaffrey, Kathleen
Vietheer, Patricia T.
Edwards, Stirling
Quinn, Charles
Coulibaly, Fásseli
Poumbourios, Pantelis
Drummer, Heidi E.
author_facet Alhammad, Yousef
Gu, Jun
Boo, Irene
Harrison, David
McCaffrey, Kathleen
Vietheer, Patricia T.
Edwards, Stirling
Quinn, Charles
Coulibaly, Fásseli
Poumbourios, Pantelis
Drummer, Heidi E.
author_sort Alhammad, Yousef
collection PubMed
description Hepatitis C virus (HCV) envelope glycoproteins E1 and E2 form a heterodimer and mediate receptor interactions and viral fusion. Both E1 and E2 are targets of the neutralizing antibody (NAb) response and are candidates for the production of vaccines that generate humoral immunity. Previous studies demonstrated that N-terminal hypervariable region 1 (HVR1) can modulate the neutralization potential of monoclonal antibodies (MAbs), but no information is available on the influence of HVR2 or the intergenotypic variable region (igVR) on antigenicity. In this study, we examined how the variable regions influence the antigenicity of the receptor binding domain of E2 spanning HCV polyprotein residues 384 to 661 (E2(661)) using a panel of MAbs raised against E2(661) and E2(661) lacking HVR1, HVR2, and the igVR (Δ123) and well-characterized MAbs isolated from infected humans. We show for a subset of both neutralizing and nonneutralizing MAbs that all three variable regions decrease the ability of MAbs to bind E2(661) and reduce the ability of MAbs to inhibit E2-CD81 interactions. In addition, we describe a new MAb directed toward the region spanning residues 411 to 428 of E2 (MAb24) that demonstrates broad neutralization against all 7 genotypes of HCV. The ability of MAb24 to inhibit E2-CD81 interactions is strongly influenced by the three variable regions. Our data suggest that HVR1, HVR2, and the igVR modulate exposure of epitopes on the core domain of E2 and their ability to prevent E2-CD81 interactions. These studies suggest that the function of HVR2 and the igVR is to modulate antibody recognition of glycoprotein E2 and may contribute to immune evasion. IMPORTANCE This study reveals conformational and antigenic differences between the Δ123 and intact E2(661) glycoproteins and provides new structural and functional data about the three variable regions and their role in occluding neutralizing and nonneutralizing epitopes on the E2 core domain. The variable regions may therefore function to reduce the ability of HCV to elicit NAbs directed toward the conserved core domain. Future studies aimed at generating a three-dimensional structure for intact E2 containing HVR1, and the adjoining NAb epitope at residues 412 to 428, together with HVR2, will reveal how the variable regions modulate antigenic structure.
format Online
Article
Text
id pubmed-4665232
institution National Center for Biotechnology Information
language English
publishDate 2015
publisher American Society for Microbiology
record_format MEDLINE/PubMed
spelling pubmed-46652322015-12-10 Monoclonal Antibodies Directed toward the Hepatitis C Virus Glycoprotein E2 Detect Antigenic Differences Modulated by the N-Terminal Hypervariable Region 1 (HVR1), HVR2, and Intergenotypic Variable Region Alhammad, Yousef Gu, Jun Boo, Irene Harrison, David McCaffrey, Kathleen Vietheer, Patricia T. Edwards, Stirling Quinn, Charles Coulibaly, Fásseli Poumbourios, Pantelis Drummer, Heidi E. J Virol Structure and Assembly Hepatitis C virus (HCV) envelope glycoproteins E1 and E2 form a heterodimer and mediate receptor interactions and viral fusion. Both E1 and E2 are targets of the neutralizing antibody (NAb) response and are candidates for the production of vaccines that generate humoral immunity. Previous studies demonstrated that N-terminal hypervariable region 1 (HVR1) can modulate the neutralization potential of monoclonal antibodies (MAbs), but no information is available on the influence of HVR2 or the intergenotypic variable region (igVR) on antigenicity. In this study, we examined how the variable regions influence the antigenicity of the receptor binding domain of E2 spanning HCV polyprotein residues 384 to 661 (E2(661)) using a panel of MAbs raised against E2(661) and E2(661) lacking HVR1, HVR2, and the igVR (Δ123) and well-characterized MAbs isolated from infected humans. We show for a subset of both neutralizing and nonneutralizing MAbs that all three variable regions decrease the ability of MAbs to bind E2(661) and reduce the ability of MAbs to inhibit E2-CD81 interactions. In addition, we describe a new MAb directed toward the region spanning residues 411 to 428 of E2 (MAb24) that demonstrates broad neutralization against all 7 genotypes of HCV. The ability of MAb24 to inhibit E2-CD81 interactions is strongly influenced by the three variable regions. Our data suggest that HVR1, HVR2, and the igVR modulate exposure of epitopes on the core domain of E2 and their ability to prevent E2-CD81 interactions. These studies suggest that the function of HVR2 and the igVR is to modulate antibody recognition of glycoprotein E2 and may contribute to immune evasion. IMPORTANCE This study reveals conformational and antigenic differences between the Δ123 and intact E2(661) glycoproteins and provides new structural and functional data about the three variable regions and their role in occluding neutralizing and nonneutralizing epitopes on the E2 core domain. The variable regions may therefore function to reduce the ability of HCV to elicit NAbs directed toward the conserved core domain. Future studies aimed at generating a three-dimensional structure for intact E2 containing HVR1, and the adjoining NAb epitope at residues 412 to 428, together with HVR2, will reveal how the variable regions modulate antigenic structure. American Society for Microbiology 2015-09-16 /pmc/articles/PMC4665232/ /pubmed/26378182 http://dx.doi.org/10.1128/JVI.02070-15 Text en Copyright © 2015 Alhammad et al. http://creativecommons.org/licenses/by-nc-sa/3.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution-Noncommercial-ShareAlike 3.0 Unported license (http://creativecommons.org/licenses/by-nc-sa/3.0/) , which permits unrestricted noncommercial use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Structure and Assembly
Alhammad, Yousef
Gu, Jun
Boo, Irene
Harrison, David
McCaffrey, Kathleen
Vietheer, Patricia T.
Edwards, Stirling
Quinn, Charles
Coulibaly, Fásseli
Poumbourios, Pantelis
Drummer, Heidi E.
Monoclonal Antibodies Directed toward the Hepatitis C Virus Glycoprotein E2 Detect Antigenic Differences Modulated by the N-Terminal Hypervariable Region 1 (HVR1), HVR2, and Intergenotypic Variable Region
title Monoclonal Antibodies Directed toward the Hepatitis C Virus Glycoprotein E2 Detect Antigenic Differences Modulated by the N-Terminal Hypervariable Region 1 (HVR1), HVR2, and Intergenotypic Variable Region
title_full Monoclonal Antibodies Directed toward the Hepatitis C Virus Glycoprotein E2 Detect Antigenic Differences Modulated by the N-Terminal Hypervariable Region 1 (HVR1), HVR2, and Intergenotypic Variable Region
title_fullStr Monoclonal Antibodies Directed toward the Hepatitis C Virus Glycoprotein E2 Detect Antigenic Differences Modulated by the N-Terminal Hypervariable Region 1 (HVR1), HVR2, and Intergenotypic Variable Region
title_full_unstemmed Monoclonal Antibodies Directed toward the Hepatitis C Virus Glycoprotein E2 Detect Antigenic Differences Modulated by the N-Terminal Hypervariable Region 1 (HVR1), HVR2, and Intergenotypic Variable Region
title_short Monoclonal Antibodies Directed toward the Hepatitis C Virus Glycoprotein E2 Detect Antigenic Differences Modulated by the N-Terminal Hypervariable Region 1 (HVR1), HVR2, and Intergenotypic Variable Region
title_sort monoclonal antibodies directed toward the hepatitis c virus glycoprotein e2 detect antigenic differences modulated by the n-terminal hypervariable region 1 (hvr1), hvr2, and intergenotypic variable region
topic Structure and Assembly
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4665232/
https://www.ncbi.nlm.nih.gov/pubmed/26378182
http://dx.doi.org/10.1128/JVI.02070-15
work_keys_str_mv AT alhammadyousef monoclonalantibodiesdirectedtowardthehepatitiscvirusglycoproteine2detectantigenicdifferencesmodulatedbythenterminalhypervariableregion1hvr1hvr2andintergenotypicvariableregion
AT gujun monoclonalantibodiesdirectedtowardthehepatitiscvirusglycoproteine2detectantigenicdifferencesmodulatedbythenterminalhypervariableregion1hvr1hvr2andintergenotypicvariableregion
AT booirene monoclonalantibodiesdirectedtowardthehepatitiscvirusglycoproteine2detectantigenicdifferencesmodulatedbythenterminalhypervariableregion1hvr1hvr2andintergenotypicvariableregion
AT harrisondavid monoclonalantibodiesdirectedtowardthehepatitiscvirusglycoproteine2detectantigenicdifferencesmodulatedbythenterminalhypervariableregion1hvr1hvr2andintergenotypicvariableregion
AT mccaffreykathleen monoclonalantibodiesdirectedtowardthehepatitiscvirusglycoproteine2detectantigenicdifferencesmodulatedbythenterminalhypervariableregion1hvr1hvr2andintergenotypicvariableregion
AT vietheerpatriciat monoclonalantibodiesdirectedtowardthehepatitiscvirusglycoproteine2detectantigenicdifferencesmodulatedbythenterminalhypervariableregion1hvr1hvr2andintergenotypicvariableregion
AT edwardsstirling monoclonalantibodiesdirectedtowardthehepatitiscvirusglycoproteine2detectantigenicdifferencesmodulatedbythenterminalhypervariableregion1hvr1hvr2andintergenotypicvariableregion
AT quinncharles monoclonalantibodiesdirectedtowardthehepatitiscvirusglycoproteine2detectantigenicdifferencesmodulatedbythenterminalhypervariableregion1hvr1hvr2andintergenotypicvariableregion
AT coulibalyfasseli monoclonalantibodiesdirectedtowardthehepatitiscvirusglycoproteine2detectantigenicdifferencesmodulatedbythenterminalhypervariableregion1hvr1hvr2andintergenotypicvariableregion
AT poumbouriospantelis monoclonalantibodiesdirectedtowardthehepatitiscvirusglycoproteine2detectantigenicdifferencesmodulatedbythenterminalhypervariableregion1hvr1hvr2andintergenotypicvariableregion
AT drummerheidie monoclonalantibodiesdirectedtowardthehepatitiscvirusglycoproteine2detectantigenicdifferencesmodulatedbythenterminalhypervariableregion1hvr1hvr2andintergenotypicvariableregion

Ejemplares similares