Structure and Recognition of a Novel HIV-1 gp120-gp41 Interface Antibody that Caused MPER Exposure through Viral Escape

A comprehensive understanding of the regions on HIV-1 envelope trimers targeted by broadly neutralizing antibodies may contribute to rational design of an HIV-1 vaccine. We previously identified a participant in the CAPRISA cohort, CAP248, who developed trimer-specific antibodies capable of neutrali...

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Autores principales: Wibmer, Constantinos Kurt, Gorman, Jason, Ozorowski, Gabriel, Bhiman, Jinal N., Sheward, Daniel J., Elliott, Debra H., Rouelle, Julie, Smira, Ashley, Joyce, M. Gordon, Ndabambi, Nonkululeko, Druz, Aliaksandr, Asokan, Mangai, Burton, Dennis R., Connors, Mark, Abdool Karim, Salim S., Mascola, John R., Robinson, James E., Ward, Andrew B., Williamson, Carolyn, Kwong, Peter D., Morris, Lynn, Moore, Penny L.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2017
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5226681/
https://www.ncbi.nlm.nih.gov/pubmed/28076415
http://dx.doi.org/10.1371/journal.ppat.1006074
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author Wibmer, Constantinos Kurt
Gorman, Jason
Ozorowski, Gabriel
Bhiman, Jinal N.
Sheward, Daniel J.
Elliott, Debra H.
Rouelle, Julie
Smira, Ashley
Joyce, M. Gordon
Ndabambi, Nonkululeko
Druz, Aliaksandr
Asokan, Mangai
Burton, Dennis R.
Connors, Mark
Abdool Karim, Salim S.
Mascola, John R.
Robinson, James E.
Ward, Andrew B.
Williamson, Carolyn
Kwong, Peter D.
Morris, Lynn
Moore, Penny L.
author_facet Wibmer, Constantinos Kurt
Gorman, Jason
Ozorowski, Gabriel
Bhiman, Jinal N.
Sheward, Daniel J.
Elliott, Debra H.
Rouelle, Julie
Smira, Ashley
Joyce, M. Gordon
Ndabambi, Nonkululeko
Druz, Aliaksandr
Asokan, Mangai
Burton, Dennis R.
Connors, Mark
Abdool Karim, Salim S.
Mascola, John R.
Robinson, James E.
Ward, Andrew B.
Williamson, Carolyn
Kwong, Peter D.
Morris, Lynn
Moore, Penny L.
author_sort Wibmer, Constantinos Kurt
collection PubMed
description A comprehensive understanding of the regions on HIV-1 envelope trimers targeted by broadly neutralizing antibodies may contribute to rational design of an HIV-1 vaccine. We previously identified a participant in the CAPRISA cohort, CAP248, who developed trimer-specific antibodies capable of neutralizing 60% of heterologous viruses at three years post-infection. Here, we report the isolation by B cell culture of monoclonal antibody CAP248-2B, which targets a novel membrane proximal epitope including elements of gp120 and gp41. Despite low maximum inhibition plateaus, often below 50% inhibitory concentrations, the breadth of CAP248-2B significantly correlated with donor plasma. Site-directed mutagenesis, X-ray crystallography, and negative-stain electron microscopy 3D reconstructions revealed how CAP248-2B recognizes a cleavage-dependent epitope that includes the gp120 C terminus. While this epitope is distinct, it overlapped in parts of gp41 with the epitopes of broadly neutralizing antibodies PGT151, VRC34, 35O22, 3BC315, and 10E8. CAP248-2B has a conformationally variable paratope with an unusually long 19 amino acid light chain third complementarity determining region. Two phenylalanines at the loop apex were predicted by docking and mutagenesis data to interact with the viral membrane. Neutralization by CAP248-2B is not dependent on any single glycan proximal to its epitope, and low neutralization plateaus could not be completely explained by N- or O-linked glycosylation pathway inhibitors, furin co-transfection, or pre-incubation with soluble CD4. Viral escape from CAP248-2B involved a cluster of rare mutations in the gp120-gp41 cleavage sites. Simultaneous introduction of these mutations into heterologous viruses abrogated neutralization by CAP248-2B, but enhanced neutralization sensitivity to 35O22, 4E10, and 10E8 by 10-100-fold. Altogether, this study expands the region of the HIV-1 gp120-gp41 quaternary interface that is a target for broadly neutralizing antibodies and identifies a set of mutations in the gp120 C terminus that exposes the membrane-proximal external region of gp41, with potential utility in HIV vaccine design.
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spelling pubmed-52266812017-01-31 Structure and Recognition of a Novel HIV-1 gp120-gp41 Interface Antibody that Caused MPER Exposure through Viral Escape Wibmer, Constantinos Kurt Gorman, Jason Ozorowski, Gabriel Bhiman, Jinal N. Sheward, Daniel J. Elliott, Debra H. Rouelle, Julie Smira, Ashley Joyce, M. Gordon Ndabambi, Nonkululeko Druz, Aliaksandr Asokan, Mangai Burton, Dennis R. Connors, Mark Abdool Karim, Salim S. Mascola, John R. Robinson, James E. Ward, Andrew B. Williamson, Carolyn Kwong, Peter D. Morris, Lynn Moore, Penny L. PLoS Pathog Research Article A comprehensive understanding of the regions on HIV-1 envelope trimers targeted by broadly neutralizing antibodies may contribute to rational design of an HIV-1 vaccine. We previously identified a participant in the CAPRISA cohort, CAP248, who developed trimer-specific antibodies capable of neutralizing 60% of heterologous viruses at three years post-infection. Here, we report the isolation by B cell culture of monoclonal antibody CAP248-2B, which targets a novel membrane proximal epitope including elements of gp120 and gp41. Despite low maximum inhibition plateaus, often below 50% inhibitory concentrations, the breadth of CAP248-2B significantly correlated with donor plasma. Site-directed mutagenesis, X-ray crystallography, and negative-stain electron microscopy 3D reconstructions revealed how CAP248-2B recognizes a cleavage-dependent epitope that includes the gp120 C terminus. While this epitope is distinct, it overlapped in parts of gp41 with the epitopes of broadly neutralizing antibodies PGT151, VRC34, 35O22, 3BC315, and 10E8. CAP248-2B has a conformationally variable paratope with an unusually long 19 amino acid light chain third complementarity determining region. Two phenylalanines at the loop apex were predicted by docking and mutagenesis data to interact with the viral membrane. Neutralization by CAP248-2B is not dependent on any single glycan proximal to its epitope, and low neutralization plateaus could not be completely explained by N- or O-linked glycosylation pathway inhibitors, furin co-transfection, or pre-incubation with soluble CD4. Viral escape from CAP248-2B involved a cluster of rare mutations in the gp120-gp41 cleavage sites. Simultaneous introduction of these mutations into heterologous viruses abrogated neutralization by CAP248-2B, but enhanced neutralization sensitivity to 35O22, 4E10, and 10E8 by 10-100-fold. Altogether, this study expands the region of the HIV-1 gp120-gp41 quaternary interface that is a target for broadly neutralizing antibodies and identifies a set of mutations in the gp120 C terminus that exposes the membrane-proximal external region of gp41, with potential utility in HIV vaccine design. Public Library of Science 2017-01-11 /pmc/articles/PMC5226681/ /pubmed/28076415 http://dx.doi.org/10.1371/journal.ppat.1006074 Text en https://creativecommons.org/publicdomain/zero/1.0/ This is an open access article, free of all copyright, and may be freely reproduced, distributed, transmitted, modified, built upon, or otherwise used by anyone for any lawful purpose. The work is made available under the Creative Commons CC0 (https://creativecommons.org/publicdomain/zero/1.0/) public domain dedication.
spellingShingle Research Article
Wibmer, Constantinos Kurt
Gorman, Jason
Ozorowski, Gabriel
Bhiman, Jinal N.
Sheward, Daniel J.
Elliott, Debra H.
Rouelle, Julie
Smira, Ashley
Joyce, M. Gordon
Ndabambi, Nonkululeko
Druz, Aliaksandr
Asokan, Mangai
Burton, Dennis R.
Connors, Mark
Abdool Karim, Salim S.
Mascola, John R.
Robinson, James E.
Ward, Andrew B.
Williamson, Carolyn
Kwong, Peter D.
Morris, Lynn
Moore, Penny L.
Structure and Recognition of a Novel HIV-1 gp120-gp41 Interface Antibody that Caused MPER Exposure through Viral Escape
title Structure and Recognition of a Novel HIV-1 gp120-gp41 Interface Antibody that Caused MPER Exposure through Viral Escape
title_full Structure and Recognition of a Novel HIV-1 gp120-gp41 Interface Antibody that Caused MPER Exposure through Viral Escape
title_fullStr Structure and Recognition of a Novel HIV-1 gp120-gp41 Interface Antibody that Caused MPER Exposure through Viral Escape
title_full_unstemmed Structure and Recognition of a Novel HIV-1 gp120-gp41 Interface Antibody that Caused MPER Exposure through Viral Escape
title_short Structure and Recognition of a Novel HIV-1 gp120-gp41 Interface Antibody that Caused MPER Exposure through Viral Escape
title_sort structure and recognition of a novel hiv-1 gp120-gp41 interface antibody that caused mper exposure through viral escape
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5226681/
https://www.ncbi.nlm.nih.gov/pubmed/28076415
http://dx.doi.org/10.1371/journal.ppat.1006074
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