Viral Escape from Neutralizing Antibodies in Early Subtype A HIV-1 Infection Drives an Increase in Autologous Neutralization Breadth

Antibodies that neutralize (nAbs) genetically diverse HIV-1 strains have been recovered from a subset of HIV-1 infected subjects during chronic infection. Exact mechanisms that expand the otherwise narrow neutralization capacity observed during early infection are, however, currently undefined. Here...

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Autores principales: Murphy, Megan K., Yue, Ling, Pan, Ruimin, Boliar, Saikat, Sethi, Anurag, Tian, Jianhui, Pfafferot, Katja, Karita, Etienne, Allen, Susan A., Cormier, Emmanuel, Goepfert, Paul A., Borrow, Persephone, Robinson, James E., Gnanakaran, S., Hunter, Eric, Kong, Xiang-Peng, Derdeyn, Cynthia A.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2013
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3585129/
https://www.ncbi.nlm.nih.gov/pubmed/23468623
http://dx.doi.org/10.1371/journal.ppat.1003173
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author Murphy, Megan K.
Yue, Ling
Pan, Ruimin
Boliar, Saikat
Sethi, Anurag
Tian, Jianhui
Pfafferot, Katja
Karita, Etienne
Allen, Susan A.
Cormier, Emmanuel
Goepfert, Paul A.
Borrow, Persephone
Robinson, James E.
Gnanakaran, S.
Hunter, Eric
Kong, Xiang-Peng
Derdeyn, Cynthia A.
author_facet Murphy, Megan K.
Yue, Ling
Pan, Ruimin
Boliar, Saikat
Sethi, Anurag
Tian, Jianhui
Pfafferot, Katja
Karita, Etienne
Allen, Susan A.
Cormier, Emmanuel
Goepfert, Paul A.
Borrow, Persephone
Robinson, James E.
Gnanakaran, S.
Hunter, Eric
Kong, Xiang-Peng
Derdeyn, Cynthia A.
author_sort Murphy, Megan K.
collection PubMed
description Antibodies that neutralize (nAbs) genetically diverse HIV-1 strains have been recovered from a subset of HIV-1 infected subjects during chronic infection. Exact mechanisms that expand the otherwise narrow neutralization capacity observed during early infection are, however, currently undefined. Here we characterized the earliest nAb responses in a subtype A HIV-1 infected Rwandan seroconverter who later developed moderate cross-clade nAb breadth, using (i) envelope (Env) glycoproteins from the transmitted/founder virus and twenty longitudinal nAb escape variants, (ii) longitudinal autologous plasma, and (iii) autologous monoclonal antibodies (mAbs). Initially, nAbs targeted a single region of gp120, which flanked the V3 domain and involved the alpha2 helix. A single amino acid change at one of three positions in this region conferred early escape. One immunoglobulin heavy chain and two light chains recovered from autologous B cells comprised two mAbs, 19.3H-L1 and 19.3H-L3, which neutralized the founder Env along with one or three of the early escape variants carrying these mutations, respectively. Neither mAb neutralized later nAb escape or heterologous Envs. Crystal structures of the antigen-binding fragments (Fabs) revealed flat epitope contact surfaces, where minimal light chain mutation in 19.3H-L3 allowed for additional antigenic interactions. Resistance to mAb neutralization arose in later Envs through alteration of two glycans spatially adjacent to the initial escape signatures. The cross-neutralizing nAbs that ultimately developed failed to target any of the defined V3-proximal changes generated during the first year of infection in this subject. Our data demonstrate that this subject's first recognized nAb epitope elicited strain-specific mAbs, which incrementally acquired autologous breadth, and directed later B cell responses to target distinct portions of Env. This immune re-focusing could have triggered the evolution of cross-clade antibodies and suggests that exposure to a specific sequence of immune escape variants might promote broad humoral responses during HIV-1 infection.
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spelling pubmed-35851292013-03-06 Viral Escape from Neutralizing Antibodies in Early Subtype A HIV-1 Infection Drives an Increase in Autologous Neutralization Breadth Murphy, Megan K. Yue, Ling Pan, Ruimin Boliar, Saikat Sethi, Anurag Tian, Jianhui Pfafferot, Katja Karita, Etienne Allen, Susan A. Cormier, Emmanuel Goepfert, Paul A. Borrow, Persephone Robinson, James E. Gnanakaran, S. Hunter, Eric Kong, Xiang-Peng Derdeyn, Cynthia A. PLoS Pathog Research Article Antibodies that neutralize (nAbs) genetically diverse HIV-1 strains have been recovered from a subset of HIV-1 infected subjects during chronic infection. Exact mechanisms that expand the otherwise narrow neutralization capacity observed during early infection are, however, currently undefined. Here we characterized the earliest nAb responses in a subtype A HIV-1 infected Rwandan seroconverter who later developed moderate cross-clade nAb breadth, using (i) envelope (Env) glycoproteins from the transmitted/founder virus and twenty longitudinal nAb escape variants, (ii) longitudinal autologous plasma, and (iii) autologous monoclonal antibodies (mAbs). Initially, nAbs targeted a single region of gp120, which flanked the V3 domain and involved the alpha2 helix. A single amino acid change at one of three positions in this region conferred early escape. One immunoglobulin heavy chain and two light chains recovered from autologous B cells comprised two mAbs, 19.3H-L1 and 19.3H-L3, which neutralized the founder Env along with one or three of the early escape variants carrying these mutations, respectively. Neither mAb neutralized later nAb escape or heterologous Envs. Crystal structures of the antigen-binding fragments (Fabs) revealed flat epitope contact surfaces, where minimal light chain mutation in 19.3H-L3 allowed for additional antigenic interactions. Resistance to mAb neutralization arose in later Envs through alteration of two glycans spatially adjacent to the initial escape signatures. The cross-neutralizing nAbs that ultimately developed failed to target any of the defined V3-proximal changes generated during the first year of infection in this subject. Our data demonstrate that this subject's first recognized nAb epitope elicited strain-specific mAbs, which incrementally acquired autologous breadth, and directed later B cell responses to target distinct portions of Env. This immune re-focusing could have triggered the evolution of cross-clade antibodies and suggests that exposure to a specific sequence of immune escape variants might promote broad humoral responses during HIV-1 infection. Public Library of Science 2013-02-28 /pmc/articles/PMC3585129/ /pubmed/23468623 http://dx.doi.org/10.1371/journal.ppat.1003173 Text en © 2013 Murphy et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Murphy, Megan K.
Yue, Ling
Pan, Ruimin
Boliar, Saikat
Sethi, Anurag
Tian, Jianhui
Pfafferot, Katja
Karita, Etienne
Allen, Susan A.
Cormier, Emmanuel
Goepfert, Paul A.
Borrow, Persephone
Robinson, James E.
Gnanakaran, S.
Hunter, Eric
Kong, Xiang-Peng
Derdeyn, Cynthia A.
Viral Escape from Neutralizing Antibodies in Early Subtype A HIV-1 Infection Drives an Increase in Autologous Neutralization Breadth
title Viral Escape from Neutralizing Antibodies in Early Subtype A HIV-1 Infection Drives an Increase in Autologous Neutralization Breadth
title_full Viral Escape from Neutralizing Antibodies in Early Subtype A HIV-1 Infection Drives an Increase in Autologous Neutralization Breadth
title_fullStr Viral Escape from Neutralizing Antibodies in Early Subtype A HIV-1 Infection Drives an Increase in Autologous Neutralization Breadth
title_full_unstemmed Viral Escape from Neutralizing Antibodies in Early Subtype A HIV-1 Infection Drives an Increase in Autologous Neutralization Breadth
title_short Viral Escape from Neutralizing Antibodies in Early Subtype A HIV-1 Infection Drives an Increase in Autologous Neutralization Breadth
title_sort viral escape from neutralizing antibodies in early subtype a hiv-1 infection drives an increase in autologous neutralization breadth
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3585129/
https://www.ncbi.nlm.nih.gov/pubmed/23468623
http://dx.doi.org/10.1371/journal.ppat.1003173
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