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Rapid Induction of Multifunctional Antibodies in Rabbits and Macaques by Clade C HIV-1 CAP257 Envelopes Circulating During Epitope-Specific Neutralization Breadth Development

We report here on HIV-1 immunization results in rabbits and macaques co-immunized with clade C gp160 DNA and gp140 trimeric envelope vaccines, a strategy similar to a recent clinical trial that showed improved speed and magnitude of humoral responses. Clade C envelopes were isolated from CAP257, an...

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Autores principales: Malherbe, Delphine C., Wibmer, Constantinos Kurt, Nonyane, Molati, Reed, Jason, Sather, D. Noah, Spencer, David A., Schuman, Jason T., Guo, Biwei, Pandey, Shilpi, Robins, Harlan, Park, Byung, Fuller, Deborah H., Sacha, Jonah B., Moore, Penny L., Hessell, Ann J., Haigwood, Nancy L.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2020
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7280454/
https://www.ncbi.nlm.nih.gov/pubmed/32582155
http://dx.doi.org/10.3389/fimmu.2020.00984
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author Malherbe, Delphine C.
Wibmer, Constantinos Kurt
Nonyane, Molati
Reed, Jason
Sather, D. Noah
Spencer, David A.
Schuman, Jason T.
Guo, Biwei
Pandey, Shilpi
Robins, Harlan
Park, Byung
Fuller, Deborah H.
Sacha, Jonah B.
Moore, Penny L.
Hessell, Ann J.
Haigwood, Nancy L.
author_facet Malherbe, Delphine C.
Wibmer, Constantinos Kurt
Nonyane, Molati
Reed, Jason
Sather, D. Noah
Spencer, David A.
Schuman, Jason T.
Guo, Biwei
Pandey, Shilpi
Robins, Harlan
Park, Byung
Fuller, Deborah H.
Sacha, Jonah B.
Moore, Penny L.
Hessell, Ann J.
Haigwood, Nancy L.
author_sort Malherbe, Delphine C.
collection PubMed
description We report here on HIV-1 immunization results in rabbits and macaques co-immunized with clade C gp160 DNA and gp140 trimeric envelope vaccines, a strategy similar to a recent clinical trial that showed improved speed and magnitude of humoral responses. Clade C envelopes were isolated from CAP257, an individual who developed a unique temporal pattern of neutralization breadth development, comprising three separate “Waves” targeting distinct Env epitopes and different HIV clades. We used phylogeny and neutralization criteria to down-select envelope vaccine candidates, and confirmed antigenicity of our antigens by interaction with well-characterized broadly neutralizing monoclonal antibodies. Using these envelopes, we performed rabbit studies that screened for immunogenicity of CAP257 Envs from timepoints preceding peak neutralization breadth in each Wave. Selected CAP257 envelopes from Waves 1 and 2, during the first 2 years of infection that were highly immunogenic in rabbits were then tested in macaques. We found that in rabbits and macaques, co-immunization of DNA, and protein envelope-based vaccines induced maximum binding and neutralizing antibody titers with three immunizations. No further benefit was obtained with additional immunizations. The vaccine strategies recapitulated the Wave-specific epitope targeting observed in the CAP257 participant, and elicited Tier 1A, 1B, and Tier 2 heterologous neutralization. CAP257 envelope immunogens also induced the development of ADCC and T(FH) responses in macaques, and these responses positively correlated with heterologous neutralization. Together, the results from two animal models in this study have implications for identifying effective vaccine immunogens. We used a multi-step strategy to (1) select an Env donor with well-characterized neutralization breadth development; (2) study Env phylogeny for potential immunogens circulating near peak breadth timepoints during the first 2 years of infection; (3) test down-selected Envs for antigenicity; (4) screen down-selected Envs in an effective vaccine regimen in rabbits; and (5) advance the most immunogenic Envs to NHP studies. The results were an induction of high titers of HIV-1 envelope-specific antibodies with increasing avidity and cross-clade neutralizing antibodies with effector functions that together may improve the potential for protection in a pre-clinical SHIV model.
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spelling pubmed-72804542020-06-23 Rapid Induction of Multifunctional Antibodies in Rabbits and Macaques by Clade C HIV-1 CAP257 Envelopes Circulating During Epitope-Specific Neutralization Breadth Development Malherbe, Delphine C. Wibmer, Constantinos Kurt Nonyane, Molati Reed, Jason Sather, D. Noah Spencer, David A. Schuman, Jason T. Guo, Biwei Pandey, Shilpi Robins, Harlan Park, Byung Fuller, Deborah H. Sacha, Jonah B. Moore, Penny L. Hessell, Ann J. Haigwood, Nancy L. Front Immunol Immunology We report here on HIV-1 immunization results in rabbits and macaques co-immunized with clade C gp160 DNA and gp140 trimeric envelope vaccines, a strategy similar to a recent clinical trial that showed improved speed and magnitude of humoral responses. Clade C envelopes were isolated from CAP257, an individual who developed a unique temporal pattern of neutralization breadth development, comprising three separate “Waves” targeting distinct Env epitopes and different HIV clades. We used phylogeny and neutralization criteria to down-select envelope vaccine candidates, and confirmed antigenicity of our antigens by interaction with well-characterized broadly neutralizing monoclonal antibodies. Using these envelopes, we performed rabbit studies that screened for immunogenicity of CAP257 Envs from timepoints preceding peak neutralization breadth in each Wave. Selected CAP257 envelopes from Waves 1 and 2, during the first 2 years of infection that were highly immunogenic in rabbits were then tested in macaques. We found that in rabbits and macaques, co-immunization of DNA, and protein envelope-based vaccines induced maximum binding and neutralizing antibody titers with three immunizations. No further benefit was obtained with additional immunizations. The vaccine strategies recapitulated the Wave-specific epitope targeting observed in the CAP257 participant, and elicited Tier 1A, 1B, and Tier 2 heterologous neutralization. CAP257 envelope immunogens also induced the development of ADCC and T(FH) responses in macaques, and these responses positively correlated with heterologous neutralization. Together, the results from two animal models in this study have implications for identifying effective vaccine immunogens. We used a multi-step strategy to (1) select an Env donor with well-characterized neutralization breadth development; (2) study Env phylogeny for potential immunogens circulating near peak breadth timepoints during the first 2 years of infection; (3) test down-selected Envs for antigenicity; (4) screen down-selected Envs in an effective vaccine regimen in rabbits; and (5) advance the most immunogenic Envs to NHP studies. The results were an induction of high titers of HIV-1 envelope-specific antibodies with increasing avidity and cross-clade neutralizing antibodies with effector functions that together may improve the potential for protection in a pre-clinical SHIV model. Frontiers Media S.A. 2020-06-02 /pmc/articles/PMC7280454/ /pubmed/32582155 http://dx.doi.org/10.3389/fimmu.2020.00984 Text en Copyright © 2020 Malherbe, Wibmer, Nonyane, Reed, Sather, Spencer, Schuman, Guo, Pandey, Robins, Park, Fuller, Sacha, Moore, Hessell and Haigwood. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Immunology
Malherbe, Delphine C.
Wibmer, Constantinos Kurt
Nonyane, Molati
Reed, Jason
Sather, D. Noah
Spencer, David A.
Schuman, Jason T.
Guo, Biwei
Pandey, Shilpi
Robins, Harlan
Park, Byung
Fuller, Deborah H.
Sacha, Jonah B.
Moore, Penny L.
Hessell, Ann J.
Haigwood, Nancy L.
Rapid Induction of Multifunctional Antibodies in Rabbits and Macaques by Clade C HIV-1 CAP257 Envelopes Circulating During Epitope-Specific Neutralization Breadth Development
title Rapid Induction of Multifunctional Antibodies in Rabbits and Macaques by Clade C HIV-1 CAP257 Envelopes Circulating During Epitope-Specific Neutralization Breadth Development
title_full Rapid Induction of Multifunctional Antibodies in Rabbits and Macaques by Clade C HIV-1 CAP257 Envelopes Circulating During Epitope-Specific Neutralization Breadth Development
title_fullStr Rapid Induction of Multifunctional Antibodies in Rabbits and Macaques by Clade C HIV-1 CAP257 Envelopes Circulating During Epitope-Specific Neutralization Breadth Development
title_full_unstemmed Rapid Induction of Multifunctional Antibodies in Rabbits and Macaques by Clade C HIV-1 CAP257 Envelopes Circulating During Epitope-Specific Neutralization Breadth Development
title_short Rapid Induction of Multifunctional Antibodies in Rabbits and Macaques by Clade C HIV-1 CAP257 Envelopes Circulating During Epitope-Specific Neutralization Breadth Development
title_sort rapid induction of multifunctional antibodies in rabbits and macaques by clade c hiv-1 cap257 envelopes circulating during epitope-specific neutralization breadth development
topic Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7280454/
https://www.ncbi.nlm.nih.gov/pubmed/32582155
http://dx.doi.org/10.3389/fimmu.2020.00984
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