Identification of Effective Subdominant Anti-HIV-1 CD8+ T Cells Within Entire Post-infection and Post-vaccination Immune Responses

Defining the components of an HIV immunogen that could induce effective CD8+ T cell responses is critical to vaccine development. We addressed this question by investigating the viral targets of CD8+ T cells that potently inhibit HIV replication in vitro, as this is highly predictive of virus contro...

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Autores principales: Hancock, Gemma, Yang, Hongbing, Yorke, Elisabeth, Wainwright, Emma, Bourne, Victoria, Frisbee, Alyse, Payne, Tamika L., Berrong, Mark, Ferrari, Guido, Chopera, Denis, Hanke, Tomas, Mothe, Beatriz, Brander, Christian, McElrath, M. Juliana, McMichael, Andrew, Goonetilleke, Nilu, Tomaras, Georgia D., Frahm, Nicole, Dorrell, Lucy
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2015
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4344337/
https://www.ncbi.nlm.nih.gov/pubmed/25723536
http://dx.doi.org/10.1371/journal.ppat.1004658
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author Hancock, Gemma
Yang, Hongbing
Yorke, Elisabeth
Wainwright, Emma
Bourne, Victoria
Frisbee, Alyse
Payne, Tamika L.
Berrong, Mark
Ferrari, Guido
Chopera, Denis
Hanke, Tomas
Mothe, Beatriz
Brander, Christian
McElrath, M. Juliana
McMichael, Andrew
Goonetilleke, Nilu
Tomaras, Georgia D.
Frahm, Nicole
Dorrell, Lucy
author_facet Hancock, Gemma
Yang, Hongbing
Yorke, Elisabeth
Wainwright, Emma
Bourne, Victoria
Frisbee, Alyse
Payne, Tamika L.
Berrong, Mark
Ferrari, Guido
Chopera, Denis
Hanke, Tomas
Mothe, Beatriz
Brander, Christian
McElrath, M. Juliana
McMichael, Andrew
Goonetilleke, Nilu
Tomaras, Georgia D.
Frahm, Nicole
Dorrell, Lucy
author_sort Hancock, Gemma
collection PubMed
description Defining the components of an HIV immunogen that could induce effective CD8+ T cell responses is critical to vaccine development. We addressed this question by investigating the viral targets of CD8+ T cells that potently inhibit HIV replication in vitro, as this is highly predictive of virus control in vivo. We observed broad and potent ex vivo CD8+ T cell-mediated viral inhibitory activity against a panel of HIV isolates among viremic controllers (VC, viral loads <5000 copies/ml), in contrast to unselected HIV-infected HIV Vaccine trials Network (HVTN) participants. Viral inhibition of clade-matched HIV isolates was strongly correlated with the frequency of CD8+ T cells targeting vulnerable regions within Gag, Pol, Nef and Vif that had been identified in an independent study of nearly 1000 chronically infected individuals. These vulnerable and so-called “beneficial” regions were of low entropy overall, yet several were not predicted by stringent conservation algorithms. Consistent with this, stronger inhibition of clade-matched than mismatched viruses was observed in the majority of subjects, indicating better targeting of clade-specific than conserved epitopes. The magnitude of CD8+ T cell responses to beneficial regions, together with viral entropy and HLA class I genotype, explained up to 59% of the variation in viral inhibitory activity, with magnitude of the T cell response making the strongest unique contribution. However, beneficial regions were infrequently targeted by CD8+ T cells elicited by vaccines encoding full-length HIV proteins, when the latter were administered to healthy volunteers and HIV-positive ART-treated subjects, suggesting that immunodominance hierarchies undermine effective anti-HIV CD8+ T cell responses. Taken together, our data support HIV immunogen design that is based on systematic selection of empirically defined vulnerable regions within the viral proteome, with exclusion of immunodominant decoy epitopes that are irrelevant for HIV control.
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spelling pubmed-43443372015-03-04 Identification of Effective Subdominant Anti-HIV-1 CD8+ T Cells Within Entire Post-infection and Post-vaccination Immune Responses Hancock, Gemma Yang, Hongbing Yorke, Elisabeth Wainwright, Emma Bourne, Victoria Frisbee, Alyse Payne, Tamika L. Berrong, Mark Ferrari, Guido Chopera, Denis Hanke, Tomas Mothe, Beatriz Brander, Christian McElrath, M. Juliana McMichael, Andrew Goonetilleke, Nilu Tomaras, Georgia D. Frahm, Nicole Dorrell, Lucy PLoS Pathog Research Article Defining the components of an HIV immunogen that could induce effective CD8+ T cell responses is critical to vaccine development. We addressed this question by investigating the viral targets of CD8+ T cells that potently inhibit HIV replication in vitro, as this is highly predictive of virus control in vivo. We observed broad and potent ex vivo CD8+ T cell-mediated viral inhibitory activity against a panel of HIV isolates among viremic controllers (VC, viral loads <5000 copies/ml), in contrast to unselected HIV-infected HIV Vaccine trials Network (HVTN) participants. Viral inhibition of clade-matched HIV isolates was strongly correlated with the frequency of CD8+ T cells targeting vulnerable regions within Gag, Pol, Nef and Vif that had been identified in an independent study of nearly 1000 chronically infected individuals. These vulnerable and so-called “beneficial” regions were of low entropy overall, yet several were not predicted by stringent conservation algorithms. Consistent with this, stronger inhibition of clade-matched than mismatched viruses was observed in the majority of subjects, indicating better targeting of clade-specific than conserved epitopes. The magnitude of CD8+ T cell responses to beneficial regions, together with viral entropy and HLA class I genotype, explained up to 59% of the variation in viral inhibitory activity, with magnitude of the T cell response making the strongest unique contribution. However, beneficial regions were infrequently targeted by CD8+ T cells elicited by vaccines encoding full-length HIV proteins, when the latter were administered to healthy volunteers and HIV-positive ART-treated subjects, suggesting that immunodominance hierarchies undermine effective anti-HIV CD8+ T cell responses. Taken together, our data support HIV immunogen design that is based on systematic selection of empirically defined vulnerable regions within the viral proteome, with exclusion of immunodominant decoy epitopes that are irrelevant for HIV control. Public Library of Science 2015-02-27 /pmc/articles/PMC4344337/ /pubmed/25723536 http://dx.doi.org/10.1371/journal.ppat.1004658 Text en © 2015 Hancock 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
Hancock, Gemma
Yang, Hongbing
Yorke, Elisabeth
Wainwright, Emma
Bourne, Victoria
Frisbee, Alyse
Payne, Tamika L.
Berrong, Mark
Ferrari, Guido
Chopera, Denis
Hanke, Tomas
Mothe, Beatriz
Brander, Christian
McElrath, M. Juliana
McMichael, Andrew
Goonetilleke, Nilu
Tomaras, Georgia D.
Frahm, Nicole
Dorrell, Lucy
Identification of Effective Subdominant Anti-HIV-1 CD8+ T Cells Within Entire Post-infection and Post-vaccination Immune Responses
title Identification of Effective Subdominant Anti-HIV-1 CD8+ T Cells Within Entire Post-infection and Post-vaccination Immune Responses
title_full Identification of Effective Subdominant Anti-HIV-1 CD8+ T Cells Within Entire Post-infection and Post-vaccination Immune Responses
title_fullStr Identification of Effective Subdominant Anti-HIV-1 CD8+ T Cells Within Entire Post-infection and Post-vaccination Immune Responses
title_full_unstemmed Identification of Effective Subdominant Anti-HIV-1 CD8+ T Cells Within Entire Post-infection and Post-vaccination Immune Responses
title_short Identification of Effective Subdominant Anti-HIV-1 CD8+ T Cells Within Entire Post-infection and Post-vaccination Immune Responses
title_sort identification of effective subdominant anti-hiv-1 cd8+ t cells within entire post-infection and post-vaccination immune responses
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4344337/
https://www.ncbi.nlm.nih.gov/pubmed/25723536
http://dx.doi.org/10.1371/journal.ppat.1004658
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