Analysis of V2 antibody responses induced in vaccinees in the ALVAC/AIDSVAX HIV-1 vaccine efficacy trial.
The RV144 clinical trial of a prime/boost immunizing regimen using recombinant canary pox (ALVAC-HIV) and two gp120 proteins (AIDSVAX B and E) was previously shown to have a 31.2% efficacy rate. Plasma specimens from vaccine and placebo recipients were used in an extensive set of assays to identify...
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doaj-3f8bd381cf2f4c4e9cbc7c43ba28e4062020-11-25T00:44:18ZengPublic Library of Science (PLoS)PLoS ONE1932-62032013-01-0181e5362910.1371/journal.pone.0053629Analysis of V2 antibody responses induced in vaccinees in the ALVAC/AIDSVAX HIV-1 vaccine efficacy trial.Susan Zolla-PaznerAllan C deCampTimothy CardozoNicos KarasavvasRaphael GottardoConstance WilliamsDaryl E MorrisGeorgia TomarasMangala RaoErik BillingsPhillip BermanXiaoying ShenCharla AndrewsRobert J O'ConnellViseth NgauySorachai NitayaphanMark de SouzaBette KorberRichard KoupRobert T BailerJohn R MascolaAbraham PinterDavid MontefioriBarton F HaynesMerlin L RobbSupachai Rerks-NgarmNelson L MichaelPeter B GilbertJerome H KimThe RV144 clinical trial of a prime/boost immunizing regimen using recombinant canary pox (ALVAC-HIV) and two gp120 proteins (AIDSVAX B and E) was previously shown to have a 31.2% efficacy rate. Plasma specimens from vaccine and placebo recipients were used in an extensive set of assays to identify correlates of HIV-1 infection risk. Of six primary variables that were studied, only one displayed a significant inverse correlation with risk of infection: the antibody (Ab) response to a fusion protein containing the V1 and V2 regions of gp120 (gp70-V1V2). This finding prompted a thorough examination of the results generated with the complete panel of 13 assays measuring various V2 Abs in the stored plasma used in the initial pilot studies and those used in the subsequent case-control study. The studies revealed that the ALVAC-HIV/AIDSVAX vaccine induced V2-specific Abs that cross-react with multiple HIV-1 subgroups and recognize both conformational and linear epitopes. The conformational epitope was present on gp70-V1V2, while the predominant linear V2 epitope mapped to residues 165-178, immediately N-terminal to the putative α4β7 binding motif in the mid-loop region of V2. Odds ratios (ORs) were calculated to compare the risk of infection with data from 12 V2 assays, and in 11 of these, the ORs were ≤1, reaching statistical significance for two of the variables: Ab responses to gp70-V1V2 and to overlapping V2 linear peptides. It remains to be determined whether anti-V2 Ab responses were directly responsible for the reduced infection rate in RV144 and whether anti-V2 Abs will prove to be important with other candidate HIV vaccines that show efficacy, however, the results support continued dissection of Ab responses to the V2 region which may illuminate mechanisms of protection from HIV-1 infection and may facilitate the development of an effective HIV-1 vaccine.http://europepmc.org/articles/PMC3547933?pdf=render |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Susan Zolla-Pazner Allan C deCamp Timothy Cardozo Nicos Karasavvas Raphael Gottardo Constance Williams Daryl E Morris Georgia Tomaras Mangala Rao Erik Billings Phillip Berman Xiaoying Shen Charla Andrews Robert J O'Connell Viseth Ngauy Sorachai Nitayaphan Mark de Souza Bette Korber Richard Koup Robert T Bailer John R Mascola Abraham Pinter David Montefiori Barton F Haynes Merlin L Robb Supachai Rerks-Ngarm Nelson L Michael Peter B Gilbert Jerome H Kim |
spellingShingle |
Susan Zolla-Pazner Allan C deCamp Timothy Cardozo Nicos Karasavvas Raphael Gottardo Constance Williams Daryl E Morris Georgia Tomaras Mangala Rao Erik Billings Phillip Berman Xiaoying Shen Charla Andrews Robert J O'Connell Viseth Ngauy Sorachai Nitayaphan Mark de Souza Bette Korber Richard Koup Robert T Bailer John R Mascola Abraham Pinter David Montefiori Barton F Haynes Merlin L Robb Supachai Rerks-Ngarm Nelson L Michael Peter B Gilbert Jerome H Kim Analysis of V2 antibody responses induced in vaccinees in the ALVAC/AIDSVAX HIV-1 vaccine efficacy trial. PLoS ONE |
author_facet |
Susan Zolla-Pazner Allan C deCamp Timothy Cardozo Nicos Karasavvas Raphael Gottardo Constance Williams Daryl E Morris Georgia Tomaras Mangala Rao Erik Billings Phillip Berman Xiaoying Shen Charla Andrews Robert J O'Connell Viseth Ngauy Sorachai Nitayaphan Mark de Souza Bette Korber Richard Koup Robert T Bailer John R Mascola Abraham Pinter David Montefiori Barton F Haynes Merlin L Robb Supachai Rerks-Ngarm Nelson L Michael Peter B Gilbert Jerome H Kim |
author_sort |
Susan Zolla-Pazner |
title |
Analysis of V2 antibody responses induced in vaccinees in the ALVAC/AIDSVAX HIV-1 vaccine efficacy trial. |
title_short |
Analysis of V2 antibody responses induced in vaccinees in the ALVAC/AIDSVAX HIV-1 vaccine efficacy trial. |
title_full |
Analysis of V2 antibody responses induced in vaccinees in the ALVAC/AIDSVAX HIV-1 vaccine efficacy trial. |
title_fullStr |
Analysis of V2 antibody responses induced in vaccinees in the ALVAC/AIDSVAX HIV-1 vaccine efficacy trial. |
title_full_unstemmed |
Analysis of V2 antibody responses induced in vaccinees in the ALVAC/AIDSVAX HIV-1 vaccine efficacy trial. |
title_sort |
analysis of v2 antibody responses induced in vaccinees in the alvac/aidsvax hiv-1 vaccine efficacy trial. |
publisher |
Public Library of Science (PLoS) |
series |
PLoS ONE |
issn |
1932-6203 |
publishDate |
2013-01-01 |
description |
The RV144 clinical trial of a prime/boost immunizing regimen using recombinant canary pox (ALVAC-HIV) and two gp120 proteins (AIDSVAX B and E) was previously shown to have a 31.2% efficacy rate. Plasma specimens from vaccine and placebo recipients were used in an extensive set of assays to identify correlates of HIV-1 infection risk. Of six primary variables that were studied, only one displayed a significant inverse correlation with risk of infection: the antibody (Ab) response to a fusion protein containing the V1 and V2 regions of gp120 (gp70-V1V2). This finding prompted a thorough examination of the results generated with the complete panel of 13 assays measuring various V2 Abs in the stored plasma used in the initial pilot studies and those used in the subsequent case-control study. The studies revealed that the ALVAC-HIV/AIDSVAX vaccine induced V2-specific Abs that cross-react with multiple HIV-1 subgroups and recognize both conformational and linear epitopes. The conformational epitope was present on gp70-V1V2, while the predominant linear V2 epitope mapped to residues 165-178, immediately N-terminal to the putative α4β7 binding motif in the mid-loop region of V2. Odds ratios (ORs) were calculated to compare the risk of infection with data from 12 V2 assays, and in 11 of these, the ORs were ≤1, reaching statistical significance for two of the variables: Ab responses to gp70-V1V2 and to overlapping V2 linear peptides. It remains to be determined whether anti-V2 Ab responses were directly responsible for the reduced infection rate in RV144 and whether anti-V2 Abs will prove to be important with other candidate HIV vaccines that show efficacy, however, the results support continued dissection of Ab responses to the V2 region which may illuminate mechanisms of protection from HIV-1 infection and may facilitate the development of an effective HIV-1 vaccine. |
url |
http://europepmc.org/articles/PMC3547933?pdf=render |
work_keys_str_mv |
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