Vaccine-induced human antibodies specific for the third variable region of HIV-1 gp120 impose immune pressure on infecting viruses
© 2014 The Authors. To evaluate the role of V3-specific IgG+antibodies (Abs) in the RV144 clinical HIV vaccine trial, which reducedHIV-1 infection by 31.2%, the anti-V3 Ab response was assessed. Vaccinees' V3 Abs were highly cross-reactivewith cyclic V3 peptides (cV3s) from diverse virus subtyp...
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th-mahidol.334962018-11-09T09:00:46Z Vaccine-induced human antibodies specific for the third variable region of HIV-1 gp120 impose immune pressure on infecting viruses Susan Zolla-Pazner Paul T. Edlefsen Morgane Rolland Xiang Peng Kong Allan deCamp Raphael Gottardo Constance Williams Sodsai Tovanabutra Sandra Sharpe-Cohen James I. Mullins Mark S. deSouza Nicos Karasavvas Sorachai Nitayaphan Supachai Rerks-Ngarm Punnee Pitisuttihumi Jaranit Kaewkungwal Robert J. O'Connell Merlin L. Robb Nelson L. Michael Jerome H. Kim Peter Gilbert New York Veterans Affairs Harbor Healthcare System NYU School of Medicine Fred Hutchinson Cancer Research Center Walter Reed Army Institute of Research University of Washington, Seattle Thai Red Cross AIDS Research Centre Armed Forces Research Institute of Medical Sciences, Thailand Thailand Ministry of Public Health Mahidol University US Military HIV Research Program Biochemistry, Genetics and Molecular Biology © 2014 The Authors. To evaluate the role of V3-specific IgG+antibodies (Abs) in the RV144 clinical HIV vaccine trial, which reducedHIV-1 infection by 31.2%, the anti-V3 Ab response was assessed. Vaccinees' V3 Abs were highly cross-reactivewith cyclic V3 peptides (cV3s) from diverse virus subtypes. Sieve analysis of CRF01_AE breakthrough virusesfrom 43 vaccine- and 66 placebo-recipients demonstrated an estimated vaccine efficacy of 85% against viruseswith amino acids mismatching the vaccine at V3 site 317 (p= 0.004) and 52% against virusesmatching the vaccineat V3 site 307 (p = 0.004). This analysis was supported by data showing that vaccinees' plasma Abs wereless reactive with I307when replaced with residues foundmore often in vaccinees' breakthrough viruses. Simultaneously, viruses with mutations at F317were less infectious, possibly due to the contribution of F317to optimalformation of the V3 hydrophobic core. These data suggest that RV144-induced V3-specific Abs imposed immunepressure on infecting viruses and inform efforts to design an HIV vaccine. 2018-11-09T02:00:46Z 2018-11-09T02:00:46Z 2014-01-01 Article EBioMedicine. Vol.1, No.1 (2014), 37-45 10.1016/j.ebiom.2014.10.022 23523964 2-s2.0-84921972284 https://repository.li.mahidol.ac.th/handle/123456789/33496 Mahidol University SCOPUS https://www.scopus.com/inward/record.uri?partnerID=HzOxMe3b&scp=84921972284&origin=inward |
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Biochemistry, Genetics and Molecular Biology Susan Zolla-Pazner Paul T. Edlefsen Morgane Rolland Xiang Peng Kong Allan deCamp Raphael Gottardo Constance Williams Sodsai Tovanabutra Sandra Sharpe-Cohen James I. Mullins Mark S. deSouza Nicos Karasavvas Sorachai Nitayaphan Supachai Rerks-Ngarm Punnee Pitisuttihumi Jaranit Kaewkungwal Robert J. O'Connell Merlin L. Robb Nelson L. Michael Jerome H. Kim Peter Gilbert Vaccine-induced human antibodies specific for the third variable region of HIV-1 gp120 impose immune pressure on infecting viruses |
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© 2014 The Authors. To evaluate the role of V3-specific IgG+antibodies (Abs) in the RV144 clinical HIV vaccine trial, which reducedHIV-1 infection by 31.2%, the anti-V3 Ab response was assessed. Vaccinees' V3 Abs were highly cross-reactivewith cyclic V3 peptides (cV3s) from diverse virus subtypes. Sieve analysis of CRF01_AE breakthrough virusesfrom 43 vaccine- and 66 placebo-recipients demonstrated an estimated vaccine efficacy of 85% against viruseswith amino acids mismatching the vaccine at V3 site 317 (p= 0.004) and 52% against virusesmatching the vaccineat V3 site 307 (p = 0.004). This analysis was supported by data showing that vaccinees' plasma Abs wereless reactive with I307when replaced with residues foundmore often in vaccinees' breakthrough viruses. Simultaneously, viruses with mutations at F317were less infectious, possibly due to the contribution of F317to optimalformation of the V3 hydrophobic core. These data suggest that RV144-induced V3-specific Abs imposed immunepressure on infecting viruses and inform efforts to design an HIV vaccine. |
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New York Veterans Affairs Harbor Healthcare System |
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New York Veterans Affairs Harbor Healthcare System Susan Zolla-Pazner Paul T. Edlefsen Morgane Rolland Xiang Peng Kong Allan deCamp Raphael Gottardo Constance Williams Sodsai Tovanabutra Sandra Sharpe-Cohen James I. Mullins Mark S. deSouza Nicos Karasavvas Sorachai Nitayaphan Supachai Rerks-Ngarm Punnee Pitisuttihumi Jaranit Kaewkungwal Robert J. O'Connell Merlin L. Robb Nelson L. Michael Jerome H. Kim Peter Gilbert |
format |
Article |
author |
Susan Zolla-Pazner Paul T. Edlefsen Morgane Rolland Xiang Peng Kong Allan deCamp Raphael Gottardo Constance Williams Sodsai Tovanabutra Sandra Sharpe-Cohen James I. Mullins Mark S. deSouza Nicos Karasavvas Sorachai Nitayaphan Supachai Rerks-Ngarm Punnee Pitisuttihumi Jaranit Kaewkungwal Robert J. O'Connell Merlin L. Robb Nelson L. Michael Jerome H. Kim Peter Gilbert |
author_sort |
Susan Zolla-Pazner |
title |
Vaccine-induced human antibodies specific for the third variable region of HIV-1 gp120 impose immune pressure on infecting viruses |
title_short |
Vaccine-induced human antibodies specific for the third variable region of HIV-1 gp120 impose immune pressure on infecting viruses |
title_full |
Vaccine-induced human antibodies specific for the third variable region of HIV-1 gp120 impose immune pressure on infecting viruses |
title_fullStr |
Vaccine-induced human antibodies specific for the third variable region of HIV-1 gp120 impose immune pressure on infecting viruses |
title_full_unstemmed |
Vaccine-induced human antibodies specific for the third variable region of HIV-1 gp120 impose immune pressure on infecting viruses |
title_sort |
vaccine-induced human antibodies specific for the third variable region of hiv-1 gp120 impose immune pressure on infecting viruses |
publishDate |
2018 |
url |
https://repository.li.mahidol.ac.th/handle/123456789/33496 |
_version_ |
1763488717001981952 |