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Are Clade Specific HIV Vaccines a Necessity? An Analysis Based on Mathematical Models

As HIV-1 envelope immune responses are critical to vaccine related protection, most candidate HIV vaccines entering efficacy trials are based upon a clade specific design. This need for clade specific vaccine prototypes markedly reduces the implementation of potentially effective HIV vaccines. We ut...

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Autores principales: Dimitrov, Dobromir, Kublin, James G., Ramsey, Scott, Corey, Lawrence
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2015
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4703729/
https://www.ncbi.nlm.nih.gov/pubmed/26844286
http://dx.doi.org/10.1016/j.ebiom.2015.11.009
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author Dimitrov, Dobromir
Kublin, James G.
Ramsey, Scott
Corey, Lawrence
author_facet Dimitrov, Dobromir
Kublin, James G.
Ramsey, Scott
Corey, Lawrence
author_sort Dimitrov, Dobromir
collection PubMed
description As HIV-1 envelope immune responses are critical to vaccine related protection, most candidate HIV vaccines entering efficacy trials are based upon a clade specific design. This need for clade specific vaccine prototypes markedly reduces the implementation of potentially effective HIV vaccines. We utilized a mathematical model to determine the effectiveness of immediate roll-out of a non-clade matched vaccine with reduced efficacy compared to constructing clade specific vaccines, which would take considerable time to manufacture and test in safety and efficacy trials. We simulated the HIV epidemic in San Francisco (SF) and South Africa (SA) and projected effectiveness of three vaccination strategies: i) immediate intervention with a 20–40% vaccine efficacy (VE) non-matched vaccine, ii) delayed intervention by developing a 50% VE clade-specific vaccine, and iii) immediate intervention with a non-matched vaccine replaced by a clade-specific vaccine when developed. Immediate vaccination with a non-clade matched vaccine, even with reduced efficacy, would prevent thousands of new infections in SF and millions in SA over 30 years. Vaccination with 50% VE delayed for five years needs six and 12 years in SA to break-even with immediate 20 and 30% VE vaccination, respectively, while not able to surpass the impact of immediate 40% VE vaccination over 30 years. Replacing a 30% VE with a 50% VE vaccine after 5 years reduces the HIV acquisition by 5% compared to delayed vaccination. The immediate use of an HIV vaccine with reduced VE in high risk communities appears desirable over a short time line but higher VE should be the pursued to achieve strong long-term impact. Our analysis illustrates the importance of developing surrogate markers (correlates of protection) to allow bridging types of immunogenicity studies to support more rapid assessment of clade specific vaccines.
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spelling pubmed-47037292016-02-03 Are Clade Specific HIV Vaccines a Necessity? An Analysis Based on Mathematical Models Dimitrov, Dobromir Kublin, James G. Ramsey, Scott Corey, Lawrence EBioMedicine Research Article As HIV-1 envelope immune responses are critical to vaccine related protection, most candidate HIV vaccines entering efficacy trials are based upon a clade specific design. This need for clade specific vaccine prototypes markedly reduces the implementation of potentially effective HIV vaccines. We utilized a mathematical model to determine the effectiveness of immediate roll-out of a non-clade matched vaccine with reduced efficacy compared to constructing clade specific vaccines, which would take considerable time to manufacture and test in safety and efficacy trials. We simulated the HIV epidemic in San Francisco (SF) and South Africa (SA) and projected effectiveness of three vaccination strategies: i) immediate intervention with a 20–40% vaccine efficacy (VE) non-matched vaccine, ii) delayed intervention by developing a 50% VE clade-specific vaccine, and iii) immediate intervention with a non-matched vaccine replaced by a clade-specific vaccine when developed. Immediate vaccination with a non-clade matched vaccine, even with reduced efficacy, would prevent thousands of new infections in SF and millions in SA over 30 years. Vaccination with 50% VE delayed for five years needs six and 12 years in SA to break-even with immediate 20 and 30% VE vaccination, respectively, while not able to surpass the impact of immediate 40% VE vaccination over 30 years. Replacing a 30% VE with a 50% VE vaccine after 5 years reduces the HIV acquisition by 5% compared to delayed vaccination. The immediate use of an HIV vaccine with reduced VE in high risk communities appears desirable over a short time line but higher VE should be the pursued to achieve strong long-term impact. Our analysis illustrates the importance of developing surrogate markers (correlates of protection) to allow bridging types of immunogenicity studies to support more rapid assessment of clade specific vaccines. Elsevier 2015-11-05 /pmc/articles/PMC4703729/ /pubmed/26844286 http://dx.doi.org/10.1016/j.ebiom.2015.11.009 Text en © 2015 The Authors http://creativecommons.org/licenses/by-nc-nd/4.0/ This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Research Article
Dimitrov, Dobromir
Kublin, James G.
Ramsey, Scott
Corey, Lawrence
Are Clade Specific HIV Vaccines a Necessity? An Analysis Based on Mathematical Models
title Are Clade Specific HIV Vaccines a Necessity? An Analysis Based on Mathematical Models
title_full Are Clade Specific HIV Vaccines a Necessity? An Analysis Based on Mathematical Models
title_fullStr Are Clade Specific HIV Vaccines a Necessity? An Analysis Based on Mathematical Models
title_full_unstemmed Are Clade Specific HIV Vaccines a Necessity? An Analysis Based on Mathematical Models
title_short Are Clade Specific HIV Vaccines a Necessity? An Analysis Based on Mathematical Models
title_sort are clade specific hiv vaccines a necessity? an analysis based on mathematical models
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4703729/
https://www.ncbi.nlm.nih.gov/pubmed/26844286
http://dx.doi.org/10.1016/j.ebiom.2015.11.009
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