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Control of Heterologous Simian Immunodeficiency Virus SIV(smE660) Infection by DNA and Protein Coimmunization Regimens Combined with Different Toll-Like-Receptor-4-Based Adjuvants in Macaques

We developed a method of simultaneous vaccination with DNA and protein resulting in robust and durable cellular and humoral immune responses with efficient dissemination to mucosal sites and protection against simian immunodeficiency virus (SIV) infection. To further optimize the DNA-protein coimmun...

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Autores principales: Singh, Shakti, Ramírez-Salazar, Eric G., Doueiri, Rami, Valentin, Antonio, Rosati, Margherita, Hu, Xintao, Keele, Brandon F., Shen, Xiaoying, Tomaras, Georgia D., Ferrari, Guido, LaBranche, Celia, Montefiori, David C., Das, Jishnu, Alter, Galit, Trinh, Hung V., Hamlin, Christopher, Rao, Mangala, Dayton, Frances, Bear, Jenifer, Chowdhury, Bhabadeb, Alicea, Candido, Lifson, Jeffrey D., Broderick, Kate E., Sardesai, Niranjan Y., Sivananthan, Sandra J., Fox, Christopher B., Reed, Steven G., Venzon, David J., Hirsch, Vanessa M., Pavlakis, George N., Felber, Barbara K.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Society for Microbiology 2018
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6052320/
https://www.ncbi.nlm.nih.gov/pubmed/29793957
http://dx.doi.org/10.1128/JVI.00281-18
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author Singh, Shakti
Ramírez-Salazar, Eric G.
Doueiri, Rami
Valentin, Antonio
Rosati, Margherita
Hu, Xintao
Keele, Brandon F.
Shen, Xiaoying
Tomaras, Georgia D.
Ferrari, Guido
LaBranche, Celia
Montefiori, David C.
Das, Jishnu
Alter, Galit
Trinh, Hung V.
Hamlin, Christopher
Rao, Mangala
Dayton, Frances
Bear, Jenifer
Chowdhury, Bhabadeb
Alicea, Candido
Lifson, Jeffrey D.
Broderick, Kate E.
Sardesai, Niranjan Y.
Sivananthan, Sandra J.
Fox, Christopher B.
Reed, Steven G.
Venzon, David J.
Hirsch, Vanessa M.
Pavlakis, George N.
Felber, Barbara K.
author_facet Singh, Shakti
Ramírez-Salazar, Eric G.
Doueiri, Rami
Valentin, Antonio
Rosati, Margherita
Hu, Xintao
Keele, Brandon F.
Shen, Xiaoying
Tomaras, Georgia D.
Ferrari, Guido
LaBranche, Celia
Montefiori, David C.
Das, Jishnu
Alter, Galit
Trinh, Hung V.
Hamlin, Christopher
Rao, Mangala
Dayton, Frances
Bear, Jenifer
Chowdhury, Bhabadeb
Alicea, Candido
Lifson, Jeffrey D.
Broderick, Kate E.
Sardesai, Niranjan Y.
Sivananthan, Sandra J.
Fox, Christopher B.
Reed, Steven G.
Venzon, David J.
Hirsch, Vanessa M.
Pavlakis, George N.
Felber, Barbara K.
author_sort Singh, Shakti
collection PubMed
description We developed a method of simultaneous vaccination with DNA and protein resulting in robust and durable cellular and humoral immune responses with efficient dissemination to mucosal sites and protection against simian immunodeficiency virus (SIV) infection. To further optimize the DNA-protein coimmunization regimen, we tested a SIV(mac251)-based vaccine formulated with either of two Toll-like receptor 4 (TLR4) ligand-based liposomal adjuvant formulations (TLR4 plus TLR7 [TLR4+7] or TLR4 plus QS21 [TLR4+QS21]) in macaques. Although both vaccines induced humoral responses of similar magnitudes, they differed in their functional quality, including broader neutralizing activity and effector functions in the TLR4+7 group. Upon repeated heterologous SIV(smE660) challenge, a trend of delayed viral acquisition was found in vaccinees compared to controls, which reached statistical significance in animals with the TRIM-5α-resistant (TRIM-5α R) allele. Vaccinees were preferentially infected by an SIV(smE660) transmitted/founder virus carrying neutralization-resistant A/K mutations at residues 45 and 47 in Env, demonstrating a strong vaccine-induced sieve effect. In addition, the delay in virus acquisition directly correlated with SIV(smE660)-specific neutralizing antibodies. The presence of mucosal V1V2 IgG binding antibodies correlated with a significantly decreased risk of virus acquisition in both TRIM-5α R and TRIM-5α-moderate/sensitive (TRIM-5α M/S) animals, although this vaccine effect was more prominent in animals with the TRIM-5α R allele. These data support the combined contribution of immune responses and genetic background to vaccine efficacy. Humoral responses targeting V2 and SIV-specific T cell responses correlated with viremia control. In conclusion, the combination of DNA and gp120 Env protein vaccine regimens using two different adjuvants induced durable and potent cellular and humoral responses contributing to a lower risk of infection by heterologous SIV challenge. IMPORTANCE An effective AIDS vaccine continues to be of paramount importance for the control of the pandemic, and it has been proven to be an elusive target. Vaccine efficacy trials and macaque challenge studies indicate that protection may be the result of combinations of many parameters. We show that a combination of DNA and protein vaccinations applied at the same time provides rapid and robust cellular and humoral immune responses and evidence for a reduced risk of infection. Vaccine-induced neutralizing antibodies and Env V2-specific antibodies at mucosal sites contribute to the delay of SIV(smE660) acquisition, and genetic makeup (TRIM-5α) affects the effectiveness of the vaccine. These data are important for the design of better vaccines and may also affect other vaccine platforms.
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spelling pubmed-60523202018-07-27 Control of Heterologous Simian Immunodeficiency Virus SIV(smE660) Infection by DNA and Protein Coimmunization Regimens Combined with Different Toll-Like-Receptor-4-Based Adjuvants in Macaques Singh, Shakti Ramírez-Salazar, Eric G. Doueiri, Rami Valentin, Antonio Rosati, Margherita Hu, Xintao Keele, Brandon F. Shen, Xiaoying Tomaras, Georgia D. Ferrari, Guido LaBranche, Celia Montefiori, David C. Das, Jishnu Alter, Galit Trinh, Hung V. Hamlin, Christopher Rao, Mangala Dayton, Frances Bear, Jenifer Chowdhury, Bhabadeb Alicea, Candido Lifson, Jeffrey D. Broderick, Kate E. Sardesai, Niranjan Y. Sivananthan, Sandra J. Fox, Christopher B. Reed, Steven G. Venzon, David J. Hirsch, Vanessa M. Pavlakis, George N. Felber, Barbara K. J Virol Vaccines and Antiviral Agents We developed a method of simultaneous vaccination with DNA and protein resulting in robust and durable cellular and humoral immune responses with efficient dissemination to mucosal sites and protection against simian immunodeficiency virus (SIV) infection. To further optimize the DNA-protein coimmunization regimen, we tested a SIV(mac251)-based vaccine formulated with either of two Toll-like receptor 4 (TLR4) ligand-based liposomal adjuvant formulations (TLR4 plus TLR7 [TLR4+7] or TLR4 plus QS21 [TLR4+QS21]) in macaques. Although both vaccines induced humoral responses of similar magnitudes, they differed in their functional quality, including broader neutralizing activity and effector functions in the TLR4+7 group. Upon repeated heterologous SIV(smE660) challenge, a trend of delayed viral acquisition was found in vaccinees compared to controls, which reached statistical significance in animals with the TRIM-5α-resistant (TRIM-5α R) allele. Vaccinees were preferentially infected by an SIV(smE660) transmitted/founder virus carrying neutralization-resistant A/K mutations at residues 45 and 47 in Env, demonstrating a strong vaccine-induced sieve effect. In addition, the delay in virus acquisition directly correlated with SIV(smE660)-specific neutralizing antibodies. The presence of mucosal V1V2 IgG binding antibodies correlated with a significantly decreased risk of virus acquisition in both TRIM-5α R and TRIM-5α-moderate/sensitive (TRIM-5α M/S) animals, although this vaccine effect was more prominent in animals with the TRIM-5α R allele. These data support the combined contribution of immune responses and genetic background to vaccine efficacy. Humoral responses targeting V2 and SIV-specific T cell responses correlated with viremia control. In conclusion, the combination of DNA and gp120 Env protein vaccine regimens using two different adjuvants induced durable and potent cellular and humoral responses contributing to a lower risk of infection by heterologous SIV challenge. IMPORTANCE An effective AIDS vaccine continues to be of paramount importance for the control of the pandemic, and it has been proven to be an elusive target. Vaccine efficacy trials and macaque challenge studies indicate that protection may be the result of combinations of many parameters. We show that a combination of DNA and protein vaccinations applied at the same time provides rapid and robust cellular and humoral immune responses and evidence for a reduced risk of infection. Vaccine-induced neutralizing antibodies and Env V2-specific antibodies at mucosal sites contribute to the delay of SIV(smE660) acquisition, and genetic makeup (TRIM-5α) affects the effectiveness of the vaccine. These data are important for the design of better vaccines and may also affect other vaccine platforms. American Society for Microbiology 2018-07-17 /pmc/articles/PMC6052320/ /pubmed/29793957 http://dx.doi.org/10.1128/JVI.00281-18 Text en Copyright © 2018 Singh et al. https://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution 4.0 International license (https://creativecommons.org/licenses/by/4.0/) .
spellingShingle Vaccines and Antiviral Agents
Singh, Shakti
Ramírez-Salazar, Eric G.
Doueiri, Rami
Valentin, Antonio
Rosati, Margherita
Hu, Xintao
Keele, Brandon F.
Shen, Xiaoying
Tomaras, Georgia D.
Ferrari, Guido
LaBranche, Celia
Montefiori, David C.
Das, Jishnu
Alter, Galit
Trinh, Hung V.
Hamlin, Christopher
Rao, Mangala
Dayton, Frances
Bear, Jenifer
Chowdhury, Bhabadeb
Alicea, Candido
Lifson, Jeffrey D.
Broderick, Kate E.
Sardesai, Niranjan Y.
Sivananthan, Sandra J.
Fox, Christopher B.
Reed, Steven G.
Venzon, David J.
Hirsch, Vanessa M.
Pavlakis, George N.
Felber, Barbara K.
Control of Heterologous Simian Immunodeficiency Virus SIV(smE660) Infection by DNA and Protein Coimmunization Regimens Combined with Different Toll-Like-Receptor-4-Based Adjuvants in Macaques
title Control of Heterologous Simian Immunodeficiency Virus SIV(smE660) Infection by DNA and Protein Coimmunization Regimens Combined with Different Toll-Like-Receptor-4-Based Adjuvants in Macaques
title_full Control of Heterologous Simian Immunodeficiency Virus SIV(smE660) Infection by DNA and Protein Coimmunization Regimens Combined with Different Toll-Like-Receptor-4-Based Adjuvants in Macaques
title_fullStr Control of Heterologous Simian Immunodeficiency Virus SIV(smE660) Infection by DNA and Protein Coimmunization Regimens Combined with Different Toll-Like-Receptor-4-Based Adjuvants in Macaques
title_full_unstemmed Control of Heterologous Simian Immunodeficiency Virus SIV(smE660) Infection by DNA and Protein Coimmunization Regimens Combined with Different Toll-Like-Receptor-4-Based Adjuvants in Macaques
title_short Control of Heterologous Simian Immunodeficiency Virus SIV(smE660) Infection by DNA and Protein Coimmunization Regimens Combined with Different Toll-Like-Receptor-4-Based Adjuvants in Macaques
title_sort control of heterologous simian immunodeficiency virus siv(sme660) infection by dna and protein coimmunization regimens combined with different toll-like-receptor-4-based adjuvants in macaques
topic Vaccines and Antiviral Agents
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6052320/
https://www.ncbi.nlm.nih.gov/pubmed/29793957
http://dx.doi.org/10.1128/JVI.00281-18
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