Abstract

An AIDS vaccine approach combining adenovirus (Ad)-HIV recombinant priming with envelope protein boosting has been pursued. Chimpanzee studies demonstrated long-lasting protection against low- and high-dose HIV challenges without intervening immunizations. Only a minimal number of immunizations were necessary to elicit protective immunity along with antibodies capable of neutralizing primary and lab-adapted isolates. A role for cytotoxic T-lymphocytes in protection against low-dose challenge was also suggested. After boosting and a third re-challenge of the 3 protected chimpanzees with a non-syncytial- inducing primary isolate, one animal was completely protected and a second exhibited a reduced viral burden compared to the naive control. This first demonstration of protection against a heterologous primary isolate is highly encouraging and strongly supports further development of this vaccine approach. Priming of rhesus macaques with an Ad host range mutant-SIV recombinant and boosting with SIV envelope protein elicited humoral, cellular and mucosal immune responses. Upon intravaginal SIV challenge, the viral burden was reduced 10 to 100-fold during the acute infection period compared to control macaques. Notably, protection in both these systems was achieved using vaccines based only on the viral envelope. Addition of other viral components should significantly increase protective immunity. Further prime-boost studies in macaques using molecularly attenuated vaccinia SIV recombinants, with or without recombinant- expressed cytokine adjuvants, have shown induction of soluble CD8+ T-cell viral suppressive activity. Pre-challenge levels of this activity were correlated with steady-state plasma viral RNA levels post-intravenous SIV challenge. Moreover, high post-challenge levels correlated with non- progressor status while low levels correlated with rapid disease progression. These findings suggest future vaccine design should include induction of this suppressive activity. AIDS title: Adenovirus and Attenuated Poxvirus Vectors in AIDS Vaccine Development

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Intramural Research (Z01)
Project #
1Z01BC005536-12
Application #
6100816
Study Section
Special Emphasis Panel (BRL)
Project Start
Project End
Budget Start
Budget End
Support Year
12
Fiscal Year
1998
Total Cost
Indirect Cost

  Institution

Name
National Cancer Institute Division of Basic Sciences
Department
Type
DUNS #
City
State
Country
United States
Zip Code

  Publications

Tuero, Iskra; Venzon, David; Robert-Guroff, Marjorie (2016) Mucosal and Systemic ??+ T Cells Associated with Control of Simian Immunodeficiency Virus Infection. J Immunol 197:4686-4695
Musich, Thomas; Robert-Guroff, Marjorie (2016) New developments in an old strategy: heterologous vector primes and envelope protein boosts in HIV vaccine design. Expert Rev Vaccines 15:1015-27
Mohanram, Venkatramanan; Demberg, Thorsten; Musich, Thomas et al. (2016) B Cell Responses Associated with Vaccine-Induced Delayed SIVmac251 Acquisition in Female Rhesus Macaques. J Immunol 197:2316-24
Musich, Thomas; Demberg, Thorsten; Morgan, Ian L et al. (2015) Purification and functional characterization of mucosal IgA from vaccinated and SIV-infected rhesus macaques. Clin Immunol 158:127-39
Demberg, Thorsten; Mohanram, Venkatramanan; Musich, Thomas et al. (2015) Loss of marginal zone B-cells in SHIVSF162P4 challenged rhesus macaques despite control of viremia to low or undetectable levels in chronic infection. Virology 484:323-33
Vargas-Inchaustegui, Diego A; Robert-Guroff, Marjorie (2013) Fc receptor-mediated immune responses: new tools but increased complexity in HIV prevention. Curr HIV Res 11:407-20
Demberg, Thorsten; Brocca-Cofano, Egidio; Kuate, Seraphin et al. (2013) Impact of antibody quality and anamnestic response on viremia control post-challenge in a combined Tat/Env vaccine regimen in rhesus macaques. Virology 440:210-21
Demberg, Thorsten; Robert-Guroff, Marjorie (2009) Mucosal immunity and protection against HIV/SIV infection: strategies and challenges for vaccine design. Int Rev Immunol 28:20-48
Florese, Ruth H; Demberg, Thorsten; Xiao, Peng et al. (2009) Contribution of nonneutralizing vaccine-elicited antibody activities to improved protective efficacy in rhesus macaques immunized with Tat/Env compared with multigenic vaccines. J Immunol 182:3718-27
Florese, Ruth H; Wiseman, Roger W; Venzon, David et al. (2008) Comparative study of Tat vaccine regimens in Mauritian cynomolgus and Indian rhesus macaques: influence of Mauritian MHC haplotypes on susceptibility/resistance to SHIV(89.6P) infection. Vaccine 26:3312-21

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