Improved Vaccine Protection from Simian AIDS by the Addition of Nonstructural Simian Immunodeficiency Virus Genes

Hel, Zdeněk; Tsai, Wen-Po; Tryniszewska, Elżbieta; Nacsa, János; Markham, Phillip D.; Lewis, Mark G.; Pavlakis, George N.; Felber, Barbara K.; Tartaglia, Jim; Franchini, Genoveffa

doi:10.4049/jimmunol.176.1.85

Cited by 63 publications

(66 citation statements)

References 80 publications

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“…These results suggest an important role for Nef and Gag cellular immune responses that appear to be driven by virus replication in the early phase of the infection. Similar results have been reported for anamnestic responses against Gag (Dale et al, 2004;Hel et al, 2006). However, for SIV Gag, pre-challenge, vaccineinduced responses were also found to correlate with suppression of virus replication when a DNA prime/ Nef-, SIV mac Nef-and SIV mac Gag-stimulated wells, per million PBMCs measured either 6 weeks after the fourth (last) immunization or 2 weeks after challenge, as well as the individual SIV Nef-and SIV Gag-specific IFN-c ELISpot responses measured 2 weeks after challenge, are plotted against the steadystate plasma virus load, measured 28 weeks after challenge.…”

Section: Discussionsupporting

confidence: 88%

“…DNA vaccines were shown to induce both humoral and cellular immune responses in rodents, but in non-human primates and in humans, only low-level immunogenicity has been reported (Estcourt et al, 2004;Robinson, 1999). Efforts have been directed at improving these responses by boosting with viral vectors (Amara et al, 2002;Brave et al, 2007;Casimiro et al, 2005;Doria-Rose et al, 2003;Hel et al, 2006;Koopman et al, 2004;Letvin et al, 2004). DNA vaccines are generally effective at stimulating CD8 responses, whilst subunit vaccines are more effective at eliciting antibody responses (Barouch et al, 2000;Earl et al, 2001Earl et al, , 2002Patterson et al, 2004;Robinson, 1999).…”

Section: Introductionmentioning

confidence: 99%

“…Strategies to improve the efficacy of HIV-1 Env singlecomponent vaccines have been directed at inclusion of gag/ pol structural and/or tat, rev and nef regulatory gene products (Calarota et al, 1998;Hel et al, 2006;Stittelaar et al, 2002;Wilson et al, 2006). Whilst immunization with simian immunodeficiency virus (SIV) Gag, alone or in combination with HIV-1 Env or Nef and Tat, has already yielded promising results, the data must be interpreted with caution as, in most cases, Mamu A*01-positive animals, which mount a particularly robust response to highly conserved Gag peptides, were used (Amara et al, 2001(Amara et al, , 2002Barouch et al, 2001;Casimiro et al, 2005;Egan et al, 2004;Montefiori et al, 1996;Mooij et al, 2004;Seth et al, 2000;Shiver et al, 2002).…”

Section: Introductionmentioning

confidence: 99%

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Immune-response profiles induced by human immunodeficiency virus type 1 vaccine DNA, protein or mixed-modality immunization: increased protection from pathogenic simian–human immunodeficiency virus viraemia with protein/DNA combination

Koopman

Mortier

Hofman

et al. 2008

Journal of General Virology

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Current data suggest that prophylactic human immunodeficiency virus type 1 (HIV) vaccines will be most efficacious if they elicit a combination of adaptive humoral and T-cell responses. Here, we explored the use of different vaccine strategies in heterologous prime–boost regimes and evaluated the breadth and nature of immune responses in rhesus monkeys induced by epidermally delivered plasmid DNA or recombinant HIV proteins formulated in the AS02A adjuvant system. These immunogens were administered alone or as either prime or boost in mixed-modality regimes. DNA immunization alone induced cell-mediated immune (CMI) responses, with a strong bias towards Th1-type cytokines, and no detectable antibodies to the vaccine antigens. Whenever adjuvanted protein was used as a vaccine, either alone or in a regime combined with DNA, high-titre antibody responses to all vaccine antigens were detected in addition to strong Th1- and Th2-type CMI responses. As the vaccine antigens included HIV-1 Env, Nef and Tat, as well as simian immunodeficiency virus (SIV)mac239 Nef, the animals were subsequently exposed to a heterologous, pathogenic simian–human immunodeficiency virus (SHIV)89.6p challenge. Protection against sustained high virus load was observed to some degree in all vaccinated groups. Suppression of virus replication to levels below detection was observed most frequently in the group immunized with protein followed by DNA immunization, and similarly in the group immunized with DNA alone. Interestingly, control of virus replication was associated with increased SIV Nef- and Gag-specific gamma interferon responses observed immediately following challenge.

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Section: Discussionsupporting

confidence: 88%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Immune-response profiles induced by human immunodeficiency virus type 1 vaccine DNA, protein or mixed-modality immunization: increased protection from pathogenic simian–human immunodeficiency virus viraemia with protein/DNA combination

Koopman

Mortier

Hofman

et al. 2008

Journal of General Virology

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“…Tat combined with other HIV antigens might better confer protection at higher challenge doses. Immunizations with Tat plus Rev and Tat plus other nonstructural HIV gene products have shown protection against SIV [45,46]. A potential synergy between Tat and Env leading to enhanced protective efficacy in rhesus macaques against SHIV 89.6P was recently reported [44].…”

Section: Discussionmentioning

confidence: 99%

“…The significantly higher peak Tat-specific T cell proliferative responses seen in vaccinated macaques with the resistant haplotypes prior to challenge suggest cellular immunity should be further explored as a possible mechanism for the observed resistance. Results of the haplotype analysis and vaccine evaluations, together with reports showing that vaccines targeting Tat in combination with other viral proteins elicit good protective efficacy in non-human primates [44][45][46], suggest that HIV Tat vaccines might be best exploited in combination with other viral antigens.…”

Section: Introductionmentioning

confidence: 98%

Comparative study of Tat vaccine regimens in Mauritian cynomolgus and Indian rhesus macaques: Influence of Mauritian MHC haplotypes on susceptibility/resistance to SHIV89.6P infection

Florese

Wiseman

Venzon

et al. 2008

Vaccine

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Protection afforded by HIV Tat-based vaccines has differed in Indian rhesus and Mauritian cynomolgus macaques. We evaluated native Tat and Ad-HIVtat priming/Tat-boosting regimens in both species. Both vaccines were immunogenic. Only the Ad-tat regimen modestly reduced acute viremia in rhesus macaques after SHIV 89.6P challenge. Confounding variables uncovered in Mauritian macaques included significant associations of susceptibility to infection with MHC class IB and class II H2 and H5 haplotypes, and resistance to infection with class IB haplotypes H3 and H6. Although protection here was limited, Tat-based vaccines incorporating other HIV components have shown greater efficacy. Combination strategies should be further explored.

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Nonhuman Primate Models for HIV/AIDS Vaccine Development

et al. 2013

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The development of HIV vaccines has been hampered by the lack of an animal model that can accurately predict vaccine efficacy. Chimpanzees can be infected with HIV-1 but are not practical for research. However, several species of macaques are susceptible to the Simian Immunodeficiency Viruses (SIV) that causes a disease in macaques that closely mimics HIV in humans. Thus, macaque-SIV models of HIV infection have become a critical foundation for AIDS vaccine development. Here, we examine the multiple variables and considerations that must be taken into account to use this NHP model effectively. These include the species and subspecies of macaques, virus strain, dose and route of administration and macaque genetics including Major Histocompatibility Complex molecules that affect immune responses and other virus restriction factors. We illustrate how these NHP models can be used to carry out studies of immune responses in mucosal and other tissues than could not easily be performed on human volunteers. Futhermore macaques are an ideal model system to optimize adjuvants, test vaccine platforms, and identify correlates of protection that can advance the HIV vaccine field. We also illustrate techniques used to identify different macaque lymphocyte populations and review some poxvirus vaccine candidates that are in various stages of clinical trials. Understanding how to effectively use this valuable model will greatly increase the likelihood of finding a successful vaccine for HIV.

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Improved Vaccine Protection from Simian AIDS by the Addition of Nonstructural Simian Immunodeficiency Virus Genes

Cited by 63 publications

References 80 publications

Immune-response profiles induced by human immunodeficiency virus type 1 vaccine DNA, protein or mixed-modality immunization: increased protection from pathogenic simian–human immunodeficiency virus viraemia with protein/DNA combination

Immune-response profiles induced by human immunodeficiency virus type 1 vaccine DNA, protein or mixed-modality immunization: increased protection from pathogenic simian–human immunodeficiency virus viraemia with protein/DNA combination

Comparative study of Tat vaccine regimens in Mauritian cynomolgus and Indian rhesus macaques: Influence of Mauritian MHC haplotypes on susceptibility/resistance to SHIV89.6P infection

Nonhuman Primate Models for HIV/AIDS Vaccine Development

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