Robust Recall and Long-Term Memory T-Cell Responses Induced by Prime-Boost Regimens with Heterologous Live Viral Vectors Expressing Human Immunodeficiency Virus Type 1 Gag and Env Proteins

Haglund, K.E.; Leiner, Ingrid; Kerksiek, Kristen M.; Buonocore, Linda; Pamer, Eric G.; Rose, John K.

doi:10.1128/jvi.76.15.7506-7517.2002

Cited by 63 publications

(56 citation statements)

References 52 publications

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“…In inbred mice, priming with VSV Gag and boosting with vaccinia virus Gag generated about five times more recall and long-term CD8 ϩ T cells than a VSV Gag prime and VSV Gag (G-exchange) boost (11). In macaques a clear trend in the same direction is evident, but the differences in the immune responses do not reach statistical significance.…”

Section: Discussionsupporting

confidence: 52%

“…These studies showed that mice immunized with an rVSV expressing HIV-1 Gag and boosted with a completely heterologous vaccinia virus recombinant expressing HIV-1 Gag generated a fivefold increase in peak Gag-specific CD8 ϩ T cells relative to the levels seen in mice immunized with a VSV vector and boosted with a VSV G protein exchange vector expressing Gag (11). The population of Gag-specific T cells persisting long term was also increased fivefold by the heterologous vaccinia boost.…”

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confidence: 83%

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Highly Effective Control of an AIDS Virus Challenge in Macaques by Using Vesicular Stomatitis Virus and Modified Vaccinia Virus Ankara Vaccine Vectors in a Single-Boost Protocol

Ramsburg

Rose

Marx

et al. 2004

J Virol

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Previous studies have shown that vaccination and boosting of rhesus macaques with attenuated vesicular stomatitis virus (VSV) vectors encoding Env and Gag proteins of simian immunodeficiency virus-human immunodeficiency virus (SHIV) hybrid viruses protect rhesus macaques from AIDS after challenge with the highly pathogenic SHIV 89.6P (23). In the present study, we compared the effectiveness of a single prime-boost protocol consisting of VSV vectors expressing SHIV Env, Gag, and Pol proteins to that of a protocol consisting of a VSV vector prime followed with a single boost with modified vaccinia virus Ankara (MVA) expressing the same SHIV proteins. After challenge with SHIV 89.6P, MVA-boosted animals controlled peak challenge viral loads to less than 2 ؋ 10 6 copies/ml (a level significantly lower than that seen with VSV-boosted animals and lower than those reported for other vaccine studies employing the same challenge). MVA-boosted animals have shown excellent preservation of CD4 ؉ T cells, while two of four VSV-boosted animals have shown significant loss of CD4 ؉ T cells. The improved protection in MVA-boosted animals correlates with trends toward stronger prechallenge CD8؉ -T-cell responses to SHIV antigens and stronger postchallenge SHIV-neutralizing antibody production.

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Section: Discussionsupporting

confidence: 52%

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confidence: 83%

Highly Effective Control of an AIDS Virus Challenge in Macaques by Using Vesicular Stomatitis Virus and Modified Vaccinia Virus Ankara Vaccine Vectors in a Single-Boost Protocol

Ramsburg

Rose

Marx

et al. 2004

J Virol

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“…We found that vaccination with STxB-OVA induced OVA-specific CD8 + T cells detected ex vivo without the need for in vitro restimulation, and this response was long-lasting, as it was still observed at least 3 months after immunization. Such robust and long-lasting memory CD8 + T cell responses have been observed with recombinant viruses [57,58] and ex vivo DC pulsed with antigens [59,60] but with very few carrier proteins [61,62].…”

Section: Discussionmentioning

confidence: 85%

The Shiga toxin B‐subunit targets antigen in vivo to dendritic cells and elicits anti‐tumor immunity

et al. 2006

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The non-toxic B-subunit of Shiga toxin (STxB) interacts with the glycolipid Gb 3 , which is preferentially expressed on dendritic cells (DC) and B cells. After administration of STxB chemically coupled to OVA (STxB-OVA) in mice, we showed that the immunodominant OVA 257-264 peptide restricted by K b molecules is specifically presented by CD11c + CD8a -DC, some of them displaying a mature phenotype. Using mice carrying a transgene encoding a diphtheria toxin receptor (DTR) under the control of the murine CD11c promoter, which allows inducible ablation of DC, we showed that DC are required for efficient priming of CTL after STxB-OVA vaccination. Immunization of mice with STxB-OVA induced OVA-specific CD8 + T cells detected ex vivo; these cells were long lasting, since they could be detected even 91 days after the last immunization and were composed of both central and memory T cells. Vaccination of mice with STxB-OVA and STxB coupled to E7, a protein derived from HPV16, inhibited tumor growth in prophylactic and therapeutic experiments. This effect was mainly mediated by CD8 + T cells. STxB therefore appears to be a powerful carrier directly targeting DC in vivo, resulting in a strong and durable CTL response associated with tumor protection.

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“…infection. 23,25 In this study, the results of CTL activity demonstrated that immunization with vaccine in combination with NLX and alum mixture did not show any significant difference vs. the alum adjuvanted group. However, the study of Molla Hassan et al showed that NLX significantly increased CTL activity for a cancer vaccine in comparison to the un-adjuvanted vaccine.…”

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confidence: 85%

Naloxone/alum mixture a potent adjuvant for HIV-1 vaccine: induction of cellular and poly-isotypic humoral immune responses

Farahani

Aghasadeghi

Memarnejadian

et al. 2016

Pathogens and Global Health

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In the present study we used a fusion peptide from HIV-1 p24 and Nef as vaccine model and adjuvant activity of Naloxone/alum mixture was evaluated in a peptide vaccine model. HIV-1 p24-Nef fusion peptide was synthesized. Female BALB/c mice were divided into five groups. The first group immunized subcutaneously with the p24-Nef fusion peptide adjuvanted with Naloxone/alum mixture and boosted with same protocol. The second was immunized with fusion peptide adjuvanted in alum. The control groups were injected with NLX (Group 3), Alum (Group 4), or PBS (Groups 5) under the same conditions. To determine the type of induced immune response, sera and splenocytes were analyzed by commercial ELISA method for total IgG and isotypes and cytokine secretion (IL-4 & IFN-γ), respectively. We have also used the ELISPOT assay to monitor changes in the frequency of IFN-γ-producing T cells. The proliferation of T cells was assessed using Brdu method and T-cell cytotoxicity was assessed with CFSE method. Immunization of mice with HIV-1 p24-Nef fusion peptide formulated in Naloxone/ alum mixture significantly increased lymphocyte proliferation and shifted cytokine responses toward Th1 profile compared to all other groups. Analysis of humoral immune responses revealed that administration of HIV-1 p24-Nef fusion peptide with Naloxone/alum mixture significantly increased specific IgG responses and also increased IgG1,IgG2a, IgG2b, IgG3, and IgM vs. alum-adjuvanted vaccine groups. Naloxone/alum mixture as an adjuvant could improve cellular and humoral immune response for HIV vaccine model and this adjuvant maybe useful for HIV vaccine model in human clinical trial.

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Robust Recall and Long-Term Memory T-Cell Responses Induced by Prime-Boost Regimens with Heterologous Live Viral Vectors Expressing Human Immunodeficiency Virus Type 1 Gag and Env Proteins

Cited by 63 publications

References 52 publications

Highly Effective Control of an AIDS Virus Challenge in Macaques by Using Vesicular Stomatitis Virus and Modified Vaccinia Virus Ankara Vaccine Vectors in a Single-Boost Protocol

Highly Effective Control of an AIDS Virus Challenge in Macaques by Using Vesicular Stomatitis Virus and Modified Vaccinia Virus Ankara Vaccine Vectors in a Single-Boost Protocol

The Shiga toxin B‐subunit targets antigen in vivo to dendritic cells and elicits anti‐tumor immunity

Naloxone/alum mixture a potent adjuvant for HIV-1 vaccine: induction of cellular and poly-isotypic humoral immune responses

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