Role of Interleukin-4 (IL-4), IL-12, and Gamma Interferon in Primary and Vaccine-Primed Immune Responses to Friend Retrovirus Infection

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Therapeutic strategies for the treatment of acute retroviral infections have relied mainly on antiviral drugs. In this study we used the Friend virus model system to demonstrate that enhancement of the immune system can also have dramatic therapeutic effects. Since resistance to Friend virus-induced leukemia in mice is associated with T helper cell type 1 (Th1) immune responses, we enhanced these responses in susceptible mice by treatment with synthetic oligodeoxynucleotides containing unmethylated CpG motifs (CpG-ODN). Treatments begun at 4 days postinfection increased recovery from 6% in the control group to 74% in the CpG-treated group. CpG-mediated recovery was associated with a significant reduction of viral loads in the blood and spleens of treated mice compared to those of control animals. The treatment promoted Th1-type cytokine production by splenocytes of Friend virus-infected mice and augmented Friend virus-specific cytotoxic T-cell responses, but no influence on the virus-specific neutralizing antibody response was observed. Friend virusspecific CD8 ؉ T cells were critical for effective treatment with CpG-ODN, since in vivo depletion of these cells from treated mice prevented their recovery. Our results demonstrate that CpG-ODN therapy can significantly enhance virus-specific cellular immune responses and prevent retrovirus-induced disease. These findings may have implications for antiviral therapy in general.

mentioning

confidence: 91%

Effective Postexposure Treatment of Retrovirus-Induced Disease with Immunostimulatory DNA Containing CpG Motifs

Olbrich

Schimmer

Heeg

et al. 2002

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“…To detect FV infection, cells were stained with tissue culture supernatant containing monoclonal antibody (MAb) 34 (7), which is specific for F-MuLV glycosylated Gag protein. MAb 34 binding was detected with allophycocyanin-labeled goat anti-mouse IgG2b-specific antiserum (Caltag Laboratories, Burlingame, Calif.) that was preabsorbed with naive mouse spleen cells to remove background activity (13). Directly labeled fluorescent antibodies specific for Ter119 (Ly-76), CD4, CD8, CD19, and CD43 were obtained from Pharmingen (San Diego, Calif.).…”

Section: Methodsmentioning

confidence: 99%

Temporal Effects of Gamma Interferon Deficiency on the Course of Friend Retrovirus Infection in Mice

Stromnes

Dittmer

Schumacher

et al. 2002

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The current studies demonstrate complex and seemingly contradictory effects by gamma interferon (IFN-␥) on Friend virus (FV) infection. Both temporal and tissue-specific effects were observed. During the first week of infection, IFN-␥-deficiency caused increased levels of FV infection in multiple tissues. Surprisingly, however, by 2 weeks postinfection, IFN-␥-deficient mice had significantly lower levels of infection in both the spleen and bone marrow compared to wild-type mice. The rapid reduction of virus in the IFN-␥-deficient mice correlated with a more rapid virus-neutralizing antibody response than was observed in the wild-type mice. Furthermore, the virus-neutralizing antibody response in wild-type mice could be accelerated by ablation of their IFN-␥ response. Although the IFN-␥-deficient mice developed an accelerated virus-neutralizing antibody response, they did not class-switch to immunoglobulin G class immunoglobulins nor could they maintain long-term virus-neutralizing antibody titers. Eventually, all of the IFN-␥-deficient mice failed to keep persistent virus in check and developed fatal FV-induced erythroleukemia.

“…For example, mice of the H-2 b/b haplotype are resistant to FV-induced disease because they mount lymphocyte responses that appear earlier and are of higher magnitude than those of mice with an H-2 a/b haplotype, which are susceptible to FV-mediated leukemia (8,21). Immunity to FV is associated with a Th1-type immune response, including the production of gamma interferon and the activation of T cells (4,21). Since CpG-ODN shift the immune system toward a Th1-dominated response, it was possible that CpG-ODN pretreatment of FV-susceptible mice might induce resistance.…”

mentioning

confidence: 99%

Preinfection Treatment of Resistant Mice with CpG Oligodeoxynucleotides Renders Them Susceptible to Friend Retrovirus-Induced Leukemia

Olbrich

Schimmer

Dittmer³

2003

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