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Research Topic : epitopes, ctl
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  • Funded Activity

    Differences In Immune Recognition Amongst EB Isolates

    Funder
    National Health and Medical Research Council
    Funding Amount
    $158,407.00
    More information
    Funded Activity

    Characterisation Of The Human Cellular And Humoral Response To The Major Latex Allergen, HEV B 5.

    Funder
    National Health and Medical Research Council
    Funding Amount
    $79,977.00
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    Funded Activity

    CTL Avidity As A Determinant Of The Mature, Antigen-specific Immune Repertoire

    Funder
    National Health and Medical Research Council
    Funding Amount
    $241,527.00
    Summary
    Killer T lymphocytes are a diverse population which vary in their ability to recognise infected cells. This study aims to determine whether vaccine dose and frequency impact on the generation of highly sensitive killer T cells. This study will improve our basic knowledge of killer T lymphocyte selection during infection and have application to improved methods of vaccination.
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    Funded Activity

    Novel Generic Vaccine Approaches Applied For The Prevention Of Hepatitis C And Influenza Virus Infections.

    Funder
    National Health and Medical Research Council
    Funding Amount
    $392,328.00
    Summary
    For the induction of good immune responses, antigens should be delivered in several copies on a defined particle. The small envelope protein (HBsAg) encoded by the hepatitis B virus (HBV) has the capacity to self-assemble with host derived lipids into VLPs. HBsAg VLPs are the sole component of one of the most successful vaccines, and clinical trials have shown that they are a successful delivery system for foreign epitopes or protein domains. Hepatitis C virus (HCV) and Influenza viruses are maj .... For the induction of good immune responses, antigens should be delivered in several copies on a defined particle. The small envelope protein (HBsAg) encoded by the hepatitis B virus (HBV) has the capacity to self-assemble with host derived lipids into VLPs. HBsAg VLPs are the sole component of one of the most successful vaccines, and clinical trials have shown that they are a successful delivery system for foreign epitopes or protein domains. Hepatitis C virus (HCV) and Influenza viruses are major human pathogens. HCV has infected 200 million people worldwide, and there is no effective vaccine available. Influenza continues to affect thousands of people each year causing epidemics with severe morbidity and considerable mortality. Current influenza vaccines are mostly inactivated formulations and they exhibit poor immunogenicity in immunological naive persons such as children and in the elderly. The influenza vaccines are not optimal for stimulation of cell-mediated immunity. We propose to use particulate antigens as a delivery platform for influenza and HCV-specific epitopes with the focus to develop approaches to target various HCV and influenza strains, including H5N1 bird influenza. We have successfully produced modified VLPs containing HCV-specific sequences, which are able to induce anti-HCV antibodies with neutralising capacity. We hypothesise that the design of VLPs with an appropriate set of HCV-specific antigens will enhance the neutralising capacity of anti-HCV sera and this may overcome strain specificity. This application will exploit a prototype delivery system to induce antibody and also cellular responses against a variety of HCV- and influenza specific target sequences (epitopes). The outcome of this study will be a prototype multivalent vaccine to a range of HCV- and influenza-specific epitopes. As a delivery system this will be ideal for vaccination against agents that are highly variable.
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    Funded Activity

    Understanding The Mechanism And Significance Of CXCL16-mediated Protection Of Tumour Cells From CTL-induced Apoptosis.

    Funder
    National Health and Medical Research Council
    Funding Amount
    $524,520.00
    Summary
    This research will begin to determine the significance of changes in the amount of a recently-discovered protein on the surface of tumour cells. We have shown that an increase in expression of this protein protects tumour cells from destruction by our immune system's killer T cells. The outcome of this research could lead to a better understanding of how the immune system recognises and kills tumour cells, and ultimately, alternate vaccine strategies for tumours.
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    Funded Activity

    Studies On Mosquito-transmitted Viruses Of Medical Impo Rtance In Australia

    Funder
    National Health and Medical Research Council
    Funding Amount
    $329,773.00
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    Funded Activity

    Epitopes Of A Major Latex Allergen And Mutagenesis To Express Hypoallergenic Variants For Immunotherapy

    Funder
    National Health and Medical Research Council
    Funding Amount
    $192,473.00
    More information
    Funded Activity

    Identification And Characterisation Of HLA-E Restricted Influenza A Virus-specific CD8+ T Cells

    Funder
    National Health and Medical Research Council
    Funding Amount
    $354,156.00
    Summary
    With seasonal epidemics and the continual threat of a pandemic, there is an urgent need for a one-shot universal vaccine that protects against different influenza strains. This can potentially be achieved by the activation of killer T cells. I will identify new virus targets presented by a highly conserved human protein. Killer T cell recognition of these targets may provide a unique opportunity to develop an improved vaccine.
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    Funded Activity

    Comparison Within The Long-term Non-progressors Of T Cell Factors Contributing To Natural Control Of HIV Infection

    Funder
    National Health and Medical Research Council
    Funding Amount
    $63,934.00
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    Funded Activity

    Epigenetic Regulation Of CD8+ T Cell Function And Memory.

    Funder
    National Health and Medical Research Council
    Funding Amount
    $578,171.00
    Summary
    Upon virus infection, a subset of white blood cells, called killer T cells, are recruited to fight the infection. This proposal aims to examine molecular changes that occur within killer T cells and impart their specific function. We also aim to understand how killer T cells are _programmed� as they establish immunological memory. This proposal will provide insights important for the design and improvement of vaccine strategies to fight pathogens such as influenza, HIV and even tumors.
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