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Research Topic : cellular interactions
Field of Research : Infectious Diseases
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  • Researchers (13)
  • Funded Activities (21)
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  • Funded Activity

    Utility And Impact Of NKT Cells In HIV-SIV Infection

    Funder
    National Health and Medical Research Council
    Funding Amount
    $89,840.00
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    Funded Activity

    West Nile Virus Replication And Host Response

    Funder
    National Health and Medical Research Council
    Funding Amount
    $560,434.00
    Summary
    We seek to gain a detailed understanding of how interactions between the West Nile virus proteins and host factors involved in the IFN response determine the outcome of virus infection. Better understanding of the mechanisms employed by this highly pathogenic virus to disable the mammalian host's IFN response will have wider implications for our understanding of other human diseases such as cancer, autoimmunity and provide new avenues for design of efficient antiviral and anticancer therapies.
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    Funded Activity

    Comparative Effectiveness Of Vaccine-induced SIV-specific CD8 T Cells

    Funder
    National Health and Medical Research Council
    Funding Amount
    $607,797.00
    Summary
    A HIV vaccine remains elusive. Although killer T cell immunity can provide partial protection from HIV disease, we don't know the best type of killer T cells to induce by vaccination. This project compares multiple HIV vaccine strategies in macaques. We will carefully study the quality of killer T cell immunity induced using novel and cutting-edge assays. We will identify the requirements for effective killer T cell immunity to HIV.
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    Funded Activity

    Practitioner Fellowship

    Funder
    National Health and Medical Research Council
    Funding Amount
    $514,013.00
    Summary
    I am a clinician-scientist studying the biological determinants of clinical outcomes in infectious diseases.
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    Funded Activity

    Gamma-ray Inactivated Influenza A Virus Vaccine For Cross-protective T Cell Immunity

    Funder
    National Health and Medical Research Council
    Funding Amount
    $239,963.00
    Summary
    Although there are new antiviral drugs that appear to be effective against influenza virus, the far more costeffective and efficient means to combat an influenza pandemic would be by vaccination. Current influenza vaccines employ virus preparations that are inactivated by chemical treatment. The inactivated vaccines, which function mostly by inducing antibody against the virus, have to be reformulated almost every year to take account of the changing virus because the antibodies recognize the vi .... Although there are new antiviral drugs that appear to be effective against influenza virus, the far more costeffective and efficient means to combat an influenza pandemic would be by vaccination. Current influenza vaccines employ virus preparations that are inactivated by chemical treatment. The inactivated vaccines, which function mostly by inducing antibody against the virus, have to be reformulated almost every year to take account of the changing virus because the antibodies recognize the viral surface which is prone to mutation. Accordingly, in terms of the threatening H5N1 avian influenza pandemic, it is not known if an inactivated vaccine based on the circulating H5N1 strain will be effective if the virus mutates to adapt to efficient growth and spread in the human population. In contrast to the antibody response against influenza virus, the cytotoxic T cell response is broadly crossreactive between heterologous influenza virus strains. Live virus infection efficiently induces cytotoxic T cell immunity which plays an important role in reducing disease severity and mortality following infection with a second, heterologous influenza virus, although infection per se is not prevented. Accordingly, vaccination strategies that elicit cytotoxic T cell memory should be given urgent consideration in the preparation against an influenza pandemic. We have found that the use of gamma-irradiation (in contrast to chemical treatment) for the preparation of inactivated experimental vaccines against influenza and other viruses does not destroy the ability of the vaccines to elicit cytotoxic T cell immunity. The gamma-ray inactivated vaccines conferred protection against lethal challenge with heterologous influenza virus strains in mice. This proposal is aimed at extending this novel finding to avian influenza viruses and to uncover the mechanisms involved in the cytotoxic T cell immunogenicity of gamma-ray inactivated vaccines.
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    Funded Activity

    Uncovering Evolutionary Defense Mechanisms In Prokaryote-eukaryote Interactions; Potential For Novel Therapeutic Targets

    Funder
    National Health and Medical Research Council
    Funding Amount
    $324,386.00
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    Funded Activity

    Understanding The Importance Of Panton-Valentine Leukocidin Production In Australian Isolates Of Staphylococcus Aureus.

    Funder
    National Health and Medical Research Council
    Funding Amount
    $118,796.00
    Summary
    New strains of the superbug methicillin-resistant Staphylococcus aureus (MRSA) have emerged in the community, causing severe, sometimes fatal infections in otherwise healthy people. These strains, called community-acquired MRSA produce a toxin (Panton-Valentine leukocidin). This project will provide important information about how this toxin promotes disease, and how the immune system responds to the toxin, providing the basis for the development of immunotherapies against this new superbug.
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    Funded Activity

    Dissemmnation Of HIV And Establishment Of Cellular Reservoirs During Transmission

    Funder
    National Health and Medical Research Council
    Funding Amount
    $394,460.00
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    Funded Activity

    The Impact Of Reduced Plasmodium Falciparum And Plasmodium Vivax Transmission On The Epidemiology Of Malaria And The Acquisition Of Antigen-specific Recall Responses In Children From Papua New Guinea.

    Funder
    National Health and Medical Research Council
    Funding Amount
    $365,166.00
    Summary
    Malaria represents a significant global health burden in endemic countries. Individuals gradually develop a level of immunity to the clinical symptoms of malaria as a result of continued exposure throughout their lifetime. Efforts to implement effective malaria control strategies are increasing, thereby reducing exposure. This project will investigate how such strategies will impact on the development of immunity to malaria and the amount of clinical disease observed in different age groups.
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    Funded Activity

    Linkage Projects - Grant ID: LP0667698

    Funder
    Australian Research Council
    Funding Amount
    $249,000.00
    Summary
    Identification of novel markers of inflammation. This project will benefit Australia as it will increase basic understanding of inflammatory processes, result in a new generation of diagnostics for inflammatory diseases that could lead to earlier diagnosis and to monitor treatment, resulting in large economic and health benefit. It may lead to development of novel new therapies using monoclonal antibodies to regulate processes in immune, cardiovascular and infectious diseases. The work will gene .... Identification of novel markers of inflammation. This project will benefit Australia as it will increase basic understanding of inflammatory processes, result in a new generation of diagnostics for inflammatory diseases that could lead to earlier diagnosis and to monitor treatment, resulting in large economic and health benefit. It may lead to development of novel new therapies using monoclonal antibodies to regulate processes in immune, cardiovascular and infectious diseases. The work will generate significant economic spin-offs to the Australian biotechnology industry and will further relationships and training between research and development.
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