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  • Funded Activity

    Uncoupled Research Fellowship

    Funder
    National Health and Medical Research Council
    Funding Amount
    $602,666.00
    Summary
    I am a molecular biologist interested in understanding how cells are able to actively kill themselves, and how cells make the decision to live or die. Understanding how cells kill themselves will ultimately lead to better therapies designed to kill cancer
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    Funded Activity

    Role Of Transformation And IAPs In Sensitivity Of Cells To TNFalpha

    Funder
    National Health and Medical Research Council
    Funding Amount
    $505,786.00
    Summary
    Current cancer treatments are ineffective and unpleasant for patients. This is because existing cancer treatments target normal as well as cancer cells. New anti-cancer drugs have been designed to encourage cancer cells to kill themselves, by a process called apoptosis, but may still target normal cells. This project aims to discover why cancer cells are susceptible to a novel anti-cancer drug and a natural ligand called TNF but normal cells are not. This will lead to better treatments.
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    Funded Activity

    Pathophysiological Significance Of Reverse Signaling Through Membrane TNF

    Funder
    National Health and Medical Research Council
    Funding Amount
    $453,055.00
    Summary
    Cytokines are molecules produced by cells that take part in immune and inflammatory responses. They coordinate the activities of leukocytes and therefore are important in the host response against infections. However, overproduction of some cytokines, particularly tumour necrosis factor, seems to cause the deleterious consequences. Tumour necrosis factor is made by cells, particularly macrophages, T lymphocytes and natural killer cells, in two stages: first, the cytokine is exposed on the surfac .... Cytokines are molecules produced by cells that take part in immune and inflammatory responses. They coordinate the activities of leukocytes and therefore are important in the host response against infections. However, overproduction of some cytokines, particularly tumour necrosis factor, seems to cause the deleterious consequences. Tumour necrosis factor is made by cells, particularly macrophages, T lymphocytes and natural killer cells, in two stages: first, the cytokine is exposed on the surface of the cell and then it is 'clipped off' and released as a smaller, soluble form. In either form it can interact with specific receptors on other cells and, in this way, change the cells' activities. We believe that binding of tumour necrosis factor receptors to the cytokine while it is in its membrane form can also send a message backwards, into the cell bearing the tumour necrosis factor. This process, known as reverse signalling, then changes the activity of this cell. In this project we will investigate this phenomenon in detail. The results will be extremely relevant to new methods of treatment of diseases, that rely either on 'masking' tumour necrosis factor by administering soluble forms of its receptor or on blocking the release of the soluble form of the molecule from the surface of the cell. Our work will enable us to understand the consequences of these approaches more fully. We will also be looking at the role of the membrane form of tumour necrosis factor in a model of infectious disease. Influenza virus is responsible for a great deal of morbidity and mortality around the world. We, and others, have shown, in a mouse model, that some cells in the lungs make tumour necrosis factor during the course of viral pneumonia. Here we will determine whether the membrane form of this cytokine plays a role in clearing virus or causing some of the complications of this disease. This also may have relevance to other inflammatory and infectious disease.
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    Funded Activity

    Apo2L/TRAIL Killing Of Tumour Cells And The Role Of Inhibitor Of Apoptosis Proteins

    Funder
    National Health and Medical Research Council
    Funding Amount
    $390,321.00
    Summary
    Melanomas and Gliomas are tumour types that respond poorly to current treatments. Current treatments are not only sometimes ineffective, but also unpleasant and may cause co-lateral damage. We will test 2 new targetted anti-cancer treatments, that so far appear to have minor side effects in small animal models, on these difficult to treat tumour types to see if and how they kill them. We also want to know whether these independent treatments can work together to kill tumours more effectively. Al .... Melanomas and Gliomas are tumour types that respond poorly to current treatments. Current treatments are not only sometimes ineffective, but also unpleasant and may cause co-lateral damage. We will test 2 new targetted anti-cancer treatments, that so far appear to have minor side effects in small animal models, on these difficult to treat tumour types to see if and how they kill them. We also want to know whether these independent treatments can work together to kill tumours more effectively. Although we will not personally test these drugs in clinical settings, these drugs or similar are currently in preclinical and clinical trials. This means that understanding how these drugs function is of paramount importance and may result in better clinical trials and possibly more rapid acceptance of the use of these drugs in patients.
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    Funded Activity

    Relevance Of The -308 TNF Promoter Polymorphism In Disease

    Funder
    National Health and Medical Research Council
    Funding Amount
    $154,042.00
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    Funded Activity

    Investigation Into The Cause Of Illness In Malaria

    Funder
    National Health and Medical Research Council
    Funding Amount
    $429,136.00
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    Funded Activity

    The Role Of TRAF2 Signal Transduction Molecule In Lymphocyte Responses

    Funder
    National Health and Medical Research Council
    Funding Amount
    $90,288.00
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    Funded Activity

    Molecular And Immunological Functions Of TRAF2 And Its Splice Variant TRAF2A

    Funder
    National Health and Medical Research Council
    Funding Amount
    $136,731.00
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    Funded Activity

    Development Of A Highly Potent, Fully Human Anti-GM-CSF Monoclonal Antibody

    Funder
    National Health and Medical Research Council
    Funding Amount
    $334,000.00
    Summary
    Many diseases, such as arthritis, have unwanted inflammatory reactions. Better drugs are needed to control inflammation. A powerful antibody to a significant pro-inflammatory cytokine will be generated; this antibody will be especially designed so that it will not be rejected by patients. Because of its properties it will cost the community less than similar therapeutics. Because inflammatory diseases are common many patients will benefit from our therapeutic.
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    Funded Activity

    Molecular Basis Of Type 2 TNF Receptor (TNFR2)-mediated Apoptosis

    Funder
    National Health and Medical Research Council
    Funding Amount
    $209,466.00
    More information

    Showing 1-10 of 48 Funded Activites

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