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Australian State/Territory : QLD
Research Topic : Murine Model
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  • Funded Activity

    Mathematical Modelling Of Nosocomial Infections To Improve Understanding Of Transmission & Optimise Infection Control.

    Funder
    National Health and Medical Research Council
    Funding Amount
    $73,842.00
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    Funded Activity

    Dopamine Neuron Ontogeny: Convergent Neurobiological Pathway For Risk Factors Of Schizophrenia

    Funder
    National Health and Medical Research Council
    Funding Amount
    $337,214.00
    Summary
    Schizophrenia is associated with changes in dopamine (a signalling molecule in the brain). These changes are present prior to psychosis, suggesting they begin early in development. Our aims are to manipulate key factors in the development of brain dopamine systems to clarify their role in psychosis and schizophrenia. This work has the potential to identify early brain changes that lead to schizophrenia, which in turn may generate better diagnoses and outcomes for people with this disorder.
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    Funded Activity

    High Penetrance Deleterious Mutations In Blinding Glaucoma

    Funder
    National Health and Medical Research Council
    Funding Amount
    $1,345,055.00
    Summary
    This project aims to identify the genes most commonly mutated in individuals with advanced glaucoma. Identification of such genes will lead to improved understanding of glaucoma pathogenesis, a better ability to predict risk, and the identification of drug targets for novel therapies.
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    Funded Activity

    Hedgehog Signalling In Limb And Craniofacial Development And Disease

    Funder
    National Health and Medical Research Council
    Funding Amount
    $494,544.00
    Summary
    Anomalies of the face and limbs are amongst the most common features of human birth defects, and their frequent association suggests that the same genes are involved in governing the development of the limbs and face during embryogenesis. We have used a genomics-based approach to identify genes involved in limb development based on their alteration in a mouse model which develops extra fingers and toes. Defects in this mouse result from changes in Gli3, a gene which is known to be important in b .... Anomalies of the face and limbs are amongst the most common features of human birth defects, and their frequent association suggests that the same genes are involved in governing the development of the limbs and face during embryogenesis. We have used a genomics-based approach to identify genes involved in limb development based on their alteration in a mouse model which develops extra fingers and toes. Defects in this mouse result from changes in Gli3, a gene which is known to be important in both limb and face development. Based on the organs in which our genes of interest are active, we believe that they will also play key roles in embryonic development of the limbs, face and other organs. We now plan to investigate the regulation of a subset of these genes based on analysis in mouse models of limb and face development. In addition, we have chosen to further analyse the function of a completely novel gene we have identified which our preliminary studies suggest may play a role in the normal development of the lip and palate. These studies have the potential to shed light on the processes governing how organs develop, as well as on the molecular basis of common birth defects such as polydactyly (extra fingers and toes) and cleft palate.
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    Funded Activity

    Delineating The Relationship Between Iron And Peroxisomal Disorders: The Role Of The Peroxisomal Enzyme GNPAT In Iron-Overload Disorders

    Funder
    National Health and Medical Research Council
    Funding Amount
    $700,767.00
    Summary
    Hereditary haemochromatosis is one of the most common genetic disorders in humans, affecting 1 in 200 Australians. We have identified a change in a peroxisomal gene which may affect iron levels in humans. The prevalence of this gene change in Australian haemochromatosis patients will be examined followed by a systematic analysis of how this protein controls iron levels in the body. Our goal is to identify and diagnose genetic changes which influence iron loading in haemochromatosis patients.
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    Funded Activity

    SARA: Delineating Its Association With The Onset And Development Of Liver Fibrosis

    Funder
    National Health and Medical Research Council
    Funding Amount
    $865,972.00
    Summary
    Liver disease, a significant burden on society, affects many in the prime of their life. Scarring of the liver is a response to injury due to many factors including alcohol, viruses, obesity, and fatty-liver disease. We have identified a protein associated with liver injury. In this project we will perform a systematic analysis to understand the role of this protein in injury progression. Ultimately we intend to develop tools to prevent and treat liver injury.
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    Showing 1-6 of 6 Funded Activites

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