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Field of Research : Medical Virology
Research Topic : MUCOSAL INFECTION
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  • Funded Activity

    Mucosal Human Immunodeficiency Virus Vaccine Late Pre-clinical Evaluation

    Funder
    National Health and Medical Research Council
    Funding Amount
    $575,315.00
    Summary
    Despite many candidate vaccines entering clinical development for protection against HIV, none has yet been successful. This proposal centres on late preclinical development for a novel mucosal vaccine strategy for HIV, which combines a preclinically-proven approach to generating strong T cell immune responses, with an existing approach to generating broadly neutralising antibody responses to HIV. Proof of synergy between these approaches will lead directly to clinical development.
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    Funded Activity

    Immune Modulatory Effects Of Vaginal Microbiota Metabolites And HIV Susceptibility

    Funder
    National Health and Medical Research Council
    Funding Amount
    $795,110.00
    Summary
    This study will advance knowledge on how acid molecules produced by beneficial and harmful bacteria are able to promote or impede HIV infection of the female genital mucosa through their effects on the barrier and immune function of cells that line the vagina and cervix. The results of this study are anticipated to augment the efficacy of topical HIV prevention strategies and lead to the development of safe vaginal hygiene products that help protect against other sexually transmitted infections.
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    Funded Activity

    The Role Of Noncoding Viral RNAs In Flavivirus Infection And Exosomal Signalling

    Funder
    National Health and Medical Research Council
    Funding Amount
    $683,447.00
    Summary
    The application is aimed at investigating the novel role for viral noncoding RNAs in exosomal antiviral signalling and associated outcome of infection with West Nile virus. We will identify host enzymes involved in generation of viral noncoding RNAs, determine which host proteins they interact with and how these interactions determine their incorporation into secreted exosomes to influence outcome of infection.
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    Funded Activity

    Virus-host Interactions Contributing To Hepatitis C Virus Chronicity

    Funder
    National Health and Medical Research Council
    Funding Amount
    $316,806.00
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    Funded Activity

    Understanding How Cytomegaloviruses Establish Systemic Infection

    Funder
    National Health and Medical Research Council
    Funding Amount
    $668,144.00
    Summary
    Human cytomegalovirus (HCMV) infects most Australians, causes birth defects and harms transplant patients. Vaccines against it have worked poorly. HCMV spreads throughout the body and is never cleared. To control infection we must identify its key checkpoints. Using mouse CMV, we find that host dendritic cells, which normally defend against infections, are taken over and spread virus to new sites. The viral gene responsible is a potential target for intervention. We will define how it works.
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    Funded Activity

    New Drug Combinations To Enhance Elimination Of Hepatitis B Infection

    Funder
    National Health and Medical Research Council
    Funding Amount
    $888,304.00
    Summary
    We have developed a therapy that kills hepatitis B virus infected cells and promotes elimination of infection. We are now testing novel drugs that can be used to maximise the efficacy of our new treatment to promote better outcomes that may be translated to other infections.
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    Funded Activity

    Burden Of Respiratory Infection In The First 2 Years Of Life: A Birth Cohort Study Of Emerging Respiratory Pathogens.

    Funder
    National Health and Medical Research Council
    Funding Amount
    $1,168,963.00
    Summary
    Respiratory illnesses are extremely common, but there is little information about patterns of infection in the community using modern diagnostic tests. Children have the highest rates of infection and transmit to all other age groups. We intend to recruit 138 newborns to monitor respiratory symptoms and collect specimens for testing in the first two years of life. This will allow us to document illnesses due to known and newly identified respiratory pathogens.
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    Funded Activity

    Characterization Of Neutralizing Antibody Responses In HCV Infected Individuals.

    Funder
    National Health and Medical Research Council
    Funding Amount
    $478,076.00
    Summary
    Hepatitis C virus is a major human pathogen infecting 200 million people world-wide. Currently, there is no vaccine to prevent infection and treatment regimes are only partially effective. IInitial HCV infection is frequently asymptomatic and 30% of people spontaneously clear the virus. The remaining 70% of people develop a life-long chronic infection that causes progressive liver disease, cirrhosis and in some cases liver cancer. The reason why some people are able to clear virus has been attri .... Hepatitis C virus is a major human pathogen infecting 200 million people world-wide. Currently, there is no vaccine to prevent infection and treatment regimes are only partially effective. IInitial HCV infection is frequently asymptomatic and 30% of people spontaneously clear the virus. The remaining 70% of people develop a life-long chronic infection that causes progressive liver disease, cirrhosis and in some cases liver cancer. The reason why some people are able to clear virus has been attributed to the development of a strong cellular immune response and antibody is belived to play a monir role in achieving viral clearance. However, measurememnt of antibody responses in HCV infected pateints is routinely performed using conventional diagnostic tests that do not measure antibody that can help neutralize and clear virus. We have developed an assay that accurately measures the level of NAb in patient sera. We have found that chronically infected patients have broadly reactive neutralizing antibodies but that patients who clear virus, naturally or through treatment do not have broadly reactive neutralizing antibodies. Possibly explaining this phenomenon is that early during infection, antibody is frequently specific only to the infecting virus therefore to detect neutralizing antibodies, homologous viral sequences must be examined. In addition, we have found evidence that HCV can evade neutralzing antibodies through masking of sites to which antibodies bind. We propose to explore whether acutely infected patients develop NAb to autologous viral sequences, and how do these viral sequences and the antibody titre change throughout the course of infection and treatment. We also plan to determine the mechanism of neutralization resistance through the use of mutagenesis of resistant HCV glycoproteins. These studies are aimed at gaining a thorough understanding of the true role of antibody in HCV infection and its influence on viral evolution.
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    Funded Activity

    Receptor Activated Conformations Of Retroviral Glycoproteins.

    Funder
    National Health and Medical Research Council
    Funding Amount
    $489,000.00
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    Funded Activity

    Clearing Chronic Infectious Diseases – Enhancing Host Immune Effector Function

    Funder
    National Health and Medical Research Council
    Funding Amount
    $92,314.00
    Summary
    Chronic infections produced by pathogens such as HIV, overwhelm our immune system leading to an exhausted state where cells responsible for the clearance of invading microorganisms are unable to respond effectively. We have recently identified a highly promising therapeutic target that enhances immune effector function. We seek to understand the underlying mechanism, and to explore the therapeutic potential of this approach for the treatment of a broad range of pathogens, including those respons .... Chronic infections produced by pathogens such as HIV, overwhelm our immune system leading to an exhausted state where cells responsible for the clearance of invading microorganisms are unable to respond effectively. We have recently identified a highly promising therapeutic target that enhances immune effector function. We seek to understand the underlying mechanism, and to explore the therapeutic potential of this approach for the treatment of a broad range of pathogens, including those responsible for chronic disease.
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