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Research Topic : MOLECULAR INTERACTIO
Field of Research : Medical Bacteriology
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Medical Bacteriology (37)
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  • Researchers (12)
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  • Funded Activity

    Molecular Epidemiology And High Resolution Surveillance Of Salmonella Enterica Serovar Typhimurium In Australia

    Funder
    National Health and Medical Research Council
    Funding Amount
    $583,180.00
    Summary
    Salmonella typhimurium is a leading cause of the food-borne disease – salmonellosis. It is responsible for considerable morbidity and has an enormous economic cost. Molecular typing is the key to rapidly identify and control outbreaks. This project will employ next generation sequencing technology to develop a new molecular typing scheme. A surveillance system that integrates molecular typing data and epidemiological data will be developed for outbreak investigation and disease prevention.
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    Funded Activity

    Optimising Temporal Genomic Surveillance Of Salmonella Infections In Australia

    Funder
    National Health and Medical Research Council
    Funding Amount
    $763,447.00
    Summary
    Salmonella is a leading cause of the food-borne disease – salmonellosis. It is responsible for considerable morbidity and has an enormous economic cost. Molecular typing is the key to rapidly identify and control outbreaks. This project will optimise the use of whole genome sequencing for outbreak investigation and long term epidemiology. A surveillance system that integrates genome sequence and epidemiological data will be highly significant for outbreak investigation and disease prevention.
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    Funded Activity

    Improving The Understanding And Management Of Important Human Bacterial Infections

    Funder
    National Health and Medical Research Council
    Funding Amount
    $204,196.00
    Summary
    This project will focus on two important bacteria, Staphylococcus aureus (Golden Staph), and Enterococcus faecium, both causes of serious infections in hospital and community patients in Australia. Using new technologies, including whole genome sequencing, this project will lead to significant advances in understanding how these bacteria evolve, spread and cause disease. This will lead to new strategies for prevention and management of infections caused by these important bacteria.
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    Funded Activity

    Molecular Mechanisms Of Persistence Of Mycobacterium Tuberculosis

    Funder
    National Health and Medical Research Council
    Funding Amount
    $398,142.00
    Summary
    Mycobacterium tuberculosis is the bacterium that causes tuberculosis (TB. It infects about third of all people in the world and kills several million people each year. People with active TB spread the mycobacteria in aerosols from their breath. When another person inhales an infected aerosol the mycobacteria enter their lungs and establish a new infection. During the course of infection M. tuberculosis is exposed to a variety of harsh environments inside the lungs which normally kill other bacte .... Mycobacterium tuberculosis is the bacterium that causes tuberculosis (TB. It infects about third of all people in the world and kills several million people each year. People with active TB spread the mycobacteria in aerosols from their breath. When another person inhales an infected aerosol the mycobacteria enter their lungs and establish a new infection. During the course of infection M. tuberculosis is exposed to a variety of harsh environments inside the lungs which normally kill other bacteria. M. tuberculosis is able to survive and adapt to those harsh environments. M. tuberculosis has an especially thick and tough cell wall which protects it. M. tuberculosis can adapt to the environments it encounters in a patient by changing their cell walls. The wall also protects mycobacteria from chemicals so it is resistant to many common antibiotics. There are some drugs to treat TB however M. tuberculosis is building up resistance to those drugs so we need to find new ones We will determine how mycobacteria synthesize their special cell wall and how they adapt during an infection. If we know how the details of how M. tuberculosis protects itself then we can find potential weakness which could be targets for the development of new drugs to treat TB.
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    Funded Activity

    Acinetobacter Baumannii Virulence From A Regulatory Perspective: The Role Of Two Component Signal Transduction Systems

    Funder
    National Health and Medical Research Council
    Funding Amount
    $608,731.00
    Summary
    Acinetobacter baumannii is becoming a significant pathogen in the hospital and more recently in the community. It is very resistant to removal from surfaces and upon entering the host is almost impossible to treat with currently available antibiotics. It causes a wide range of disease states from wound infections and pneumonia to bacteraemia; little is known of this process. This research will increase our understanding of the disease process, providing possible treatment options in the future.
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    Funded Activity

    Role In Disease Of A Novel Epigenetic Regulator Associated With The Hypervirulent Neisseria Meningitidis Clonal Complex 41/44

    Funder
    National Health and Medical Research Council
    Funding Amount
    $403,249.00
    Summary
    Neisseria meningitis is a major cause of meningococcal septicaemia and meningitis worldwide. We have identified a phase variable DNA methyltransferase present in disease isolates, some of which have caused meningococcal epidemics. This methyltransferase is involved in the regulation of proteins involved in infection and disease processes. We will investigate whether this regulation increases the ability of the bacteria to adapt to changing host environments and cause disease.
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    Funded Activity

    Understanding Virulence Of Invasive Staphylococcus Aureus

    Funder
    National Health and Medical Research Council
    Funding Amount
    $772,711.00
    Summary
    Staph aureus (Golden staph) is a major cause of disease in humans. In this project we will use state-of-the-art molecular biology and genomics to fully understand the mechanisms of virulence in this pathogen. This information will inform future approaches to development of therapeutics, as well as the use of genomics in clinical microbiology and disease management.
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    Funded Activity

    A One Health Approach To Assessing The Threat Of Clostridium Difficile To Australia’s Biosecurity: A Genomic Investigation Of Human, Animal And Environmental Isolates

    Funder
    National Health and Medical Research Council
    Funding Amount
    $318,768.00
    Summary
    Clostridium difficile is a bacterium that causes life-threatening diarrhoea in humans and animals and is a major public health issue in Australia. This project will study the genetic make-up of the bacterium and identify factors contributing to the emergence, evolution, and spread of C. difficile. This knowledge will be essential in guiding effective public health interventions and reducing deaths from C. difficile infection in humans and animals.
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    Funded Activity

    Non-coding RNA Regulation Of Virulence In Enterohaemorrhagic E. Coli

    Funder
    National Health and Medical Research Council
    Funding Amount
    $389,313.00
    Summary
    Shiga toxins cause potentially fatal haemolytic uremic syndrome (HUS) and are transferred between bacterial pathogens by bacteriophage (bacterial viruses). We have recently found that the Shiga toxin encoding bacteriophage encodes an unusually large number of non-coding RNAs (RNA regulators of gene expression). This Project aims to understand how these RNA regulators benefit the Shiga toxin bacteriophage and use this knowledge to develop interventions that will prevent expression of the toxin.
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    Funded Activity

    Genome Wide Investigations Of Mycobacterium Tuberculosis To Reveal Processes Of Pathogenesis

    Funder
    National Health and Medical Research Council
    Funding Amount
    $396,341.00
    Summary
    Tuberculosis remains a global health burden of staggering proportions. Around 1 in 3 people are infected with Mycobacteria tuberculosis, the organism responsible for the disease, which kills 2 million people annually. The emergence of strains now resistant to almost all of our front line drugs has placed extra pressure on researchers who are attempting to develop new protective vaccines and the critical antibiotics required to eradicate the disease. Furthermore the current global HIV pandemic is .... Tuberculosis remains a global health burden of staggering proportions. Around 1 in 3 people are infected with Mycobacteria tuberculosis, the organism responsible for the disease, which kills 2 million people annually. The emergence of strains now resistant to almost all of our front line drugs has placed extra pressure on researchers who are attempting to develop new protective vaccines and the critical antibiotics required to eradicate the disease. Furthermore the current global HIV pandemic is making the situation far worse as HIV kills the very cells of the body that protect us from tuberculosis. This research project will fill the significant gaps in our knowledge of M. tuberculosis infection, specifically identify the genes of the organism which allow it to invade and spread throughout the body. M. tuberculosis infection consists of 3 characteristic stages, i.e. colonisation, spread and long term survival in specialised structures called granulomas. It is from these granulomas that the bacterium can emerge after long periods of inactivity to cause clinical tuberculosis. Using a mouse model of infection I will define the genes needed by the bacterium to survive at these 3 key stages of disease thereby providing for a better knowledge base from which to design new vaccine strategies and to create effective drugs.
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