Bio21 - Research Publications

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Author: Dagley, Michael × Author: McConville, Malcolm × Author: Saunders, Eleanor ×

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    Leishmania carbon metabolism in the macrophage phagolysosome- feast or famine?
    McConville, MJ ; Saunders, EC ; Kloehn, J ; Dagley, MJ (F1000 Research Ltd, 2015)
    A number of medically important microbial pathogens target and proliferate within macrophages and other phagocytic cells in their mammalian hosts. While the majority of these pathogens replicate within the host cell cytosol or non-hydrolytic vacuolar compartments, a few, including protists belonging to the genus Leishmania, proliferate long-term within mature lysosome compartments.  How these parasites achieve this feat remains poorly defined. In this review, we highlight recent studies that suggest that Leishmania virulence is intimately linked to programmed changes in the growth rate and carbon metabolism of the obligate intra-macrophage stages. We propose that activation of a slow growth and a stringent metabolic response confers resistance to multiple stresses (oxidative, temperature, pH), as well as both nutrient limitation and nutrient excess within this niche. These studies highlight the importance of metabolic processes as key virulence determinants in Leishmania.
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    Metabolic characteristics of CD8+ T cell subsets in young and aged individuals are not predictive of functionality (vol 11, 2857, 2020)
    Quinn, KM ; Hussain, T ; Kraus, F ; Formosa, LE ; Lam, WK ; Dagley, MJ ; Saunders, EC ; Assmus, LM ; Wynne-Jones, E ; Loh, L ; van de Sandt, CE ; Cooper, L ; Good-Jacobson, KL ; Kedzierska, K ; Mackay, LK ; McConville, MJ ; Ramm, G ; Ryan, MT ; La Gruta, NL (NATURE PUBLISHING GROUP, 2020-07-09)
    An amendment to this paper has been published and can be accessed via a link at the top of the paper.
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    Metabolic characteristics of CD8+ T cell subsets in young and aged individuals are not predictive of functionality
    Quinn, KM ; Hussain, T ; Kraus, F ; Formosa, LE ; Lam, WK ; Dagley, MJ ; Saunders, EC ; Assmus, LM ; Wynne-Jones, E ; Loh, L ; van de Sandt, CE ; Cooper, L ; Good-Jacobson, KL ; Kedzierska, K ; Mackay, LK ; McConville, MJ ; Ramm, G ; Ryan, MT ; La Gruta, NL (NATURE PUBLISHING GROUP, 2020-06-05)
    Virtual memory T (TVM) cells are antigen-naïve CD8+ T cells that exist in a semi-differentiated state and exhibit marked proliferative dysfunction in advanced age. High spare respiratory capacity (SRC) has been proposed as a defining metabolic characteristic of antigen-experienced memory T (TMEM) cells, facilitating rapid functionality and survival. Given the semi-differentiated state of TVM cells and their altered functionality with age, here we investigate TVM cell metabolism and its association with longevity and functionality. Elevated SRC is a feature of TVM, but not TMEM, cells and it increases with age in both subsets. The elevated SRC observed in aged mouse TVM cells and human CD8+ T cells from older individuals is associated with a heightened sensitivity to IL-15. We conclude that elevated SRC is a feature of TVM, but not TMEM, cells, is driven by physiological levels of IL-15, and is not indicative of enhanced functionality in CD8+ T cells.
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    Characterization of Metabolically Quiescent Leishmania Parasites in Murine Lesions Using Heavy Water Labeling
    Kloehn, J ; Saunders, EC ; O'Callaghan, S ; Dagley, MJ ; McConville, MJ ; Sacks, DL (PUBLIC LIBRARY SCIENCE, 2015-02)
    Information on the growth rate and metabolism of microbial pathogens that cause long-term chronic infections is limited, reflecting the absence of suitable tools for measuring these parameters in vivo. Here, we have measured the replication and physiological state of Leishmania mexicana parasites in murine inflammatory lesions using 2H2O labeling. Infected BALB/c mice were labeled with 2H2O for up to 4 months, and the turnover of parasite DNA, RNA, protein and membrane lipids estimated from the rate of deuterium enrichment in constituent pentose sugars, amino acids, and fatty acids, respectively. We show that the replication rate of parasite stages in these tissues is very slow (doubling time of ~12 days), but remarkably constant throughout lesion development. Lesion parasites also exhibit markedly lower rates of RNA synthesis, protein turnover and membrane lipid synthesis than parasite stages isolated from ex vivo infected macrophages or cultured in vitro, suggesting that formation of lesions induces parasites to enter a semi-quiescent physiological state. Significantly, the determined parasite growth rate accounts for the overall increase in parasite burden indicating that parasite death and turnover of infected host cells in these lesions is minimal. We propose that the Leishmania response to lesion formation is an important adaptive strategy that minimizes macrophage activation, providing a permissive environment that supports progressive expansion of parasite burden. This labeling approach can be used to measure the dynamics of other host-microbe interactions in situ.