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Glycolysis is important for optimal asexual growth and formation of mature tissue cysts by Toxoplasma gondii
Authors:Anurag Shukla  Kellen L. Olszewski  Manuel Llinás  Leah M. Rommereim  Barbara A. Fox  David J. Bzik  Dong Xia  Jonathan Wastling  Daniel Beiting  David S. Roos  Dhanasekaran Shanmugam
Affiliation:1. Biochemical Sciences Division, CSIR-National Chemical Laboratory, Pune, India;2. Department of Metabolomics, Kadmon Corporation, New York, USA;3. Department of Biochemistry and Molecular Biology and Department of Chemistry, Huck Center for Malaria Research, The Pennsylvania State University, W126 Millennium Science Complex, University Park, PA, USA;4. Department of Microbiology and Immunology, Geisel School of Medicine at Dartmouth, Lebanon, NH, USA;5. The Royal Veterinary College, London NW1 0TU, UK;6. Faculty of Natural Sciences, Keele University, Keele, Staffordshire, ST5 5BG, UK;g. School of Veterinary Medicine, Dept. of Pathobiology, University of Pennsylvania, Philadelphia, PA, USA;h. Department of Biology and Penn Genome Frontiers Institute, University of Pennsylvania, Philadelphia, PA, USA
Abstract:Toxoplasma gondii can grow and replicate using either glucose or glutamine as the major carbon source. Here, we have studied the essentiality of glycolysis in the tachyzoite and bradyzoite stages of T. gondii, using transgenic parasites that lack a functional hexokinase gene (Δhk) in RH (Type-1) and Prugniaud (Type-II) strain parasites. Tachyzoite stage Δhk parasites exhibit a fitness defect similar to that reported previously for the major glucose transporter mutant, and remain virulent in mice. However, although Prugniaud strain Δhk tachyzoites were capable of transforming into bradyzoites in vitro, they were severely compromised in their ability to make mature bradyzoite cysts in the brain tissue of mice. Isotopic labelling studies reveal that glucose-deprived tacyzoites utilise glutamine to replenish glycolytic and pentose phosphate pathway intermediates via gluconeogenesis. Interestingly, while glutamine-deprived intracellular Δhk tachyzoites continued to replicate, extracellular parasites were unable to efficiently invade host cells. Further, studies on mutant tachyzoites lacking a functional phosphoenolpyruvate carboxykinase (Δpepck1) revealed that glutaminolysis is the sole source of gluconeogenic flux in glucose-deprived parasites. In addition, glutaminolysis is essential for sustaining oxidative phosphorylation in Δhk parasites, while wild type (wt) and Δpepck1 parasites can obtain ATP from either glycolysis or oxidative phosphorylation. This study provides insights into the role of nutrient metabolism during asexual propagation and development of T. gondii, and validates the versatile nature of central carbon and energy metabolism in this parasite.
Keywords:Glycolysis  Gluconeogenesis  Metabolomics  Hexokinase  ATP synthesis
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