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PknG senses amino acid availability to control metabolism and virulence of Mycobacterium tuberculosis
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نویسنده
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rieck b. ,degiacomi g. ,zimmermann m. ,cascioferro a. ,boldrin f. ,lazar-adler n.r. ,bottrill a.r. ,le chevalier f. ,frigui w. ,bellinzoni m. ,lisa m.-n. ,alzari p.m. ,nguyen l. ,brosch r. ,sauer u. ,manganelli r. ,o’hare h.m.
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منبع
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plos pathogens - 2017 - دوره : 13 - شماره : 5
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چکیده
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Sensing and response to changes in nutrient availability are essential for the lifestyle of environmental and pathogenic bacteria. serine/threonine protein kinase g (pkng) is required for virulence of the human pathogen mycobacterium tuberculosis,and its putative substrate gara regulates the tricarboxylic acid cycle in m. tuberculosis and other actinobacteria by protein-protein binding. we sought to understand the stimuli that lead to phosphorylation of gara,and the roles of this regulatory system in pathogenic and non-pathogenic bacteria. we discovered that m. tuberculosis lacking gara was severely attenuated in mice and macrophages and furthermore that gara lacking phosphorylation sites failed to restore the growth of gara deficient m. tuberculosis in macrophages. additionally we examined the impact of genetic disruption of pkng or gara upon protein phosphorylation,nutrient utilization and the intracellular metabolome. we found that phosphorylation of gara requires pkng and depends on nutrient availability,with glutamate and aspartate being the main stimuli. disruption of pkng or gara caused opposing effects on metabolism: a defect in glutamate catabolism or depletion of intracellular glutamate,respectively. strikingly,disruption of the phosphorylation sites of gara was sufficient to recapitulate defects caused by pkng deletion. the results suggest that gara is a cellular target of pkng and the metabolomics data demonstrate that the function of this signaling system is in metabolic regulation. this function in amino acid homeostasis is conserved amongst the actinobacteria and provides an example of the close relationship between metabolism and virulence. © 2017 rieck et al.
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آدرس
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department of infection,immunity and inflammation,university of leicester,leicester, United Kingdom, department of molecular medicine,university of padua,padova, Italy, institute of molecular systems biology,eth zurich,zurich,switzerland,department of microbial pathogenesis,yale university school of medicine,new haven,ct, United States, institut pasteur,integrated mycobacterial pathogenomics unit,paris, France, department of molecular medicine,university of padua,padova, Italy, core biotechnology services,university of leicester,leicester, United Kingdom, core biotechnology services,university of leicester,leicester, United Kingdom, institut pasteur,integrated mycobacterial pathogenomics unit,paris, France, institut pasteur,integrated mycobacterial pathogenomics unit,paris, France, institut pasteur,unité de microbiologie structurale and cnrs-umr3528,paris, France, institut pasteur,unité de microbiologie structurale and cnrs-umr3528,paris,france,laboratory of molecular & structural microbiology,institut pasteur de montevideo,montevideo, Uruguay, institut pasteur,unité de microbiologie structurale and cnrs-umr3528,paris, France, department of molecular biology and microbiology,case western reserve university school of medicine,cleveland,oh, United States, institut pasteur,integrated mycobacterial pathogenomics unit,paris, France, institute of molecular systems biology,eth zurich,zurich, Switzerland, department of molecular medicine,university of padua,padova, Italy, department of infection,immunity and inflammation,university of leicester,leicester,united kingdom,department of molecular and cellular bioscience,university of leicester,leicester, United Kingdom
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Authors
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