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Filamentous fungal carbon catabolite repression supports metabolic plasticity and stress responses essential for disease progression
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نویسنده
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beattie s.r. ,mark k.m.k. ,thammahong a. ,ries l.n.a. ,dhingra s. ,caffrey-carr a.k. ,cheng c. ,black c.c. ,bowyer p. ,bromley m.j. ,obar j.j. ,goldman g.h. ,cramer r.a.
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منبع
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plos pathogens - 2017 - دوره : 13 - شماره : 4
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چکیده
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Aspergillus fumigatus is responsible for a disproportionate number of invasive mycosis cases relative to other common filamentous fungi. while many fungal factors critical for infection establishment are known,genes essential for disease persistence and progression are ill defined. we propose that fungal factors that promote navigation of the rapidly changing nutrient and structural landscape characteristic of disease progression represent untapped clinically relevant therapeutic targets. to this end,we find that a. fumigatus requires a carbon catabolite repression (ccr) mediated genetic network to support in vivo fungal fitness and disease progression. while ccr as mediated by the transcriptional repressor crea is not required for pulmonary infection establishment,loss of ccr inhibits fungal metabolic plasticity and the ability to thrive in the dynamic infection microenvironment. our results suggest a model whereby ccr in an environmental filamentous fungus is dispensable for initiation of pulmonary infection but essential for infection maintenance and disease progression. conceptually,we argue these data provide a foundation for additional studies on fungal factors required to support fungal fitness and disease progression and term such genes and factors,dpfs (disease progression factors). © 2017 beattie et al.
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آدرس
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department of microbiology and immunology,geisel school of medicine at dartmouth,hanover,nh, United States, department of molecular and systems biology,geisel school of medicine at dartmouth,hanover,nh, United States, department of microbiology and immunology,geisel school of medicine at dartmouth,hanover,nh, United States, faculdade de ciências farmacêuticas de ribeirão preto,universidade de são paulo, Brazil, department of microbiology and immunology,geisel school of medicine at dartmouth,hanover,nh, United States, department of microbiology and immunology,geisel school of medicine at dartmouth,hanover,nh,united states,department of microbiology and immunology,montana state university,bozeman,mt, United States, department of molecular and systems biology,geisel school of medicine at dartmouth,hanover,nh,united states,norris cotton cancer center,geisel school of medicine at dartmouth,lebanon,nh,united states,institute for quantitative biomedical sciences,geisel school of medicine at dartmouth,lebanon,nh, United States, department of pathology,dartmouth-hitchcock medical center,lebanon,nh, United States, manchester fungal infection group,school of biological sciences,university of manchester,manchester, United Kingdom, manchester fungal infection group,school of biological sciences,university of manchester,manchester, United Kingdom, department of microbiology and immunology,geisel school of medicine at dartmouth,hanover,nh, United States, faculdade de ciências farmacêuticas de ribeirão preto,universidade de são paulo, Brazil, department of microbiology and immunology,geisel school of medicine at dartmouth,hanover,nh, United States
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Authors
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