| Literature DB >> 35316647 |
De-Dong Li1, Chetan V Jawale1, Chunsheng Zhou1, Li Lin1, Giraldina J Trevejo-Nunez2, Syed A Rahman3, Steven J Mullet4, Jishnu Das3, Stacy G Wendell4, Greg M Delgoffe5, Michail S Lionakis6, Sarah L Gaffen1, Partha S Biswas7.
Abstract
Combating fungal pathogens poses metabolic challenges for neutrophils, key innate cells in anti-Candida albicans immunity, yet how host-pathogen interactions cause remodeling of the neutrophil metabolism is unclear. We show that neutrophils mediate renal immunity to disseminated candidiasis by upregulating glucose uptake via selective expression of glucose transporter 1 (Glut1). Mechanistically, dectin-1-mediated recognition of β-glucan leads to activation of PKCδ, which triggers phosphorylation, localization, and early glucose transport by a pool of pre-formed Glut1 in neutrophils. These events are followed by increased Glut1 gene transcription, leading to more sustained Glut1 accumulation, which is also dependent on the β-glucan/dectin-1/CARD9 axis. Card9-deficient neutrophils show diminished glucose incorporation in candidiasis. Neutrophil-specific Glut1-ablated mice exhibit increased mortality in candidiasis caused by compromised neutrophil phagocytosis, reactive oxygen species (ROS), and neutrophil extracellular trap (NET) formation. In human neutrophils, β-glucan triggers metabolic remodeling and enhances candidacidal function. Our data show that the host-pathogen interface increases glycolytic activity in neutrophils by regulating Glut1 expression, localization, and function.Entities:
Keywords: Candida albicans; fungus; glucose; glucose transporter 1; immunometabolism; kidney; neutrophils
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Year: 2022 PMID: 35316647 PMCID: PMC9026661 DOI: 10.1016/j.chom.2022.02.017
Source DB: PubMed Journal: Cell Host Microbe ISSN: 1931-3128 Impact factor: 31.316