Candida auris uses metabolic strategies to escape and kill macrophages while avoiding robust activation of the NLRP3 inflammasome response

Harshini Weerasinghe, Claudia Simm, Tirta Mario Djajawi, Irma Tedja, Tricia L. Lo, Daniel S. Simpson, David Shasha, Naama Mizrahi, Françios A.B. Olivier, Mary Speir, Kate E. Lawlor, Ronen Ben-Ami, Ana Traven*

*Corresponding author for this work

Research output: Contribution to journalArticlepeer-review

19 Scopus citations

Abstract

Metabolic adaptations regulate the response of macrophages to infection. The contributions of metabolism to macrophage interactions with the emerging fungal pathogen Candida auris are poorly understood. Here, we show that C. auris-infected macrophages undergo immunometabolic reprogramming and increase glycolysis but fail to activate a strong interleukin (IL)-1β cytokine response or curb C. auris growth. Further analysis shows that C. auris relies on its own metabolic capacity to escape from macrophages and proliferate in vivo. Furthermore, C. auris kills macrophages by triggering host metabolic stress through glucose starvation. However, despite causing macrophage cell death, C. auris does not trigger robust activation of the NLRP3 inflammasome. Consequently, inflammasome-dependent responses remain low throughout infection. Collectively, our findings show that C. auris uses metabolic regulation to eliminate macrophages while remaining immunologically silent to ensure its own survival. Thus, our data suggest that host and pathogen metabolism could represent therapeutic targets for C. auris infections.

Original languageEnglish
Article number112522
JournalCell Reports
Volume42
Issue number5
DOIs
StatePublished - 30 May 2023

Funding

FundersFunder number
Monash-Warwick Alliance
National Health and Medical Research CouncilAPP2002520, APP1181089, APP1158678
Ministry of Science and Technology88555
Israel Science Foundation442/18

    Keywords

    • CP: Immunology
    • Candida auris
    • NLRP3 inflammasome
    • immunometabolism
    • innate immunity
    • macrophage

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