| Literature DB >> 34262174 |
Kyla S Ost1,2, Teresa R O'Meara3, W Zac Stephens1,2, Tyson Chiaro1,2, Haoyang Zhou1,2, Jourdan Penman1,2, Rickesha Bell1,2, Jason R Catanzaro4, Deguang Song5, Shakti Singh6, Daniel H Call7, Elizabeth Hwang-Wong8, Kimberly E Hanson9, John F Valentine10, Kenneth A Christensen7, Ryan M O'Connell1,2, Brendan Cormack8, Ashraf S Ibrahim6,11, Noah W Palm5, Suzanne M Noble12, June L Round13,14.
Abstract
Pathogenic fungi reside in the intestinal microbiota but rarely cause disease. Little is known about the interactions between fungi and the immune system that promote commensalism. Here we investigate the role of adaptive immunity in promoting mutual interactions between fungi and host. We find that potentially pathogenic Candida species induce and are targeted by intestinal immunoglobulin A (IgA) responses. Focused studies on Candida albicans reveal that the pathogenic hyphal morphotype, which is specialized for adhesion and invasion, is preferentially targeted and suppressed by intestinal IgA responses. IgA from mice and humans directly targets hyphal-enriched cell-surface adhesins. Although typically required for pathogenesis, C. albicans hyphae are less fit for gut colonization1,2 and we show that immune selection against hyphae improves the competitive fitness of C. albicans. C. albicans exacerbates intestinal colitis3 and we demonstrate that hyphae and an IgA-targeted adhesin exacerbate intestinal damage. Finally, using a clinically relevant vaccine to induce an adhesin-specific immune response protects mice from C. albicans-associated damage during colitis. Together, our findings show that adaptive immunity suppresses harmful fungal effectors, with benefits to both C. albicans and its host. Thus, IgA uniquely uncouples colonization from pathogenesis in commensal fungi to promote homeostasis.Entities:
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Year: 2021 PMID: 34262174 PMCID: PMC8904204 DOI: 10.1038/s41586-021-03722-w
Source DB: PubMed Journal: Nature ISSN: 0028-0836 Impact factor: 49.962