Replicative Aging Remodels the Cell Wall and Is Associated with Increased Intracellular Trafficking in Human Pathogenic Yeasts

Replicative Aging Remodels the Cell Wall and Is Associated with Increased Intracellular Trafficking in Human Pathogenic Yeasts

Replicative aging is an underexplored field of research in medical mycology. Cryptococcus neoformans ( ) and Candida glabrata ( ) are dreaded fungal pathogens that cause fatal invasive infections. The fungal cell wall is essential for yeast viability and pathogenesis. In this study, we provide data...

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Published in:mBio Vol. 13; no. 1; p. e0019022
Main Authors: Silva, Vanessa K A, Bhattacharya, Somanon, Oliveira, Natalia Kronbauer, Savitt, Anne G, Zamith-Miranda, Daniel, Nosanchuk, Joshua D, Fries, Bettina C
Format: Journal Article
Language:English
Published: United States American Society for Microbiology 15-02-2022
Subjects:
Candida glabrata
cell wall
Cryptococcus neoformans
Molecular and Cellular Biology
replicative lifespan
Research Article
vesicle trafficking
Candida glabrata
Cryptococcus neoformans
cell wall
replicative lifespan
vesicle trafficking
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Summary:Replicative aging is an underexplored field of research in medical mycology. Cryptococcus neoformans ( ) and Candida glabrata ( ) are dreaded fungal pathogens that cause fatal invasive infections. The fungal cell wall is essential for yeast viability and pathogenesis. In this study, we provide data characterizing age-associated modifications to the cell wall of and . Here, we report that old yeast cells upregulate genes of cell wall biosynthesis, leading to cell wall reorganization and increased levels of all major components, including glucan, chitin, and its derivatives, as well as mannan. This results in a significant thickening of the cell wall in aged cells. Old-generation yeast cells exhibited drastic ultrastructural changes, including the presence of abundant vesicle-like particles in the cytoplasm, and enlarged vacuoles with altered pH homeostasis. Our findings suggest that the cell wall modifications could be enabled by augmented intracellular trafficking. This work furthers our understanding of the cell phenotype that emerges during aging. It highlights differences in these two fungal pathogens and elucidates mechanisms that explain the enhanced resistance of old cells to antifungals and phagocytic attacks. Cryptococcus neoformans and Candida glabrata are two opportunistic human fungal pathogens that cause life-threatening diseases. During infection, both microorganisms have the ability to persist for long periods, and treatment failure can occur even if standard testing identifies the yeasts to be sensitive to antifungals. Replicative life span is a trait that is measured by the number of divisions a cell undergoes before death. Aging in fungi is associated with enhanced tolerance to antifungals and resistance to phagocytosis, and characterization of old cells may help identify novel antifungal targets. The cell wall remains an attractive target for new therapies because it is essential for fungi and is not present in humans. This study shows that the organization of the fungal cell wall changes remarkably during aging and becomes thicker and is associated with increased intracellular trafficking as well as the alteration of vacuole morphology and pH homeostasis.
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The authors declare no conflict of interest.
Vanessa K. A. Silva and Somanon Bhattacharya share first authorship. Both have generated the majority of the data. Vanessa is in first position because she led the investigations and wrote the majority of the manuscript.
ISSN:2150-7511
2150-7511
DOI:10.1128/MBIO.00190-22