Stress-induced phenotypic switching in Candida albicans

Candida albicans is both a common commensal and an opportunistic pathogen, being a prevalent cause of mucosal and systemic infections in humans. Phenotypic switching between white and opaque forms is a reversible transition that influences virulence, mating behavior, and biofilm formation. In this w...

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Bibliographic Details
Published in:Molecular biology of the cell 2009-07, Vol.20 (14), p.3178-3191
Main Authors: Alby, Kevin, Bennett, Richard J
Format: Article
Language:English
Subjects:
Candida albicans - drug effects
Candida albicans - genetics
Candida albicans - growth & development
DNA Damage
Gene Deletion
Gene Dosage
Gene Expression Regulation, Fungal - drug effects
Genes, Fungal
Genes, Switch
Hydroxyurea - pharmacology
Methyl Methanesulfonate - pharmacology
Oxidative Stress - drug effects
Phenotype
S Phase - drug effects
Stress, Physiological - drug effects
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Summary:Candida albicans is both a common commensal and an opportunistic pathogen, being a prevalent cause of mucosal and systemic infections in humans. Phenotypic switching between white and opaque forms is a reversible transition that influences virulence, mating behavior, and biofilm formation. In this work, we show that a wide range of factors induces high rates of switching from white to opaque. These factors include different forms of environmental stimuli such as genotoxic and oxidative stress, as well as intrinsic factors such as mutations in DNA repair genes. We propose that these factors increase switching to the opaque phase via a common mechanism-inhibition of cell growth. To confirm this hypothesis, growth rates were artificially manipulated by varying expression of the CLB4 cyclin gene; slowing cell growth by depleting CLB4 resulted in a concomitant increase in white-opaque switching. Furthermore, two clinical isolates of C. albicans, P37005 and L26, were found to naturally exhibit both slow growth and high rates of white-opaque switching. Notably, suppression of the slow growth phenotype suppressed hyperswitching in the P37005 isolate. Based on the sensitivity of the switch to levels of the master regulator Wor1, we propose a model for how changes in cellular growth modulate white-opaque switching frequencies.
ISSN:1059-1524
1939-4586
DOI:10.1091/mbc.E09-01-0040