Candida albicans Biofilm-Defective Mutants

doi:10.1128/EC.4.8.1493-1502.2005

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Candida albicans Biofilm-Defective Mutants

Mathias L. Richard,¹^, Clarissa J. Nobile,¹^,2 Vincent M. Bruno,¹^,3 and Aaron P. Mitchell¹^*

Department of Microbiology, Columbia University, New York, New York 10032,¹ Biological Sciences Program, Department of Biological Sciences, Columbia University, New York, New York 10027,² Program in Cellular, Molecular, and Biophysical Studies, Columbia University, New York, New York 10032³

Received 4 June 2004/ Accepted 17 June 2005

Biofilm formation plays a key role in the life cycles and subsistenceof many microorganisms. For the human fungal pathogen Candidaalbicans, biofilm development is arguably a virulence trait,because medical implants that serve as biofilm substrates aresignificant risk factors for infection. The development of C.albicans biofilms in vitro proceeds through an early phase,in which yeast cells populate a substrate, an intermediate phase,in which pseudohyphal and hyphal cell types are produced, anda maturation phase, in which continued cell growth is accompaniedby accumulation of an extracellular matrix. Here we report theresults of a screen for C. albicans biofilm-defective mutants,in which homozygous insertions in NUP85, MDS3, KEM1, and SUV3were found to block biofilm development. Confocal microscopicexamination suggests that nup85, suv3, and mds3 mutations causeearly-phase arrest, whereas the kem1 mutation causes intermediate-phasearrest. All of the mutants are defective in hypha productionin several media. Analysis of mixed-biofilm development indicatesthat all of the mutants are defective in the production of hyphaein the context of a biofilm. Because all of the mutants aredefective in the retention of cells in the biofilm, we inferthat hyphae provide an adherent scaffold that stabilizes thebiofilm structure.

* Corresponding author. Mailing address: Department of Microbiology, Columbia University, Hammer Building, Room no. 906, 701 West 168th Street, New York, NY 10032. Phone: (212) 305-8251. Fax: (212) 342-4070. E-mail: apm4{at}columbia.edu.

Present address: Laboratoire de Microbiologie et GénétiqueMoléculaire, INA P-G, UMR-INRA216, URA-CNRS1925, BP01,78850 Thiverval-Grignon, France.

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