Transcriptional Response of Saccharomyces cerevisiae to the Plasma Membrane-Perturbing Compound Chitosan

doi:10.1128/EC.4.4.703-715.2005

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Eukaryotic Cell, April 2005, p. 703-715, Vol. 4, No. 4
1535-9778/05/$08.00+0 doi:10.1128/EC.4.4.703-715.2005
Copyright © 2005, American Society for Microbiology. All Rights Reserved.

Transcriptional Response of Saccharomyces cerevisiae to the Plasma Membrane-Perturbing Compound Chitosan

Anna Zakrzewska,¹^* Andre Boorsma,¹ Stanley Brul,² Klaas J. Hellingwerf,¹ and Frans M. Klis²

Molecular Microbial Physiology,¹ Molecular Biology and Microbial Food Safety, Swammerdam Institute of Life Sciences, Amsterdam, The Netherlands²

Received 2 December 2004/ Accepted 14 February 2005

Chitosan is a plasma membrane-perturbing compound consistingof linear chains of ß-1,4-linked glucosamine residues,which at acidic pHs become positively charged. It is extensivelyused as an antimicrobial compound, yet its mode of action isstill unresolved. Chitosan strongly affected the growth of theyeast Saccharomyces cerevisiae, the food spoilage yeast Zygosaccharomycesbailii, and two human-pathogenic yeasts, Candida albicans andCandida glabrata. Microarray analysis of yeast cells treatedwith sublethal concentrations of chitosan revealed inductionof the environmental stress response and three more major transcriptionalresponses. The first was a rapid and stable Cin5p-mediated response.Cin5p/Yap4p is a transcription factor involved in various stressresponses. Deletion of CIN5 led to increased chitosan sensitivity.The second was a Crz1p-mediated response, which is delayed comparedto the Cin5p response. Crz1p is a transcription factor of thecalcineurin pathway. Cells deleted for CRZ1 or treated withthe calcineurin inhibitor FK506 became hypersensitive to chitosan,supporting the notion that the Crz1p-controlled response offersprotection against chitosan. The third was a strong Rlm1p-mediatedresponse which ran parallel in time with the Crz1p-regulatedresponse. Rlm1p is a transcription factor of the cell wall integritypathway, which is activated by cell wall stress. Importantly,chitosan-treated cells became more resistant to ß-1,3-glucanase,which is a well-known response to cell wall stress. We proposethat the transcriptional response to chitosan may be representativeof other plasma membrane-perturbing compounds.

* Corresponding author. Mailing address: Molecular Microbial Physiology and Molecular Biology and Microbial Food Safety, Swammerdam Institute of Life Sciences, Nieuwe Achtergracht 166, 1018WV Amsterdam, The Netherlands. Phone: 31205256424. Fax: 31205257056. E-mail: A.M.Zakrzewska{at}uva.nl.

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