The CRH Family Coding for Cell Wall Glycosylphosphatidylinositol Proteins with a Predicted Transglycosidase Domain Affects Cell Wall Organization and Virulence of Candida albicans

The CRH Family Coding for Cell Wall Glycosylphosphatidylinositol Proteins with a Predicted Transglycosidase Domain Affects Cell Wall Organization and Virulence of Candida albicans

In Candida albicans UTR2 (CSF4), CRH11, and CRH12 are members of a gene family (the CRH family) that encode glycosylphosphatidylinositol-dependent cell wall proteins with putative transglycosidase activity. Deletion of genes of this family resulted in additive sensitivity to compounds interfering wi...

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Veröffentlicht in:The Journal of biological chemistry 2006-12, Vol.281 (52), p.40399-40411
Hauptverfasser: Pardini, Giacomo, De Groot, Piet W.J., Coste, Alix T., Karababa, Mahir, Klis, Frans M., de Koster, Chris G., Sanglard, Dominique
Format: Artikel
Sprache:eng
Schlagworte:
Animals
Candida albicans
Candida albicans - enzymology
Candida albicans - genetics
Candida albicans - growth & development
Candida albicans - pathogenicity
Candidiasis - enzymology
Candidiasis - metabolism
Candidiasis - mortality
Cell Wall - enzymology
Cell Wall - genetics
Cell Wall - metabolism
Congo Red - chemistry
Fungal Proteins - chemistry
Fungal Proteins - genetics
Fungal Proteins - physiology
Gene Deletion
Glycoside Hydrolases - chemistry
Glycoside Hydrolases - genetics
Glycoside Hydrolases - physiology
Glycosylphosphatidylinositols - chemistry
Glycosylphosphatidylinositols - physiology
Mice
Multienzyme Complexes - chemistry
Multienzyme Complexes - physiology
Multigene Family
Protein Structure, Tertiary
Transferases - chemistry
Transferases - physiology
Virulence Factors - chemistry
Virulence Factors - physiology
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Zusammenfassung:In Candida albicans UTR2 (CSF4), CRH11, and CRH12 are members of a gene family (the CRH family) that encode glycosylphosphatidylinositol-dependent cell wall proteins with putative transglycosidase activity. Deletion of genes of this family resulted in additive sensitivity to compounds interfering with normal cell wall formation (Congo red, calcofluor white, SDS, and high Ca2+ concentrations), suggesting that these genes contribute to cell wall organization. A triple mutant lacking UTR2, CRH11, and CRH12 produced a defective cell wall, as inferred from increased sensitivity to cell wall-degrading enzymes, decreased ability of protoplasts to regenerate a new wall, constitutive activation of Mkc1p, the mitogen-activated protein kinase of the cell wall integrity pathway, and an increased chitin content of the cell wall. Importantly, this was accompanied by a decrease in alkali-insoluble 1,3-β-glucan but not total glucan content, suggesting that formation of the linkage between 1,3-β-glucan and chitin might be affected. In support of this idea, localization of a Utr2p-GFP fusion protein largely coincided with areas of chitin incorporation in C. albicans.As UTR2 and CRH11 expression is regulated by calcineurin, a serine/threonine protein phosphatase involved in tolerance to antifungal drugs, cell wall morphogenesis, and virulence, this points to a possible relationship between calcineurin and the CRH family. Deletion of UTR2, CRH11, and CRH12 resulted in only a partial overlap with calcineurin-dependent phenotypes, suggesting that calcineurin has additional targets. Interestingly, cells deleted for UTR2, CRH11, and CRH12 were, like a calcineurin mutant, avirulent in a mouse model of systemic infection but retained the capacity to colonize target organs (kidneys) as the wild type. In conclusion, this work establishes the role of UTR2, CRH11, and CRH12 in cell wall organization and integrity.
ISSN:0021-9258
1083-351X
DOI:10.1074/jbc.M606361200