Taxonomic group: fungi / Ascomycota (Phylum: Ascomycota)
Organ / tissue: cell wall
 
NCBI PubMed ID: 30082817
Publication DOI: 10.1038/s41467-018-05497-7
Journal NLM ID: 101528555
Publisher: London: Nature Publishing Group
Correspondence: j.wagenerhygiene.uni-wuerzburg.de
Institutions: Max von Pettenkofer-Institut für Hygiene und Medizinische Mikrobiologie, Medizinische Fakultät, LMU München, Munich, Germany, Zell- und Entwicklungsbiologie, Department Biologie II, LMU München, Planegg-Martinsried, Germany, Institut für Hygiene und Mikrobiologie, Julius-Maximilians-Universität Würzburg, Würzburg, Germany, National Reference Center for Invasive Fungal Infections (NRZMyk), Leibniz-Institut für Naturstoff-Forschung und Infektionsbiologie, Hans-Knöll-Institut, Jena, Germany, Molecular Microbiology and Biotechnology, Institute of Biology Leiden, Leiden University, Leiden, The Netherlands

Azole antifungals inhibit the fungal ergosterol biosynthesis pathway, resulting in either growth inhibition or killing of the pathogen, depending on the species. Here we report that azoles have an initial growth-inhibitory (fungistatic) activity against the pathogen Aspergillus fumigatus that can be separated from the succeeding fungicidal effects. At a later stage, the cell wall salvage system is induced. This correlates with successive cell integrity loss and death of hyphal compartments. Time-lapse fluorescence microscopy reveals excessive synthesis of cell wall carbohydrates at defined spots along the hyphae, leading to formation of membrane invaginations and eventually rupture of the plasma membrane. Inhibition of β-1,3-glucan synthesis reduces the formation of cell wall carbohydrate patches and delays cell integrity failure and fungal death. We propose that azole antifungals exert their fungicidal activity by triggering synthesis of cell wall carbohydrate patches that penetrate the plasma membrane, thereby killing the fungus. The elucidated mechanism may be potentially exploited as a novel approach for azole susceptibility testing.

cell wall, Microscopy, antifungal activity, azoles

Structure type: structural motif or average structure
Location inside paper: p.2, column 2, paragraph 3
Trivial name: β-1,3-glucan
Compound class: EPS, O-polysaccharide, cell wall polysaccharide, glucan
Contained glycoepitopes: IEDB_1397514,IEDB_142488,IEDB_146664,IEDB_153543,IEDB_158555,IEDB_161166,IEDB_558869,IEDB_857743,IEDB_983931,SB_192
 
Methods: genetic methods, microscopy, fluorescence microscopy
Biological activity: under the effect of fungicidal azoles forms patches on the cell wall that rupture it
Enzymes that release or process the structure: Fks1p
 
Related record ID(s): 48689
NCBI Taxonomy refs (TaxIDs): 746128
Reference(s) to other database(s): GTC:G51056AN
Show glycosyltransferases
 

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