Fungal siderophore biosynthesis is partially localized in peroxisomes |
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Authors: | Mario Gründlinger Sabiha Yasmin Beatrix Elisabeth Lechner Stephan Geley Markus Schrettl Michael Hynes Hubertus Haas |
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Affiliation: | 1. Division of Molecular Biology/Biocenter, Innsbruck Medical University, , A‐6020 Innsbruck, Austria;2. Division of Molecular Pathophysiology/Biocenter, Innsbruck Medical University, , A‐6020 Innsbruck, Austria;3. Department of Genetics, University of Melbourne, , Parkville, 3010 Australia |
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Abstract: | Siderophores play a central role in iron metabolism and virulence of most fungi. Both Aspergillus fumigatus and Aspergillus nidulans excrete the siderophore triacetylfusarinine C (TAFC) for iron acquisition. In A. fumigatus, green fluorescence protein‐tagging revealed peroxisomal localization of the TAFC biosynthetic enzymes SidI (mevalonyl‐CoA ligase), SidH (mevalonyl‐CoA hydratase) and SidF (anhydromevalonyl‐CoA transferase), while elimination of the peroxisomal targeting signal (PTS) impaired both, peroxisomal SidH‐targeting and TAFC biosynthesis. The analysis of A. nidulans mutants deficient in peroxisomal biogenesis, ATP import or protein import revealed that cytosolic mislocalization of one or two but, interestingly, not all three enzymes impairs TAFC production during iron starvation. The PTS motifs are conserved in fungal orthologues of SidF, SidH and SidI. In agreement with the evolutionary conservation of the partial peroxisomal compartmentalization of fungal siderophore biosynthesis, the SidI orthologue of coprogen‐type siderophore‐producing Neurospora crassa was confirmed to be peroxisomal. Taken together, this study identified and characterized a novel, evolutionary conserved metabolic function of peroxisomes. |
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