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High-Throughput Profiling of Candida auris Isolates Reveals Clade-Specific Metabolic Differences

Candida auris, a multidrug-resistant human fungal pathogen that causes outbreaks of invasive infections, emerged as four distinct geographical clades. Previous studies identified genomic and proteomic differences in nutrient utilization on comparison to Candida albicans, suggesting that certain meta...

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Autores principales: Brandt, Philipp, Mirhakkak, Mohammad H., Wagner, Lysett, Driesch, Dominik, Möslinger, Anna, Fänder, Pauline, Schäuble, Sascha, Panagiotou, Gianni, Vylkova, Slavena
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Society for Microbiology 2023
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10269459/
https://www.ncbi.nlm.nih.gov/pubmed/37097196
http://dx.doi.org/10.1128/spectrum.00498-23
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author Brandt, Philipp
Mirhakkak, Mohammad H.
Wagner, Lysett
Driesch, Dominik
Möslinger, Anna
Fänder, Pauline
Schäuble, Sascha
Panagiotou, Gianni
Vylkova, Slavena
author_facet Brandt, Philipp
Mirhakkak, Mohammad H.
Wagner, Lysett
Driesch, Dominik
Möslinger, Anna
Fänder, Pauline
Schäuble, Sascha
Panagiotou, Gianni
Vylkova, Slavena
author_sort Brandt, Philipp
collection PubMed
description Candida auris, a multidrug-resistant human fungal pathogen that causes outbreaks of invasive infections, emerged as four distinct geographical clades. Previous studies identified genomic and proteomic differences in nutrient utilization on comparison to Candida albicans, suggesting that certain metabolic features may contribute to C. auris emergence. Since no high-throughput clade-specific metabolic characterization has been described yet, we performed a phenotypic screening of C. auris strains from all 4 clades on 664 nutrients, 120 chemicals, and 24 stressors. We identified common and clade- or strain-specific responses, including the preferred utilization of various dipeptides as nitrogen source and the inability of the clade II isolate AR 0381 to withstand chemical stress. Further analysis of the metabolic properties of C. auris isolates showed robust growth on intermediates of the tricarboxylic acid cycle, such as citrate and succinic and malic acids. However, there was reduced or no growth on pyruvate, lactic acid, or acetate, likely due to the lack of the monocarboxylic acid transporter Jen1, which is conserved in most pathogenic Candida species. Comparison of C. auris and C. albicans transcriptomes of cells grown on alternative carbon sources and dipeptides as a nitrogen source revealed common as well as species-unique responses. C. auris induced a significant number of genes with no ortholog in C. albicans, e.g., genes similar to the nicotinic acid transporter TNA1 (alternative carbon sources) and to the oligopeptide transporter (OPT) family (dipeptides). Thus, C. auris possesses unique metabolic features which could have contributed to its emergence as a pathogen. IMPORTANCE Four main clades of the emerging, multidrug-resistant human pathogen Candida auris have been identified, and they differ in their susceptibilities to antifungals and disinfectants. Moreover, clade- and strain-specific metabolic differences have been identified, but a comprehensive overview of nutritional characteristics and resistance to various stressors is missing. Here, we performed high-throughput phenotypic characterization of C. auris on various nutrients, stressors, and chemicals and obtained transcriptomes of cells grown on selected nutrients. The generated data sets identified multiple clade- and strain-specific phenotypes and induction of C. auris-specific metabolic genes, showing unique metabolic properties. The presented work provides a large amount of information for further investigations that could explain the role of metabolism in emergence and pathogenicity of this multidrug-resistant fungus.
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spelling pubmed-102694592023-06-16 High-Throughput Profiling of Candida auris Isolates Reveals Clade-Specific Metabolic Differences Brandt, Philipp Mirhakkak, Mohammad H. Wagner, Lysett Driesch, Dominik Möslinger, Anna Fänder, Pauline Schäuble, Sascha Panagiotou, Gianni Vylkova, Slavena Microbiol Spectr Research Article Candida auris, a multidrug-resistant human fungal pathogen that causes outbreaks of invasive infections, emerged as four distinct geographical clades. Previous studies identified genomic and proteomic differences in nutrient utilization on comparison to Candida albicans, suggesting that certain metabolic features may contribute to C. auris emergence. Since no high-throughput clade-specific metabolic characterization has been described yet, we performed a phenotypic screening of C. auris strains from all 4 clades on 664 nutrients, 120 chemicals, and 24 stressors. We identified common and clade- or strain-specific responses, including the preferred utilization of various dipeptides as nitrogen source and the inability of the clade II isolate AR 0381 to withstand chemical stress. Further analysis of the metabolic properties of C. auris isolates showed robust growth on intermediates of the tricarboxylic acid cycle, such as citrate and succinic and malic acids. However, there was reduced or no growth on pyruvate, lactic acid, or acetate, likely due to the lack of the monocarboxylic acid transporter Jen1, which is conserved in most pathogenic Candida species. Comparison of C. auris and C. albicans transcriptomes of cells grown on alternative carbon sources and dipeptides as a nitrogen source revealed common as well as species-unique responses. C. auris induced a significant number of genes with no ortholog in C. albicans, e.g., genes similar to the nicotinic acid transporter TNA1 (alternative carbon sources) and to the oligopeptide transporter (OPT) family (dipeptides). Thus, C. auris possesses unique metabolic features which could have contributed to its emergence as a pathogen. IMPORTANCE Four main clades of the emerging, multidrug-resistant human pathogen Candida auris have been identified, and they differ in their susceptibilities to antifungals and disinfectants. Moreover, clade- and strain-specific metabolic differences have been identified, but a comprehensive overview of nutritional characteristics and resistance to various stressors is missing. Here, we performed high-throughput phenotypic characterization of C. auris on various nutrients, stressors, and chemicals and obtained transcriptomes of cells grown on selected nutrients. The generated data sets identified multiple clade- and strain-specific phenotypes and induction of C. auris-specific metabolic genes, showing unique metabolic properties. The presented work provides a large amount of information for further investigations that could explain the role of metabolism in emergence and pathogenicity of this multidrug-resistant fungus. American Society for Microbiology 2023-04-25 /pmc/articles/PMC10269459/ /pubmed/37097196 http://dx.doi.org/10.1128/spectrum.00498-23 Text en Copyright © 2023 Brandt et al. https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution 4.0 International license (https://creativecommons.org/licenses/by/4.0/) .
spellingShingle Research Article
Brandt, Philipp
Mirhakkak, Mohammad H.
Wagner, Lysett
Driesch, Dominik
Möslinger, Anna
Fänder, Pauline
Schäuble, Sascha
Panagiotou, Gianni
Vylkova, Slavena
High-Throughput Profiling of Candida auris Isolates Reveals Clade-Specific Metabolic Differences
title High-Throughput Profiling of Candida auris Isolates Reveals Clade-Specific Metabolic Differences
title_full High-Throughput Profiling of Candida auris Isolates Reveals Clade-Specific Metabolic Differences
title_fullStr High-Throughput Profiling of Candida auris Isolates Reveals Clade-Specific Metabolic Differences
title_full_unstemmed High-Throughput Profiling of Candida auris Isolates Reveals Clade-Specific Metabolic Differences
title_short High-Throughput Profiling of Candida auris Isolates Reveals Clade-Specific Metabolic Differences
title_sort high-throughput profiling of candida auris isolates reveals clade-specific metabolic differences
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10269459/
https://www.ncbi.nlm.nih.gov/pubmed/37097196
http://dx.doi.org/10.1128/spectrum.00498-23
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