An integrated transcriptomic and metabolomic approach to investigate the heterogeneous Candida albicans biofilm phenotype

Candida albicans is the most prevalent and notorious of the Candida species involved in bloodstream infections, which is characterised by its capacity to form robust biofilms. Biofilm formation is an important clinical entity shown to be highly variable among clinical isolates. There are various env...

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Autores principales: Delaney, Christopher, Short, Bryn, Rajendran, Ranjith, Kean, Ryan, Burgess, Karl, Williams, Craig, Munro, Carol A., Ramage, Gordon
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2023
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10034394/
https://www.ncbi.nlm.nih.gov/pubmed/36969800
http://dx.doi.org/10.1016/j.bioflm.2023.100112
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author Delaney, Christopher
Short, Bryn
Rajendran, Ranjith
Kean, Ryan
Burgess, Karl
Williams, Craig
Munro, Carol A.
Ramage, Gordon
author_facet Delaney, Christopher
Short, Bryn
Rajendran, Ranjith
Kean, Ryan
Burgess, Karl
Williams, Craig
Munro, Carol A.
Ramage, Gordon
author_sort Delaney, Christopher
collection PubMed
description Candida albicans is the most prevalent and notorious of the Candida species involved in bloodstream infections, which is characterised by its capacity to form robust biofilms. Biofilm formation is an important clinical entity shown to be highly variable among clinical isolates. There are various environmental and physiological factors, including nutrient availability which influence the phenotype of Candida species. However, mechanisms underpinning adaptive biofilm heterogeneity have not yet been fully explored. Within this study we have profiled previously characterised and phenotypically distinct C. albicans bloodstream isolates. We assessed the dynamic susceptibility of these differing populations to antifungal treatments using population analysis profiling in addition to assessing biofilm formation and morphological changes. High throughput methodologies of RNA-Seq and LC-MS were employed to map and integrate the transcriptional and metabolic reprogramming undertaken by heterogenous C. albicans isolates in response to biofilm and hyphal inducing serum. We found a significant relationship between biofilm heterogeneity and azole resistance (P < 0.05). In addition, we observed that in response to serum our low biofilm forming (LBF) C. albicans exhibited a significant increase in biofilm formation and hyphal elongation. The transcriptional reprogramming of LBF strains compared to high biofilm forming (HBF) was distinct, indicating a high level of plasticity and variation in stress responses by heterogenous strains. The metabolic responses, although variable between LBF and HBF, shared many of the same responses to serum. Notably, a high upregulation of the arachidonic acid cascade, part of the COX pathway, was observed and this pathway was found to induce biofilm formation in LBF 3-fold. C. albicans is a highly heterogenous bloodstream pathogen with clinical isolates varying in antifungal tolerance and biofilm formation. In addition to this, C. albicans is capable of highly complex and variable regulation of transcription and metabolic pathways and heterogeneity across isolates further increases the complexity of these pathways. Here we have shown with a dual and integrated approach, the importance of studying a diverse panel of C. albicans isolates, which has the potential to reveal distinct pathways that can harnessed for drug discovery.
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spelling pubmed-100343942023-03-24 An integrated transcriptomic and metabolomic approach to investigate the heterogeneous Candida albicans biofilm phenotype Delaney, Christopher Short, Bryn Rajendran, Ranjith Kean, Ryan Burgess, Karl Williams, Craig Munro, Carol A. Ramage, Gordon Biofilm Article Candida albicans is the most prevalent and notorious of the Candida species involved in bloodstream infections, which is characterised by its capacity to form robust biofilms. Biofilm formation is an important clinical entity shown to be highly variable among clinical isolates. There are various environmental and physiological factors, including nutrient availability which influence the phenotype of Candida species. However, mechanisms underpinning adaptive biofilm heterogeneity have not yet been fully explored. Within this study we have profiled previously characterised and phenotypically distinct C. albicans bloodstream isolates. We assessed the dynamic susceptibility of these differing populations to antifungal treatments using population analysis profiling in addition to assessing biofilm formation and morphological changes. High throughput methodologies of RNA-Seq and LC-MS were employed to map and integrate the transcriptional and metabolic reprogramming undertaken by heterogenous C. albicans isolates in response to biofilm and hyphal inducing serum. We found a significant relationship between biofilm heterogeneity and azole resistance (P < 0.05). In addition, we observed that in response to serum our low biofilm forming (LBF) C. albicans exhibited a significant increase in biofilm formation and hyphal elongation. The transcriptional reprogramming of LBF strains compared to high biofilm forming (HBF) was distinct, indicating a high level of plasticity and variation in stress responses by heterogenous strains. The metabolic responses, although variable between LBF and HBF, shared many of the same responses to serum. Notably, a high upregulation of the arachidonic acid cascade, part of the COX pathway, was observed and this pathway was found to induce biofilm formation in LBF 3-fold. C. albicans is a highly heterogenous bloodstream pathogen with clinical isolates varying in antifungal tolerance and biofilm formation. In addition to this, C. albicans is capable of highly complex and variable regulation of transcription and metabolic pathways and heterogeneity across isolates further increases the complexity of these pathways. Here we have shown with a dual and integrated approach, the importance of studying a diverse panel of C. albicans isolates, which has the potential to reveal distinct pathways that can harnessed for drug discovery. Elsevier 2023-03-12 /pmc/articles/PMC10034394/ /pubmed/36969800 http://dx.doi.org/10.1016/j.bioflm.2023.100112 Text en © 2023 The Authors https://creativecommons.org/licenses/by/4.0/This is an open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Delaney, Christopher
Short, Bryn
Rajendran, Ranjith
Kean, Ryan
Burgess, Karl
Williams, Craig
Munro, Carol A.
Ramage, Gordon
An integrated transcriptomic and metabolomic approach to investigate the heterogeneous Candida albicans biofilm phenotype
title An integrated transcriptomic and metabolomic approach to investigate the heterogeneous Candida albicans biofilm phenotype
title_full An integrated transcriptomic and metabolomic approach to investigate the heterogeneous Candida albicans biofilm phenotype
title_fullStr An integrated transcriptomic and metabolomic approach to investigate the heterogeneous Candida albicans biofilm phenotype
title_full_unstemmed An integrated transcriptomic and metabolomic approach to investigate the heterogeneous Candida albicans biofilm phenotype
title_short An integrated transcriptomic and metabolomic approach to investigate the heterogeneous Candida albicans biofilm phenotype
title_sort integrated transcriptomic and metabolomic approach to investigate the heterogeneous candida albicans biofilm phenotype
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10034394/
https://www.ncbi.nlm.nih.gov/pubmed/36969800
http://dx.doi.org/10.1016/j.bioflm.2023.100112
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