
Genomic and metabolomic analyses of the marine fungus Emericellopsis cladophorae : insights into saltwater adaptability mechanisms and its biosynthetic potential
- Author
- Micael F. M. Gonçalves, Sandra Hilário, Yves Van de Peer (UGent) , Ana C. Esteves and Artur Alves
- Organization
- Abstract
- The genus Emericellopsis is found in terrestrial, but mainly in marine, environments with a worldwide distribution. Although Emericellopsis has been recognized as an important source of bioactive compounds, the range of metabolites expressed by the species of this genus, as well as the genes involved in their production are still poorly known. Untargeted metabolomics, using UPLC- QToF-MS/MS, and genome sequencing (Illumina HiSeq) was performed to unlock E. cladophorae MUM 19.33 chemical diversity. The genome of E. cladophorae is 26.9 Mb and encodes 8572 genes. A large set of genes encoding carbohydrate-active enzymes (CAZymes), secreted proteins, transporters, and secondary metabolite biosynthetic gene clusters were identified. Our analysis also revealed genomic signatures that may reflect a certain fungal adaptability to the marine environment, such as genes encoding for (1) the high-osmolarity glycerol pathway; (2) osmolytes' biosynthetic processes; (3) ion transport systems, and (4) CAZymes classes allowing the utilization of marine polysaccharides. The fungal crude extract library constructed revealed a promising source of antifungal (e.g., 9,12,13-Trihydroxyoctadec-10-enoic acid, hymeglusin), antibacterial (e.g., NovobiocinA), anticancer (e.g., daunomycinone, isoreserpin, flavopiridol), and anti-inflammatory (e.g., 2'-O-Galloylhyperin) metabolites. We also detected unknown compounds with no structural match in the databases used. The metabolites' profiles of E. cladophorae MUM 19.33 fermentations were salt dependent. The results of this study contribute to unravel aspects of the biology and ecology of this marine fungus. The genome and metabolome data are relevant for future biotechnological exploitation of the species.
- Keywords
- antimicrobial, anticancer, marine fungi, metabolites, whole genome sequencing, ANTIFUNGAL PEPTAIBOL, ACID, TRANSPORTER, ADAPTATION, LEUCINOSTATIN, BERGOFUNGIN, RIBOFLAVIN, ANNOTATION, PATHWAY, PROTEIN
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Citation
Please use this url to cite or link to this publication: http://hdl.handle.net/1854/LU-8734116
- MLA
- Gonçalves, Micael F. M., et al. “Genomic and Metabolomic Analyses of the Marine Fungus Emericellopsis Cladophorae : Insights into Saltwater Adaptability Mechanisms and Its Biosynthetic Potential.” JOURNAL OF FUNGI, vol. 8, no. 1, 2022, doi:10.3390/jof8010031.
- APA
- Gonçalves, M. F. M., Hilário, S., Van de Peer, Y., Esteves, A. C., & Alves, A. (2022). Genomic and metabolomic analyses of the marine fungus Emericellopsis cladophorae : insights into saltwater adaptability mechanisms and its biosynthetic potential. JOURNAL OF FUNGI, 8(1). https://doi.org/10.3390/jof8010031
- Chicago author-date
- Gonçalves, Micael F. M., Sandra Hilário, Yves Van de Peer, Ana C. Esteves, and Artur Alves. 2022. “Genomic and Metabolomic Analyses of the Marine Fungus Emericellopsis Cladophorae : Insights into Saltwater Adaptability Mechanisms and Its Biosynthetic Potential.” JOURNAL OF FUNGI 8 (1). https://doi.org/10.3390/jof8010031.
- Chicago author-date (all authors)
- Gonçalves, Micael F. M., Sandra Hilário, Yves Van de Peer, Ana C. Esteves, and Artur Alves. 2022. “Genomic and Metabolomic Analyses of the Marine Fungus Emericellopsis Cladophorae : Insights into Saltwater Adaptability Mechanisms and Its Biosynthetic Potential.” JOURNAL OF FUNGI 8 (1). doi:10.3390/jof8010031.
- Vancouver
- 1.Gonçalves MFM, Hilário S, Van de Peer Y, Esteves AC, Alves A. Genomic and metabolomic analyses of the marine fungus Emericellopsis cladophorae : insights into saltwater adaptability mechanisms and its biosynthetic potential. JOURNAL OF FUNGI. 2022;8(1).
- IEEE
- [1]M. F. M. Gonçalves, S. Hilário, Y. Van de Peer, A. C. Esteves, and A. Alves, “Genomic and metabolomic analyses of the marine fungus Emericellopsis cladophorae : insights into saltwater adaptability mechanisms and its biosynthetic potential,” JOURNAL OF FUNGI, vol. 8, no. 1, 2022.
@article{8734116, abstract = {{The genus Emericellopsis is found in terrestrial, but mainly in marine, environments with a worldwide distribution. Although Emericellopsis has been recognized as an important source of bioactive compounds, the range of metabolites expressed by the species of this genus, as well as the genes involved in their production are still poorly known. Untargeted metabolomics, using UPLC- QToF-MS/MS, and genome sequencing (Illumina HiSeq) was performed to unlock E. cladophorae MUM 19.33 chemical diversity. The genome of E. cladophorae is 26.9 Mb and encodes 8572 genes. A large set of genes encoding carbohydrate-active enzymes (CAZymes), secreted proteins, transporters, and secondary metabolite biosynthetic gene clusters were identified. Our analysis also revealed genomic signatures that may reflect a certain fungal adaptability to the marine environment, such as genes encoding for (1) the high-osmolarity glycerol pathway; (2) osmolytes' biosynthetic processes; (3) ion transport systems, and (4) CAZymes classes allowing the utilization of marine polysaccharides. The fungal crude extract library constructed revealed a promising source of antifungal (e.g., 9,12,13-Trihydroxyoctadec-10-enoic acid, hymeglusin), antibacterial (e.g., NovobiocinA), anticancer (e.g., daunomycinone, isoreserpin, flavopiridol), and anti-inflammatory (e.g., 2'-O-Galloylhyperin) metabolites. We also detected unknown compounds with no structural match in the databases used. The metabolites' profiles of E. cladophorae MUM 19.33 fermentations were salt dependent. The results of this study contribute to unravel aspects of the biology and ecology of this marine fungus. The genome and metabolome data are relevant for future biotechnological exploitation of the species.}}, articleno = {{31}}, author = {{Gonçalves, Micael F. M. and Hilário, Sandra and Van de Peer, Yves and Esteves, Ana C. and Alves, Artur}}, issn = {{2309-608X}}, journal = {{JOURNAL OF FUNGI}}, keywords = {{antimicrobial,anticancer,marine fungi,metabolites,whole genome sequencing,ANTIFUNGAL PEPTAIBOL,ACID,TRANSPORTER,ADAPTATION,LEUCINOSTATIN,BERGOFUNGIN,RIBOFLAVIN,ANNOTATION,PATHWAY,PROTEIN}}, language = {{eng}}, number = {{1}}, pages = {{20}}, title = {{Genomic and metabolomic analyses of the marine fungus Emericellopsis cladophorae : insights into saltwater adaptability mechanisms and its biosynthetic potential}}, url = {{http://doi.org/10.3390/jof8010031}}, volume = {{8}}, year = {{2022}}, }
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