Your search keyword '"Kjærbølling I"' showing total 2 results

1. Strategies to establish the link between biosynthetic gene clusters and secondary metabolites.

Author

Kjærbølling I, Mortensen UH, Vesth T, and Andersen MR

Subjects

Biosynthetic Pathways genetics, Fungal Proteins genetics, Fungi enzymology, Gene Expression Regulation, Fungal, Genome, Fungal, Genomics, Peptide Synthases genetics, Polyketide Synthases genetics, Fungi genetics, Fungi metabolism, Multigene Family, Secondary Metabolism genetics

Abstract

Filamentous fungi produce a vast number of bioactive secondary metabolites (SMs), some of which have found applications in the pharmaceutical industry including as antibiotics and immunosuppressants. As more and more species are whole genome sequenced the number of predicted clusters of genes for SM biosynthesis is ever increasing - holding a promise of novel useful bioactive SMs. To be able to fully utilize the potential of novel SMs, it is necessary to link the SM and the genes responsible for producing it. This can be challenging, but many strategies and tools have been developed for this purpose. Here we provide an overview of the methods used to establish the link between SM and biosynthetic gene cluster (BGC) and vice versa, along with the challenges and advantages of each of the methods. Part I of the review, associating BCG with SM, is divided into gene manipulations native strain and heterologous expression strategies, depending on the fungal species. Part II, associating SM with BGC, is divided into three main approaches: (1) homology search (2) retro-biosynthesis and (3) comparative genomics., (Copyright © 2019 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2019

2. Linking secondary metabolites to gene clusters through genome sequencing of six diverse Aspergillus species.

Author

Kjærbølling I, Vesth TC, Frisvad JC, Nybo JL, Theobald S, Kuo A, Bowyer P, Matsuda Y, Mondo S, Lyhne EK, Kogle ME, Clum A, Lipzen A, Salamov A, Ngan CY, Daum C, Chiniquy J, Barry K, LaButti K, Haridas S, Simmons BA, Magnuson JK, Mortensen UH, Larsen TO, Grigoriev IV, Baker SE, and Andersen MR

Subjects

Aflatoxins biosynthesis, Allergens genetics, Aspergillus pathogenicity, DNA Methylation, Evolution, Molecular, Flavonoids biosynthesis, Genome, Fungal, Indole Alkaloids metabolism, Phylogeny, Terpenes metabolism, Whole Genome Sequencing, Aflatoxins genetics, Aspergillus genetics, Aspergillus metabolism, Multigene Family, Secondary Metabolism genetics

Abstract

The fungal genus of Aspergillus is highly interesting, containing everything from industrial cell factories, model organisms, and human pathogens. In particular, this group has a prolific production of bioactive secondary metabolites (SMs). In this work, four diverse Aspergillus species ( A. campestris , A. novofumigatus , A. ochraceoroseus , and A. steynii ) have been whole-genome PacBio sequenced to provide genetic references in three Aspergillus sections. A. taichungensis and A. candidus also were sequenced for SM elucidation. Thirteen Aspergillus genomes were analyzed with comparative genomics to determine phylogeny and genetic diversity, showing that each presented genome contains 15-27% genes not found in other sequenced Aspergilli. In particular, A. novofumigatus was compared with the pathogenic species A. fumigatus This suggests that A. novofumigatus can produce most of the same allergens, virulence, and pathogenicity factors as A. fumigatus , suggesting that A. novofumigatus could be as pathogenic as A. fumigatus Furthermore, SMs were linked to gene clusters based on biological and chemical knowledge and analysis, genome sequences, and predictive algorithms. We thus identify putative SM clusters for aflatoxin, chlorflavonin, and ochrindol in A. ochraceoroseus , A. campestris , and A. steynii , respectively, and novofumigatonin, ent -cycloechinulin, and epi -aszonalenins in A. novofumigatus Our study delivers six fungal genomes, showing the large diversity found in the Aspergillus genus; highlights the potential for discovery of beneficial or harmful SMs; and supports reports of A. novofumigatus pathogenicity. It also shows how biological, biochemical, and genomic information can be combined to identify genes involved in the biosynthesis of specific SMs., Competing Interests: The authors declare no conflict of interest.

Published

2018