Global analysis of adenylate-forming enzymes reveals β-lactone biosynthesis pathway in pathogenic Nocardia

Mapping Intimacies ◽

10.1101/856955 ◽

2019 ◽

Cited By ~ 2

Author(s):

Serina L. Robinson ◽

Barbara R. Terlouw ◽

Megan D. Smith ◽

Sacha J. Pidot ◽

Tim P. Stinear ◽

...

Keyword(s):

Machine Learning ◽

Natural Product ◽

Sequence Similarity ◽

Global Analysis ◽

Gene Clusters ◽

Acid Activation ◽

Biosynthetic Gene ◽

Biosynthetic Gene Clusters ◽

Predictive Tool ◽

Wide Range

ABSTRACTEnzymes that cleave ATP to activate carboxylic acids play essential roles in primary and secondary metabolism in all domains of life. Class I adenylate-forming enzymes share a conserved structural fold but act on a wide range of substrates to catalyze reactions involved in bioluminescence, nonribosomal peptide biosynthesis, fatty acid activation, and β-lactone formation. Despite their metabolic importance, the substrates and catalytic functions of the vast majority of adenylate-forming enzymes are unknown without tools available to accurately predict them. Given the crucial roles of adenylate-forming enzymes in biosynthesis, this also severely limits our ability to predict natural product structures from biosynthetic gene clusters. Here we used machine learning to predict adenylate-forming enzyme function and substrate specificity from protein sequence. We built a web-based predictive tool and used it to comprehensively map the biochemical diversity of adenylate-forming enzymes across >50,000 candidate biosynthetic gene clusters in bacterial, fungal, and plant genomes. Ancestral enzyme reconstruction and sequence similarity networking revealed a ‘hub’ topology suggesting radial divergence of the adenylate-forming superfamily from a core enzyme scaffold most related to contemporary aryl-CoA ligases. Our classifier also predicted β-lactone synthetases in novel biosynthetic gene clusters conserved across >90 different strains of Nocardia. To test our computational predictions, we purified a candidate β-lactone synthetase from Nocardia brasiliensis and reconstituted the biosynthetic pathway in vitro to link the gene cluster to the β-lactone natural product, nocardiolactone. We anticipate our machine learning approach will aid in functional classification of enzymes and advance natural product discovery.

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Global analysis of adenylate-forming enzymes reveals β-lactone biosynthesis pathway in pathogenic Nocardia

Journal of Biological Chemistry ◽

10.1074/jbc.ra120.013528 ◽

2020 ◽

Vol 295 (44) ◽

pp. 14826-14839

Author(s):

Serina L. Robinson ◽

Barbara R. Terlouw ◽

Megan D. Smith ◽

Sacha J. Pidot ◽

Timothy P. Stinear ◽

...

Keyword(s):

Machine Learning ◽

Natural Product ◽

Global Analysis ◽

Gene Clusters ◽

Divergent Evolution ◽

Acid Activation ◽

Biosynthetic Gene ◽

Biosynthetic Gene Clusters ◽

Predictive Tool ◽

Wide Range

Enzymes that cleave ATP to activate carboxylic acids play essential roles in primary and secondary metabolism in all domains of life. Class I adenylate-forming enzymes share a conserved structural fold but act on a wide range of substrates to catalyze reactions involved in bioluminescence, nonribosomal peptide biosynthesis, fatty acid activation, and β-lactone formation. Despite their metabolic importance, the substrates and functions of the vast majority of adenylate-forming enzymes are unknown without tools available to accurately predict them. Given the crucial roles of adenylate-forming enzymes in biosynthesis, this also severely limits our ability to predict natural product structures from biosynthetic gene clusters. Here we used machine learning to predict adenylate-forming enzyme function and substrate specificity from protein sequences. We built a web-based predictive tool and used it to comprehensively map the biochemical diversity of adenylate-forming enzymes across >50,000 candidate biosynthetic gene clusters in bacterial, fungal, and plant genomes. Ancestral phylogenetic reconstruction and sequence similarity networking of enzymes from these clusters suggested divergent evolution of the adenylate-forming superfamily from a core enzyme scaffold most related to contemporary CoA ligases toward more specialized functions including β-lactone synthetases. Our classifier predicted β-lactone synthetases in uncharacterized biosynthetic gene clusters conserved in >90 different strains of Nocardia. To test our prediction, we purified a candidate β-lactone synthetase from Nocardia brasiliensis and reconstituted the biosynthetic pathway in vitro to link the gene cluster to the β-lactone natural product, nocardiolactone. We anticipate that our machine learning approach will aid in functional classification of enzymes and advance natural product discovery.

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Discovery and characterisation of an amidine-containing ribosomally-synthesised peptide that is widely distributed in nature

Chemical Science ◽

10.1039/d1sc01456k ◽

2021 ◽

Author(s):

Alicia H Russell ◽

Natalia Miguel Vior ◽

Edward Steven Hems ◽

Rodney Lacret ◽

Andrew William Truman

Keyword(s):

Natural Product ◽

Genome Mining ◽

Gene Clusters ◽

Biosynthetic Gene ◽

Biosynthetic Gene Clusters ◽

Wide Range ◽

Modified Peptides

Ribosomally synthesised and post-translationally modified peptides (RiPPs) are a structurally diverse class of natural product with a wide range of bioactivities. Genome mining for RiPP biosynthetic gene clusters (BGCs) is...

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Understanding and manipulating antibiotic production in actinomycetes

Biochemical Society Transactions ◽

10.1042/bst20130214 ◽

2013 ◽

Vol 41 (6) ◽

pp. 1355-1364 ◽

Cited By ~ 29

Author(s):

Mervyn J. Bibb

Keyword(s):

Natural Product ◽

Biological Activities ◽

Antibiotic Production ◽

Gene Clusters ◽

Biosynthetic Gene ◽

Biosynthetic Gene Clusters ◽

Natural Product Biosynthesis ◽

Genomic Technologies ◽

Wide Range ◽

Recent Developments

Actinomycetes are prolific producers of natural products with a wide range of biological activities. Many of the compounds that they make (and derivatives thereof) are used extensively in medicine, most notably as clinically important antibiotics, and in agriculture. Moreover, these organisms remain a source of novel and potentially useful molecules, but maximizing their biosynthetic potential requires a better understanding of natural product biosynthesis. Recent developments in genome sequencing have greatly facilitated the identification of natural product biosynthetic gene clusters. In the present article, I summarize the recent contributions of our laboratory in applying genomic technologies to better understand and manipulate natural product biosynthesis in a range of different actinomycetes.

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Mining metagenomes for natural product biosynthetic gene clusters: unlocking new potential with ultrafast techniques

10.1101/2021.01.20.427441 ◽

2021 ◽

Author(s):

Emiliano Pereira-Flores ◽

Marnix Medema ◽

Pier Luigi Buttigieg ◽

Peter Meinicke ◽

Frank Oliver Glöckner ◽

...

Keyword(s):

Natural Products ◽

Natural Product ◽

Human Microbiome ◽

Gene Clusters ◽

Human Microbiome Project ◽

Biosynthetic Gene Cluster ◽

Metagenomic Data ◽

Biosynthetic Gene ◽

Biosynthetic Gene Clusters ◽

Wide Range

Microorganisms produce an immense variety of natural products through the expression of Biosynthetic Gene Clusters (BGCs): physically clustered genes that encode the enzymes of a specialized metabolic pathway. These natural products cover a wide range of chemical classes (e.g., aminoglycosides, lantibiotics, nonribosomal peptides, oligosaccharides, polyketides, terpenes) that are highly valuable for industrial and medical applications1. Metagenomics, as a culture-independent approach, has greatly enhanced our ability to survey the functional potential of microorganisms and is growing in popularity for the mining of BGCs. However, to effectively exploit metagenomic data to this end, it will be crucial to more efficiently identify these genomic elements in highly complex and ever-increasing volumes of data2. Here, we address this challenge by developing the ultrafast Biosynthetic Gene cluster MEtagenomic eXploration toolbox (BiG-MEx). BiG-MEx rapidly identifies a broad range of BGC protein domains, assess their diversity and novelty, and predicts the abundance profile of natural product BGC classes in metagenomic data. We show the advantages of BiG-MEx compared to standard BGC-mining approaches, and use it to explore the BGC domain and class composition of samples in the TARA Oceans3 and Human Microbiome Project datasets4. In these analyses, we demonstrate BiG-MEx’s applicability to study the distribution, diversity, and ecological roles of BGCs in metagenomic data, and guide the exploration of natural products with clinical applications.

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Survey of Biosynthetic Gene Clusters from Sequenced Myxobacteria Reveals Unexplored Biosynthetic Potential

Microorganisms ◽

10.3390/microorganisms7060181 ◽

2019 ◽

Vol 7 (6) ◽

pp. 181 ◽

Cited By ~ 5

Author(s):

Katherine Gregory ◽

Laura A. Salvador ◽

Shukria Akbar ◽

Barbara I. Adaikpoh ◽

D. Cole Stevens

Keyword(s):

Natural Product ◽

Chemical Space ◽

Sequence Similarity ◽

Gene Clusters ◽

Biologically Active ◽

Critical Component ◽

Biosynthetic Gene ◽

Bacterial Genomes ◽

Biosynthetic Gene Clusters ◽

Natural Product Discovery

Coinciding with the increase in sequenced bacteria, mining of bacterial genomes for biosynthetic gene clusters (BGCs) has become a critical component of natural product discovery. The order Myxococcales, a reputable source of biologically active secondary metabolites, spans three suborders which all include natural product producing representatives. Utilizing the BiG-SCAPE-CORASON platform to generate a sequence similarity network that contains 994 BGCs from 36 sequenced myxobacteria deposited in the antiSMASH database, a total of 843 BGCs with lower than 75% similarity scores to characterized clusters within the MIBiG database are presented. This survey provides the biosynthetic diversity of these BGCs and an assessment of the predicted chemical space yet to be discovered. Considering the mere snapshot of myxobacteria included in this analysis, these untapped BGCs exemplify the potential for natural product discovery from myxobacteria.

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Mining of Cyanobacterial Genomes Indicates That Plasmids Are Involved in the Production of Natural Products

10.21203/rs.3.rs-121751/v1 ◽

2020 ◽

Author(s):

Rafael Popin ◽

Danillo Alvarenga ◽

Raquel Castelo-Branco ◽

David Fewer ◽

Kaarina Sivonen

Keyword(s):

Natural Products ◽

Natural Product ◽

Biological Activities ◽

Gene Clusters ◽

Biosynthetic Pathways ◽

Biosynthetic Gene ◽

Biosynthetic Gene Clusters ◽

Chemical Structures ◽

Wide Range ◽

Genes Encoding

Abstract Background Microbial natural products have unique chemical structures and diverse biological activities. Cyanobacteria commonly possess a wide range of biosynthetic gene clusters to produce natural products. Several studies have mapped the distribution of natural product biosynthetic gene clusters in cyanobacterial genomes. However, little attention has been paid to natural product biosynthesis in plasmids. Some genes encoding cyanobacterial natural product biosynthetic pathways are believed to be dispersed by plasmids through horizontal gene transfer. Thus, we examined complete cyanobacterial genomes to assess if plasmids are involved in the production and dissemination of natural products by cyanobacteria.Results The 185 analyzed genomes possessed 1 to 42 gene clusters and an average of 10. In total, 1816 biosynthetic gene clusters were found. Approximately 95% of these clusters were present in chromosomes. The remaining 5% were present in plasmids, from which homologs of the biosynthetic pathways for aeruginosin, anabaenopeptin, ambiguine, cryptophycin, hassallidin, geosmin, and microcystin were manually curated. The cryptophycin pathway was previously described as active while the other gene cluster include all genes for biosynthesis. Approximately 12% of the 424 analyzed cyanobacterial plasmids contained homologs of genes involved in conjugation. Large plasmids, previously named as “chromids”, were also observed to be widespread in cyanobacteria. Sixteen cryptic natural product biosynthetic gene clusters and geosmin biosynthetic gene clusters were located in those mobile plasmids.Conclusion Homologues of genes involved in the production of toxins, protease inhibitors, odorous compounds, antimicrobials, antitumorals, and other unidentified natural products are located in cyanobacterial plasmids. Some of these plasmids are predicted to be conjugative. The present study provides in silico evidence that plasmids are involved in the distribution of natural product biosynthetic pathways in cyanobacteria.

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Complete genome sequences of Streptomyces spp. isolated from disease-suppressive soils

BMC Genomics ◽

10.1186/s12864-019-6279-8 ◽

2019 ◽

Vol 20 (1) ◽

Cited By ~ 1

Author(s):

Stephen C. Heinsch ◽

Szu-Yi Hsu ◽

Lindsey Otto-Hanson ◽

Linda Kinkel ◽

Michael J. Smanski

Keyword(s):

Microbial Communities ◽

Natural Product ◽

De Novo ◽

Sequence Similarity ◽

Gene Clusters ◽

Biosynthetic Gene ◽

Sequencing Data ◽

Biosynthetic Gene Clusters ◽

Contig Assembly ◽

Sample Number

Abstract Background Bacteria within the genus Streptomyces remain a major source of new natural product discovery and as soil inoculants in agriculture where they promote plant growth and protect from disease. Recently, Streptomyces spp. have been implicated as important members of naturally disease-suppressive soils. To shine more light on the ecology and evolution of disease-suppressive microbial communities, we have sequenced the genome of three Streptomyces strains isolated from disease-suppressive soils and compared them to previously sequenced isolates. Strains selected for sequencing had previously showed strong phenotypes in competition or signaling assays. Results Here we present the de novo sequencing of three strains of the genus Streptomyces isolated from disease-suppressive soils to produce high-quality complete genomes. Streptomyces sp. GS93–23, Streptomyces sp. 3211–3, and Streptomyces sp. S3–4 were found to have linear chromosomes of 8.24 Mb, 8.23 Mb, and greater than 7.5 Mb, respectively. In addition, two of the strains were found to have large, linear plasmids. Each strain harbors between 26 and 38 natural product biosynthetic gene clusters, on par with previously sequenced Streptomyces spp. We compared these newly sequenced genomes with those of previously sequenced organisms. We see substantial natural product biosynthetic diversity between closely related strains, with the gain/loss of episomal DNA elements being a primary driver of genome evolution. Conclusions Long read sequencing data facilitates large contig assembly for high-GC Streptomyces genomes. While the sample number is too small for a definitive conclusion, we do not see evidence that disease suppressive soil isolates are particularly privileged in terms of numbers of biosynthetic gene clusters. The strong sequence similarity between GS93–23 and previously isolated Streptomyces lydicus suggests that species recruitment may contribute to the evolution of disease-suppressive microbial communities.

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Activation of three natural product biosynthetic gene clusters from Streptomyces lavendulae CGMCC 4.1386 by a reporter-guided strategy

Synthetic and Systems Biotechnology ◽

10.1016/j.synbio.2018.10.010 ◽

2018 ◽

Vol 3 (4) ◽

pp. 254-260 ◽

Cited By ~ 1

Author(s):

Pengwei Li ◽

Zhengyan Guo ◽

Wei Tang ◽

Yihua Chen

Keyword(s):

Natural Product ◽

Gene Clusters ◽

Biosynthetic Gene ◽

Biosynthetic Gene Clusters ◽

Streptomyces Lavendulae

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Pan-Genome of the Genus Streptomyces and Prioritization of Biosynthetic Gene Clusters With Potential to Produce Antibiotic Compounds

Frontiers in Microbiology ◽

10.3389/fmicb.2021.677558 ◽

2021 ◽

Vol 12 ◽

Author(s):

Carlos Caicedo-Montoya ◽

Monserrat Manzo-Ruiz ◽

Rigoberto Ríos-Estepa

Keyword(s):

Comparative Genomics ◽

Sequence Similarity ◽

Experimental Studies ◽

Gene Clusters ◽

Antibiotic Activity ◽

Genomic Diversity ◽

Biosynthetic Gene ◽

Biosynthetic Gene Clusters ◽

Genus Streptomyces ◽

Pan Genome

Species of the genus Streptomyces are known for their ability to produce multiple secondary metabolites; their genomes have been extensively explored to discover new bioactive compounds. The richness of genomic data currently available allows filtering for high quality genomes, which in turn permits reliable comparative genomics studies and an improved prediction of biosynthetic gene clusters (BGCs) through genome mining approaches. In this work, we used 121 genome sequences of the genus Streptomyces in a comparative genomics study with the aim of estimating the genomic diversity by protein domains content, sequence similarity of proteins and conservation of Intergenic Regions (IGRs). We also searched for BGCs but prioritizing those with potential antibiotic activity. Our analysis revealed that the pan-genome of the genus Streptomyces is clearly open, with a high quantity of unique gene families across the different species and that the IGRs are rarely conserved. We also described the phylogenetic relationships of the analyzed genomes using multiple markers, obtaining a trustworthy tree whose relationships were further validated by Average Nucleotide Identity (ANI) calculations. Finally, 33 biosynthetic gene clusters were detected to have potential antibiotic activity and a predicted mode of action, which might serve up as a guide to formulation of related experimental studies.

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