Authors
Rudenko, A., Mohite, O., Yun, B., Lee, B. T., Lee, B., Kwon, J. Y., Kang, H.-S., Santos, A., Weber, T., Kim, H. U., Charusanti, P.
Abstract
Actinomycetota are major sources of specialized metabolites with applications in drug discovery and agriculture, yet much of their biosynthetic potential remains silent under standard laboratory conditions. Limited understanding of the mechanisms controlling biosynthetic gene cluster (BGC) activation constrains metabolite discovery and production. Here, we generated 1432 RNA-seq datasets from 132 Actinomycetota strains grown in eight media to identify patterns associated with BGC expression. On average, strains expressed 44% of their encoded BGCs across the tested conditions, with more expression observed among known BGCs (61%) compared to uncharacterized BGCs (35%). Co-expression analyses revealed frequent associations between BGCs and transporters, transcriptional regulators, and proteins containing DUF397 and DUF742 domains. Targeted overexpression of candidate genes selected from BGC-associated co-expression modules increased metabolite production, with DUF397- and DUF742-containing operons showing the broadest effects by boosting the levels of several different specialized metabolites. Other genes boosted levels in a metabolite-specific manner. Together, our results support a multilayered model of BGC regulation in Actinomycetota in which BGC expression is shaped by medium composition, BGC-specific regulators, and integration of BGCs into broader transcriptional network modules. By connecting BGC expression to specific media and co-expressed genes, this study also provides a resource for selecting growth conditions and engineering specialized metabolism.
Preprint server:
bioRxiv
The authors list and abstract were imported from bioRxiv on 18 Jun 2026.
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