The cyanobacterial hepatotoxin microcystin is assembled at a non-ribosomal peptide synthetase (NRPS) complex. The enormous structural diversity of this peptide, which is also found in closely related strains, is the result of frequent recombination events and point mutations. Here, we have compared the in vitro activation profiles of related monospecific and multispecific modules that either strictly incorporate leucine or arginine or incorporate chemically diverse amino acids in parallel into microcystin. By analyzing di- and tri-domain proteins we have dissected the role of adenylation and condensation domains for substrate specificity. We have further analyzed the role of subdomains and provide evidence for an extended gatekeeping function for the condensation domains of multispecific modules. By reproducing natural point mutations, we could convert a monospecific module into a multispecific module. Our findings may inspire novel synthetic biology approaches and demonstrate how recombination platforms of NRPSs have developed in nature.
Filamentous
cyanobacteria belong to the most prolific producers
of structurally unique and biologically active natural products, yet
the majority of biosynthetic gene clusters predicted for these multicellular
collectives are currently orphan. Here, we present a systems analysis
of secondary metabolite gene expression in the model strain Nostoc punctiforme PCC73102 using RNA-seq and fluorescence
reporter analysis. Our data demonstrate that the majority of the cryptic
gene clusters are not silent but are expressed with regular or sporadic
pattern. Cultivation of N. punctiforme using high-density
fermentation overrules the spatial control and leads to a pronounced
upregulation of more than 50% of biosynthetic gene clusters. Our data
suggest that a combination of autocrine factors, a high CO2 level, and high light account for the upregulation of individual
pathways. Our overarching study not only sheds light on the strategies
of filamentous cyanobacteria to share the enormous metabolic burden
connected with the production of specialized molecules but provides
an avenue for the genome-based discovery of natural products in multicellular
cyanobacteria as exemplified by the discovery of highly unusual variants
of the tricyclic peptide microviridin.
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