4.7 Article

Discovery and Heterologous Expression of Microginins from Microcystis aeruginosa LEGE 91341

Journal

ACS SYNTHETIC BIOLOGY
Volume -, Issue -, Pages -

Publisher

AMER CHEMICAL SOC
DOI: 10.1021/acssynbio.2c00389

Keywords

cyanobacteria; natural products; direct pathway cloning (DiPaC); heterologous expression; microginins; biosynthesis

Funding

  1. Fundacao para a Ciencia e a Tecnologia [PTDC/BIA-BQM/29710/2017, UIDB/04423/2021, UIDP/04423/2021, SFRH/BD/136367/2018]
  2. European Union [952374]
  3. German Research Foundation
  4. State Ministry of Science and Cultural Affairs of Saxony [SAB 100589439]

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A study discovered 12 new variants of microginins in a cyanobacterium, containing uncommon amino acids. Heterologous expression of the relevant biosynthetic gene cluster led to the production of several microginins, providing a pathway for accessing new variants through genome data or pathway engineering.
Microginins are a large family of cyanobacterial lipopeptide protease inhibitors. A hybrid polyketide synthase/non-ribosomal peptide synthetase biosynthetic gene cluster (BGC) found in several microginin-producing strains-mic-was proposed to encode the production of microginins, based on bioinformatic analysis. Here, we explored a cyanobacterium, Microcystis aeruginosa LEGE 91341, which contains a mic BGC, to discover 12 new microginin variants. The new compounds contain uncommon amino acids, namely, homophenylalanine (Hphe), homotyrosine (Htyr), or methylproline, as well as a 3-aminodecanoic acid (Ada) residue, which in some variants was chlorinated at its terminal methyl group. We have used direct pathway cloning (DiPaC) to heterologously express the mic BGC from M. aeruginosa LEGE 91341 in Escherichia coli, which led to the production of several microginins. This proved that the mic BGC is, in fact, responsible for the biosynthesis of microginins and paves the way to accessing new variants from (meta)genome data or through pathway engineering.

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