AI Article Synopsis

  • Naringenin and its derivative naringin are flavonoids made via the phenylpropanoid pathway, and recent findings show that actinobacteria, used in producing clavulanic acid, can also synthesize naringenin.
  • The biosynthesis in these bacteria involves key enzymes like chalcone synthase and tyrosine ammonia lyase, and specific genes are crucial for this process.
  • Comparative analysis of naringenin-producing enzymes in actinobacteria and plants suggests evolutionary conservation but different mechanisms for the same reactions, paving the way for developing new antibacterial and antitumor compounds.

Article Abstract

Naringenin and its glycosylated derivative naringin are flavonoids that are synthesized by the phenylpropanoid pathway in plants. We found that naringenin is also formed by the actinobacterium , a well-known microorganism used to industrially produce clavulanic acid. The production of naringenin in involves a chalcone synthase that uses -coumaric as a starter unit and a P monoxygenase, encoded by two adjacent genes (). The -coumaric acid starter unit is formed by a tyrosine ammonia lyase encoded by an unlinked, , gene. Deletion and complementation studies demonstrate that these three genes are required for biosynthesis of naringenin in . Other actinobacteria chalcone synthases use caffeic acid, ferulic acid, sinapic acid or benzoic acid as starter units in the formation of different antibiotics and antitumor agents. The biosynthesis of naringenin is restricted to a few species and the encoding gene cluster is present also in some and species. Phylogenetic comparison of naringenin chalcone synthase with homologous proteins of other actinobacteria reveal that this protein is closely related to chalcone synthases that use malonyl-CoA as a starter unit for the formation of red-brown pigment. The function of the core enzymes in the pathway, such as the chalcone synthase and the tyrosine ammonia lyase, is conserved in plants and actinobacteria. However, use a P monooxygenase proposed to complete the cyclization step of the naringenin chalcone, whereas this reaction in plants is performed by a chalcone isomerase. Comparison of the plant and chalcone synthases indicates that they have not been transmitted between these organisms by a recent horizontal gene transfer phenomenon. We provide a comprehensive view of the molecular genetics and biochemistry of chalcone synthases and their impact on the development of antibacterial and antitumor compounds. These advances allow new bioactive compounds to be obtained using combinatorial strategies. In addition, processes of heterologous expression and bioconversion for the production of naringenin and naringenin-derived compounds in yeasts are described.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8773403PMC
http://dx.doi.org/10.3390/antibiotics11010082DOI Listing

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