Acta Pharmaceutica Sinica B (Aug 2023)

P450-mediated dehydrotyrosine formation during WS9326 biosynthesis proceeds via dehydrogenation of a specific acylated dipeptide substrate

  • Songya Zhang,
  • Lin Zhang,
  • Anja Greule,
  • Julien Tailhades,
  • Edward Marschall,
  • Panward Prasongpholchai,
  • Daniel J. Leng,
  • Jingfan Zhang,
  • Jing Zhu,
  • Joe A. Kaczmarski,
  • Ralf B. Schittenhelm,
  • Oliver Einsle,
  • Colin J. Jackson,
  • Fabrizio Alberti,
  • Andreas Bechthold,
  • Youming Zhang,
  • Manuela Tosin,
  • Tong Si,
  • Max J. Cryle

Journal volume & issue
Vol. 13, no. 8
pp. 3561 – 3574

Abstract

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WS9326A is a peptide antibiotic containing a highly unusual N-methyl-E-2-3-dehydrotyrosine (NMet-Dht) residue that is incorporated during peptide assembly on a non-ribosomal peptide synthetase (NRPS). The cytochrome P450 encoded by sas16 (P450Sas) has been shown to be essential for the formation of the alkene moiety in NMet-Dht, but the timing and mechanism of the P450Sas-mediated α,β-dehydrogenation of Dht remained unclear. Here, we show that the substrate of P450Sas is the NRPS-associated peptidyl carrier protein (PCP)-bound dipeptide intermediate (Z)-2-pent-1′-enyl-cinnamoyl-Thr-N-Me-Tyr. We demonstrate that P450Sas-mediated incorporation of the double bond follows N-methylation of the Tyr by the N-methyl transferase domain found within the NRPS, and further that P450Sas appears to be specific for substrates containing the (Z)-2-pent-1′-enyl-cinnamoyl group. A crystal structure of P450Sas reveals differences between P450Sas and other P450s involved in the modification of NRPS-associated substrates, including the substitution of the canonical active site alcohol residue with a phenylalanine (F250), which in turn is critical to P450Sas activity and WS9326A biosynthesis. Together, our results suggest that P450Sas catalyses the direct dehydrogenation of the NRPS-bound dipeptide substrate, thus expanding the repertoire of P450 enzymes that can be used to produce biologically active peptides.

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