1. Academic Validation
  2. A lesion-mimic mutant of Catharanthus roseus accumulates the opioid agonist, akuammicine

A lesion-mimic mutant of Catharanthus roseus accumulates the opioid agonist, akuammicine

  • Phytochemistry. 2022 Nov:203:113422. doi: 10.1016/j.phytochem.2022.113422.
Fanfan Li 1 Stephen Bordeleau 2 Kyung Hee Kim 3 Jonathan Turcotte 1 Benjamin Davis 3 Lan Liu 4 Stéphane Bayen 4 Vincenzo De Luca 3 Mehran Dastmalchi 5
Affiliations

Affiliations

  • 1 Plant Science, McGill University, Sainte-Anne-de-Bellevue, QC, H9X 3V9, Canada.
  • 2 Cell and Systems Biology, University of Toronto, Toronto, ON, M5S 3B2, Canada.
  • 3 Biological Sciences, Brock University, St. Catharines, ON, L2S 3A1, Canada.
  • 4 Food Science and Agricultural Chemistry, McGill University, Sainte-Anne-de-Bellevue, QC, H9X 3V9, Canada.
  • 5 Plant Science, McGill University, Sainte-Anne-de-Bellevue, QC, H9X 3V9, Canada. Electronic address: mehran.dastmalchi@mcgill.ca.
Abstract

Catharanthus roseus is a medicinal plant that produces an abundance of monoterpenoid Indole Alkaloids (MIAs), notably including the Anticancer compounds vinblastine and vincristine. While the canonical pathway leading to these drugs has been resolved, the regulatory and catalytic mechanisms controlling many lateral branches of MIA biosynthesis remain largely unknown. Here, we describe an ethyl methanesulfonate (EMS) C. roseus mutant (M2-117523) that accumulates high levels of MIAs. The mutant exhibited stunted growth, partially chlorotic leaves, with deficiencies in chlorophyll biosynthesis, and a lesion-mimic phenotype. The lesions were sporadic and spontaneous, appearing after the first true bifoliate and continuing throughout development. The lesions are also the site of high concentrations of akuammicine, a minor constituent of wild type C. roseus leaves. In addition to akuammicine, the lesions were enriched in 25 other MIAs, resulting, in part, from a higher metabolic flux through the pathway. The unique metabolic shift was associated with significant upregulation of biosynthetic and regulatory genes involved in the MIA pathway, including the transcription factors WRKY1, CrMYC2, and ORCA2, and the biosynthetic genes STR, GO, and Redox1. Following the lesion-mimic mutant (LMM) phenotype, the accumulation of akuammicine is jasmonate (JA)-inducible, suggesting a role in plant defence response. Akuammicine is medicinally significant, as a weak opioid agonist, with a preference for the κ-opioid receptor, and a potential anti-diabetic. Further study of akuammicine biosynthesis and regulation can guide plant and heterologous engineering for medicinal uses.

Keywords

Akuammicine; Apocynaceae; Catharanthus roseus; Jasmonic acid; Lesion mimic mutant; Monoterpenoid indole alkaloids; Opioid; Programmed cell death; WRKY.

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