4.5 Article

New azodyrecins identified by a genome mining-directed reactivity-based screening

BEILSTEIN JOURNAL OF ORGANIC CHEMISTRY (2022)

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Journal

BEILSTEIN JOURNAL OF ORGANIC CHEMISTRY
Volume 18, Issue -, Pages 1017-1025

Publisher

BEILSTEIN-INSTITUT
DOI: 10.3762/bjoc.18.102

Keywords

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Categories

Chemistry, Organic

Funding

  1. Hokkaido University
  2. Global Facility Center (GFC)
  3. Pharma Science Open Unit (PSOU)
  4. MEXT under Support Program for Imple-mentation of New Equipment Sharing System
  5. Global Station for Biosurfaces and Drug Discovery, a project of Global Institution for Collaborative Research and Education in Hokkaido University
  6. Asahi Glass Foundation
  7. Naito Foundation
  8. Uehara Memorial Foundation
  9. Sumitomo Foundation-Grant for Basic Science Research Projects
  10. Daiichi Sankyo Foundation of Life Science
  11. japan Agency for Medical Research and Development
  12. Ministry of Education, Culture, Sports, Science and Technology (MEXT)
  13. Japan Science and Technology Agency Japan
  14. [JP19ae0101045]
  15. [ACT-X JPMJAX201F]
  16. [JP16H06448]
  17. [JP18H02581]
  18. [JP19K16390]
  19. [JP21H02635]
  20. [JP22K15302]
  21. [A-STEP JPMJTR20US]

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This study identified four new analogs of aliphatic azoxides through a reactivity-based screening. The study found that the double bond in the alkyl side chain is crucial for the cytotoxicity of azodyrecins. Additionally, the study elucidated the tailoring step of azodyrecin biosynthesis.
Only a few azoxy natural products have been identified despite their intriguing biological activities. Azodyrecins D-G, four new analogs of aliphatic azoxides, were identified from two Streptomyces species by a reactivity-based screening that targets azoxy bonds. A biological activity evaluation demonstrated that the double bond in the alkyl side chain is important for the cytotoxicity of azodyrecins. An in vitro assay elucidated the tailoring step of azodyrecin biosynthesis, which is mediated by the S-adenosylmethionine (SAM)-dependent methyltransferase Ady1. This study paves the way for the targeted isolation of aliphatic azoxy natural products through a genome-mining approach and further investigations of their biosynthetic mechanisms.

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