| Literature DB >> 29256515 |
Ken Mukai1, Danilo Pereira de Sant'Ana1, Yasuo Hirooka1, Eduardo V Mercado-Marin1, David E Stephens1, Kevin G M Kou1, Sven C Richter1, Naomi Kelley1, Richmond Sarpong1.
Abstract
Stephacidin A and its congeners are a collection of secondary metabolites that possess intriguing structural motifs. They stem from unusual biosynthetic sequences that lead to the incorporation of a prenyl or reverse-prenyl group into a bicyclo[2.2.2]diazaoctane framework, a chromene unit or the vestige thereof. To complement biosynthetic studies, which normally play a significant role in unveiling the biosynthetic pathways of natural products, here we demonstrate that chemical synthesis can provide important insights into biosynthesis. We identify a short total synthesis of congeners in the reverse-prenylated indole alkaloid family related to stephacidin A by taking advantage of a direct indole C6 halogenation of the related ketopremalbrancheamide. This novel strategic approach has now made possible the syntheses of several natural products, including malbrancheamides B and C, notoamides F, I and R, aspergamide B, and waikialoid A, which is a heterodimer of avrainvillamide and aspergamide B. Our approach to the preparation of these prenylated and reverse-prenylated indole alkaloids is bioinspired, and may also inform the as-yet undetermined biosynthesis of several congeners.Entities:
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Year: 2017 PMID: 29256515 PMCID: PMC6317722 DOI: 10.1038/nchem.2862
Source DB: PubMed Journal: Nat Chem ISSN: 1755-4330 Impact factor: 24.427