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Characterization and Synthesis of Eudistidine C, a Bioactive Marine Alkaloid with an Intriguing Molecular Scaffold

  • Susanna T. S. Chan
  • , Roger R. Nani
  • , Evan A. Schauer
  • , Gary E. Martin
  • , R. Thomas Williamson
  • , Josep Sauri
  • , Alexei V. Buevich
  • , Wes A. Schafer
  • , Leo A. Joyce
  • , Andrew K. L. Goey
  • , William D. Figg
  • , Tanya T. Ransom
  • , Curtis J. Henrich
  • , Tawnya C. Mckee
  • , Arvin Moser
  • , Scott A. MacDonald
  • , Shabana Khan
  • , James B. McMahon
  • , Martin J. Schnermann
  • , Kirk R. Gustafson

Producción científica: Artículo en revista indizadaArtículorevisión exhaustiva

33 Citas (Scopus)

Resumen

An extract of Eudistoma sp. provided eudistidine C (1), a heterocyclic alkaloid with a novel molecular framework. Eudistidine C (1) is a racemic natural product composed of a tetracyclic core structure further elaborated with a p-methoxyphenyl group and a phenol-substituted aminoimidazole moiety. This compound presented significant structure elucidation challenges due to the large number of heteroatoms and fully substituted carbons. These issues were mitigated by application of a new NMR pulse sequence (LR-EISQMBC) optimized to detect four- and five-bond heteronuclear correlations and the use of computer-assisted structure elucidation software. Synthesis of eudistidine C (1) was accomplished in high yield by treating eudistidine A (2) with 4(2-amino-1H-irnidazol-5-yl)phenol (4) in DMSO. Synthesis of eudistidine C (1) confirmed the proposed structure and provided material for further biological characterization. Treatment of 2 with various nitrogen heterocycles and electron-rich arenes provided a series of analogues (5-10) of eudistidine C. Chiral-phase HPLC resolution of epimeric eudistidine C provided (+)-(R)-eudistidine C (la) and (-)-(S)-eudistidine C (1b). The absolute configuration of these enantiomers was assigned by ECD analysis. (-)-(S)-Eudistidine C (lb) modestly inhibited interaction between the protein binding domains of HIF-1 alpha and p300. Compounds 1, 2, and 6-10 exhibited significant antimalarial activity against Plasmodium falciparum.
Idioma originalInglés
Páginas (desde-hasta)10631-10640
Número de páginas10
PublicaciónJournal of Organic Chemistry
Volumen81
N.º22
DOI
EstadoPublicada - 18 nov 2016
Publicado de forma externa

ODS de las Naciones Unidas

Este resultado contribuye a los siguientes Objetivos de Desarrollo Sostenible

  1. ODS 14: Vida submarina
    ODS 14: Vida submarina

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