| Literature DB >> 28379712 |
Alexandros Kiriazis1, Ingo B Aumüller1, Ralica Arnaudova1,2, Vanessa Brito3, Tobias Rüffer4, Heinrich Lang4, Samuel M Silvestre3,5, Päivi J Koskinen2, Jari Yli-Kauhaluoma1.
Abstract
The built-in o- and p-QM (QM = quinone methide) moieties in benzo[cd]azulen-3-ones account for an easy switch between the bridged 10π- and 6π-aromatic systems in organic synthesis. We report conjugate additions, oxidative nucleophilic substitutions of hydrogen, and reversible Michael additions under very mild conditions. In the presence of thiol nucleophiles, the protonated σH-adducts could be isolated and characterized. The typical preference for either the o- or p-QM moiety led to high regioselectivity. Furthermore, the inhibitory potency of the novel benzo[cd]azulenes against the human Pim-1 kinase was evaluated.Entities:
Year: 2017 PMID: 28379712 DOI: 10.1021/acs.orglett.7b00588
Source DB: PubMed Journal: Org Lett ISSN: 1523-7052 Impact factor: 6.005