| Literature DB >> 24795803 |
Zebin Xia1, Xihua Cao1, Elizabeth Rico-Bautista1, Jinghua Yu1, Liqun Chen1, Jiebo Chen1, Andrey Bobkov1, Dieter A Wolf1, Xiao-Kun Zhang1, Marcia I Dawson1.
Abstract
A novel and the shortest route, thus far, for preparing cytosporone B (Csn-B) is reported. Csn-B and two analogs were used to probe the importance of hydroxyl groups at the 3- and 5-positions of the Csn-B benzene ring in inhibiting the viability of human H460 lung cancer and LNCaP prostate cancer cells, inducing H460 cell apoptosis, and interacting with the NR4A1 (TR3) ligand-binding domain (LBD). These studies indicate that Csn-B and 5-Me-Csn-B, having a phenolic hydroxyl at the 3-position of their aromatic rings, had similar activities in inhibiting cancer cell viability and in inducing apoptosis, whereas 3,5-(Me)2-Csn-B was unable to do so. These results are in agreement with ligand-binding experiments showing that the interaction with the NR4A1 LBD required the presence of the 3-hydroxyl group.Entities:
Year: 2012 PMID: 24795803 PMCID: PMC4005383 DOI: 10.1039/C2MD20243C
Source DB: PubMed Journal: Medchemcomm ISSN: 2040-2503 Impact factor: 3.597