Issue 2, 2013

Relative impact of 3- and 5-hydroxyl groups of cytosporone B on cancer cell viability

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.

Graphical abstract: Relative impact of 3- and 5-hydroxyl groups of cytosporone B on cancer cell viability

Supplementary files

Article information

Article type
Concise Article
Submitted
17 Aug 2012
Accepted
07 Nov 2012
First published
12 Nov 2012

Med. Chem. Commun., 2013,4, 332-339

Relative impact of 3- and 5-hydroxyl groups of cytosporone B on cancer cell viability

Z. Xia, X. Cao, E. Rico-Bautista, J. Yu, L. Chen, J. Chen, A. Bobkov, D. A. Wolf, X. Zhang and M. I. Dawson, Med. Chem. Commun., 2013, 4, 332 DOI: 10.1039/C2MD20243C

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