| Literature DB >> 22506594 |
Satoshi Endo1, Toshiyuki Matsunaga, Ayano Kanamori, Yoko Otsuji, Hiroko Nagai, Krithika Sundaram, Ossama El-Kabbani, Naoki Toyooka, Shozo Ohta, Akira Hara.
Abstract
The human aldo-keto reductase (AKR) 1C3, also known as type-5 17β-hydroxysteroid dehydrogenase and prostaglandin F synthase, has been suggested as a therapeutic target in the treatment of prostate and breast cancers. In this study, AKR1C3 inhibition was examined by Brazilian propolis-derived cinnamic acid derivatives that show potential antitumor activity, and it was found that baccharin (1) is a potent competitive inhibitor (K(i) 56 nM) with high selectivity, showing no significant inhibition toward other AKR1C isoforms (AKR1C1, AKR1C2, and AKR1C4). Molecular docking and site-directed mutagenesis studies suggested that the nonconserved residues Ser118, Met120, and Phe311 in AKR1C3 are important for determining the inhibitory potency and selectivity of 1. The AKR1C3-mediated metabolism of 17-ketosteroid and farnesal in cancer cells was inhibited by 1, which was effective from 0.2 μM with an IC(50) value of about 30 μM. Additionally, 1 suppressed the proliferation of PC3 prostatic cancer cells stimulated by AKR1C3 overexpression. This study is the first demonstration that 1 is a highly selective inhibitor of AKR1C3.Entities:
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Year: 2012 PMID: 22506594 DOI: 10.1021/np201002x
Source DB: PubMed Journal: J Nat Prod ISSN: 0163-3864 Impact factor: 4.050