Title | Identification of a Raloxifene Analog That Promotes AhR-Mediated Apoptosis in Cancer Cells. |
Publication Type | Journal Article |
Year of Publication | 2017 |
Authors | Jang HSang, Pearce M, O'Donnell EF, Nguyen BDuc, Truong L, Mueller MJ, Bisson WH, Kerkvliet NI, Tanguay RL, Kolluri SKumar |
Journal | Biology (Basel) |
Volume | 6 |
Issue | 4 |
Date Published | 2017 Dec 01 |
ISSN | 2079-7737 |
Abstract | We previously reported that raloxifene, an estrogen receptor modulator, is also a ligand for the aryl hydrocarbon receptor (AhR). Raloxifene induces apoptosis in estrogen receptor-negative human cancer cells through the AhR. We performed structure-activity studies with seven raloxifene analogs to better understand the structural requirements of raloxifene for induction of AhR-mediated transcriptional activity and apoptosis. We identified Y134 as a raloxifene analog that activates AhR-mediated transcriptional activity and induces apoptosis in MDA-MB-231 human triple negative breast cancer cells. Suppression of AhR expression strongly reduced apoptosis induced by Y134, indicating the requirement of AhR for Y134-induced apoptosis. Y134 also induced apoptosis in hepatoma cells without having an effect on cell cycle regulation. Toxicity testing on zebrafish embryos revealed that Y134 has a significantly better safety profile than raloxifene. Our studies also identified an analog of raloxifene that acts as a partial antagonist of the AhR, and is capable of inhibiting AhR agonist-induced transcriptional activity. We conclude that Y134 is a promising raloxifene analog for further optimization as an anti-cancer agent targeting the AhR. |
DOI | 10.3390/biology6040041 |
Alternate Journal | Biology (Basel) |
PubMed ID | 29194351 |
PubMed Central ID | PMC5745446 |
Grant List | R01 ES016651 / ES / NIEHS NIH HHS / United States T32 ES007060 / ES / NIEHS NIH HHS / United States |