Broad anti-tumor activity of a small molecule that selectively targets the warburg effect and lipogenesis
Cancer Cell • 2015
Publication Information
Authors
Colin A Flaveny, Kristine Griffett, Bahaa El-Dien M El-Gendy, Melissa Kazantzis, Monideepa Sengupta, Antonio L Amelio, Arindam Chatterjee, John Walker, Laura A Solt, Theodore M Kamenecka, Thomas P Burris
Keywords
Not Available
Journal
Cancer Cell
Publisher
Cell Press
Volume
28
Issue
1
Pages
42-56
publication.type
International
Paper Link
Open Link
Supplementary Materials
Not Available
Abstract
Malignant cells exhibit aerobic glycolysis (the Warburg effect) and become dependent on de novo lipogenesis, which sustains rapid proliferation and resistance to cellular stress. The nuclear receptor liver-X-receptor (LXR) directly regulates expression of key glycolytic and lipogenic genes. To disrupt these oncogenic metabolism pathways, we designed an LXR inverse agonist SR9243 that induces LXR-corepressor interaction. In cancer cells, SR9243 significantly inhibited the Warburg effect and lipogenesis by reducing glycolytic and lipogenic gene expression. SR9243 induced apoptosis in tumors without inducing weight loss, hepatotoxicity, or inflammation. Our results suggest that LXR inverse agonists may be an effective cancer treatment approach.
Staff Members - Benha University