Disruption of TCF/{beta}-Catenin Binding Impairs Wnt Signaling and Induces Apoptosis in Soft Tissue Sarcoma Cells
In this study, we have tested pharmacologic inhibition of Wnt signaling mediated by disruption of TCF/β-catenin binding and AXIN stabilization, being the first strategy more efficient in reducing cell viability and downstream effects. We have shown that disruption of TCF/β-catenin binding with PKF118-310 produces in vitro antitumor activity in a panel of prevalent representative STS cell lines and primary cultures. At the molecular level, PKF118-310 treatment reduced β-catenin nuclear localization, reporter activity, and target genes, resulting in an increase in apoptosis. Importantly, combination of PKF118-310 with doxorubicin resulted in enhanced reduction of cell viability, suggesting that Wnt inhibition could be a new combination regime in these patients. Our findings support the usefulness of Wnt inhibitors as new therapeutic strategies for the prevalent STS. Mol Cancer Ther; 16(6); 1166–76. ©2017 AACR.
Source: Molecular Cancer Therapeutics - Category: Cancer & Oncology Authors: Martinez-Font, E., Felipe-Abrio, I., Calabuig-Farinas, S., Ramos, R., Terrasa, J., Vögler, O., Alemany, R., Martin-Broto, J., Obrador-Hevia, A. Tags: Cancer Biology and Signal Transduction Source Type: research
More News: Biology | Cancer | Cancer & Oncology | Genetics | Molecular Biology | Sarcomas | Soft Tissue Sarcoma | Stem Cell Therapy | Stem Cells | Study
MedWorm Privacy Policy
Disclaimer
Copyright © MedWorm 2006-2024