Blocking the Formation of Radiation-induced Breast Cancer Stem Cells

Overview

Journal Oncotarget

Specialty Oncology

Date 2014 Jul 9

PMID 25003837

Citations 52

Authors

Yangyang Wang

Wende Li

Shalin S Patel

Juan Cong

Nan Zhang

Francesco Sabbatino

Xiaoyan Liu

Yuan Qi

Peigen Huang

Hang Lee

Alphonse Taghian

Jian-Jian Li

Albert B DeLeo

Soldano Ferrone

Michael W Epperly

Cristina R Ferrone

Amy Ly

Elena F Brachtel

Xinhui Wang

Affiliations

Soon will be listed here.

Abstract

The goal of adjuvant (post-surgery) radiation therapy (RT) for breast cancer (BC) is to eliminate residual cancer cells, leading to better local tumor control and thus improving patient survival. However, radioresistance increases the risk of tumor recurrence and negatively affects survival. Recent evidence shows that breast cancer stem cells (BCSCs) are radiation-resistant and that relatively differentiated BC cells can be reprogrammed into induced BCSCs (iBCSCs) via radiation-induced re-expression of the stemness genes. Here we show that in irradiation (IR)-treated mice bearing syngeneic mammary tumors, IR-induced stemness correlated with increased spontaneous lung metastasis (51.7%). However, IR-induced stemness was blocked by targeting the NF-κB- stemness gene pathway with disulfiram (DSF)and Copper (Cu2+). DSF is an inhibitor of aldehyde dehydrogenase (ALDH) and an FDA-approved drug for treating alcoholism. DSF binds to Cu2+ to form DSF-Cu complexes (DSF/Cu), which act as a potent apoptosis inducer and an effective proteasome inhibitor, which, in turn, inhibits NF-κB activation. Treatment of mice with RT and DSF significantly inhibited mammary primary tumor growth (79.4%) and spontaneous lung metastasis (89.6%) compared to vehicle treated mice. This anti-tumor efficacy was associated with decreased stem cell properties (or stemness) in tumors. We expect that these results will spark clinical investigation of RT and DSF as a novel combinatorial treatment for breast cancer.

Citing Articles

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