S6K1 inhibition enhances the apoptotic cell death of breast cancer cells in response to Bcl‑2/Bcl‑xL inhibition by the downregulation of survivin

Park,Jin‑Ah; Jin,Hyeon‑Ok; Lee,Ha‑Na; Kim,Jin‑Hee; Park,In‑Chul; Noh,Woo Chul; Chang,Yoon  Hwan; Hong,Young Jun; Kim,Keun‑Chul; Lee,Jin  Kyung

doi:10.3892/ol.2015.3369

S6K1 inhibition enhances the apoptotic cell death of breast cancer cells in response to Bcl‑2/Bcl‑xL inhibition by the downregulation of survivin

Authors:
- Jin‑Ah Park
- Hyeon‑Ok Jin
- Ha‑Na Lee
- Jin‑Hee Kim
- In‑Chul Park
- Woo Chul Noh
- Yoon Hwan Chang
- Young Jun Hong
- Keun‑Chul Kim
- Jin Kyung Lee
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Affiliations: KIRAMS Radiation Biobank, Korea Institute of Radiological and Medical Sciences, Seoul 139‑706, Republic of Korea, Division of Radiation Cancer Research, Korea Institute of Radiological and Medical Sciences, Seoul 139‑706, Republic of Korea, Department of Surgery, Korea Cancer Center Hospital, Korea Institute of Radiological and Medical Sciences, Seoul 139‑706, Republic of Korea , Department of Laboratory Medicine, Korea Cancer Center Hospital, Korea Institute of Radiological and Medical Sciences, Seoul 139‑706, Republic of Korea , Department of Biological Sciences, College of Natural Sciences, Kangwon National University, Chuncheon 200‑701, Republic of Korea
Published online on: June 11, 2015 https://doi.org/10.3892/ol.2015.3369
Pages: 829-834

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Abstract

Breast cancer cells possess a deregulated apoptotic pathway with increased expression levels of anti‑apoptotic B‑cell lymphoma‑2 (Bcl‑2) family proteins and ribosomal S6 kinase 1 (S6K1) protein activity. Therefore, combined interference of anti‑apoptotic Bcl‑2 family and S6K1 protein expression may be a reasonable therapeutic strategy for the treatment of patients with breast cancer. In the present study, it was identified that the administration of a combination of ABT263 [navitoclax; a Bcl‑2/Bcl‑extra large (Bcl‑xL) inhibitor] and PF4708671 (an S6K1 inhibitor) markedly increased apoptotic cell death in the BT474 breast cancer cells compared with the administration of either agent alone. Furthermore, the downregulation of Bcl‑2/Bcl‑xL and S6K1 with small interfering RNA induced a significant increase in cell death compared with RNA interference of either agent alone. Notably, combination treatment with ABT263 and PF4708671 decreased the expression level of survivin protein, with this ectopic expression of survivin attenuating cell death. Thus, the present study determined that the combined inhibition of Bcl‑2/Bcl‑xL and S6K1 may be a good strategy for treating patients with breast cancer.

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