Inhibition of ERα/ERK/P62 cascades induces “autophagic switch” in the estrogen receptor-positive breast cancer cells exposed to gemcitabine

Several clinical trials revealed that estrogen receptor (ER) status had relevance to the response of mammary malignancy to chemotherapy. Autophagy has emerged as an important cellular mechanism of tumor cells in response to anticancer therapy. The aim of this study is to investigate whether gemcitab...

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Autores principales: Shen, Peng, Chen, Ming, He, Mengye, Chen, Luoquan, Song, Yinjing, Xiao, Peng, Wan, Xiaopeng, Dai, Feng, Pan, Ting, Wang, Qingqing
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2016
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5217034/
https://www.ncbi.nlm.nih.gov/pubmed/27384485
http://dx.doi.org/10.18632/oncotarget.10363
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author Shen, Peng
Chen, Ming
He, Mengye
Chen, Luoquan
Song, Yinjing
Xiao, Peng
Wan, Xiaopeng
Dai, Feng
Pan, Ting
Wang, Qingqing
author_facet Shen, Peng
Chen, Ming
He, Mengye
Chen, Luoquan
Song, Yinjing
Xiao, Peng
Wan, Xiaopeng
Dai, Feng
Pan, Ting
Wang, Qingqing
author_sort Shen, Peng
collection PubMed
description Several clinical trials revealed that estrogen receptor (ER) status had relevance to the response of mammary malignancy to chemotherapy. Autophagy has emerged as an important cellular mechanism of tumor cells in response to anticancer therapy. The aim of this study is to investigate whether gemcitabine induces autophagy, and more importantly, whether such autophagy is functional relevant to the therapeutic effects of gemcitabine in breast cancer cells in relation to the ER status. In our study, autophagy was induced both in ER(+) MCF-7 and ER(−) MDA-MB-231 cells by gemcitabine markedly, while the autophagy plays distinct roles – cytoprotective in ER(−) MDA-MB-231 and cytotoxic in ER+ MCF-7 cells. Gemcitabine treatment leads to the activation of ERα-ERK-P62 signal pathway in MCF-7 cells which may augment the autophagic degradation, thus results in the excessive activation of autophagy and irreversible autophagic cell death eventually. Inhibition of ERα-ERK-P62 cascades in MCF-7 cells by small interfering RNA or PD98059 impairs the autophagic degradation, and leads to “autophagic switch” – from cytotoxic autophagy to cytoprotection. Moreover, stable overexpression of ERα in the ER(−) BCap37 breast cancer cell line enhances the gemcitabine-induced autophagy flux and switches the autophagic cytoprotection in ER(−) BCap37 to cytotoxicity effect in ER(+) BCap37 cells. Our study firstly demonstrated that ER status influences gemcitabine efficacy via modulating the autophagy in breast cancer cells.
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spelling pubmed-52170342017-01-17 Inhibition of ERα/ERK/P62 cascades induces “autophagic switch” in the estrogen receptor-positive breast cancer cells exposed to gemcitabine Shen, Peng Chen, Ming He, Mengye Chen, Luoquan Song, Yinjing Xiao, Peng Wan, Xiaopeng Dai, Feng Pan, Ting Wang, Qingqing Oncotarget Research Paper Several clinical trials revealed that estrogen receptor (ER) status had relevance to the response of mammary malignancy to chemotherapy. Autophagy has emerged as an important cellular mechanism of tumor cells in response to anticancer therapy. The aim of this study is to investigate whether gemcitabine induces autophagy, and more importantly, whether such autophagy is functional relevant to the therapeutic effects of gemcitabine in breast cancer cells in relation to the ER status. In our study, autophagy was induced both in ER(+) MCF-7 and ER(−) MDA-MB-231 cells by gemcitabine markedly, while the autophagy plays distinct roles – cytoprotective in ER(−) MDA-MB-231 and cytotoxic in ER+ MCF-7 cells. Gemcitabine treatment leads to the activation of ERα-ERK-P62 signal pathway in MCF-7 cells which may augment the autophagic degradation, thus results in the excessive activation of autophagy and irreversible autophagic cell death eventually. Inhibition of ERα-ERK-P62 cascades in MCF-7 cells by small interfering RNA or PD98059 impairs the autophagic degradation, and leads to “autophagic switch” – from cytotoxic autophagy to cytoprotection. Moreover, stable overexpression of ERα in the ER(−) BCap37 breast cancer cell line enhances the gemcitabine-induced autophagy flux and switches the autophagic cytoprotection in ER(−) BCap37 to cytotoxicity effect in ER(+) BCap37 cells. Our study firstly demonstrated that ER status influences gemcitabine efficacy via modulating the autophagy in breast cancer cells. Impact Journals LLC 2016-07-01 /pmc/articles/PMC5217034/ /pubmed/27384485 http://dx.doi.org/10.18632/oncotarget.10363 Text en Copyright: © 2016 Shen et al. http://creativecommons.org/licenses/by/2.5/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Paper
Shen, Peng
Chen, Ming
He, Mengye
Chen, Luoquan
Song, Yinjing
Xiao, Peng
Wan, Xiaopeng
Dai, Feng
Pan, Ting
Wang, Qingqing
Inhibition of ERα/ERK/P62 cascades induces “autophagic switch” in the estrogen receptor-positive breast cancer cells exposed to gemcitabine
title Inhibition of ERα/ERK/P62 cascades induces “autophagic switch” in the estrogen receptor-positive breast cancer cells exposed to gemcitabine
title_full Inhibition of ERα/ERK/P62 cascades induces “autophagic switch” in the estrogen receptor-positive breast cancer cells exposed to gemcitabine
title_fullStr Inhibition of ERα/ERK/P62 cascades induces “autophagic switch” in the estrogen receptor-positive breast cancer cells exposed to gemcitabine
title_full_unstemmed Inhibition of ERα/ERK/P62 cascades induces “autophagic switch” in the estrogen receptor-positive breast cancer cells exposed to gemcitabine
title_short Inhibition of ERα/ERK/P62 cascades induces “autophagic switch” in the estrogen receptor-positive breast cancer cells exposed to gemcitabine
title_sort inhibition of erα/erk/p62 cascades induces “autophagic switch” in the estrogen receptor-positive breast cancer cells exposed to gemcitabine
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5217034/
https://www.ncbi.nlm.nih.gov/pubmed/27384485
http://dx.doi.org/10.18632/oncotarget.10363
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