"Transcriptional Modulation of BCRP Gene to Reverse Multidrug Resistanc" by Yuhua Zhang, Huaiping Wang et al.

ETSU Faculty Works

Title

Transcriptional Modulation of BCRP Gene to Reverse Multidrug Resistance by Toremifene in Breast Adenocarcinoma Cells

Creator(s)

Yuhua Zhang, Shandong University
Huaiping Wang, China PLA General Hospital
Lijing Wei, Shandong Provincial Hospital
Guang Li, Beijing Tiantan Hospital, Capital Medical University
Jin Yu, Beijing Tiantan Hospital, Capital Medical University
Yan Gao, Shandong Cancer Hospital
Peng Gao, Shandong University
Xiaofang Zhang, Shandong University
Fulan Wei, Shandong University
Deling Yin, East Tennessee State University
Gengyin Zhou, Shandong University

Document Type

Article

Publication Date

10-1-2010

Description

Breast cancer resistance protein (BCRP/ ABCG2), an ATP-binding cassette half transporter, confers multidrug resistance (MDR) to a series of antitumor agents such as mitoxantrone, daunorubicin, SN-38, and topotecan, and often limits the efficacy of chemotherapy. Recent studies have indicated that a putative estrogen response element (ERE) is located in the promoter region of the BCRP gene. However, whether and how BCRP is regulated transcriptionally by toremifene (TOR) remains unknown. In the present study, two plasmid vectors have been designed to express the wild-Type full-length BCRP cDNA enforced driven by its endogenous promoter containing a functional ERE and a constitutive cytomegalovirus (CMV) promoter as control, respectively, which were transfected into estrogenresponsive MCF-7 and estrogen-independent MDA-MB-231 human breast adenocarcinoma cell lines. We showed that toremifene alone significantly downregulated BCRP mRNA and protein levels in estrogen receptor a (ERa)-positiveMCF- 7 cells in a dose-dependent manner, and the inhibitory effect was partially reversed by estrone (E1). Furthermore, gel shift assays demonstrated that specific binding of ERa to the ERE in the BCRP promoter is essential for transcriptional inhibition of BCRP by toremifene. Interestingly, toremifene alone increased the cellular accumulation of mitoxantrone inBCRPtransfected cells, suggesting that TOR indeed inhibits BCRPmediated drug efflux and overcome drug resistance. To the best of our knowledge, this is the first report describing a direct effect of toremifene on BCRP. Our results thus indicate that toremifene by itself downregulates BCRP expression to reverse BCRP-mediated atypical multidrug resistance via a novel transcriptionally mechanism, which might be involved inTOR-ERcomplexes binding to theEREofBCRP promoter to repress transcription of BCRP gene.

Citation Information

Zhang, Yuhua; Wang, Huaiping; Wei, Lijing; Li, Guang; Yu, Jin; Gao, Yan; Gao, Peng; Zhang, Xiaofang; Wei, Fulan; Yin, Deling; and Zhou, Gengyin. 2010. Transcriptional Modulation of BCRP Gene to Reverse Multidrug Resistance by Toremifene in Breast Adenocarcinoma Cells. Breast Cancer Research and Treatment. Vol.123(3). 679-689. https://doi.org/10.1007/s10549-009-0660-2 PMID: 19967559 ISSN: 0167-6806

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