| Literature DB >> 26180042 |
Kideok Jin1, Sunju Park1, Wei Wen Teo1, Preethi Korangath1, Sean Soonweng Cho1, Takahiro Yoshida1, Balázs Győrffy2, Chirayu Pankaj Goswami3, Harikrishna Nakshatri3, Leigh-Ann Cruz1, Weiqiang Zhou4, Hongkai Ji4, Ying Su5, Muhammad Ekram5, Zhengsheng Wu6, Tao Zhu6, Kornelia Polyak5, Saraswati Sukumar7.
Abstract
UNLABELLED: Why breast cancers become resistant to tamoxifen despite continued expression of the estrogen receptor-α (ERα) and what factors are responsible for high HER2 expression in these tumors remains an enigma. HOXB7 chromatin immunoprecipitation analysis followed by validation showed that HOXB7 physically interacts with ERα, and that the HOXB7-ERα complex enhances transcription of many ERα target genes, including HER2. Investigating strategies for controlling HOXB7, our studies revealed that MYC, stabilized via phosphorylation mediated by EGFR-HER2 signaling, inhibits transcription of miR-196a, a HOXB7 repressor. This leads to increased expression of HOXB7, ER target genes, and HER2. Repressing MYC using small-molecule inhibitors reverses these events and causes regression of breast cancer xenografts. The MYC-HOXB7-HER2 signaling pathway is eminently targetable in endocrine-resistant breast cancer. SIGNIFICANCE: HOXB7 acts as an ERα cofactor regulating a myriad of ER target genes, including HER2, in tamoxifen-resistant breast cancer. HOXB7 expression is controlled by MYC via transcriptional regulation of the HOXB7 repressor miR-196a; consequently, antagonists of MYC cause reversal of selective ER modulator resistance both in vitro and in vivo. ©2015 American Association for Cancer Research.Entities:
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Year: 2015 PMID: 26180042 PMCID: PMC4560624 DOI: 10.1158/2159-8290.CD-15-0090
Source DB: PubMed Journal: Cancer Discov ISSN: 2159-8274 Impact factor: 39.397