SHARPIN stabilizes estrogen receptor a and promotes breast cancer cell proliferation

Ting Zhuang, Sifan Yu, Lichen Zhang, Huijie Yang, Xin Li, Yingxiang Hou, Zhenhua Liu, Yuanyuan Shi, Weilong Wang, Na Yu, Anqi Li, Xuefeng Li, Xiumin Li, Gang Niu, Juntao Xu, Muhammad Sharif Hasni, Kun Mu, Hui Wang, Jian Zhu

Research output: Contribution to journalArticlepeer-review

Abstract

Estrogen receptor a is expressed in the majority of breast cancers and promotes estrogen-dependent cancer progression. In our study, we identified the novel E3 ubiquitin ligase SHARPIN function to facilitate ERα signaling. SHARPIN is highly expressed in human breast cancer and correlates with ERα protein level by immunohistochemistry. SHARPIN expression level correlates with poor prognosis in ERα positive breast cancer patients. SHARPIN depletion based RNA-sequence data shows that ERα signaling is a potential SHARPIN target. SHARPIN depletion significantly decreases ERα protein level, ERα target genes expression and estrogen response element activity in breast cancer cells, while SHARPIN overexpression could reverse these effects. SHARPIN depletion significantly decreases estrogen stimulated cell proliferation in breast cancer cells, which effect could be further rescued by ERα overexpression. Further mechanistic study reveals that SHARPIN mainly localizes in the cytosol and interacts with ERα both in the cytosol and the nuclear. SHARPIN regulates ERα signaling through protein stability, not through gene expression. SHARPIN stabilizes ERα protein via prohibiting ERα protein poly-ubiquitination. Further study shows that SHARPIN could facilitate the mono-ubiquitinaiton of ERα at K302/303 sites and facilitate ERE luciferase activity. Together, our findings propose a novel ERα modulation mechanism in supporting breast cancer cell growth, in which SHARPIN could be one suitable target for development of novel therapy for ERα positive breast cancer.

Original languageEnglish
Pages (from-to)77137-77151
Number of pages15
JournalOncotarget
Volume8
Issue number44
DOIs
Publication statusPublished - 2017

Subject classification (UKÄ)

  • Cancer and Oncology
  • Hematology

Free keywords

  • Breast cancer
  • ER alpha
  • Protein stability
  • SHARPIN
  • Ubiquitination

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