Oncotarget

Research Papers:

Embigin, regulated by HOXC8, plays a suppressive role in breast tumorigenesis

Fengmei Chao, Jun Zhang, Yang Zhang, Houli Liu, Chenchen Yang, Juan Wang, Yanjun Guo, Xiaohong Wen, Kaiye Zhang, Bei Huang, Daihai Liu and Yong Li _

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Oncotarget. 2015; 6:23496-23509. https://doi.org/10.18632/oncotarget.4360

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Abstract

Fengmei Chao1, Jun Zhang2,3, Yang Zhang1, Houli Liu1, Chenchen Yang1, Juan Wang2, Yanjun Guo2, Xiaohong Wen2, Kaiye Zhang2, Bei Huang1, Daihai Liu1 and Yong Li1

1 Anhui University, School of Life Sciences, Center for Stem Cell and Translational Medicine, Hefei, Anhui Province, P. R. China

2 Anhui University, School of Life Sciences, Hefei, Anhui Province, P. R. China

3 The Key Laboratory of Developmental Genes and Human Disease, Ministry of Education, Institute of Life Science, Southeast University, Nanjing, P. R. China

Correspondence to:

Yong Li, email:

Keywords: EMB, transcription, HOXC8, breast cancer, tumorigenesis

Received: February 05, 2015 Accepted: May 30, 2015 Published: June 08, 2015

Abstract

The transmembrane glycoprotein embigin (EMB) belongs to the immunoglobulin superfamily (IgSF) and a number of IgSF members have been identified as biomarkers for cancer progression. In this study, we show that embigin is transcriptionally regulated by Homeobox C8 (HOXC8) in breast cancer cells and embigin expression suppresses breast tumorigenesis. With aid of Western blot, luciferase reporter gene assay and chromatin immunoprecipitation, we reveal that HOXC8 binds to the EMB promoter at the region of nucleotides −2303 to −2315 and acts as a transcription inhibitor to suppress embigin expression. Depletion of embigin leads to increase in proliferation, anchorage-independent growth and migration of breast cancer cells, and the inhibitory effects mediated by HOXC8 knockdown on breast tumorigenesis can be largely rescued by depletion of embigin expression in breast cancer cells, suggesting that HOXC8 regulates breast tumorigenesis, at least partly, through regulating embigin expression. Moreover, we show that loss of embigin promotes proliferation, anchorage-independent growth, and migration ability of normal mammary epithelial MCF10A cells. The analyses of publically available human breast tumor microarray gene expression database show that low embigin levels correlate with short survival of breast tumor patients, particularly with basal-like tumor patients, and embigin expression is low specifically in patients with basal-like, ER-/HER2- tumors. Taken together, our study demonstrates that low/loss of embigin plays an important role in the progression of breast tumors.


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