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01-04-2015 | Original Paper

G protein-coupled estrogen receptor (GPER) mediates NSCLC progression induced by 17β-estradiol (E₂) and selective agonist G1

Authors: Changyu Liu, Yongde Liao, Sheng Fan, Hexiao Tang, Zhixiao Jiang, Bo Zhou, Jing Xiong, Sheng Zhou, Man Zou, Jianmiao Wang

Published in: Medical Oncology | Issue 4/2015

Abstract

Estrogen classically drives lung cancer development via estrogen receptor β (ERβ). However, fulvestrant, an anti-estrogen-based endocrine therapeutic treatment, shows limited effects for non-small cell lung cancer (NSCLC) in phase II clinical trials. G protein-coupled estrogen receptor (GPER), a third estrogen receptor that binds to estrogen, has been found to be activated by fulvestrant, stimulating the progression of breast, endometrial, and ovarian cancers. We here demonstrated that cytoplasm-GPER (cGPER) (80.49 %) and nucleus-GPER (53.05 %) were detected by immunohistochemical analysis in NSCLC samples. cGPER expression was related to stages IIIA–IV, lymph node metastasis, and poorly differentiated NSCLC. Selective agonist G1 and 17β-estradiol (E₂) promoted the GPER-mediated proliferation, invasion, and migration of NSCLC cells. Additionally, in vitro administration of E₂ and G1 increased the number of tumor nodules, tumor grade, and tumor index in a urethane-induced adenocarcinoma model. Importantly, the pro-tumorigenic effects of GPER induced by E₂ were significantly reduced by co-administering the GPER inhibitor G15 and the ERβ inhibitor fulvestrant, as compared to administering fulvestrant alone both in vitro and in vivo. Moreover, the phosphorylation of MAPK and Akt was involved in E₂/G1-induced GPER activation. In conclusion, our results indicated that a pro-tumor function of GPER exists that mediated E₂-/G1-dependent NSCLC progression and showed better efficiency regarding the co-targeting of GPER and ERβ, providing a rationale for further investigation of anti-estrogen clinical therapy.

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Title: G protein-coupled estrogen receptor (GPER) mediates NSCLC progression induced by 17β-estradiol (E2) and selective agonist G1
Authors: Changyu Liu
Yongde Liao
Sheng Fan
Hexiao Tang
Zhixiao Jiang
Bo Zhou
Jing Xiong
Sheng Zhou
Man Zou
Jianmiao Wang
Publication date: 01-04-2015
Publisher: Springer US
Published in: Medical Oncology / Issue 4/2015
Print ISSN: 1357-0560
Electronic ISSN: 1559-131X
DOI: https://doi.org/10.1007/s12032-015-0558-2

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