Sex-determining region Y-box3 (SOX3) functions as an oncogene in promoting epithelial ovarian cancer by targeting Src kinase
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- 作者:Qin Yan ; Fangyuan Wang ; Yi Miao ; Xiaomei Wu ; Mingzhu Bai ; Xiaowei Xi…
- 关键词:SOX3 ; Epithelial ovarian cancer ; Proliferation ; Migration ; Invasion ; Src
- 刊名:Tumor Biology
- 出版年:2016
- 出版时间:September 2016
- 年:2016
- 卷:37
- 期:9
- 页码:12263-12271
- 全文大小:3,416 KB
- 刊物主题:Cancer Research;
- 出版者:Springer Netherlands
- ISSN:1423-0380
- 卷排序:37
文摘
Ovarian cancer is one of the most common cancers which cause female mortality. The knowledge of ovarian cancer initiation and progression is critical to develop new therapeutic strategies to treat and prevent it. Recently, SOX3 has been reported to play a pivotal role in tumor progression. However, the clinical significance of SOX3 in human ovarian cancer remains elusive, and the identity of SOX3 in ovarian cancer initiation, progression, and the related underlying mechanism is unknown. In this study, we showed that SOX3 expression increased from benign and borderline to malignant ovarian tumors. Subsequently, we found that overexpression of SOX3 in EOC cells promoted proliferation, migration, and invasion, while restrained apoptosis and adhesion of ovarian cancer cells. In contrast, silencing of SOX3 gained the opposite results. Finally, we discovered SOX3 targeted Src kinase in EOC cells. These data imply that SOX3, acting as an oncogene in EOC, is not only a crucial factor in the carcinogenesis but also a promising therapeutic target for EOC.