The roles EpCAM plays to enhance the malignancy of gastric cancer

Author:

Zhao Xuewei1,Zhao Ruixia1,Feng Yang1,Qiu Zuchun1,Liu Niu2,Zhou Yujuan1,Bai Xue1,Zhang Danying1,Chen Lirong1,Jia Chenshuang1,Yuan Yue1,Li Xinyao1,Duan Wei3,Nie Guochao4,Hou Yingchun1

Affiliation:

1. Shaanxi Normal University

2. Beijing Normal University

3. Deakin University

4. Guangxi Key Laboratory of Agricultural Resource Chemistry and Biotechnology

Abstract

Abstract Background Gastric cancer (GC) remains a global challenge due to its high morbidity and mortality rates especially in Asia as well as poor response to treatment. As a member of the adhesion protein family and transmembrane glycoprotein, EpCAM expressed excessively in cancer cells including GC cells. The database assay showed that EpCAM is excessively expressed and easily mutated in cancers, especially in early stage of GC. Methods To explore the roles EpCAM plays in oncogenesis and progression of GC, the expression of EpCAM was deleted in GC cells with CRISPR/Cas9 method, and then the changes of cell proliferation, apoptosis, motility and motility associated microstructures in EpCAM deleted GC cells (EpCAM-/-SGC7901) were detected to evaluate the rules EpCAM played. Results The results showed that EpCAM deletion caused cell proliferation, motility and the development of motility relevant microstructures inhibited significantly, apoptotic trend and contact inhibition enhanced in EpCAM deleted GC cells. The results of western blot suggested that EpCAM modulates the expression of epithelial/endothelial mesenchymal transition (EMT) correlated genes. All results as above indicated that EpCAM plays important roles to enhance the oncogenesis, malignancy and progression as a GC enhancer. Conclusions Combining our results and published data together, the interaction of EpCAM with other proteins was also discussed and concluded in the discussion. Our results support that EpCAM can be considered as a novel target for the diagnosis and therapy of GC in future.

Publisher

Research Square Platform LLC

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