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C-terminus of MUC16 interacts with β-catenin to activate Wnt signaling pathway, tumorigenesis and metastasis
Liu Qi,Yang Yun,Ma Huanhuan,Li Xiaotong #,Li Qinxi *
State Key Laboratory for Cellular Stress Biology, School of Life Sciences, Xiamen University, Fujian 361102, China
*Correspondence author
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Funding: none
Opened online: 2 June 2016
Accepted by: none
Citation: Liu Qi,Yang Yun,Ma Huanhuan.C-terminus of MUC16 interacts with β-catenin to activate Wnt signaling pathway, tumorigenesis and metastasis[OL]. [ 2 June 2016] http://en.paper.edu.cn/en_releasepaper/content/4692324
 
 
MUC16/CA125 has been identified as a prominent cancer biomarker, especially for epithelial ovarian cancers, in clinical test for over three decades. Due to its huge mass, limited knowledge of MUC16 was acquired previously. By utilizing a well characterized self-made MUC16 monoclonal antibody, we identified the endogenous interaction between a C-terminal fragment of MUC16 (MUC16C) and β-catenin for the first time, and further elucidated that trans-activation domain of β-catenin is required for this interaction. Such interaction could activate the Wnt/β-catenin signaling pathway by facilitating cytosol-nucleus transportation of β-catenin, consequently induce cell proliferation and migration, eventually lead to tumorigenesis and metastasis in nude mice. Consistently, knockdown of MUC16 significantly weakened the capabilities of cells for proliferation and migration. Based on our discovery, we suggest that MUC16 appears as an attractive target for the development of effective anticancer drugs.
Keywords:MUC16; β-catenin; Wnt signaling; tumor cell
 
 
 

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