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An Autocrine Mechanism for Constitutive Wnt Pathway Activation in Human Cancer Cells

Overview
Journal Cancer Cell
Publisher Cell Press
Specialty Oncology
Date 2004 Nov 16
PMID 15542433
Citations 162
Authors
Anna Bafico
Guizhong Liu
Luba Goldin
Violaine Harris
Stuart A Aaronson
Affiliations
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Abstract

Autocrine Wnt signaling in the mouse mammary tumor virus model was the first identified mechanism of canonical pathway activation in cancer. In search of this transformation mechanism in human cancer cells, we identified breast and ovarian tumor lines with upregulation of the uncomplexed transcriptionally active form of beta-catenin without mutations afflicting downstream components. Extracellular Wnt antagonists FRP1 and DKK1 caused a dramatic downregulation of beta-catenin levels in these tumor cells associated with alteration of biological properties and increased expression of epithelial differentiation markers. Colorectal carcinoma cells with knockout of the mutant beta-catenin allele retained upregulated beta-catenin levels, which also could be inhibited by these Wnt antagonists. Together, these findings establish the involvement of autocrine Wnt signaling in human cancer cells.

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