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The rac activator Tiam1 is a Wnt-responsive gene that modifies intestinal tumor development.

Angeliki Malliri ,
Tomasz P Rygiel ,
Rob A van der Kammen ,
Ji-Ying Song ,
Rainer Engers ,
Adam F L Hurlstone ,
Hans Clevers ,
John G Collard

Abstract

Mutations in the canonical Wnt signaling pathway leading to its activation are known to cause the majority of intestinal tumors. However, few genes targeted by this pathway have been demonstrated to affect tumor development in vivo. Here we show that Tiam1, a selective Rac GTPase activator, is a Wnt-responsive gene expressed in the base of intestinal crypts and up-regulated in mouse intestinal tumors and human colon adenomas. Moreover, by comparing tumor development in APC mutant Min (multiple intestinal neoplasia) mice expressing or lacking Tiam1, we found that Tiam1 deficiency significantly reduces the formation and growth of polyps in vivo. However, invasion of malignant intestinal tumors is enhanced by a lack of Tiam1. In line with this, knock-down of Tiam1 reduced the growth potential of human colorectal cancer cells and their ability to form E-cadherin-based adhesions, a prerequisite for local invasion of tumor cells. Our data indicate a novel cross-talk between Tiam1-Rac and canonical Wnt-signaling pathways that influences intestinal tumor formation and progression.

More about this publication

The Journal of biological chemistry

Volume 281
Issue nr. 1
Pages 543-8
Publication date 06-01-2006

Full text links

Publisher website (DOI) 10.1074/jbc.M507582200
Europe PubMed Central 16249175
Pubmed 16249175

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