Author:
Sansom Owen J.,Reed Karen R.,Hayes Anthony J.,Ireland Heather,Brinkmann Hannah,Newton Ian P.,Batlle Eduard,Simon-Assmann Patricia,Clevers Hans,Nathke Inke S.,Clarke Alan R.,Winton Douglas J.
Abstract
Although Apc is well characterized as a tumor-suppressor gene in the intestine, the precise mechanism of this suppression remains to be defined. Using a novel inducible Ahcre transgenic line in conjunction with a loxP-flanked Apc allele we, show that loss of Apc acutely activates Wnt signaling through the nuclear accumulation of β-catenin. Coincidentally, it perturbs differentiation, migration, proliferation, and apoptosis, such that Apc-deficient cells maintain a “crypt progenitor-like” phenotype. Critically, for the first time we confirm a series of Wnt target molecules in an in vivo setting and also identify a series of new candidate targets within the same setting.
Publisher
Cold Spring Harbor Laboratory
Subject
Developmental Biology,Genetics
Cited by
692 articles.
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