Axin facilitates Smad3 activation in the transforming growth factor β signaling pathway

Axin acts as a negative regulator in Wnt signaling through interaction with various molecules involved in this pathway, including beta -catenin, adenomatous polyposis coli, and glycogen synthase kinase 3 beta. We show here that Axin also regulates the effects of Smad3 on the transforming growth factor beta (TGF-beta) signaling pathway. In the absence of activated TGF-beta receptors. Axin physically interacted with Smad3 through its C-terminal region located between the beta -catenin binding site and Dishevelled-homologous domain. An Axin homologue, Axil (also called conductin), also interacted with Smad3. In the absence of ligand stimulation, Axin was colocalized with Smad3 in the cytoplasm in who. Upon receptor activation, Smad3 mas strongly phosphorylated by TGF-beta type I receptor (T betaR-I) in the presence of Axin, and dissociated from T betaR-I and Axin. Moreover, the transcriptional activity of TGF-beta was enhanced by Axin and repressed by an Axin mutant which is able to bind to Smad3. Axin may thus function as an adapter of Smad3, facilitating its activation by TGF-beta receptors for efficient TGF-beta signaling.