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Publication : Caveolin-1 is required for TGF-β-induced transactivation of the EGF receptor pathway in hepatocytes through the activation of the metalloprotease TACE/ADAM17.

First Author  Moreno-Càceres J Year  2014
Journal  Cell Death Dis Volume  5
Pages  e1326 PubMed ID  25032849
Mgi Jnum  J:318294 Mgi Id  MGI:6859103
Doi  10.1038/cddis.2014.294 Citation  Moreno-Caceres J, et al. (2014) Caveolin-1 is required for TGF-beta-induced transactivation of the EGF receptor pathway in hepatocytes through the activation of the metalloprotease TACE/ADAM17. Cell Death Dis 5:e1326
abstractText  Transforming growth factor-beta (TGF-beta) plays a dual role in hepatocytes, inducing both pro- and anti-apoptotic responses, whose balance decides cell fate. Survival signals are mediated by the epidermal growth factor receptor (EGFR) pathway, which is activated by TGF-beta in these cells. Caveolin-1 (Cav1) is a structural protein of caveolae linked to TGF-beta receptors trafficking and signaling. Previous results have indicated that in hepatocytes, Cav1 is required for TGF-beta-induced anti-apoptotic signals, but the molecular mechanism is not fully understood yet. In this work, we show that immortalized Cav1(-/-) hepatocytes were more sensitive to the pro-apoptotic effects induced by TGF-beta, showing a higher activation of caspase-3, higher decrease in cell viability and prolonged increase through time of intracellular reactive oxygen species (ROS). These results were coincident with attenuation of TGF-beta-induced survival signals in Cav1(-/-) hepatocytes, such as AKT and ERK1/2 phosphorylation and NFkappa-B activation. Transactivation of the EGFR pathway by TGF-beta was impaired in Cav1(-/-) hepatocytes, which correlated with lack of activation of TACE/ADAM17, the metalloprotease responsible for the shedding of EGFR ligands. Reconstitution of Cav1 in Cav1(-/-) hepatocytes rescued wild-type phenotype features, both in terms of EGFR transactivation and TACE/ADAM17 activation. TACE/ADAM17 was localized in detergent-resistant membrane (DRM) fractions in Cav1(+/+) cells, which was not the case in Cav1(-/-) cells. Disorganization of lipid rafts after treatment with cholesterol-binding agents caused loss of TACE/ADAM17 activation after TGF-beta treatment. In conclusion, in hepatocytes, Cav1 is required for TGF-beta-mediated activation of the metalloprotease TACE/ADAM17 that is responsible for shedding of EGFR ligands and activation of the EGFR pathway, which counteracts the TGF-beta pro-apoptotic effects. Therefore, Cav1 contributes to the pro-tumorigenic effects of TGF-beta in liver cancer cells.
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