E-cadherin-dependent transcriptional control of apolipoprotein A-IV gene expression in intestinal epithelial cells: A role for the hepatic nuclear factor 4

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Abstract

Cell-matrix and cell-cell adhesion play a central role in the control of cell proliferation, differentiation, and gene expression. Integrins and E-cadherin are the key components involved in these processes in epithelial cells. We recently showed that integrin-dependent adhesion to the extracellular matrix reinforces the formation of E-cadherin-actin complexes inducing the polarization of Caco-2 enterocytes and increases the expression of a marker of enterocyte differentiation, the apolipoprotein A-IV (apoA-IV) gene. By impairing or enhancing E-cadherin-dependent cell adhesion, we demonstrate in the present study its involvement in the transcriptional activation of the apoA-IV gene in Caco-2 cells. This control requires the regulatory sequence that we have previously identified as necessary and sufficient to drive and restrict apoA-IV gene expression in enterocytes in vivo. Furthermore, using chimeric E-cadherin-Fc homophilic ligand-coated surfaces, we show that a direct activation of E-cadherin triggers the transcriptional activation of the apoA-IV promoter. Finally, E-cadherin-dependent cell-cell adhesion controls the nuclear abundance of the transcription factor hepatic nuclear factor 4α, which is involved in the enterocyte-specific expression of apoA-IV gene. Altogether, our results suggest that E-cadherin controls enterocyte-specific expression of genes, such as the apoA-IV gene, through the control of hepatic nuclear factor 4α nuclear abundance. © 2006 by The American Society for Biochemistry and Molecular Biology, Inc.

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APA

Peignon, G., Thenet, S., Schreider, C., Fouquet, S., Ribeiro, A., Dussaulx, E., … Le Beyec, J. (2006). E-cadherin-dependent transcriptional control of apolipoprotein A-IV gene expression in intestinal epithelial cells: A role for the hepatic nuclear factor 4. Journal of Biological Chemistry, 281(6), 3560–3568. https://doi.org/10.1074/jbc.M506360200

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