Ernst–Otto Riecken scite author profile

Mutations in the adenomatous polyposis coli or ␤-catenin gene lead to cytosolic accumulation of ␤-catenin and, subsequently, to increased transcriptional activity of the ␤-catenin-T cell-factor/lymphoid-enhancer-factor complex. This process seems to play an essential role in the development of most colorectal carcinomas. To identify genes activated by ␤-catenin overexpression, we used colorectal cell lines for transfection with the ␤-catenin gene and searched for genes differentially expressed in the transfectants. There are four genes affected by ␤-catenin overexpression; three overexpressed genes code for two components of the AP-1 transcription complex, c-jun and fra-1, and for the urokinase-type plasminogen activator receptor (uPAR), whose transcription is activated by AP-1. The direct interaction of the ␤-catenin-T cell-factor͞lymphoid-enhancerfactor complex with the promoter region of c-jun and fra-1 was shown in a gel shift assay. The concomitant increase in ␤-catenin expression and the amount of uPAR was confirmed in primary colon carcinomas and their liver metastases at both the mRNA and the protein levels. High expression of ␤-catenin in transfectants, as well as in additionally analyzed colorectal cell lines, was associated with decreased expression of ZO-1, which is involved in epithelial polarization. Thus, accumulation of ␤-catenin indirectly affects the expression of uPAR in vitro and in vivo. Together with the other alterations, ␤-catenin accumulation may contribute to the development and progression of colon carcinoma both by dedifferentiation and through proteolytic activity.

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Altered tight junction structure contributes to the impaired epithelial barrier function in ulcerative colitis

Schmitz

et al. 1999

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Ernst–Otto Riecken

Target genes of β-catenin–T cell-factor/lymphoid-enhancer-factor signaling in human colorectal carcinomas

Altered tight junction structure contributes to the impaired epithelial barrier function in ulcerative colitis

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