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Variations of protein kinase C (PKC) expression greatly influence the proliferation-to-differentiation transition (PDT) of intestinal epithelial cells and might have an important impact on intestinal tumorigenesis. We demonstrate here that the expression of PKC
JCS ePress
online publication date 9 Jun 2009
doi: 10.1242/jcs.036483
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jcs.036483v1
122/13/2191
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Articles by Dupasquier, S.
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Articles by Quittau-Prévostel, C.
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Short Report
A new mechanism of SOX9 action to regulate PKC
expression in the intestine epithelium
* Author for correspondence (e-mail: Corinne.Quittau-Prevostel{at}igf.cnrs.fr)
in proliferating intestinal epithelial cells is repressed both in vitro and in vivo by the SOX9 transcription factor. This repression does not require DNA binding of the SOX9 high-mobility group (HMG) domain but is mediated through a new mechanism of SOX9 action requiring the central and highly conserved region of SOXE members. Because SOX9 expression is itself upregulated by Wnt-APC signaling in intestinal epithelial cells, the present study points out this transcription factor as a molecular link between the Wnt-APC pathway and PKC
. These results provide a potential explanation for the decrease of PKC
expression in colorectal cancers with constitutive activation of the Wnt-APC pathway.
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© The Company of Biologists Ltd 2009