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Ectopic Expression of Oct-4 Blocks Progenitor-cell Differentiation and Causes Dysplasia in Epithelial Tissues

Overview
Journal Cell
Publisher Cell Press
Specialty Cell Biology
Date 2005 May 11
PMID 15882627
Citations 423
Authors
Konrad Hochedlinger
Yasuhiro Yamada
Caroline Beard
Rudolf Jaenisch
Affiliations
Soon will be listed here.
Abstract

The POU-domain transcription factor Oct-4 is normally expressed in pluripotent cells of the mammalian embryo. In addition, germ-cell tumors and a few somatic tumors show detectable expression of Oct-4. While Oct-4's role during preimplantation development is to maintain embryonic cells in a pluripotent state, little is known about its potential oncogenic properties. Here we investigate the effect of ectopic Oct-4 expression on somatic tissues of adult mice using a doxycycline-dependent expression system. Activation of Oct-4 results in dysplastic growths in epithelial tissues that are dependent on continuous Oct-4 expression. Dysplastic lesions show an expansion of progenitor cells and increased beta-catenin transcriptional activity. In the intestine, Oct-4 expression causes dysplasia by inhibiting cellular differentiation in a manner similar to that in embryonic cells. These data show that certain adult progenitors remain competent to interpret key embryonic signals and support the notion that progenitor cells are a driving force in tumorigenesis.

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