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Overexpression of YAP1 induces immortalization of normal human keratinocytes by blocking clonal evolution

Authors
  • D’Addario, Irene1
  • Abbruzzese, Claudia1
  • Lo Iacono, Marco2
  • Teson, Massimo3
  • Golisano, Osvaldo4
  • Barone, Virginia1, 5
  • 1 Istituto Dermopatico dell’Immacolata, IRCCS, Laboratory of Tissue Engineering and Cutaneous Physiopathology, Rome, Italy , Rome (Italy)
  • 2 University of Turin, Department of Biological and Clinical Sciences, Turin, Italy , Turin (Italy)
  • 3 Istituto Dermopatico dell’Immacolata, IRCCS, Laboratory of Molecular and Cell Biology, Rome, Italy , Rome (Italy)
  • 4 IDI Farmaceutici SPA, Pomezia, RM, Italy , Pomezia (Italy)
  • 5 University of Siena, Molecular Medicine Section, Department of Neuroscience, Via Aldo Moro, Siena, Italy , Siena (Italy)
Type
Published Article
Journal
Histochemistry and Cell Biology
Publisher
Springer-Verlag
Publication Date
Jul 31, 2010
Volume
134
Issue
3
Pages
265–276
Identifiers
DOI: 10.1007/s00418-010-0728-4
Source
Springer Nature
Keywords
License
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Abstract

YAP1 is a transcriptional co-activator able to bind several transcription factors. YAP1 was termed a candidate oncogene after it was shown to be in human chromosome 11q22 amplicon; besides the genomic amplification, several experiments indicated that it has oncogenic function. However, YAP1 was also reported to be a tumor suppressor as its gene locus is deleted in some breast cancers. To clarify the role of this protein in the physiology of rapidly renewal cells, we investigated YAP1 in human keratinocytes. Here, we show that YAP1 overexpression in primary human keratinocytes blocks clonal evolution and induces cell immortalization, but not malignant transformation. YAP1 overexpression led to an increase in cell proliferation, colony forming efficiency and holoclone percentage. Cells escaped from senescence, immortalized but still remained unable to grow in soft agar or express mesenchymal markers, suggesting that YAP1 overexpression is not sufficient to promote a complete epithelial–mesenchymal transition and tumorigenic transformation. Protein analysis showed an increase in epithelial proliferation markers and a decrease in epithelial differentiation markers. The expression of LEKTI, a late differentiation marker, dramatically dropped to undetectable levels. Taken together, these data suggest that YAP1-overexpressing keratinocytes are maintained in the proliferative compartment.

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