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The tumor suppressor functions of p27(kip1) include control of the mesenchymal/amoeboid transition

Authors :
Alfonso Colombatti
Peter Friedl
Stefania Berton
Andrea Vecchione
Gustavo Baldassarre
Vincenzo Canzonieri
Katarina Wolf
Francesca Lovat
Barbara Belletti
Berton, S
Belletti, B
Wolf, K
Canzonieri, V
Lovat, F
Vecchione, A
Colombatti, A
Friedl, P
Baldassarre, G
Source :
Molecular and Cellular Biology, 29, 5031-45, Molecular and Cellular Biology, 29, 18, pp. 5031-45
Publication Year :
2009

Abstract

Contains fulltext : 81143.pdf (Publisher’s version ) (Open Access) In many human cancers, p27 downregulation correlates with a worse prognosis, suggesting that p27 levels could represent an important determinant in cell transformation and cancer development. Using a mouse model system based on v-src-induced transformation, we show here that p27 absence is always linked to a more aggressive phenotype. When cultured in three-dimensional contexts, v-src-transformed p27-null fibroblasts undergo a morphological switch from an elongated to a rounded cell shape, accompanied by amoeboid-like morphology and motility. Importantly, the acquisition of the amoeboid motility is associated with a greater ability to move and colonize distant sites in vivo. The reintroduction of different p27 mutants in v-src-transformed p27-null cells demonstrates that the control of cell proliferation and motility represents two distinct functions of p27, both necessary for it to fully act as a tumor suppressor. Thus, we highlight here a new p27 function in driving cell plasticity that is associated with its C-terminal portion and does not depend on the control of cyclin-dependent kinase activity.

Details

ISSN :
02707306
Database :
OpenAIRE
Journal :
Molecular and Cellular Biology, 29, 5031-45, Molecular and Cellular Biology, 29, 18, pp. 5031-45
Accession number :
edsair.doi.dedup.....6e1e16ecefc337fb8dab058c2c600e38
Full Text :
https://doi.org/10.1128/MCB.00144-09