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Identification of PHLPP1 as a tumor suppressor reveals the role of feedback activation in PTEN-mutant prostate cancer progression

Authors :
Martha E. Zeeman
Nikolaus Schultz
Adam Naguib
Jernej Murn
Chris Sander
William L. Gerald
Gurinder S. Atwal
Nicholas Navin
Barry S. Taylor
Carlos Cordon-Cardo
Lloyd C. Trotman
Brett S. Carver
Dawid G. Nowak
Alexandra C. Newton
Audrey K. O’Neill
Mireia Castillo-Martin
Christopher P. Pratt
Danielle M. Grace
Muhan Chen
Source :
Cancer cell. 20(2)
Publication Year :
2011

Abstract

SummaryHyperactivation of the PI 3-kinase/AKT pathway is a driving force of many cancers. Here we identify the AKT-inactivating phosphatase PHLPP1 as a prostate tumor suppressor. We show that Phlpp1-loss causes neoplasia and, on partial Pten-loss, carcinoma in mouse prostate. This genetic setting initially triggers a growth suppressive response via p53 and the Phlpp2 ortholog, and reveals spontaneous Trp53 inactivation as a condition for full-blown disease. Surprisingly, the codeletion of PTEN and PHLPP1 in patient samples is highly restricted to metastatic disease and tightly correlated to deletion of TP53 and PHLPP2. These data establish a conceptual framework for progression of PTEN mutant prostate cancer to life-threatening disease.

Details

ISSN :
18783686
Volume :
20
Issue :
2
Database :
OpenAIRE
Journal :
Cancer cell
Accession number :
edsair.doi.dedup.....c922e1556c3857af7d9a493fb234e124