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

Overview

abstract

Hyperactivation 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.

authors

Castillo-Martin, Mireia

Nowak, Dawid
Naguib, Adam
Grace, Danielle M
Murn, Jernej
Navin, Nick
Atwal, Gurinder S
Sander, Chris
Gerald, William L
Cordon-Cardo, Carlos
Newton, Alexandra C
Carver, Brett
Trotman, Lloyd C

publication date

August 16, 2011

published in

Cancer cell Journal

Research

keywords

Mutation
Nuclear Proteins
PTEN Phosphohydrolase
Phosphoprotein Phosphatases
Prostatic Neoplasms

Identity

PubMed Central ID

PMC3176728

Scopus Document Identifier

80051579092

Digital Object Identifier (DOI)

10.1016/j.ccr.2011.07.013

PubMed ID

21840483

Additional Document Info

has global citation frequency

138

volume

20

issue

2

VIVO Weill Cornell Medical College

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

Overview

abstract

authors

publication date

published in

Research

keywords

Identity

PubMed Central ID

Scopus Document Identifier

Digital Object Identifier (DOI)

PubMed ID

Additional Document Info

has global citation frequency

volume

issue