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Androgen deprivation–mediated activation of AKT is enhanced in prostate cancer with TMPRSS2:ERG fusion

by Russo, Joshua W , Yuan, Xin , Ye, Huihui , Ma, Fen , Karzai, Fatima , Voznesensky, Olga , Xie, Fang , Calagua, Carla , Ersoy-Fazlioglu, Betul , Chen, Sen , Arai, Seiji , Ball, Steven P , Einstein, David J , Ku, Anson T , Taplin, Mary-Ellen , Poluben, Larysa , Cai, Changmeng , Awad, Seifeldin , Toker, Alex , Cecchi, Luigi , Sowalsky, Adam G

in Adenocarcinoma / AKT protein / Androgen receptors / Androgens / Cancer / Clinical trials / Combination therapy / Down-regulation / ERG gene / Gene expression / Gene fusion / Kinases / Phosphatase / Phosphorylation / Prostate / Prostate cancer / Prostatectomy / Proteins / PTEN protein / Tumors

2025

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Androgen deprivation–mediated activation of AKT is enhanced in prostate cancer with TMPRSS2:ERG fusion

2025

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Androgen deprivation–mediated activation of AKT is enhanced in prostate cancer with TMPRSS2:ERG fusion

2025

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Journal Article

Androgen deprivation–mediated activation of AKT is enhanced in prostate cancer with TMPRSS2:ERG fusion

Russo, Joshua W,

Yuan, Xin,

Ye, Huihui,

Ma, Fen,

Karzai, Fatima,

Voznesensky, Olga,

Xie, Fang,

Calagua, Carla,

Ersoy-Fazlioglu, Betul,

Chen, Sen,

Arai, Seiji,

Ball, Steven P,

Einstein, David J,

Ku, Anson T,

Taplin, Mary-Ellen,

Poluben, Larysa,

Cai, Changmeng,

Awad, Seifeldin,

Toker, Alex,

Cecchi, Luigi,

Sowalsky, Adam G

2025

Overview

TMPRSS2:ERG gene fusion (T:E fusion) in prostate adenocarcinoma (PCa) puts ERG under androgen receptor-regulated (AR-regulated) TMPRSS2 expression. T:E fusion is associated with PTEN loss and is highly associated with decreased INPP4B expression, which together may compensate for ERG-mediated suppression of AKT signaling. We confirmed in PCa cells and a mouse PCa model that ERG suppresses IRS2 and AKT activation. In contrast, ERG downregulation did not increase INPP4B, suggesting its decrease is indirect and reflects selective pressure to suppress INPP4B function. Notably, INPP4B expression was decreased in PTEN-intact and PTEN-deficient T:E fusion tumors, suggesting selection for a nonredundant function. As ERG in T:E fusion tumors is AR regulated, we further assessed whether AR inhibition increases AKT activity in T:E fusion tumors. A T:E fusion-positive PDX had increased AKT activity in vivo and response to AKT inhibition in vitro after androgen deprivation. Moreover, two clinical trials of neoadjuvant AR inhibition prior to radical prostatectomy showed greater increases in AKT activation in the T:E fusion-positive versus -negative tumors. These findings indicate that AKT activation may mitigate the efficacy of AR-targeted therapy in T:E fusion PCa and that these patients may most benefit from combination therapy targeting AR and AKT.

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Publisher

American Society for Clinical Investigation

Subject

/ Cancer

/ Combination therapy