| Literature DB >> 26235627 |
Shusuke Akamatsu1, Alexander W Wyatt1, Dong Lin2, Summer Lysakowski1, Fan Zhang1, Soojin Kim1, Charan Tse1, Kendric Wang1, Fan Mo1, Anne Haegert1, Sonal Brahmbhatt1, Robert Bell1, Hans Adomat1, Yoshihisa Kawai1, Hui Xue3, Xin Dong3, Ladan Fazli1, Harrison Tsai4, Tamara L Lotan4, Myriam Kossai5, Juan Miguel Mosquera5, Mark A Rubin5, Himisha Beltran6, Amina Zoubeidi1, Yuzhuo Wang2, Martin E Gleave7, Colin C Collins8.
Abstract
More potent targeting of the androgen receptor (AR) in advanced prostate cancer is driving an increased incidence of neuroendocrine prostate cancer (NEPC), an aggressive and treatment-resistant AR-negative variant. Its molecular pathogenesis remains poorly understood but appears to require TP53 and RB1 aberration. We modeled the development of NEPC from conventional prostatic adenocarcinoma using a patient-derived xenograft and found that the placental gene PEG10 is de-repressed during the adaptive response to AR interference and subsequently highly upregulated in clinical NEPC. We found that the AR and the E2F/RB pathway dynamically regulate distinct post-transcriptional and post-translational isoforms of PEG10 at distinct stages of NEPC development. In vitro, PEG10 promoted cell-cycle progression from G0/G1 in the context of TP53 loss and regulated Snail expression via TGF-β signaling to promote invasion. Taken together, these findings show the mechanistic relevance of RB1 and TP53 loss in NEPC and suggest PEG10 as a NEPC-specific target.Entities:
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Year: 2015 PMID: 26235627 DOI: 10.1016/j.celrep.2015.07.012
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423