Cell Reports (Apr 2016)

Activation of P-TEFb by Androgen Receptor-Regulated Enhancer RNAs in Castration-Resistant Prostate Cancer

  • Yu Zhao,
  • Liguo Wang,
  • Shancheng Ren,
  • Lan Wang,
  • Patrick R. Blackburn,
  • Melissa S. McNulty,
  • Xu Gao,
  • Meng Qiao,
  • Robert L. Vessella,
  • Manish Kohli,
  • Jun Zhang,
  • R. Jeffrey Karnes,
  • Donald J. Tindall,
  • Youngsoo Kim,
  • Robert MacLeod,
  • Stephen C. Ekker,
  • Tiebang Kang,
  • Yinghao Sun,
  • Haojie Huang

DOI
https://doi.org/10.1016/j.celrep.2016.03.038
Journal volume & issue
Vol. 15, no. 3
pp. 599 – 610

Abstract

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The androgen receptor (AR) is required for castration-resistant prostate cancer (CRPC) progression, but the function and disease relevance of AR-bound enhancers remain unclear. Here, we identify a group of AR-regulated enhancer RNAs (e.g., PSA eRNA) that are upregulated in CRPC cells, patient-derived xenografts (PDXs), and patient tissues. PSA eRNA binds to CYCLIN T1, activates P-TEFb, and promotes cis and trans target gene transcription by increasing serine-2 phosphorylation of RNA polymerase II (Pol II-Ser2p). We define an HIV-1 TAR RNA-like (TAR-L) motif in PSA eRNA that is required for CYCLIN T1 binding. Using TALEN-mediated gene editing we further demonstrate that this motif is essential for increased Pol II-Ser2p occupancy levels and CRPC cell growth. We have uncovered a P-TEFb activation mechanism and reveal altered eRNA expression that is related to abnormal AR function and may potentially be a therapeutic target in CRPC.