Cancers (Aug 2021)

Antithetic hTERT Regulation by Androgens in Prostate Cancer Cells: hTERT Inhibition Is Mediated by the ING1 and ING2 Tumor Suppressors

  • Sophie Bartsch,
  • Kimia Mirzakhani,
  • Laura Neubert,
  • Alexander Stenzel,
  • Marzieh Ehsani,
  • Mohsen Esmaeili,
  • Thanakorn Pungsrinont,
  • Merve Kacal,
  • Seyed Mohammad Mahdi Rasa,
  • Julia Kallenbach,
  • Divya Damodaran,
  • Federico Ribaudo,
  • Marc-Oliver Grimm,
  • Francesco Neri,
  • Aria Baniahmad

DOI
https://doi.org/10.3390/cancers13164025
Journal volume & issue
Vol. 13, no. 16
p. 4025

Abstract

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The human telomerase is a key factor during tumorigenesis in prostate cancer (PCa). The androgen receptor (AR) is a key drug target controlling PCa growth and regulates hTERT expression, but is described to either inhibit or to activate. Here, we reveal that androgens repress and activate hTERT expression in a concentration-dependent manner. Physiological low androgen levels activate, while, notably, supraphysiological androgen levels (SAL), used in bipolar androgen therapy (BAT), repress hTERT expression. We confirmed the SAL-mediated gene repression of hTERT in PCa cell lines, native human PCa samples derived from patients treated ex vivo, as well as in cancer spheroids derived from androgen-dependent or castration resistant PCa (CRPC) cells. Interestingly, chromatin immuno-precipitation (ChIP) combined with functional assays revealed a positive (pARE) and a negative androgen response element (nARE). The nARE was narrowed down to 63 bp in the hTERT core promoter region. AR and tumor suppressors, inhibitor of growth 1 and 2 (ING1 and ING2, respectively), are androgen-dependently recruited. Mechanistically, knockdown indicates that ING1 and ING2 mediate AR-regulated transrepression. Thus, our data suggest an oppositional, biphasic function of AR to control the hTERT expression, while the inhibition of hTERT by androgens is mediated by the AR co-repressors ING1 and ING2.

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