1. Academic Validation
  2. Ack1-mediated androgen receptor phosphorylation modulates radiation resistance in castration-resistant prostate cancer

Ack1-mediated androgen receptor phosphorylation modulates radiation resistance in castration-resistant prostate cancer

  • J Biol Chem. 2012 Jun 22;287(26):22112-22. doi: 10.1074/jbc.M112.357384.
Kiran Mahajan 1 Domenico Coppola Bhupendra Rawal Y Ann Chen Harshani R Lawrence Robert W Engelman Nicholas J Lawrence Nupam P Mahajan
Affiliations

Affiliation

  • 1 Department of Drug Discovery, Moffitt Cancer Center, Tampa, Florida 33612, USA.
Abstract

Androgen deprivation therapy has been the standard of care in prostate Cancer due to its effectiveness in initial stages. However, the disease recurs, and this recurrent Cancer is referred to as castration-resistant prostate Cancer (CRPC). Radiotherapy is the treatment of choice; however, in addition to androgen independence, CRPC is often resistant to radiotherapy, making radioresistant CRPC an incurable disease. The molecular mechanisms by which CRPC cells acquire radioresistance are unclear. Androgen Receptor (AR)-tyrosine 267 phosphorylation by Ack1 tyrosine kinase (also known as TNK2) has emerged as an important mechanism of CRPC growth. Here, we demonstrate that pTyr(267)-AR is recruited to the ATM (ataxia telangiectasia mutated) enhancer in an Ack1-dependent manner to up-regulate ATM expression. Mice engineered to express activated Ack1 exhibited a significant increase in pTyr(267)-AR and ATM levels. Furthermore, primary human CRPCs with up-regulated activated Ack1 and pTyr(267)-AR also exhibited significant increase in ATM expression. The Ack1 Inhibitor AIM-100 not only inhibited Ack1 activity but also was able to suppress AR Tyr(267) phosphorylation and its recruitment to the ATM enhancer. Notably, AIM-100 suppressed Ack1 mediated ATM expression and mitigated the growth of radioresistant CRPC tumors. Thus, our study uncovers a previously unknown mechanism of radioresistance in CRPC, which can be therapeutically reversed by a new synergistic approach that includes radiotherapy along with the suppression of Ack1/AR/ATM signaling by the Ack1 Inhibitor, AIM-100.

Figures
Products
  • Cat. No.
    Product Name
    Description
    Target
    Research Area
  • HY-15290
    99.95%, Ack1 Inhibitor