There is an unmet need for better therapeutic strategies for advanced prostate cancer. Poly (ADP-ribose) polymerase-1 (PARP-1) is a chromatin-binding DNA repair enzyme overexpressed in prostate cancer. This study evaluates whether PARP-1, on account of its proximity to the cell's DNA, would be a good target for delivering high-linear energy transfer Auger radiation to induce lethal DNA damage in prostate cancer cells. We analyzed the correlation between PARP-1 expression and Gleason score in a prostate cancer tissue microarray. A radio-brominated Auger emitting inhibitor ([ 77 Br]Br-WC-DZ) targeting PARP-1 was synthesized. The ability of [ 77 Br]Br-WC-DZ to induce cytotoxicity and DNA damage was assessed in vitro. The antitumor efficacy of [ 77 Br]Br-WC-DZ was investigated in prostate cancer xenograft models. PARP-1 expression was found to be positively correlated with the Gleason score, thus making it an attractive target for Auger therapy in advanced diseases. The Auger emitter, [ 77 Br]Br-WC-DZ, induced DNA damage, G2-M cell cycle phase arrest, and cytotoxicity in PC-3 and IGR-CaP1 prostate cancer cells. A single dose of [ 77 Br]Br-WC-DZ inhibited the growth of prostate cancer xenografts and improved the survival of tumor-bearing mice. Our studies establish the fact that PARP-1 targeting Auger emitters could have therapeutic implications in advanced prostate cancer and provides a strong rationale for future clinical investigation.
Keyphrases
- prostate cancer
- dna damage
- dna repair
- radical prostatectomy
- cell cycle
- oxidative stress
- dna damage response
- energy transfer
- poor prognosis
- quantum dots
- cancer therapy
- clinical trial
- stem cells
- gene expression
- transcription factor
- drug delivery
- adipose tissue
- single cell
- mass spectrometry
- smoking cessation
- radiation induced
- replacement therapy
- long non coding rna
- circulating tumor cells
- circulating tumor