Feed-forward alpha particle radiotherapy ablates androgen receptor-addicted prostate cancer.
Michael R McDevittDaniel L J ThorekTakeshi HashimotoTatsuo GondoDarren R VeachSai Kiran SharmaTeja Muralidhar KalidindiDiane S AbouPhilip A WatsonBradley J BeattieOskar Vilhemsson TimmermandSven-Erik StrandJason S LewisPeter T ScardinoHoward I ScherHans G LiljaSteven M LarsonDavid UlmertPublished in: Nature communications (2018)
Human kallikrein peptidase 2 (hK2) is a prostate specific enzyme whose expression is governed by the androgen receptor (AR). AR is the central oncogenic driver of prostate cancer (PCa) and is also a key regulator of DNA repair in cancer. We report an innovative therapeutic strategy that exploits the hormone-DNA repair circuit to enable molecularly-specific alpha particle irradiation of PCa. Alpha-particle irradiation of PCa is prompted by molecularly specific-targeting and internalization of the humanized monoclonal antibody hu11B6 targeting hK2 and further accelerated by inherent DNA-repair that up-regulate hK2 (KLK2) expression in vivo. hu11B6 demonstrates exquisite targeting specificity for KLK2. A single administration of actinium-225 labeled hu11B6 eradicates disease and significantly prolongs survival in animal models. DNA damage arising from alpha particle irradiation induces AR and subsequently KLK2, generating a unique feed-forward mechanism, which increases binding of hu11B6. Imaging data in nonhuman primates support the possibility of utilizing hu11B6 in man.
Keyphrases
- dna repair
- dna damage
- prostate cancer
- monoclonal antibody
- dna damage response
- radical prostatectomy
- poor prognosis
- cancer therapy
- high glucose
- endothelial cells
- oxidative stress
- transcription factor
- early stage
- binding protein
- high resolution
- drug delivery
- papillary thyroid
- squamous cell carcinoma
- photodynamic therapy
- dna binding
- free survival
- benign prostatic hyperplasia