Author:
Bidkar Anil P.,Wang Sinan,Bobba Kondapa Naidu,Chan Emily,Bidlingmaier Scott,Egusa Emily A.,Peter Robin,Ali Umama,Meher Niranjan,Wadhwa Anju,Dhrona Suchi,Beckford-Vera Denis,Su Yang,Tang Ryan,Zhang Li,He Jiang,Wilson David M.,Aggarwal Rahul,VanBrocklin Henry F.,Seo Youngho,Chou Jonathan,Liu Bin,Flavell Robert R.
Abstract
AbstractRadiopharmaceutical therapy is changing the standard of care in prostate cancer (PCa) and other malignancies. We previously reported high CD46 expression in PCa and developed an antibody-drug conjugate and immunoPET agent based on the YS5 antibody, which targets a tumor-selective CD46 epitope. Here, we present the preparation, preclinical efficacy, and toxicity evaluation of [225Ac]DOTA-YS5, a radioimmunotherapy agent based on the YS5 antibody. Our radiolabeled antibody retains binding efficacy and shows a high tumor to background ratio in PCa xenografts. Furthermore, we show that radiolabeled antibody was able to suppress the growth of cell-derived and patient-derived xenografts, including PSMA-positive and deficient models. Nephrotoxicity, not seen at low radioactive doses, is evident at higher radioactivity dose levels, likely due to redistribution of daughter isotope213Bi. Overall, this preclinical study confirms that [225Ac]DOTA-YS5 is a highly effective treatment and suggests feasibility for clinical translation of CD46 targeted radioligand therapy in PCa.
Publisher
Cold Spring Harbor Laboratory