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Treatment of prostate cancer with CD46 targeted 225Ac alpha particle radioimmunotherapy
- 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;
- Dasari, Chandrashekhar;
- 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
- et al.
Published Web Location
https://doi.org/10.1158/1078-0432.ccr-22-3291Abstract
Purpose
Radiopharmaceutical therapy is changing the standard of care in prostate cancer and other malignancies. We previously reported high CD46 expression in prostate cancer 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.Experimental design
[225Ac]DOTA-YS5 was developed, and its therapeutic efficiency was tested on cell-derived (22Rv1, DU145), and patient-derived (LTL-545, LTL484) prostate cancer xenograft models. Biodistribution studies were carried out on 22Rv1 tumor xenograft models to confirm the targeting efficacy. Toxicity analysis of the [225Ac]DOTA-YS5 was carried out on nu/nu mice to study short-term (acute) and long-term (chronic) toxicity.Results
Biodistribution study shows that [225Ac]DOTA-YS5 agent delivers high levels of radiation to the tumor tissue (11.64% ± 1.37%ID/g, 28.58% ± 10.88%ID/g, 29.35% ± 7.76%ID/g, and 31.78% ± 5.89%ID/g at 24, 96, 168, and 408 hours, respectively), compared with the healthy organs. [225Ac]DOTA-YS5 suppressed tumor size and prolonged survival in cell line-derived and patient-derived xenograft models. Toxicity analysis revealed that the 0.5 μCi activity levels showed toxicity to the kidneys, likely due to redistribution of daughter isotope 213Bi.Conclusions
[225Ac]DOTA-YS5 suppressed the growth of cell-derived and patient-derived xenografts, including prostate-specific membrane antigen-positive and prostate-specific membrane antigen-deficient models. 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 prostate cancer.Many UC-authored scholarly publications are freely available on this site because of the UC's open access policies. Let us know how this access is important for you.
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