Preclinical Evaluation of 213Bi- and 225Ac-Labeled Low-Molecular-Weight Compounds for Radiopharmaceutical Therapy of Prostate Cancer

Sangeeta Ray Banerjee; Ala Lisok; Il Minn; Anders Josefsson; Vivek Kumar; Mary Brummet; Srikanth Boinapally; Cory Brayton; Ronnie C Mease; George Sgouros; Robert F Hobbs; Martin G Pomper

doi:10.2967/jnumed.120.256388

Preclinical Evaluation of ²¹³Bi- and ²²⁵Ac-Labeled Low-Molecular-Weight Compounds for Radiopharmaceutical Therapy of Prostate Cancer

J Nucl Med. 2021 Jul 1;62(7):980-988. doi: 10.2967/jnumed.120.256388. Epub 2020 Nov 27.

Authors

Sangeeta Ray Banerjee^{1

2}, Ala Lisok³, Il Minn³, Anders Josefsson³, Vivek Kumar³, Mary Brummet³, Srikanth Boinapally³, Cory Brayton⁴, Ronnie C Mease^{3

2}, George Sgouros³, Robert F Hobbs^{3

5}, Martin G Pomper^{3

2

5}

Affiliations

¹ Russell H. Morgan Department of Radiology and Radiological Science, Johns Hopkins University School of Medicine, Baltimore, Maryland; [email protected].
² Sidney Kimmel Comprehensive Cancer Center, Johns Hopkins University School of Medicine, Baltimore, Maryland.
³ Russell H. Morgan Department of Radiology and Radiological Science, Johns Hopkins University School of Medicine, Baltimore, Maryland.
⁴ Department of Molecular and Comparative Pathobiology, Johns Hopkins University School of Medicine, Baltimore, Maryland; and.
⁵ Department of Radiation Oncology, Johns Hopkins University School of Medicine, Baltimore, Maryland.

Abstract

Prostate-specific membrane antigen (PSMA)-targeted radiopharmaceutical therapy is a new option for patients with advanced prostate cancer refractory to other treatments. Previously, we synthesized a β-particle-emitting low-molecular-weight compound, ¹⁷⁷Lu-L1 which demonstrated reduced off-target effects in a xenograft model of prostate cancer. Here, we leveraged that scaffold to synthesize α-particle-emitting analogs of L1, ²¹³Bi-L1 and ²²⁵Ac-L1, to evaluate their safety and cell kill effect in PSMA-positive (+) xenograft models. Methods: The radiochemical synthesis, cell uptake, cell kill, and biodistribution of ²¹³Bi-L1 and ²²⁵Ac-L1 were evaluated. The efficacy of ²²⁵Ac-L1 was determined in human PSMA+ subcutaneous and micrometastatic models. Subacute toxicity at 8 wk and chronic toxicity at 1 y after administration were evaluated for ²²⁵Ac-L1. The absorbed radiation dose of ²²⁵Ac-L1 was determined using the biodistribution data and α-camera imaging. Results:²¹³Bi- and ²²⁵Ac-L1 demonstrated specific cell uptake and cell kill in PSMA+ cells. The biodistribution of ²¹³Bi-L1 and ²²⁵Ac-L1 revealed specific uptake of radioactivity within PSMA+ lesions. Treatment studies of ²²⁵Ac-L1 demonstrated activity-dependent, specific inhibition of tumor growth in the PSMA+ flank tumor model. ²²⁵Ac-L1 also showed an increased survival benefit in the micrometastatic model compared with ¹⁷⁷Lu-L1. Activity-escalated acute and chronic toxicity studies of ²²⁵Ac-L1 revealed off-target radiotoxicity, mainly in kidneys and liver. The estimated maximum tolerated activity was about 1 MBq/kg. α-Camera imaging of ²²⁵Ac-L1 revealed high renal cortical accumulation at 2 h followed by fast clearance at 24 h. Conclusion:²²⁵Ac-L1 demonstrated activity-dependent efficacy with minimal treatment-related organ radiotoxicity. ²²⁵Ac-L1 is a promising therapeutic for further clinical evaluation.

Keywords: long-term toxicity; murine; prostate carcinoma; prostate-specific membrane antigen (PSMA); α-particle.

MeSH terms

Actinium* / chemistry
Actinium* / therapeutic use
Animals
Bismuth* / chemistry
Bismuth* / therapeutic use
Cell Line, Tumor
Humans
Isotope Labeling
Male
Mice
Molecular Weight
Prostatic Neoplasms* / drug therapy
Prostatic Neoplasms* / pathology
Prostatic Neoplasms* / radiotherapy
Radioisotopes* / therapeutic use
Radiopharmaceuticals* / pharmacokinetics
Radiopharmaceuticals* / therapeutic use
Tissue Distribution

Substances

Radiopharmaceuticals
Actinium
Actinium-225
Radioisotopes
Bismuth
Bismuth-213

Abstract

MeSH terms

Substances

Grants and funding