A High Separation Factor for <sup>165</sup>Er from Ho for Targeted Radionuclide Therapy
oleh: Isidro Da Silva, Taylor R. Johnson, Jason C. Mixdorf, Eduardo Aluicio-Sarduy, Todd E. Barnhart, R. Jerome Nickles, Jonathan W. Engle, Paul A. Ellison
| Format: | Article |
|---|---|
| Diterbitkan: | MDPI AG 2021-12-01 |
Deskripsi
<b>Background:</b> Radionuclides emitting Auger electrons (AEs) with low (0.02–50 keV) energy, short (0.0007–40 µm) range, and high (1–10 keV/µm) linear energy transfer may have an important role in the targeted radionuclide therapy of metastatic and disseminated disease. Erbium-165 is a pure AE-emitting radionuclide that is chemically matched to clinical therapeutic radionuclide <sup>177</sup>Lu, making it a useful tool for fundamental studies on the biological effects of AEs. This work develops new biomedical cyclotron irradiation and radiochemical isolation methods to produce <sup>165</sup>Er suitable for targeted radionuclide therapeutic studies and characterizes a new such agent targeting prostate-specific membrane antigen. <b>Methods:</b> Biomedical cyclotrons proton-irradiated spot-welded Ho<sub>(m)</sub> targets to produce <sup>165</sup>Er, which was isolated via cation exchange chromatography (AG 50W-X8, 200–400 mesh, 20 mL) using alpha-hydroxyisobutyrate (70 mM, pH 4.7) followed by LN2 (20–50 µm, 1.3 mL) and bDGA (50–100 µm, 0.2 mL) extraction chromatography. The purified <sup>165</sup>Er was radiolabeled with standard radiometal chelators and used to produce and characterize a new AE-emitting radiopharmaceutical, [<sup>165</sup>Er]PSMA-617. <b>Results:</b> Irradiation of 80–180 mg <sup>nat</sup>Ho targets with 40 µA of 11–12.5 MeV protons produced <sup>165</sup>Er at 20–30 MBq·µA<sup>−1</sup>·h<sup>−1</sup>. The 4.9 ± 0.7 h radiochemical isolation yielded <sup>165</sup>Er in 0.01 M HCl (400 µL) with decay-corrected (DC) yield of 64 ± 2% and a Ho/<sup>165</sup>Er separation factor of (2.8 ± 1.1) · 10<sup>5</sup>. Radiolabeling experiments synthesized [<sup>165</sup>Er]PSMA-617 at DC molar activities of 37–130 GBq·µmol<sup>−1</sup>. <b>Conclusions:</b> A 2 h biomedical cyclotron irradiation and 5 h radiochemical separation produced GBq-scale <sup>165</sup>Er suitable for producing radiopharmaceuticals at molar activities satisfactory for investigations of targeted radionuclide therapeutics. This will enable fundamental radiation biology experiments of pure AE-emitting therapeutic radiopharmaceuticals such as [<sup>165</sup>Er]PSMA-617, which will be used to understand the impact of AEs in PSMA-targeted radionuclide therapy of prostate cancer.