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An Eighteen‐Membered Macrocyclic Ligand for Actinium‐225 Targeted Alpha Therapy
268
Zitationen
16
Autoren
2017
Jahr
Abstract
The 18-membered macrocycle H<sub>2</sub> macropa was investigated for <sup>225</sup> Ac chelation in targeted alpha therapy (TAT). Radiolabeling studies showed that macropa, at submicromolar concentration, complexed all <sup>225</sup> Ac (26 kBq) in 5 min at RT. [<sup>225</sup> Ac(macropa)]<sup>+</sup> remained intact over 7 to 8 days when challenged with either excess La<sup>3+</sup> ions or human serum, and did not accumulate in any organ after 5 h in healthy mice. A bifunctional analogue, macropa-NCS, was conjugated to trastuzumab as well as to the prostate-specific membrane antigen-targeting compound RPS-070. Both constructs rapidly radiolabeled <sup>225</sup> Ac in just minutes at RT, and macropa-Tmab retained >99 % of its <sup>225</sup> Ac in human serum after 7 days. In LNCaP xenograft mice, <sup>225</sup> Ac-macropa-RPS-070 was selectively targeted to tumors and did not release free <sup>225</sup> Ac over 96 h. These findings establish macropa to be a highly promising ligand for <sup>225</sup> Ac chelation that will facilitate the clinical development of <sup>225</sup> Ac TAT for the treatment of soft-tissue metastases.
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