Boosting Bismuth(III) Complexation for Targeted α-Therapy (TAT) Applications with the Mesocyclic Chelating Agent AAZTA.
Dávid HorváthAdrienn VágnerDezsö SzikraGyörgy TrencsényiNicola DemitriNicol GuidolinAlessandro MaiocchiSimona GhianiFabio TravaginGiovanni Battista GiovenzanaZsolt BaranyaiPublished in: Angewandte Chemie (International ed. in English) (2022)
Targeted α therapy (TAT) is a promising tool in the therapy of cancer. The radionuclide <sup>213</sup> Bi<sup>III</sup> shows favourable physical properties for this application, but the fast and stable chelation of this metal ion remains challenging. Herein, we demonstrate that the mesocyclic chelator AAZTA quickly coordinates Bi<sup>III</sup> at room temperature, leading to a robust complex. A comprehensive study of the structural, thermodynamic and kinetic properties of [Bi(AAZTA)]<sup>-</sup> is reported, along with bifunctional [Bi(AAZTA-C4-COO<sup>-</sup> )]<sup>2-</sup> and the targeted agent [Bi(AAZTA-C4-TATE)]<sup>-</sup> , which incorporates the SSR agonist Tyr<sup>3</sup> -octreotate. An unexpected increase in the stability and kinetic inertness of the metal chelate was observed for the bifunctional derivative and was maintained for the peptide conjugate. A cyclotron-produced <sup>205/206</sup> Bi mixture was used as a model of <sup>213</sup> Bi in labelling, stability, and biodistribution experiments, allowing the efficiency of [<sup>213</sup> Bi(AAZTA-C4-TATE)]<sup>-</sup> to be estimated. High accumulation in AR42J tumours and reduced kidney uptake were observed with respect to the macrocyclic chelate [<sup>213</sup> Bi(DOTA-TATE)]<sup>-</sup> .