Pretargeted Alpha Therapy of Disseminated Cancer Combining Click Chemistry and Astatine-211

To enhance targeting efficacy in the radioimmunotherapy of disseminated cancer, several pretargeting strategies have been developed. In pretargeted radioimmunotherapy, the tumor is pretargeted with a modified monoclonal antibody that has an affinity for both tumor antigens and radiolabeled carriers....

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Main Authors: Chiara Timperanza (Author), Holger Jensen (Author), Tom Bäck (Author), Sture Lindegren (Author), Emma Aneheim (Author)
Format: Book
Published: MDPI AG, 2023-04-01T00:00:00Z.
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Summary:To enhance targeting efficacy in the radioimmunotherapy of disseminated cancer, several pretargeting strategies have been developed. In pretargeted radioimmunotherapy, the tumor is pretargeted with a modified monoclonal antibody that has an affinity for both tumor antigens and radiolabeled carriers. In this work, we aimed to synthesize and evaluate poly-L-lysine-based effector molecules for pretargeting applications based on the tetrazine and trans-cyclooctene reaction using <sup>211</sup>At for targeted alpha therapy and <sup>125</sup>I as a surrogate for the imaging radionuclides <sup>123, 124</sup>I. Poly-L-lysine in two sizes was functionalized with a prosthetic group, for the attachment of both radiohalogens, and tetrazine, to allow binding to the trans-cyclooctene-modified pretargeting agent, maintaining the structural integrity of the polymer. Radiolabeling resulted in a radiochemical yield of over 80% for astatinated poly-L-lysines and a range of 66-91% for iodinated poly-L-lysines. High specific astatine activity was achieved without affecting the stability of the radiopharmaceutical or the binding between tetrazine and transcyclooctene. Two sizes of poly-L-lysine were evaluated, which displayed similar blood clearance profiles in a pilot in vivo study. This work is a first step toward creating a pretargeting system optimized for targeted alpha therapy with <sup>211</sup>At.
Item Description:10.3390/ph16040595
1424-8247