International Journal of Molecular Sciences (Sep 2022)

Oxidation of <i>p</i>-[<sup>125</sup>I]Iodobenzoic Acid and <i>p</i>-[<sup>211</sup>At]Astatobenzoic Acid Derivatives and Evaluation In Vivo

  • Yawen Li,
  • Ming-Kuan Chyan,
  • Donald K. Hamlin,
  • Holly Nguyen,
  • Eva Corey,
  • D. Scott Wilbur

DOI
https://doi.org/10.3390/ijms231810655
Journal volume & issue
Vol. 23, no. 18
p. 10655

Abstract

Read online

The alpha particle-emitting radionuclide astatine-211 (211At) is of interest for targeted radiotherapy; however, low in vivo stability of many 211At-labeled cancer-targeting molecules has limited its potential. As an alternative labeling method, we evaluated whether a specific type of astatinated aryl compound that has the At atom in a higher oxidation state might be stable to in vivo deastatination. In the research effort, para-iodobenzoic acid methyl ester and dPEG4-amino acid methyl ester derivatives were prepared as HPLC standards. The corresponding para-stannylbenzoic acid derivatives were also prepared and labeled with 125I and 211At. Oxidization of the [125I]iodo- and [211At]astato-benzamidyl-dPEG4-acid methyl ester derivatives provided materials for in vivo evaluation. A biodistribution was conducted in mice with coinjected oxidized 125I- and 211At-labeled compounds. The oxidized radioiodinated derivative was stable to in vivo deiodination, but unfortunately the oxidized [211At]astatinated benzamide derivative was found to be unstable under the conditions of isolation by radio-HPLC (post animal injection). Another biodistribution study in mice evaluated the tissue concentrations of coinjected [211At]NaAtO3 and [125I]NaIO3. Comparison of the tissue concentrations of the isolated material from the oxidized [211At]benzamide derivative with those of [211At]astatate indicated the species obtained after isolation was likely [211At]astatate.

Keywords