Pharmaceuticals (Jun 2024)

Automated Radiosynthesis of [<sup>18</sup>F]FluoFAPI and Its Dosimetry and Single Acute Dose Toxicological Evaluation

  • Jason A. Witek,
  • Allen F. Brooks,
  • Sahil M. Kapila,
  • Wade P. Winton,
  • Jenelle R. Stauff,
  • Peter J. H. Scott,
  • Benjamin L. Viglianti

DOI
https://doi.org/10.3390/ph17070833
Journal volume & issue
Vol. 17, no. 7
p. 833

Abstract

Read online

Background: Cancer-associated fibroblasts have become a new target for therapy. Fibroblasts present within malignancies express the fibroblast activation protein (FAP). Inhibitors to FAP (FAPI) are small molecules recently developed as a theranostic agents for imaging and radiotherapy. All currently used FAPI rely on a linker–chelator complex attached to the ‘inhibitor’. We describe a new automated method of the direct attachment of the radioisotope to the inhibitor, resulting in a >50% MW reduction with the hope of an improved tumor-to-background ratio and tumor uptake. Methods: [18F]FluroFAPI was developed from a Sn precursor. This allowed for subsequent automated radioflourination. We obtained the biodistribution of [18F]FluroFAPI in rats, performed estimated human radiation dosimetry, and performed a 100× expected single dose toxicology analysis for eventual first-in-human experiments. Results: The synthesis of the Sn precursor for FluorFAPI and the automated synthesis of [18F]FluroFAPI was demonstrated. [18F]FluroFAPI had favorable estimated human radiation dosimetry, and demonstrated no adverse effects when injected at a dose of 100× that planned for [18F]FluroFAPI. Conclusions: With the successful development of an automated synthesis of [18F]FluroFAPI, first-in-human testing can be planned with the hope of an improved tumor-to-background performance compared to other FAPI agents.

Keywords