Guzik, Patrycja, Benešová, Martina, Ratz, Magdalena, Monné Rodríguez, Josep M., Deberle, Luisa M., Schibli, Roger, and Müller, Cristina
Purpose The folate receptor (FR) is frequently overexpressed in a variety of tumor types and, hence, an interesting target for radionuclide therapy. The aim of this study was to evaluate a new class of albumin-binding radioconjugates comprising 5-methyltetrahydrofolate (5-MTHF) as a targeting agent and to compare their properties with those of the previously established folic acid-based [Lu-177]Lu-OxFol-1. Methods [Lu-177]Lu-6R-RedFol-1 and [Lu-177]Lu-6S-RedFol-1 were investigated in vitro using FR-positive KB tumor cells. Biodistribution studies were performed in KB tumor-bearing mice, and the areas under the curve (AUC(0 -> 120h)) were determined for the uptake in tumors and kidneys. [Lu-177]Lu-6R-RedFol-1 was compared with [Lu-177]Lu-OxFol-1 in a therapy study over 8 weeks using KB tumor-bearing mice. Results Both radioconjugates demonstrated similar in vitro properties as [Lu-177]Lu-OxFol-1; however, the tumor uptake of [Lu-177]Lu-6R-RedFol-1 and [Lu-177]Lu-6S-RedFol-1 was significantly increased in comparison with [Lu-177]Lu-OxFol-1. In the case of [Lu-177]Lu-6S-RedFol-1, also the kidney uptake was increased; however, renal retention of [Lu-177]Lu-6R-RedFol-1 was similar to that of [Lu-177]Lu-OxFol-1. This led to an almost 4-fold increased tumor-to-kidney AUC(0 -> 120h)ratio of [Lu-177]Lu-6R-RedFol-1 as compared with [Lu-177]Lu-6S-RedFol-1 and [Lu-177]Lu-OxFol-1. At equal activity, the therapeutic effect of [Lu-177]Lu-6R-RedFol-1 was better than that of [Lu-177]Lu-OxFol-1, reflected by a slower tumor growth and, consequently, an increased median survival time (49 days vs. 34 days). Conclusion This study demonstrated the promising potential of 5-MTHF-based radioconjugates for FR-targeting. Application of [Lu-177]Lu-6R-RedFol-1 resulted in unprecedentedly high tumor-to-kidney ratios and, as a consequence, a superior therapeutic effect as compared with [Lu-177]Lu-OxFol-1. These findings, together with the absence of early side effects, make [Lu-177]Lu-6R-RedFol-1 attractive in view of a future clinical translation., European Journal of Nuclear Medicine and Molecular Imaging, 48 (4), ISSN:1619-7070, ISSN:1619-7089