Biodistribution of the Bombesin Receptor-Targeted Radiopharmaceutical Precursor BBN/C1-C2 in a Prostate Cancer Model
E.A. Beloborodov, E.V. Iurova, D.R. Dolgova, A.A. Ermakova, D.E. Sugak, A.N. Fomin, Y.V. Saenko

TL;DR
This study examines a new radiopharmaceutical molecule that targets prostate cancer cells while minimizing uptake in healthy organs.
Contribution
The paper introduces a novel GRPR-targeted radiopharmaceutical with prolonged tumor retention and low normal tissue uptake.
Findings
BBN/C1-C2 showed selective tumor binding and remained on the tumor surface for up to 5 days.
The molecule exhibited low accumulation in normal organs and tissues.
The use of U5-Sth1a toxin may pose a risk to the heart due to its ion channel tropism.
Abstract
Gastrin-releasing peptide receptor (GRPR) is a G protein-coupled receptor expressed in the central nervous system, the gastrointestinal tract, the pancreas, and the adrenal cortical tissue regulating their physiological functions. In addition to normal tissues, GRPR is overexpressed in many solid cancers. At present, several radiolabeled ligands targeting GRPR have been introduced into clinical practice for cancer diagnostics and radioligand therapy. However, there were found the high uptake of radiopharmaceuticals in normal organs and low bioavailability of the drugs caused by their stability. Therefore, GRPR radioantagonists with improved proteolytic stability and longer residence time in tumor foci with low uptake in non-target organs are currently being sought to improve the therapeutic efficacy. The aim of the study was to analyze the biodistribution of the BBN/C1-C2 molecule…
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Taxonomy
TopicsNeuropeptides and Animal Physiology · Radiopharmaceutical Chemistry and Applications · Prostate Cancer Treatment and Research
