A 99mTc(I)-postlabeled high affinity bombesin analogue as a potential tumor imaging agent

The overexpression of neuropeptide receptors observed in many cancers provides an attractive target for tumor imaging and therapy. Bombesin is a peptide exhibiting a high affinity for the gastrin releasing peptide (GRP) receptor, which is overexpressed by a variety of tumors such as breast or prostate cancer. In the present study, we have evaluated if the bombesin analogue [N-alpha-histidinyl acetate]bombesin(7-14), radiolabeled with the novel [Tc-99m(OH2)(3)(CO)(3)](+), has the potential to be used as a diagnostic radiopharmaceutical. Receptor saturation studies, carried out on the GRP receptor-expressing PC-3 human prostate cancer cell line, revealed for [Tc-99m(CO)(3)-N-alpha-histidinyl acetate]bombesin(7-14) K-d values in the subnanomolar range. Competitive binding assays, using the cold rhenium(I)-labeled analogue as a surrogate for the Tc-99m-conjugate, also showed high affinity binding. Incubation of the radioconjugate with PC-3 cells resulted in a rapid temperature- and time-dependent specific internalization. At 37 degreesC more than 70% was internalized within the first 15 min and remained constant up to 2 h. Despite the weak proteolytic stability of [Tc-99m(CO)(3)-N-alpha-histidinyl acetate] bombesin(7-14) in vitro, biodistribution studies, performed in PC-3 tumor-bearing mice, showed low uptake in the tumor (0.89 +/- 0.27% ID/g 30 min pi) but high uptake into the pancreas (7.11 +/- 3.93% ID/g 30 min pi), a GRP receptor-positive organ. Blockade experiment (coinjection of 300 mug bombesin/mouse with the radioligand) showed specificity of the uptake. Despite the low tumor uptake, tumor-to-blood ratios of 2.0 and 2.7 and tumor-to-muscle ratios of 8.9 and 8.0 were obtained at 30 min and 1.5 h postinjection, respectively. The promising results merit the future in vivo investigation of Tc-99m/Re-188-tricarbonyl-labeled bombesin analogues.