Development of a hydroxamamide-based bifunctional chelating agent to prepare technetium-99m-labeled bivalent ligand probes.

Hydroxamamide (Ham) is a thiol-free chelating agent that forms technetium-99m (Tc)-complexes with a metal-to-ligand ratio of 1:2 under moderate reaction conditions. Therefore, Ham-based chelating agents will produce Tc-labeled compounds with a bivalent targeting scaffold. For their universal usage, we developed a novel Ham-based bifunctional chelating agent, "Ham-Mal", with a maleimide group that can easily conjugate with a thiol group, for to preparing Tc-labeled bivalent ligand probes. Ham-Mal was synthesized by a four-step reaction, and then reacted with cysteine or c(RGDfC) to produce Ham-Cys or Ham-RGD. These precursors were reacted with TcO for 10 min under room temperature to obtain Tc-(Ham-Cys) and Tc -(Ham-RGD). The cellular uptake level of Tc-(Ham-RGD) by U87MG (high Integrin ɑβ expression) cells was significantly higher than that by PC3 (low Integrin ɑβ expression) cells at 60 min after the incubation, and the uptake was significantly suppressed by pre-treatment for 15 min with excess c(RGDfK) peptide. In the in vivo study with U87MG/PC3 dual xenografted BALB/c-nu mice, the radioactivity of U87MG tumor tissue was significantly higher than that of PC3 tumor tissue at 360 min after the administration of Tc-(Ham-RGD). These results suggest Ham-Mal may have potential as a bifunctional chelating agent for Tc-labeled bivalent ligand probes.