Copper-free click bioconjugation of technetium-99m complexes using strained cyclononyne derivatives

Abstract

Click chemistry, in particular copper-free click reactions, has gained growing interest for radiolabelling purposes in the field of radiopharmaceutical sciences. [^99mTc][Tc(CO)₃(H₂O)₃]⁺ works as an excellent starting complex for the radiolabelling of biomolecules under mild conditions. A new chelator, investigated for the copper-free strain-promoted cycloaddition (SPAAC), was synthesised containing the 2,2′-dipicolylamine (DPA) moiety for the ^99mTc-tricarbonyl core and compared with a DPA chelator based on activated esters for conventional radiolabelling. For the copper-free click labelling procedure, a DPA containing 4,8-diazacyclononyne moiety was prepared from a sulfonyl-modified diamide (four steps, 64% yield) followed by the Nicholas reaction with butyne-1,3-diol. The ^99mTc-DPA-DACN-complex was prepared with a radiochemical conversion (RCC) of 89% after 30 min. The following SPAAC reaction with an azide-functionalised PSMA molecule was performed within 4–5 hours at 100 °C to obtain the PSMA (prostate-specific membrane antigen) targeting ^99mTc-complex with 79% RCC and without side products. For comparison, a second DPA-chelator based on a tetrafluorophenyl (TFP) ester was prepared (three steps, 64% yield) and was successfully radiolabelled with [[^99mTc]Tc(CO)₃(H₂O)₃]⁺ with 89% RCC after 20 min and >99% radiochemical purity after separation using an RP18 cartridge. The subsequent conjugation of an amine-functionalised PSMA targeting molecule was performed with 23% RCC after 150 min. Two other unknown side products were observed indicating the decomposition of the TFP ester during the labelling. All nonradioactive Re(CO)₃ complexes were synthesised from (Et₄N)₂[ReBr₃(CO)₃] (91% yield for the ^natRe-DPA-TFP ester, 76% yield for ^natRe-DPA-DACN) and characterised to confirm the identity of the ^99mTc-complexes.