Easy Access to Bioorthogonal Click-to-Release Reagent Bishydroxy-trans-cyclooctene (C2TCO) and Harnessing of Its Rapid Labeling and Dissecting Feature in Multicycle Imaging
Bifunctional trans-cyclooctene (bTCO) with a carbamate or carbonate at the allylic position and tetrazine provide a promising bioorthogonal click chemistry pair for the click-to-release approach, successfully employed in various biotechnological applications. Herein, we demonstrate a simple and straightforward method to synthesize C2TCO, a symmetrical bTCO derivative with two hydroxyl groups at the allylic positions. The efficiently synthesized C2TCO at first was selectively functionalized with a fluorophore (C2TCO-FL), and the conjugate was labeled onto monoclonal antibodies (Ab-C2TCO-FL). The fluorophore of Ab-C2TCO-FL was easily removed from the antibody through the mild treatment of tetrazine, enabling multicycle fluorescent bioimaging. Next, an antibody-drug conjugate targeting PD-L1 was prepared using the linker based on C2TCO. The cytotoxic payload was efficiently released from the antibody upon tetrazine treatment, which induced cellular cytotoxicity.
This study was supported by the National Research Foundation of Korea (NRF) grants (RS-2024-00411474, RS-2023-00208819, RS-2024-004400824) funded by the Ministry of Science and ICT, GRRC program of Gyeonggi province (GRRCAjou2023-B03), and by the Ajou University research fund. This work was supported by Samsung Research Funding & Incubation Center of Samsung Electronics under Project Number SRFC-MA2202-07.
