ScholarWorks@성균관대학교

초록

Dimeric fibroblast activation protein inhibitor (FAPI) radioligands are promising candidates for theranostic applications because of their enhanced tumor uptake and prolonged retention compared to monomeric radioligands. Several linker strategies have been investigated to connect two FAPI motifs and a radiometal chelator in a dimer design. In this study, we report the development of a novel dimeric FAPI radioligand, [68Ga]Ga-1, which utilizes a triazine core as a trifunctional linker. The ligand [ nat Ga/68Ga]Ga-1 was synthesized by chelating gallium or gallium-68 to 2-(DOTAGA-NH-ethyl-NH)-4,6-bis(Gly-FAPI)-1,3,5-triazine (1). [ nat Ga]Ga-1, a nonradioactive ligand, exhibited FAP-binding affinity comparable to that of FAPI-04 (IC50 = 2.42 nM vs 1.57 nM). [68Ga]Ga-1 was synthesized in high decay-corrected radiochemical yields (91.7-94.7%) with high molar activities (40.8-50.0 GBq/mu mol) and showed good stability in phosphate-buffered saline and fetal bovine serum. In vitro studies confirmed FAP-specific cellular uptake of [68Ga]Ga-1. Positron emission tomography (PET) imaging and ex vivo biodistribution of [68Ga]Ga-1 in U87MG tumor-bearing mice demonstrated high tumor uptake and retention, which were significantly blocked by FAPI-04, confirming FAP specificity. Notably, [68Ga]Ga-1 demonstrated superior and more sustained tumor uptake than monomeric [68Ga]Ga-FAPI-04, indicating improved pharmacokinetics. Altogether, the triazine linker is well suited for constructing dimeric FAPI radioligands, and [68Ga]Ga-1 holds potential as a FAP-targeted radioligand for theranostic applications.

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