Scandium-44 has emerged as an attractive, novel PET radioisotope with ideal emission properties and half-life ( = 3.97 h, β = 632 keV) well matched to the pharmacokinetics of small molecules, peptides and small biologics. Conjugates of the current gold-standard chelator for Sc, 1,4,7,10-tetraaza-cyclododecane-1,4,7,10-tetraacetic acid (DOTA), require heating to achieve radiochemical complexation, limiting application of this isotope in conjunction with temperature-sensitive biologics. To establish Sc(iii) isotopes as broadly applicable tools for nuclear medicine, development of alternative bifunctional chelators is required. To address this need, we characterized the Sc(iii)-chelation properties of the small-cavity triaza-macrocycle-based, picolinate-functionalized chelator Hmpatcn. Spectroscopic and radiochemical studies establish the [Sc(mpatcn)] complex as kinetically inert and appropriate for biological applications. A proof-of-concept bifunctional conjugate targeting the prostate-specific membrane antigen (PSMA), picaga-DUPA, chelates Sc to form Sc(picaga)-DUPA at room temperature with an apparent molar activity of 60 MBq μmol and formation of inert -Λ and -Δ-twist isomers. Sc(picaga)-DUPA exhibits a of 1.6 nM for PSMA, comparable to the F-based imaging probe DCFPyL ( = 1.1 nM) currently in phase 3 clinical trials for imaging prostate cancer. Finally, we successfully employed Sc(picaga)-DUPA to image PSMA-expressing tumors in a preclinical mouse model, establishing the picaga bifunctional chelator as an optimal choice for the Sc PET nuclide.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC7472660PMC
http://dx.doi.org/10.1039/c9sc04655kDOI Listing

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