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Cyclam-Based Chelators Bearing Phosphonated Pyridine Pendants for 64Cu-PET Imaging: Synthesis, Physicochemical Studies, Radiolabeling, and Bioimaging
Author(s) -
Richard C. Knighton,
Thibault Troadec,
Valérie Mazan,
Patricia Le Saëc,
Séverine MarionneauLambot,
Thomas Le Bihan,
Nathalie Saffon-Merceron,
Nathalie Le Bris,
Michel Chérel,
Alain Faivre-Chauvet,
Mourad Elhabiri,
Loı̈c J. Charbonnière,
Raphaël Tripier
Publication year - 2021
Publication title -
inorganic chemistry
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.348
H-Index - 233
eISSN - 1520-510X
pISSN - 0020-1669
DOI - 10.1021/acs.inorgchem.0c03492
Subject(s) - cyclam , chemistry , phosphonate , dota , lipophilicity , chelation , pyridine , ligand (biochemistry) , chemical stability , combinatorial chemistry , context (archaeology) , preclinical imaging , copper , in vivo , stereochemistry , inorganic chemistry , organic chemistry , metal , paleontology , biochemistry , receptor , microbiology and biotechnology , biology
Herein we present the preparation of two novel cyclam-based macrocycles ( e1pyp and cb-te1pyp ), bearing phosphonate-appended pyridine side arms for the coordination of copper(II) ions in the context of 64 Cu PET imaging. The two ligands have been prepared through conventional protection-alkylation sequences on cyclam, and their coordination properties have been thoroughly investigated. The corresponding copper complexes have been fully characterized in the solid state (X-ray diffraction analysis) and in solution (EPR and UV-vis spectroscopies). Potentiometric studies combined with spectrometry have also allowed us to determine their thermodynamic stability constants, confirming their high affinity for copper(II) cations. The kinetic inertness of the complexes has been verified by acid-assisted dissociation experiments, enabling their use in 64 Cu-PET imaging in mice for the first time. Indeed, the two ligands could be quantitatively radiolabeled under mild conditions, and the resulting 64 Cu complexes have demonstrated excellent stability in serum. PET imaging demonstrated a set of features emerging from the combination of picolinates and phosphonate units: high stability in vivo , fast clearance from the body via renal elimination, and most interestingly, very low fixation in the liver. This is in contrast with what was observed for monopicolinate cyclam ( e1pa ), which had a non-negligible accumulation in the liver, owing probably to its different charge and lipophilicity. These results thus pave the way for the use of such phosphonated pyridine chelators for in vivo 64 Cu-PET imaging.

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