4-N-Alkanoyl and 4-N-alkyl gemcitabine analogues with NOTA chelators for 68-gallium labelling

The positron-emitting radionuclide gallium-68 has become increasingly utilised in both preclinical and clinical settings with positron emission tomography (PET). The synthesis of radiochemically pure gallium-68 radiopharmaceuticals relies on careful consideration of the coordination chemistry. The short half-life of 68 min necessitates rapid quantitative radiolabelling (≤10 min). Desirable radiolabelling conditions include near-neutral pH, ambient temperatures, and low chelator concentrations to achieve the desired apparent molar activity. This review presents a broad overview of the requirements of an efficient bifunctional chelator in relation to the aqueous coordination chemistry of gallium. Developments in bifunctional chelator design and application are then presented and grouped according to eight categories of bifunctional chelator: the macrocyclic chelators DOTA and TACN; the acyclic HBED, pyridinecarboxylates, siderophores, tris(hydroxypyridinones), and DTPA; and the mesocyclic diazepines.

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4-N-Alkanoyl and 4-N-alkyl gemcitabine analogues with NOTA chelators for 68-gallium labelling

Cited by 2 publications

References 36 publications

Synthesis and ¹⁸F-radiolabeling of thymidine AMBF₃ conjugates

Synthesis and ¹⁸F-radiolabeling of thymidine AMBF₃ conjugates

Modern Developments in Bifunctional Chelator Design for Gallium Radiopharmaceuticals

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4-N-Alkanoyl and 4-N-alkyl gemcitabine analogues with NOTA chelators for 68-gallium labelling

Cited by 2 publications

References 36 publications

Synthesis and 18F-radiolabeling of thymidine AMBF3 conjugates

Synthesis and 18F-radiolabeling of thymidine AMBF3 conjugates

Modern Developments in Bifunctional Chelator Design for Gallium Radiopharmaceuticals

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Synthesis and ¹⁸F-radiolabeling of thymidine AMBF₃ conjugates

Synthesis and ¹⁸F-radiolabeling of thymidine AMBF₃ conjugates