Synthesis, Fluorine-18 Radiolabeling, and In Vivo PET Imaging of a Hydrophilic Fluorosulfotetrazine

The development of 18F-fluorotetrazines, suitable for the radiolabeling of biologics such as proteins and antibodies by IEDDA ligation, represents a major challenge, especially for pre-targeting applications. The hydrophilicity of the tetrazine has clearly become a crucial parameter for the performa...

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Published inPharmaceuticals (Basel, Switzerland) Vol. 16; no. 5; p. 636
Main Authors Beaufrez, Jason, Guillouet, Stéphane, Seimbille, Yann, Perrio, Cécile
Format Journal Article
LanguageEnglish
Published Switzerland MDPI AG 22.04.2023
MDPI
Subjects
Acids
bioconjugation
Chemical properties
Chemical Sciences
Fluorides
Fluorine
Fluorine compounds
fluorine-18
hydrophilicity
Life Sciences
Medicinal Chemistry
Methods
PET imaging
Pharmaceutical sciences
Pharmacokinetics
Pharmacology
Potassium
pre-targeting
Radioactive tracers
Reagents
Sodium
Structure
Temperature
tetrazine
France
bioconjugation
fluorine-18
pre-targeting
PET imaging
sultone
sulfonic acid salt
tetrazine
hydrophilicity
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Summary:The development of 18F-fluorotetrazines, suitable for the radiolabeling of biologics such as proteins and antibodies by IEDDA ligation, represents a major challenge, especially for pre-targeting applications. The hydrophilicity of the tetrazine has clearly become a crucial parameter for the performance of in vivo chemistry. In this study, we present the design, the synthesis, the radiosynthesis, the physicochemical characterization, the in vitro and in vivo stability, as well as the pharmacokinetics and the biodistribution determined by PET imaging in healthy animals of an original hydrophilic 18F-fluorosulfotetrazine. This tetrazine was prepared and radiolabelled with fluorine-18 according to a three-step procedure, starting from propargylic butanesultone as the precursor. The propargylic sultone was converted into the corresponding propargylic fluorosulfonate by a ring-opening reaction with 18/19F-fluoride. Propargylic 18/19F-fluorosulfonate was then subject to a CuACC reaction with an azidotetrazine, followed by oxidation. The overall automated radiosynthesis afforded the 18F-fluorosulfotetrazine in 29–35% DCY, within 90–95 min. The experimental LogP and LogD7.4 values of −1.27 ± 0.02 and −1.70 ± 0.02, respectively, confirmed the hydrophilicity of the 18F-fluorosulfotetrazine. In vitro and in vivo studies displayed a total stability of the 18F-fluorosulfotetrazine without any traces of metabolization, the absence of non-specific retention in all organs, and the appropriate pharmacokinetics for pre-targeting applications.
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ISSN:1424-8247
1424-8247
DOI:10.3390/ph16050636