[18F]F2 – New production methods and applications
Krzyczmonik, Anna (2018-12-19)
[18F]F2 – New production methods and applications
(19.12.2018)
Turun yliopisto
Julkaisun pysyvä osoite on:
https://urn.fi/URN:ISBN:978-951-29-7496-2
https://urn.fi/URN:ISBN:978-951-29-7496-2
Tiivistelmä
Fluorine-18 is a positron emitting radioisotope. It has a half-life of 109.8 min, a simple decay profile and low positron energy as a result of which properties fluorine-18 is an excellent candidate for use in the production of tracers for positron emission tomography (PET). Radiochemistry with fluorine-18 starts from the production of the radioactive isotope, which is then used for the labelling of bioactive molecules. The labelling can be done by nucleophilic or electrophilic methods. Nucleophilic 18F-fluorination, using [18F]F-, is the most popular approach due to the effective production method. Production of [18F]F2 is more challenging and is one of the limiting factors for the use of electrophilic 18F-fluorination. Production of [18F]F2 requires the addition of carrier F2, which reduces the molar activity of the product. The electrophilic labelling method that gives the highest molar activity utilizes a high voltage discharge in the production of [18F]F2.
In this study, the first of the methods developed for the production of [18F]F2 replaces the high voltage discharge with a milder, more reliable excitation source i.e., high energy photons. In a second method, the toxic, very reactive F2 gas used as a carrier is replaced by the very inert SF6 gas. In addition, new applications of [18F]F2 based labelling syntheses were developed. [18F]F2 and its derivatives were used for stereoselective 18F-fluorination, for the production of [18F]-4-fluorosydnone, a new reagent for click chemistry as well as, for the production of 6-[18F]fluoro-marsanidine, a PET tracer candidate for brain α2A-adrenoceptors imaging.
Both methods developed for the production of [18F]F2 resulted in the production of the desire product in low yield and with moderated molar activity (Am). Stereoselective 18Ffluorination resulted in high yield and products in high enantiomeric excess. [18F]-4- fluorosydnone, was successfully used for a click reaction, resulting in rapid complete cycloaddition. 6-[18F]fluoro-marsanidine was synthetized with a quality sufficient for preclinical evaluation. However, rapid in vivo metabolism limits its usefulness for brain α2Aadrenoceptor imaging in rodents.
In this study, the first of the methods developed for the production of [18F]F2 replaces the high voltage discharge with a milder, more reliable excitation source i.e., high energy photons. In a second method, the toxic, very reactive F2 gas used as a carrier is replaced by the very inert SF6 gas. In addition, new applications of [18F]F2 based labelling syntheses were developed. [18F]F2 and its derivatives were used for stereoselective 18F-fluorination, for the production of [18F]-4-fluorosydnone, a new reagent for click chemistry as well as, for the production of 6-[18F]fluoro-marsanidine, a PET tracer candidate for brain α2A-adrenoceptors imaging.
Both methods developed for the production of [18F]F2 resulted in the production of the desire product in low yield and with moderated molar activity (Am). Stereoselective 18Ffluorination resulted in high yield and products in high enantiomeric excess. [18F]-4- fluorosydnone, was successfully used for a click reaction, resulting in rapid complete cycloaddition. 6-[18F]fluoro-marsanidine was synthetized with a quality sufficient for preclinical evaluation. However, rapid in vivo metabolism limits its usefulness for brain α2Aadrenoceptor imaging in rodents.
Kokoelmat
- Väitöskirjat [2944]