Synthesis of 18F labelled fluoro-m-tyrosine, fluoro-m-tyramine and fluoro-3-hydroxyphenylacetic acid

## Abstract A new method for the preparation of 6‐[^18^F]fluorodopamine (3) and [^18^F]fluorinated analogs of __m__‐tyramine based on a regioselective radiofluorodestannylation reaction has been developed. The radiofluorodestannylation of 6‐trimethylstannyldopamine derivative 1 was carried out with

S e c t i o n o f R a d i o l o g y a n d N u c l e a r M e d i c i n e and Department o f C h e m i s t r y , H a m i l t o n , O n t a r i o , Canada, L8N 325 SUHMARY R e a c t i o n o f d i l u t e [ F -l 8 ] f l u o r i n e gas w i t h e i t h e r m e l g t o n i n o r 5 -h y d r o x y -t r y p

The regioselective radiofluorodestannylation of 6-trimethylstannyl-L-m-tyrosine derivative 6 with [18F]F2 and [18F]acetyl hypofluorite afforded, after acid hydrolysis, 6-[18F]fluoro-L-m-tyrosine (8a) in radiochemical yields of 23 and 17%, respectively. Similarly, 4-[18F]fluoro-L-m-tyrosine (13a) was

## Abstract Progression of Parkinson's disease symptoms is imperfectly correlated with positron emission tomography biomarkers for dopamine biosynthetic pathways. The radiopharmaceutical 6‐[^18^F]fluoro‐m‐tyrosine is not a substrate for catechol‐__O__‐methyltransferase and therefore has a more favo

A combined study of the labelling methods of two important glucose-derivatives i.e. [18F]2-deoxy-2-fluoro-D-glucose ([laF]2-FDG) and [lSF]3-deoxy-3-fluoro-D-glucose ([18F]3-FDG) is described. Using [ISF]fluoride as reacting agent produced in a water target via the 180(p, n)'SF and ~60(3He, p)~SF rea