Synthesis of tritium labelled (−)-3-PPP, a selective dopamine autoreceptor agonist

Effect of 3-PPP, a putative dopamine autoreceptor agonist, on [3H]ligand binding to dopamine receptors of calf and rat striatum. Drug Dev. Res. 3:177-184, 1983. 3-(3-Hydroxyphenyl)-N-n-propyliperidine (3-PPP) is most effective in inhibiting I3HJapomorphine binding in rat striatal membranes, with Ki

DSP 4 (N-( 2-Chl oroethyl 1 -N-ethyl -2-bromobenzyl ami ne, 1) i s a neurotoxin, selective f o r neuronal noradrenaline (NAI. Tritium l a b e l l e d DSP 4 (Q) w i t h a specific a c t i v i t y o f 105 m C i / m l was prepared. The key step i n the synthesis i s a reduction o f the m i n o e s t e

The epimeric gibberellin-A 7-aldehydes 1 and 2 were silylated, enolised with KH and 3labelled with -3 H20 to give after desilylation the tritium-labelled epimeric gibberellin-A ?-aldehydes 2 and 2. Subsequent acetylation, oxidation and deacetylation afforded [ 6-3H] gibberellin-A3 (6) and [ 6-3H]6-e

## Conclusions The synthesis of AZD4619 included 14 steps with an overall yield of 13%. To reach the requirements of an increase in molecular weight by at least nine, both 13 C and 2 H had to be incorporated. According to our previous experiences the loss of deuterium in acidic positions necessita