Design and Synthesis of a Potential Dopamine D-1 Antagonist

A r a d i o b r o d n a t e d analog of SCH 23390, a s e l e c t i v e dopamine D1/DAI a n t a g o n i s t was prepared. were obtained w i t h i n 15 minutes r e a c t i o n a t r o m temperature. The s y n t h e s i s was v a l i d a t e d by performing both p h y s i c a l (MR and mass spectroscop

## Abstract A ^14^C labelled form of (+)‐8‐chloro‐5‐(2,3‐dihydrobenzofuran‐7‐yl)‐7‐hydroxy‐3‐methyl‐2,3,4,5‐tetrahydro‐1H‐3‐benzazepine (NNC 756) (8) was synthesized in 7 steps, including resolvation of the active (+)‐form, starting from [^14^C]methyl iodide and 7‐benzofurancarbaldehyde. The overal

## Abstract The synthesis of a designed, sterically congested geminal dimethyl‐bearing PAR‐1 antagonist was achieved by a route of ten steps, with the oxidation of an electron‐rich benzaldehyde, the construction of a tertiary alkyl azide, and the selective hydrogenolysis of a 1,5‐fused tetrazole to