Synthesis of 4-allyloxy-3-chlorophenylacetic-1-14C acid

Specifically labelled phenylacetic acid and mandelic acid derivatives, metabolites of L-Dopa, have been synthesized via the intermediary labelled benzyl alcohols, which were prepared by reduction of the methyl esters of the appropriate benzoic acids. The benzyl alcohols have been converted to the co

1-14C-Ca oxy]-4-benzoylbenzoic acid has been prepared v i a a Grignard r e a c t i o n w i t h %Oz. 4-Bromobenzophenone was converted t o (4-braopheny1)phenyldichloranethane using phosphorus pentachloride. was reacted w i t h methoxide i o n t o form 4-bromobenzophenone dimethyl k e t a l which was

## Abstract The title work proceeds in five steps and 16% overall yield from sodium [1‐^14^C]acetate, which was converted by bromination followed by ethoxide displacement and reaction with phthaloyl dichloride to ethoxy[1‐^14^C]acetyl chloride. The thermal[2+2]cycloaddition of tetraethoxyethene wit

During p r e l i m i n a r y work with u n l a b e l l e d compounds, an attempt was made t o carbonate t h e Grignard r e a g e n t prepared from 2-bromo-2-methylpropane according t o i. No a c i d was i s o l a t e d .

## Abstract 1,4‐Dihydro‐1‐methoxy‐6,7‐methylenedioxy‐4‐oxoquinoline‐3‐carboxylic acid (I) (AB‐206), a new synthetic antimicrobial agent, was labelled with carbon‐14 at C‐3 position of the quinolinone ring for metabolic studies. The synthesis was achieved according to the reaction schemes shown in F

## Abstract 1‐Ethyl‐6‐fluoro‐1,4‐dihydro‐4‐oxo‐7‐(1‐piperazinyl)‐ 3‐quinolinecarboxylic acid (__I__, AM‐715), a new potent antibacterial agent, was labelled with carbon‐14 at the C‐1 position of the N‐ethyl group for metabolic studies. The synthesis was achieved according to two reaction routes. Th