Synthesis of [14C]2-pipecolinyl-5-amino-4′-chloro-benzophenone (LF.1695)

## Abstract A convenient synthesis of the ^14^C‐labelled chloromethyl ketone analog of leucine is reported. Modification of previously published conditions allowed for the facile synthesis of: 2–^14^C‐3‐amino‐1‐chloro‐5‐methylhexan‐2‐one hydrochloride in four steps from 1‐^14^C‐DL‐leucine in 85.7%

## Abstract The carbon of the N‐ethyl group of the side‐chain of atabrine (I) has been labelled with carbon‐14 as part of a metabolic study of this compound. The overall radiochemical yield was 38% based on ethyl‐1–^14^C iodide.

## Abstract The title compound (1) was synthesized by a 7‐step sequence. 4‐Amino‐2‐hydroxy‐[carbonyl‐^14^C]benzoic acid (1) was selectively methylated to provide the ether ester 2, which was smoothly chlorinated in acetic acid to give 3. The ester was hydrolyzed with aqueous potassium hydroxide to

FFBu, a pro-drug o f the d i u r e t i c furosemide, has been prepared by reaction o f the l a t t e r with n-butanol and formaldehyde. A much improved synthesis o f furosemide-[ C02H] i s described based on a new, high y i e l d i n g route t o the key intermediate, 2-fluoro-Cchlorobenzoic acid-[ C

## Abstract The syntheses of 4‐amino‐3,2′‐dimethyl‐biphenyl‐3‐methyl‐^14^C, a potent carcinogen and mutagen, and 4‐amino‐2′‐methylbiphenyl‐2′‐methyl‐^14^C, an analogue having weaker activity, are described. In both cases, label was introduced with Cu^14^ CN.