Preparation of enantiomerically-active deuterium-labelled ibuprofen

The preparations o f [ar-2H4]-ibuprofen and Car, 3,3,3-2H7]-i buprofen are described. The deuterium was incorporated i n t o t h e aromatic ri,Fg o f [ar-2H+ ibuprofen which i s a m e t a b o l i c a l l y s t a b l e p o s i t i o n . [ar,3,3,3-H ]-ibuprofen was synthesized by t h e same r o u t e

## Abstract The preparation of deuterium labelled catecholamines and their metabolites is described. The procedures involve simple treatment of the compounds in DC1/D~2~O solution. Mass spectra of these labelled compounds — as their PFP or TFA derivative — are presented. The relative intensity of i

## Abstract The synthesis of d, l, ‐12‐bromocamptothecin (**2d**) from camptothecin (**1**) is described. Reduction of the bromo derivative **2d** with tritium gas in the presence of palladium on carbon afforded d, l‐camptothecin 12‐^3^H having a specific activity of 29 Ci/mmol. A simpler labelling

## Abstract The preparations of guvacine hydrochloride, in which a proton in position 2 (**11**) and protons in positions 2 and 5 (**10**) are selectively exchanged by deuterium, and of [2,6‐^2^H]isoguvacine hydrobromide (**14a**) are described. The deuterium labelled guvacine salts 10 and 11 were

## Abstract Optically active α‐deuterated serine dipeptide active ester derivatives were prepared to study the racemization mechanism. N‐Acetyl‐O‐benzyl‐DL‐serine, __1__, was converted to 5(4H)‐oxazolone __2__ and deuterated with CH~3~‐COOD in α‐position. 5(4^2^H)‐Oxazolone __3__ was converted to Z