Synthesis of carbon-14 and deuterium labeled 3-nitro-6-propoxyimidazo [1, 2-b]pyridazine — An antiparasitic agent

%Methyl -6-[3-( t r i f 1 uoromethyl ) phenyl 1-1,2,4-triazolo[4,3-b] p y r i d a z i n e ($), c u r r e n t l y being evaluated as a p o t e n t i a l anxiol y t i c agent was synthesized, l a b e l e d w i t h carbon-14 i n the 3p o s i t i o n o f t h e t r i a z o l o nucleus. i n 67% radiochemi

## Abstract Methods of preparation of carbon‐14 and deuterium labeled N‐nitroso‐2(3′,7′‐dimethyl‐2′,6′‐octadienyl)aminoethanols are described. The primary synthetic method involved alkylation of ethanolamine or ethylglycine with suitable chlorides and subsequent mild nitrosation. Isomeric ^14^C‐nit

In order to study the metabolic fate of 3-isobutyryl-2-isopropylpyrazolo~1,5-aJpyridine [I, in experimental animals and humans, the synthesis of I labeled with carbon-14 or deuterium was investiqated. Carbon-14 labeled I was obtained from 5 mCi of isobutyric acid-l-14C sodium salt with a 6 7 . 7 % y

## Abstract 5‐Methoxy‐2‐methyl‐1‐(3,4‐methylenedioxybenzoyl)indole‐3‐acetic acid (ID‐955)(I), a new anti‐inflammatory agent, was labelled with carbon‐14 at C‐2 position of indole nucleus for the use of metabolic studies. The procedure used is shown in Fig. 1 and 2. Levulinic‐4‐^14^C acid was synthe

S W 86002, 6-(4-f luorophenyl) -5-(4-pyridyl) -2,3-dihydroimidazo[2,l-b] thiazole, was synthesized labeled pith carbon-14 at C-1 or 14-2,3 using either [ C] thiourea or 1,2-dibromo [ C 3 ethane, respectively. The synthetic route, invogving the condensation of an asymmetric benzoin with thiourea foll

## Abstract 6‐[3‐(1‐Adamantyl)‐4‐methoxyphenyl]‐2‐naphthoic acid (1), a promising new compound for the treatment of disorders of keratinization, has been synthesized in [^14^C]‐labelled form from barium [^14^C]‐carbonate via labelled benzene. Benzene‐[U‐^14^C] was converted to 4‐bromo‐methoxybenzen