Abstract

Abstract Condensation of 2,4,6‐triaminopyrimidine ( 8 ) with bromomalonaldehyde ( 9 ) afforded, after pivaloylation, 2,4‐dipivaloyl‐6‐bromopyrido[2,3‐ d ]pyrimidine ( 11 ). This 6‐bromo derivative served as a key intermediate for the synthesis of 2,4‐diamino‐6‐[2‐(3′,4′‐dimethoxyphenyl)ethenyl]pyrido[2,3‐ d ]pyrimidine ( 5 ) via a palladium catalyzed carbon‐carbon coupling with 3,4‐dimethoxystyrene ( 12 ). Compound 5 , its 9,10‐dihydro analogue 6 and the 5,6,7,8,9,10‐hexahydro analogue 7 were of interest as potential inhibitors of dihydrofolate reductase. Compounds 6 and 7 were synthesized from 5 by catalytic hydrogenation over 5% Pd‐C.