Synthesis of New Isoxazolo[4,5‐d]pyrimidines as Antitumor Agents

The present paper (publication) concerns the synthesis of new isoxazole[4,5‐d]pyrimidine derivatives. There are only a few publications in the chemical literature that report the derivatives of the [4,5‐d] isomer. Our new compounds, the derivatives of this isomer, were obtained using a new manner that differs from those reported in the aforementioned publications in that we used the tautomers of 3‐arylo‐4‐imino‐5‐carbethoxy isxazole 3 and 4 as the starting compounds instead of using their 4‐amino forms. Their tautomeric form proved chemically stable, and, as a result of ammonolysis, we obtained the compounds 5 and 6 . The cyclization of the amides of 5 and 6 with various aldehydes yielded new derivatives, 10 – 19 , with good yields. As a by‐product, the 4‐amino tautomer form in by degrees and was reacted also with aldehydes, and we isolated Schiff bases 20 – 25 with low yields. Some of these compounds were tested for their antitumor activity at National Cancer Institute, Bethesda, MD, USA.