Abstract: | The diazonium salt derived from 4‐amino‐N,1,3‐trimethyl‐N‐(3‐methyl‐1‐phenyl‐1H‐pyrazol‐5‐yl)‐1H‐pyrazole‐5‐carboxamide ( 14 ) was reacted with a mixture of CuSO4 and NaCl, with ascorbic acid as an initiator to afford the planar derivative 4,6‐dihydro‐1,4,6,8‐tetramethyl‐3‐phenyldipyrazolo3,4‐b:4′,3′‐d]pyridin‐5(3H)‐one ( 16 ) and its unexpected isomer 4,6‐dihydro‐3,4,6,8‐tetramethyl‐1‐phenyldipyrazolo4,3‐b:4′,3′‐d]pyridin‐5(1H)‐one ( 17 ), as well as the epimers (3S,4S)‐ (or (3S,4R)‐) and (3S,4R)‐ (or (3S,4S)‐) 4‐chloro‐2,4‐dihydro‐1′,3′,5,5′‐tetramethyl‐2‐phenylspiropyrazole‐3,4′(1′H)‐pyrrolo3,4‐c]pyrazol]‐6′(5′H)‐one ( 18a and b , respectively). Epimers 18a and b were converted under basic conditions to 4′‐chloro‐N,1,3,3′‐tetramethyl‐1′‐phenyl‐4,5′‐bi‐1H‐pyrazole]‐5‐carboxamide ( 19 ). The structures of isomers 16 and 17 determined by single‐crystal X‐ray analysis are also reported. Linear dichroism (LD) measurements for the above isomers suggest that 17 intercalates into DNA, and 17 exhibited antiproliferation activity against human NCI‐H460 pulmonary carcinoma cells. |