Dal Piaz V, Ciciani G, Giovannoni M P
Dipartimento di Scienze Farmaceutiche, Università di Firenze, Italy.
Drug Des Discov. 1996 Mar;14(1):53-75.
A series of 5-acyl-6-phenyl-2,4-substituted-3(2H)-pyridazinones and analogous benzo[h]cinnolin-3,5-diones with reduced flexibility has been prepared and evaluated as human platelet aggregation inhibitors. The 4-methylsulfoxide 13b was the most potent compound of the series (IC50 = 1.2 microM). SAR studies have shown the primary importance of an electronegative substituent at position 4 and an acetyl group at position 5 of the pyridazine system for potent platelet aggregation inhibitory activity. Biological tests performed on a group of representative compounds showed these products have not effects on prostaglandins, thromboxanes and nitric oxide biosynthetic pathways. Some of synthesized compounds produced a moderate increase of cAMP level in platets which does not depend on the adenylate-cyclase stimulation. Tests performed on human platelet PDE III have shown that these compounds are not inhibitors of this enzyme.
已制备了一系列具有降低柔韧性的5-酰基-6-苯基-2,4-取代-3(2H)-哒嗪酮以及类似的苯并[h]噌啉-3,5-二酮,并将其作为人类血小板聚集抑制剂进行了评估。4-甲亚砜基-13b是该系列中最有效的化合物(IC50 = 1.2微摩尔)。构效关系研究表明,哒嗪系统4位的电负性取代基和5位的乙酰基对于有效的血小板聚集抑制活性至关重要。对一组代表性化合物进行的生物学测试表明,这些产物对前列腺素、血栓烷和一氧化氮生物合成途径没有影响。一些合成化合物使血小板中的cAMP水平适度升高,这并不依赖于腺苷酸环化酶的刺激。对人血小板磷酸二酯酶III进行的测试表明,这些化合物不是该酶的抑制剂。
