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Design and Synthesis of Imidazopyrazolopyridines as Novel Selective COX-2 Inhibitors

机译:新型选择性COX-2抑制剂咪唑并吡唑并吡啶的设计与合成

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摘要

The usefulness of non-steroidal anti-inflammatory drugs (NSAIDs) is hampered by their gastrointestinal side effects. Non-selective cyclooxygenases inhibitors interfere with both COX-1 and COX-2 isozymes. Since COX-1 mediates cytoprotection of gastric mucosa, its inhibition leads to the undesirable side effects. On the other hand, COX-2 is undetectable in normal tissues and selectively induced by inflammatory stimuli. Therefore, it is strongly believed that the therapeutic benefits derive from inhibition of COX-2 only. The presence of a strong connection between reported COX-2 inhibitors and cardiac toxicity encourages medicinal chemists to explore new scaffolds. In the present study, we introduced imidazopyrazolopyridines as new potent and selective COX-2 inhibitors that lack the standard pharmacophoric binding features to hERG. Starting from our lead compound >5a, structure-based drug-design was conducted and more potent analogues were obtained with high COX-2 selectivity and almost full edema protection, in carrageenan-induced edema assay, in case of compound >5e. Increased bulkiness around imidazopyrazolopyridines by adding a substituted phenyl ring(s) afforded less active compounds.
机译:非甾体抗炎药(NSAIDs)的胃肠道副作用阻碍了其有效性。非选择性环氧合酶抑制剂会干扰COX-1和COX-2同工酶。由于COX-1介导胃粘膜的细胞保护作用,因此其抑制作用会导致不良的副作用。另一方面,COX-2在正常组织中无法检测到,并由炎症刺激选择性诱导。因此,强烈认为治疗益处仅源​​自抑制COX-2。报道的COX-2抑制剂与心脏毒性之间存在很强的联系,这鼓励药物化学家探索新的支架。在本研究中,我们引入了咪唑并吡唑并吡啶作为新型有效且选择性的COX-2抑制剂,这些抑制剂缺乏与hERG的标准药效结合特性。从角叉菜胶诱导的水肿试验中,从我们的先导化合物> 5a 开始,进行了基于结构的药物设计,并获得了更有效的类似物,具有高COX-2选择性和几乎完全的浮肿保护作用。复合> 5e 。通过添加取代的苯环增加咪唑并吡唑并吡啶周围的体积,提供的活性较低。

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