一些生物活性肉桂酰腙的计算机辅助药物设计方法,作为COX-2选择性抑制剂的硅和对接研究

B. Banu, G. Rajitha, K. Bharathi
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引用次数: 5

摘要

近年来,基于结构类似物的药物发现已成为设计更有效药物的重要工具。本研究利用SAR、药效团研究和基于结构类似物的新型药物,利用互联网工具设计选择性抑制剂分子。取代酰基腙具有广泛的生物活性,如镇痛、抗炎、抗微生物、抗惊厥、抗血小板、抗结核、抗病毒、血吸虫病和抗肿瘤活性。在过去的十年中,几种肉桂酸衍生物被报道为有效的脂氧合酶抑制剂,抗氧化剂和抗炎剂。我们发现结合这些特殊的分子并设计肉桂酰腙是很有趣的,这是一系列N-[(1E)-2-取代苯基-1-{N'-[(1E)-苯基甲基]肼羰基}-1-烯-1-基]苯酰胺。对所设计的化合物进行了药物相似性和口服生物利用度的预测。选定的化合物与COX-2酶对接,发现它们表现出与sc - 558,1000倍选择性标准COX-2抑制剂相似的相互作用。
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An Approach to Computer Aided Drug Design of some Bioactive Cinnamoyl Hydrazones, In Silico and Docking Studies as Possible COX-2 Selective Inhibitors
Recently structural analogue-based drug discovery has become an important tool for designing more potent drugs. This study uses SAR, pharmacophore study and structural analogue-based novel drugs to design selective inhibitor molecules using internet-based tools. Substituted acyl hydrazones are known for wide variety of biological activities, such as analgesic, anti–inflammatory, anti-microbial, anti-convulsant, anti-platelet, anti-tubercular, antiviral, schistomiasis and anti-tumoral activities. In the last decade several cinnamic acid derivatives were reported as potent lipoxygenase inhibitors, antioxidants and anti-inflammatory agents. We found it interesting to combine these particular molecules and design cinnamoyl hydrazones, a series of N-[(1E)-2-substituted phenyl-1-{N'-[(1E)-phenyl methylidene] hydrazine carbonyl} eth-1-en-1-yl] benzamides. The designed compounds were predicted for their drug likeness and oral bioavailability. Selected compounds were docked with COX-2 enzyme and found that they were showing similar interactions as that of SC-558, 1000 time selective standard COX-2 inhibitor.
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