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Virtual Screening for Finding Novel COX-2 Inhibitors as AntitumorAgents

机译:虚拟筛选,用于寻找新型COX-2抑制剂作为抗肿瘤剂

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The cyclooxygenase-2 (COX-2) enzyme binds to arachidonic acid resulting in the release of metabolites that induce pain and inflammatory responses. Recent studies have shown that strong COX-2 expression is highly correlated with increased tumor risk. Therefore, the development of potent COX-2 inhibitors to relieve pain and treat cancers requires further investigation. We used virtual screening to find three COX-2 inhibitors (Phar-95239, T0511-4424 and Zu- 4280011) from a huge zinc database containing 2000000 compounds. The effects of the compounds on COX-2 were compared to those on COX-1 using a colorimetric COX (ovine) screening assay kit. The selectivity index, the ratio of IC50 for COX-1 inhibition to that of COX-2, calculated were MTT assay was used to evaluate the cytotoxic activity of the compounds using different dilutions. The IC50 values were calculated. Based on the results of the MTT assay, the IC50 values for compounds Phar-95239, T0511-4424 and Zu-4280011 were 178.52, 143 and 97.61 μM, respectively, and the selectivity indices of the compounds were 11.36, 12.20 and 20.03, respectively. These results indicated a relationship between the selectivity index and anticancer activity. Zu-4280011 displayed the highest selectivity index and the best results in the MTT assay among selected componds.
机译:环氧合酶2(COX-2)酶与花生四烯酸结合,导致释放出引起疼痛和炎症反应的代谢产物。最近的研究表明,强大的COX-2表达与增加的肿瘤风险高度相关。因此,开发有效的COX-2抑制剂以减轻疼痛和治疗癌症需要进一步的研究。我们使用虚拟筛选从包含2000000种化合物的庞大锌数据库中找到了三种COX-2抑制剂(Phar-95239,T0511-4424和Zu- 4280011)。使用比色COX(绵羊)筛选测定试剂盒,将化合物对COX-2的作用与对COX-1的作用进行了比较。计算出的选择性指数,即抑制COX-1的IC50与COX-2的IC50之比,用MTT分析法评估使用不同稀释度的化合物的细胞毒活性。计算IC 50值。根据MTT分析的结果,化合物Phar-95239,T0511-4424和Zu-4280011的IC50值分别为178.52、143和97.61μM,化合物的选择性指数分别为11.36、12.20和20.03。 。这些结果表明选择性指数与抗癌活性之间的关系。在MTT分析中,Zu-4280011在所选化合物中显示出最高的选择性指数和最佳结果。

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