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首页> 外文期刊>Journal of Medicinal Chemistry >Novel cyclooxygenase-1 inhibitors discovered using affinity fingerprints.
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Novel cyclooxygenase-1 inhibitors discovered using affinity fingerprints.

机译:使用亲和指纹图谱发现了新型环氧合酶-1抑制剂。

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We used protein affinity fingerprints to discover structurally novel inhibitors of cyclooxygenase-1 (COX-1) by screening a selected number of compounds, thus providing an alternative to extensive screening. From the affinity fingerprints of 19 known COX-1 inhibitors, a computational model for COX-1 inhibition was constructed and used to select candidate inhibitors from our compound library to be tested in the COX-1 assay. Subsequent refinement of the model by including affinity fingerprints of inactive compounds identified three molecules that were more potent than ibuprofen, a commonly used COX-1 inhibitor. These compounds are structurally distinct from those used to build the model and were discovered by testing only 62 library compounds. The discovery of these leads demonstrates the efficiency with which affinity fingerprints can identify novel bioactive chemotypes from known drugs.
机译:我们使用蛋白质亲和力指纹图谱通过筛选选定数量的化合物来发现结构新颖的环氧合酶-1(COX-1)抑制剂,从而为广泛筛选提供了另一种选择。根据19种已知COX-1抑制剂的亲和指纹图谱,构建了COX-1抑制的计算模型,并用于从我们的化合物库中选择候选抑制剂,以在COX-1分析中进行测试。随后通过包括非活性化合物的亲和力指纹图谱对模型进行了改进,确定出三个分子比通常使用的COX-1抑制剂布洛芬更有效。这些化合物在结构上与用于构建模型的化合物不同,并且仅通过测试62个文库化合物而发现。这些线索的发现证明了亲和指纹可以从已知药物中识别新型生物活性化学型的效率。

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