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首页> 外文期刊>Journal of Medicinal Chemistry >Development of potent non-carbohydrate imidazole-based small molecule selectin inhibitors with antiinflammatory activity.
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Development of potent non-carbohydrate imidazole-based small molecule selectin inhibitors with antiinflammatory activity.

机译:具有抗炎活性的有效的非碳水化合物咪唑基小分子选择素抑制剂的开发。

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A novel series of non-carbohydrate imidazole-based selectin inhibitors has been discovered via high-throughput screening using a P-selectin ELISA-based assay system. The initial lead 1 had an IC(50) of 17 microM in the P-selectin ELISA; this potency was significantly improved via an extensive SAR exploration. One of the current lead compounds (29) has an IC(50) of 300 nM in a P-selectin ELISA; it also has good activity in P- and E-selectin cell adhesion assays and shows efficacy in vivo. These compounds represent a novel series of sLe(X) mimetics with antiinflammatory activity. Their unique profile supports our interest in their further evaluation as drug candidates for the treatment of inflammation. Herein we describe the syntheses, optimization, and SAR of this series of novel potent selectin antagonists.
机译:通过使用基于P选择素ELISA的分析系统进行高通量筛选,已发现了一系列新型的非基于咪唑的非选择素抑制剂。初始导线1在P-选择素ELISA中的IC(50)为17 microM;通过广泛的SAR探索,这种效能得到了显着改善。目前的一种先导化合物(29)在P-选择素ELISA中的IC(50)为300 nM;它在P-和E-选择素细胞粘附测定中也具有良好的活性,并在体内显示出功效。这些化合物代表了一系列具有抗炎活性的sLe(X)模拟物。它们的独特特征支持我们对作为炎症治疗候选药物进行进一步评估的兴趣。本文中,我们描述了这一系列新型有效的选择素拮抗剂的合成,优化和SAR。

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