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基于高通量筛选的整合素 CD11b/CD18 配体结合的小分子拮抗剂的鉴定。

High-throughput screening based identification of small molecule antagonists of integrin CD11b/CD18 ligand binding.

机构信息

Division of Nephrology and Hypertension, Department of Medicine, University of Miami, Peggy and Harold Katz Family Drug Discovery Center, Miami, FL 33136, USA.

出版信息

Biochem Biophys Res Commun. 2010 Mar 26;394(1):194-9. doi: 10.1016/j.bbrc.2010.02.151. Epub 2010 Feb 25.

Abstract

Binding of leukocyte specific integrin CD11b/CD18 to its physiologic ligands is important for the development of normal immune response in vivo. Integrin CD11b/CD18 is also a key cellular effector of various inflammatory and autoimmune diseases. However, small molecules selectively inhibiting the function of integrin CD11b/CD18 are currently lacking. We used a newly described cell-based high-throughput screening assay to identify a number of highly potent antagonists of integrin CD11b/CD18 from chemical libraries containing >100,000 unique compounds. Computational analyses suggest that the identified compounds cluster into several different chemical classes. A number of the newly identified compounds blocked adhesion of wild-type mouse neutrophils to CD11b/CD18 ligand fibrinogen. Mapping the most active compounds against chemical fingerprints of known antagonists of related integrin CD11a/CD18 shows little structural similarity, suggesting that the newly identified compounds are novel and unique.

摘要

白细胞特异性整合素 CD11b/CD18 与其生理配体的结合对于体内正常免疫反应的发展非常重要。整合素 CD11b/CD18 也是各种炎症和自身免疫性疾病的关键细胞效应物。然而,目前缺乏选择性抑制整合素 CD11b/CD18 功能的小分子。我们使用新描述的基于细胞的高通量筛选测定法,从包含超过 100,000 个独特化合物的化学文库中鉴定了许多整合素 CD11b/CD18 的高效拮抗剂。计算分析表明,鉴定出的化合物可分为几个不同的化学类别。许多新鉴定的化合物可阻止野生型小鼠中性粒细胞与 CD11b/CD18 配体纤维蛋白原的粘附。针对已知相关整合素 CD11a/CD18 的拮抗剂的化学指纹图对最活跃的化合物进行映射,显示出很少的结构相似性,这表明新鉴定的化合物是新颖且独特的。

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