通过FieldScreen虚拟筛选获得的p38丝裂原活化蛋白激酶的新型先导结构

Novel lead structures for p38 MAP kinase via FieldScreen virtual screening.

作者信息

Cheeseright Timothy J, Holm Melanie, Lehmann Frank, Luik Sabine, Göttert Marcia, Melville James L, Laufer Stefan

机构信息

Cresset BioMolecular Discovery Ltd., BioPark Hertfordshire, Welwyn Garden City, Hertfordshire AL7 3AX, UK.

出版信息

J Med Chem. 2009 Jul 23;52(14):4200-9. doi: 10.1021/jm801399r.

DOI:10.1021/jm801399r

PMID:19489590

Abstract

p38 MAP kinase has received considerable interest in the pharmaceutical industry and remains a valid and interesting target for the treatment of inflammation. To discover novel p38 inhibitors, we applied the ligand-based virtual screening technique, FieldScreen, to 1.2 million commercially available compounds. Fifty-eight diverse compounds were selected for biological analysis, using molecular field similarity to known inhibitors, while explicitly removing any structure that shared a scaffold with previously reported p38 inhibitors. Of these, 11 (19%) showed >or=20% inhibition of p38 at 10 microM. We chose to prepare analogues of two distinct chemical series resulting in a potential lead compound with pIC(50) of 6.4. Modeling of SAR using FieldAlign, a ligand alignment protocol, was used to rationalize the SAR of the series of thiadiazole based inhibitors.

摘要

p38丝裂原活化蛋白激酶已在制药行业引起了相当大的关注，并且仍然是治疗炎症的一个有效的、令人感兴趣的靶点。为了发现新型p38抑制剂，我们将基于配体的虚拟筛选技术FieldScreen应用于120万种市售化合物。利用与已知抑制剂的分子场相似性，同时明确去除与先前报道的p38抑制剂具有相同骨架的任何结构，选择了58种不同的化合物进行生物学分析。其中，11种（19%）在10微摩尔浓度下对p38的抑制率≥20%。我们选择制备两个不同化学系列的类似物，得到了一个pIC(50)为6.4的潜在先导化合物。使用配体比对方案FieldAlign对构效关系进行建模，以阐明基于噻二唑的抑制剂系列的构效关系。

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通过FieldScreen虚拟筛选获得的p38丝裂原活化蛋白激酶的新型先导结构

Novel lead structures for p38 MAP kinase via FieldScreen virtual screening.

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