通过高通量对接和连续静电计算发现β-分泌酶的细胞可渗透非肽抑制剂。

Discovery of cell-permeable non-peptide inhibitors of beta-secretase by high-throughput docking and continuum electrostatics calculations.

作者信息

Huang Danzhi, Lüthi Urs, Kolb Peter, Edler Karin, Cecchini Marco, Audetat Stephan, Barberis Alcide, Caflisch Amedeo

机构信息

Department of Biochemistry, University of Zürich, Winterthurerstrasse 190, CH-8057 Zürich, Switzerland.

出版信息

J Med Chem. 2005 Aug 11;48(16):5108-11. doi: 10.1021/jm050499d.

DOI:10.1021/jm050499d

PMID:16078830

Abstract

A fragment-based docking procedure followed by substructure search were used to identify active-site beta-secretase inhibitors from a composite set of about 300 000 and a library of nearly 180 000 small molecules, respectively. EC(50) values less than 10 microM were measured in at least one of two different mammalian cell-based assays for 12 of the 72 purchased compounds. In particular, the phenylureathiadiazole 2 and the diphenylurea derivative 3 are promising lead compounds for beta-secretase inhibition.

摘要

基于片段的对接程序，随后进行子结构搜索，分别用于从约300000个化合物的组合集和近180000个小分子的文库中识别活性位点β-分泌酶抑制剂。在两种不同的基于哺乳动物细胞的检测方法中，至少有一种检测方法测得72种购买化合物中的12种的EC(50)值小于10 microM。特别是，苯基脲噻二唑2和二苯基脲衍生物3是有前景的β-分泌酶抑制先导化合物。

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通过高通量对接和连续静电计算发现β-分泌酶的细胞可渗透非肽抑制剂。

Discovery of cell-permeable non-peptide inhibitors of beta-secretase by high-throughput docking and continuum electrostatics calculations.

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