Nonpeptide inhibitors of cathepsin G:: Optimization of a novel β-ketophosphonic acid lead by structure-based drug design

被引:44
作者
Greco, MN [1 ]
Hawkins, MJ
Powell, ET
Almond, HR
Corcoran, TW
de Garavilla, L
Kauffman, JA
Recacha, R
Chattopadhyay, D
Andrade-Gordon, P
Maryanoff, BE
机构
[1] Johnson & Johnson Pharmaceut Res & Dev, Spring House, PA 19477 USA
[2] Univ Alabama Birmingham, Ctr Biophys Sci & Engn, Birmingham, AL 35294 USA
来源
JOURNAL OF THE AMERICAN CHEMICAL SOCIETY | 2002年 / 124卷 / 15期
关键词
D O I
10.1021/ja017506h
中图分类号
O6 [化学];
学科分类号
0703 ;
摘要
The serine protease cathepsin G (EC 3.4.21.20; Cat G), which is stored in the azurophilic granules of neutrophils (polymorphonuclear leukocytes) and released on degranulation, has been implicated in various pathological conditions associated with inflammation. By employing high-throughput screening, we identified β-ketophosphonic acid 1 as a moderate inhibitor of Cat G (IC50 = 4.1 μM). We were fortunate to obtain a cocrystal of 1 with Cat G and solve its structure by X-ray crystallography (3.5 Å). Structural details from the X-ray analysis of 1·Cat G served as a platform for optimization of this lead compound by structure-based drug design. With the aid of molecular modeling, substituents were attached to the 3-position of the 2-naphthyl ring of 1, which occupies the S1 pocket of Cat G, to provide an extension into the hydrophobic S3 region. Thus, we arrived at analogue 7 with an 80-fold potency improvement over 1 (IC50 = 53 nM). From these results, it is evident that the β-ketophosphonic acid unit can form the basis for a novel class of serine protease inhibitors. Copyright © 2002 American Chemical Society.
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收藏
页码:3810 / 3811
页数:2
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