Novel pyrrolyl 2-aminopyridines as potent and selective human β-secretase (BACE1) inhibitors

被引:39
作者
Malamas, Michael S. [1 ]
Barnes, Keith [2 ]
Hui, Yu [2 ]
Johnson, Matthew [2 ]
Lovering, Frank [1 ]
Condon, Jeff [1 ]
Fobare, William [1 ]
Solvibile, William [1 ]
Turner, Jim [3 ]
Hu, Yun [3 ]
Manas, Eric S. [1 ]
Fan, Kristi [1 ]
Olland, Andrea [4 ]
Chopra, Rajiv [4 ]
Bard, Jonathan [3 ]
Pangalos, Menelas N. [3 ]
Reinhart, Peter [3 ]
Robichaud, Albert J. [1 ]
机构
[1] Wyeth, Dept Chem Sci, Princeton, NJ 08543 USA
[2] Albany Mol Res, Albany, NY USA
[3] Wyeth, Neurosci, Princeton, NJ 08543 USA
[4] Wyeth, Dept Chem Sci, Cambridge, MA 02140 USA
来源
BIOORGANIC & MEDICINAL CHEMISTRY LETTERS | 2010年 / 20卷 / 07期
关键词
Alzheimer's disease (AD); BACE1; inhibitors; Beta-amyloid peptide (A beta); 2-Aminopyridines; ALZHEIMERS-DISEASE; ACYLGUANIDINE INHIBITORS; OPTIMIZATION; S-1;
D O I
10.1016/j.bmcl.2010.02.075
中图分类号
R914 [药物化学];
学科分类号
100701 ;
摘要
The proteolytic enzyme beta-secretase (BACE1) plays a central role in the synthesis of the pathogenic beta-amyloid in Alzheimer's disease. Recently, we reported small molecule acylguanidines as potent BACE1 inhibitors. However, many of these acylguanidines have a high polar surface area (e. g. as measured by the topological polar surface area or TPSA), which is unfavorable for crossing the blood-brain barrier. Herein, we describe the identification of the 2-aminopyridine moiety as a bioisosteric replacement of the acylguanidine moiety, which resulted in inhibitors with lower TPSA values and superior brain penetration. X-ray crystallographic studies indicated that the 2-aminopyridine moiety interacts directly with the catalytic aspartic acids Asp32 and Asp228 via a hydrogen-bonding network. (C) 2010 Elsevier Ltd. All rights reserved.
引用
收藏
页码:2068 / 2073
页数:6
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