A novel class of orally active non-peptide bradykinin B2 receptor antagonist.: 2.: Overcoming the species difference between guinea pig and man

被引:51
作者
Abe, Y
Kayakiri, H
Satoh, S
Inoue, T
Sawada, Y
Inamura, N
Asano, M
Hatori, C
Sawai, H
Oku, T
Tanaka, H
机构
[1] Fujisawa Pharmaceut Co Ltd, Exploratory Res Labs, Dept Med Chem, Ibaraki, Osaka 3002698, Japan
[2] Fujisawa Pharmaceut Co Ltd, Exploratory Res Labs, Dept Pharmacol, Ibaraki, Osaka 3002698, Japan
关键词
D O I
10.1021/jm980214f
中图分类号
R914 [药物化学];
学科分类号
100701 ;
摘要
Recently we reported the identification of a series of 8-[[3-(N-acylglycyl-N-methylamino)-2,6-dichlorobenzyl]oxy]-3-halo-2-methylimidazo[1,2-a]pyridines as the first orally active non-peptide bradykinin (BK) B-2 receptor antagonists (1-3). These compounds inhibited the specific binding of [H-3]BK to guinea pig ileum membrane preparations expressing B-2 receptors with nanomolar IC50's and also displayed in vivo functional antagonistic activities against BK-induced bronchoconstriction in guinea pigs at 1 mg/kg by oral administration. However, it was found that their affinities for the B-2 receptors in human A-431 cells (human epidermoid carcinoma) were much lower. Intensive modifications of the terminal substituents at the glycine moiety elucidated the structure-activity relationships (SAR) for human B-2 receptors, leading to an extended basic framework which incorporated a novel key pharmacophore. Thus, we overcame the species difference and identified the first clinical candidate 18c (FR167344) with IC50's of 0.66 and 1.4 nM for guinea pig ileum and human A-431 cells, respectively. This compound displayed in vivo functional antagonistic activity against BK-induced bronchoconstriction in guinea pigs with an ED50 value of 0.17 mg/kg by oral administration. This novel non-peptide B-2 antagonist is extremely potent both in vitro and in vivo by oral administration and is expected to be the first member of a new class of drug for the treatment of various inflammatory diseases.
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页码:4053 / 4061
页数:9
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