Synthesis and biological evaluation of bradykinin B1/B2 and selective B1 receptor antagonists

被引:10
|
作者
Amblard, M
Bedos, P
Olivier, C
Daffx, I
Luccarini, JM
Dodey, P
Pruneau, D
Paquet, JL
Martinez, J
机构
[1] Univ Montpellier 1, Fac Pharm,Lab Aminoacides Peptides & Prot, CNRS, UMR 5810, F-34060 Montpellier, France
[2] Univ Montpellier 2, Fac Pharm,Lab Aminoacides Peptides & Prot, CNRS, UMR 5810, F-34060 Montpellier, France
[3] Lab Rech FOURNIER, F-21121 Daix, France
关键词
D O I
10.1021/jm990961s
中图分类号
R914 [药物化学];
学科分类号
100701 ;
摘要
We recently described a potent bradykinin B-2 receptor agonist (JMVI116) obtained by replacing the D-Tic-Oic dipeptide moiety of HOE140 by a (3S)-amino-5-(carbonylmethyl)-2,3-dihydro-1,5-benzothiazepin-4(5H)-one (D-BT) moiety. This compound inhibited the specific binding of [H-3]BK on membranes of CHO cells expressing the human cloned B-2 receptor with nanomolar affinity and contracted both isolated rat uterus and human umbilical vein. These data demonstrated that D-BT could be a good mimic of the Pro-Phe dipeptide. In the present study we characterized B-1 receptor antagonists containing the D-BT moiety. We prepared an analogue of compound JMV1116 deleting the C-terminal arginine residue. The resulting compound (1) had an affinity of 83 nM for the human cloned B-1 receptor. The most remarkable property of 1 is its ability to bind also the B-2 receptor with an affinity of 4.4 nM despite the absence of the C-terminal arginine residue. Modifications at the N-terminal part of 1 associated with the substitution of the thienylalanine residue by alpha-(2-indanyl)glycine resulted in analogues selectively binding to the B-1 receptor with an affinity in the picomolar range.
引用
收藏
页码:2382 / 2386
页数:5
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