非肽类缓激肽B2受体拮抗剂：将啮齿动物选择性缓激肽类似物转化为强效、口服活性的人缓激肽B2受体拮抗剂。

Nonpeptide bradykinin B2 receptor antagonists: conversion of rodent-selective bradyzide analogues into potent, orally-active human bradykinin B2 receptor antagonists.

作者信息

Dziadulewicz Edward K, Ritchie Timothy J, Hallett Allan, Snell Christopher R, Davies John W, Wrigglesworth Roger, Dunstan Andrew R, Bloomfield Graham C, Drake Gillian S, McIntyre Peter, Brown Michael C, Burgess Gillian M, Lee Wai, Davis Clare, Yaqoob Mohammed, Phagoo Steve B, Phillips Elsa, Perkins Martin N, Campbell Elizabeth A, Davis Andrew J, Rang Humphrey P

机构信息

Novartis Institute for Medical Sciences, 5 Gower Place, London WC1E 6BS, England.

出版信息

J Med Chem. 2002 May 23;45(11):2160-72. doi: 10.1021/jm0111088.

DOI:10.1021/jm0111088

PMID:12014954

Abstract

The 1-(2-nitrophenyl)thiosemicarbazide (TSC) derivative, (S)-1-[4-(4-benzhydrylthiosemicarbazido)-3-nitrobenzenesulfonyl]pyrrolidine-2-carboxylic acid [2-[(2-dimethylaminoethyl)methylamino]ethyl]amide (bradyzide; (S)-4), was recently disclosed as a novel, potent, orally active nonpeptide bradykinin (BK) B2 receptor antagonist. The compound inhibited the specific binding of [3H]BK to NG108-15 cell membrane preparations (rodent neuroblastoma-glioma) expressing B2 receptors with a K(i) of 0.5 +/- 0.2 nM. Compound (S)-4 also demonstrated oral efficacy against Freund's complete adjuvant (FCA)-induced mechanical hyperalgesia in rats with an ED50 value of 0.84 micromol/kg. After we optimized the terminal binding determinants projecting from the TSC framework, we found that it was possible to replace the potentially toxicophoric nitro and divalent sulfur moieties with only a 15-fold loss in binding affinity ((S)-14a). However, bradyzide and its congeners were found to have much lower affinities for cloned human B2 receptors, expressed in Cos-7 cells. The hitherto synthesized TSC series was screened against the human B2 receptor, and the dibenzosuberane (DBS) pharmacophore emerged as the key structural requirement for potency. Incorporation of this group resulted in a series of derivatives ((S)-14d,e and 19b-d) with K(i) ranges of 10.7-176 nM in NG108-15 cells (expressing the rodent B2 receptor) and 0.79-253 nM in Cos-7 cells (expressing the human B2 receptor). There was no evidence of agonist activity with any of the nonpeptides in any of the cell lines tested. In vivo, oral administration of compound 19c reversed FCA-induced and turpentine-induced mechanical hyperalgesia in rodents with ED50 values of 0.027 and 0.32 micromol/kg, respectively. The selectivity profiles of compounds (S)-14f and (S)-14g were also assessed to determine the conformational and/or steric preferences of the double-ring arrangement. The affinity of (S)-14 g for the human B2 receptor suggested that it may be a hydrophobic interaction with the ethane bridge of the DBS moiety that accounts for the increased potency of compounds (S)-14d,e and 19b,c at this receptor, by favoring a binding mode inaccessible to the unsubstituted diphenylmethyl derivative, (S)-4.

摘要

1-(2-硝基苯基)硫代氨基脲（TSC）衍生物，(S)-1-[4-(4-二苯甲基硫代氨基脲基)-3-硝基苯磺酰基]吡咯烷-2-羧酸[2-[(2-二甲基氨基乙基)甲基氨基]乙基]酰胺（缓激肽抑制剂；(S)-4），最近被披露为一种新型、强效、口服活性的非肽类缓激肽（BK）B2受体拮抗剂。该化合物抑制[3H]BK与表达B2受体的NG108-15细胞膜制剂（啮齿动物神经母细胞瘤-胶质瘤）的特异性结合，其抑制常数（K(i)）为0.5±0.2 nM。化合物(S)-4在大鼠中对弗氏完全佐剂（FCA）诱导的机械性痛觉过敏也显示出口服疗效，半数有效剂量（ED50）值为0.84 μmol/kg。在优化了从TSC骨架伸出的末端结合决定簇后，我们发现用仅15倍的结合亲和力损失就可以取代潜在的毒性硝基和二价硫部分（(S)-14a）。然而，发现缓激肽抑制剂及其同系物对在Cos-7细胞中表达的克隆人B2受体的亲和力要低得多。对迄今合成的TSC系列针对人B2受体进行了筛选，二苯并环庚烷（DBS）药效团成为效力的关键结构要求。引入该基团产生了一系列衍生物（(S)-14d、e和19b-d），在NG108-15细胞（表达啮齿动物B2受体）中的K(i)范围为10.7-176 nM，在Cos-7细胞（表达人B2受体）中的K(i)范围为0.79-253 nM。在所测试的任何细胞系中，没有任何非肽类表现出激动剂活性的证据。在体内，口服化合物19c可逆转啮齿动物中FCA诱导和松节油诱导的机械性痛觉过敏，ED50值分别为0.027和0.32 μmol/kg。还评估了化合物(S)-14f和(S)-14g的选择性谱，以确定双环排列的构象和/或空间偏好。(S)-14 g对人B2受体的亲和力表明，可能是与DBS部分的乙烷桥的疏水相互作用导致化合物(S)-14d、e和19b、c在该受体上效力增加，这是通过有利于未取代的二苯甲基衍生物(S)-4无法进入的结合模式实现的。