Emedastine:一种有效的,高亲和力的组胺h1受体选择性拮抗剂用于眼部:受体结合和第二信使研究。

N A Sharif, S X Su, J M Yanni
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引用次数: 55

摘要

研究了抗组胺药艾美司丁对鼠脑H1、H2和H3组胺受体结合的[3H]吡啶胺、[3H]噻替丁和[3H] n -甲基组胺的竞争能力。Emedastine对h1受体(解离常数Ki = 1.3 +/- 0.1 nM)的亲和力最高,对H2- (K1 = 49,067 +/- 11,113 nM)和h3受体(Ki = 12,430 +/- 1,282 nM)的亲和力较弱。这些数据得出H2:H1、H3:H1和H2:H3受体亲和率分别为37744、9562和4,从而使艾美司汀成为一种非常选择性的H1受体拮抗剂。艾美司汀的H1选择性明显优于吡啶胺(H2:H1、H3:H1和H2:H3的比值分别为11887、12709和1)。同样,酮替芬(858,1752,0.5)、左旋巴巴斯丁(420,82,5)、苯那敏(430,312,1)、氯苯那敏(5700,2216,3)和安他唑啉(1163,1110,1)的受体亲和比表明,这些抗组胺药的h1选择性也明显低于艾美司汀。艾美达斯汀(IC50 = 1.44 +/- 0.3 nM)对组胺诱导的人小梁网细胞磷酸肌肽转换的拮抗作用与其对h1受体的结合亲和力比较好。这些数据表明,emedastine是一种高亲和力和高效的组胺拮抗剂,对h1 -组胺受体具有最高的选择性。
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Emedastine: a potent, high affinity histamine H1-receptor-selective antagonist for ocular use: receptor binding and second messenger studies.

The antihistaminic agent, emedastine, was tested for its ability to compete for [3H]pyrilamine, [3H]tiotidine and [3H]N-methyl histamine binding to rodent brain H1, H2 and H3 histamine receptors, respectively. Emedastine exhibited the highest affinity for H1-receptors (dissociation constant, Ki = 1.3 +/- 0.1 nM), and was considerably weaker at H2- (K1 = 49,067 +/- 11,113 nM) and H3-receptors (Ki = 12,430 +/- 1,282 nM). These data yielded ratios of 37744, 9562 and 4 for H2:H1, H3:H1 and H2:H3 receptor affinities, respectively, thus making emedastine a very selective H1-receptor antagonist. The H1-selectivity of emedastine was considerably superior to that of pyrilamine (H2:H1, H3:H1 and H2:H3 ratios of 11887, 12709 and 1, respectively). Similarly, the respective receptor affinity ratios for ketotifen (858, 1752, 0.5), levocabastine (420, 82, 5), pheniramine (430, 312, 1), chlorpheniramine (5700, 2216, 3) and antazoline (1163, 1110, 1) showed these antihistamines to be also markedly less H1-selective than emedastine. The potency of emedastine (IC50 = 1.44 +/- 0.3 nM) for antagonizing histamine-induced phosphoinositide turnover in human trabecular meshwork cells compared well with its binding affinity at the H1-receptor. These data indicate emedastine to be a high affinity and high potency histamine antagonist with the highest selectivity for the H1-histamine receptor.

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