Distinct pharmacology of rat and human histamine H3 receptors:: role of two amino acids in the third transmembrane domain

被引:139
|
作者
Ligneau, X
Morisset, S
Tardivel-Lacombe, J
Gbahou, F
Ganellin, CR
Stark, H
Schunack, W
Schwartz, JC
Arrang, JM
机构
[1] Ctr Paul Broca, INSERM, U109, Unite Neurobiol & Pharmacol Mol, F-75014 Paris, France
[2] UCL, Dept Chem, London WC1H 0AJ, England
[3] Free Univ Berlin, Inst Pharm, D-14195 Berlin, Germany
[4] Bioprojet, F-75003 Paris, France
关键词
histamine; H-3; receptor; G protein-coupled receptors; ciproxifan; thioperamide; I-125]iodoproxyfan; FUB; 349; clobenpropit; site-directed mutagenesis;
D O I
10.1038/sj.bjp.0703712
中图分类号
R9 [药学];
学科分类号
1007 ;
摘要
Starting from the sequence of the human histamine H-3 receptor (hH(3)R) cDNA, we have cloned the corresponding rat cDNA. Whereas the two deduced proteins show 93.5% overall homology and differ only by five amino acid residues at the level of the transmembrane domains (TMs), some ligands displayed distinct affinities. Thioperamide and ciproxifan were about 10 fold more potent at the rat than at the human receptor, whereas FUB 349 displayed a reverse preference. Histamine, (R)alpha -methylhistamine, proxyfan or clobenpropit were nearly equipotent at H-3 receptors of both species. The inverse discrimination patterns of ciproxifan and FUB 349 were partially changed by mutation of one amino acid (V122A), and fully abolished by mutation of two amino acids (A119T and V122A), in TM3 of the rH(3)R located in the vicinity of Asp(114) purported to salt-link the ammonium group of histamine. Therefore, these two residues appear to be responsible for the distinct pharmacology of the H3R in the two species.
引用
收藏
页码:1247 / 1250
页数:4
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