SYNTHESIS, ABSOLUTE-CONFIGURATION, STEREOSELECTIVITY, AND RECEPTOR SELECTIVITY OF (ALPHA-R,BETA-S)-ALPHA,BETA-DIMETHYLHISTAMINE, A NOVEL HIGHLY POTENT HISTAMINE H-3 RECEPTOR AGONIST

被引:35
作者
LIPP, R
ARRANG, JM
GARBARG, M
LUGER, P
SCHWARTZ, JC
SCHUNACK, W
机构
[1] FREE UNIV BERLIN, INST PHARM, W-1000 BERLIN 33, GERMANY
[2] INSERM, CTR PAUL BROCA, UNITE NEUROBIOL, F-75014 PARIS, FRANCE
[3] FREE UNIV BERLIN, INST CRYSTALLOG, W-1000 BERLIN 33, GERMANY
关键词
D O I
10.1021/jm00101a021
中图分类号
R914 [药物化学];
学科分类号
100701 ;
摘要
Depending on the selected synthetic pathway, structural variations of the neurotransmitter histamine led to mixtures of alpha,beta-dimethylhistamines as well as to the corresponding pure optical isomers. One of these isomers, namely (alphaR,betaS)-alpha,beta-dimethylhistamine, proved to be a highly potent H-3 receptor agonist with exceptional receptor selectivity. The absolute configuration of the compound was determined by X-ray structure analysis of its dihydrobromide using the anomalous dispersion of bromine. The optical purity of both enantiomers of erythro-alpha,beta-dimethylhistamine was checked by H-1 NMR investigations after acylation of the amines with (R)-2-methoxy-2-phenylacetyl chloride. As expected H-3 receptors distinguish in a very strong way between the title compound and its alphaS,betaR-configured enantiomer. The agonistic potency of the latter is 2 orders of magnitude lower than the potency of (alphaR,betaS)-alpha,beta-dimethylhistamine.
引用
收藏
页码:4434 / 4441
页数:8
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