STRUCTURE‐ACTIVITY RELATIONSHIPS OF CLONIDINE‐ AND TOLAZOLINE‐LIKE COMPOUNDS AT HISTAMINE AND α‐ADRENOCEPTOR SITES
Open Access
- 1 August 1980
- journal article
- Published by Wiley in British Journal of Pharmacology
- Vol. 69 (4) , 679-688
- https://doi.org/10.1111/j.1476-5381.1980.tb07922.x
Abstract
1 Thirty clonidine- and tolazoline-like compounds with differing phenyl ring substituents were tested for agonistic actions at histamine H1-receptors (guinea-pig ileum), histamine H2-receptors (guinea-pig driven right ventricular strips), post-junctional α-adrenoceptors (rat desheathed vas deferens) and pre-junctional α-adrenoceptors (inhibition of sympathetic stimulation in guinea-pig driven left atria). 2 All compounds were inactive at histamine H1-receptors, while 21 of the 30 compounds displayed varying stimulant activity at H2-receptors. 3 At post-junctional α-receptors all 30 compounds produced stimulant actions, whereas at prejunctional α-receptors the compounds displayed either agonistic or antagonistic actions. 4 Thus structure-activity relationships (SAR) could only be validated for histamine H2- and post-junctional α-receptor effects. These studies show that the most potent compounds are those with 2,6-phenyl substituents in which rotation is restricted so that the two rings are aplanar. Electronic effects of the substituents have a greater influence on activity at H2- than at α-receptors. 5 The major difference in SAR involves the influence of substituents in the 3, 4 or 5 positions on the phenyl ring. The presence of these substituents abolish significant activity at H2-receptors, while α-receptor stimulant activity is retained.Keywords
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