Separation of alpha-adrenergic and imidazoline/guanidinium receptive sites 4IGRS) activity in a series of imidazoline analogues of cirazoline

To characterize the structure-activity relationship between alpha(1)-adrenergic receptors and the family of imidazoline/guanidinium receptive sites (IGRS), we synthesized and characterized a series of analogues of cirazoline, an imidazoline with high affinity for alpha(1)-adrenergic receptors and IGRS. Analysis of potency, affinity and efficacy of the synthesized molecules indicate different structure-activity relationships for IGRS and alpha-adrenergic receptors. Cirazoline exhibits a 25-fold higher affinity for IGRS (pK(i) 7.9) than for alpha(1)-adrenergic receptors. Replacement of the cyclopropyl ring with an isopropoxy group resulted in a molecule that was 20-fold more selective for alpha(1)-adrenergic receptors than for IGRS, i.e. a 500-fold increase in selectivity relative to cirazoline. The unsubstituted derivative 3 and the methyl and allyl substituted analogues 4 and 12 are of particular interest: compounds 3 and 4 recognize IGRS with high affinity (pK(i) 7.83 and 8.17) and high selectivity (398 and 123) with respect to the alpha(1)-adrenergic receptor; compound 12 also recognizes IGRS with high affinity (pK(i) 8.08) and high selectivity (228 and 138) with respect to the alpha(2B), and alpha 2(C)-adrenergic receptor subtypes. Thanks to their IGRS selectivity, these compounds represent novel and valuable pharmacological tools for the characterization and elucidation of the physiological role of these novel sites.