Characterization of the interaction of the cervane alkaloid, imperialine, at muscarinic receptors in vitro

Abstract

The action of the cervane alkaloid, imperialine, has been assessed at M₁, M₂ and M₃ receptors in functional assays and at M₁, M₂, M₃ and putative M₄ sites in binding studies. In functional studies, imperialine acted as a selective surmountable antagonist at M₂ receptors in guinea-pig isolated atria and uterus (−log K_B = 7.7 and 7.4, respectively), in comparison to M₁, receptors in canine isolated saphenous vein (−log K_B = 6.9) or M3 receptors in a range of guinea-pig isolated smooth muscles including ileum, trachea, fundus, seminal vesicle or oesophagus (−log K_B = 6.6–6.8). In rat aorta, the −log K_B value at the M₃ receptor (5.9) was slightly, but significantly, lower. In competition radioligand binding studies, imperialine was also selective toward to M2 sites in rat myocardium (−log K_i = 7.2) with respect to M₁ and M₃ sites (rat cerebral cortex, rat submaxillary gland; −log K_i = 6.1 and 5.7, respectively). However, it did not significantly discriminate between rat cardiac M₂ sites and putative M₄ sites in rabbit lung (−log K_i = 6.9). Imperialine resembles the alkaloid himbacine in terms of its pharmacological profile at muscarinic receptor subtypes in that it acts as an M2 selective antagonist with respect to M₁ or M₃ sites. It may also provide a second, commercially available, antagonist with which to discriminate between M₁ and M₄ receptors.