New selective ligands of human cloned melatonin MT1 and MT2 receptors

Abstract

Melatonin has a key role in the circadian rhythm relay to periphery organs. Melatonin exerts its multiple roles mainly through two seven transmembrane domain, G-coupled receptors, namely MT₁ or MT₂ receptors. A pharmacological characterization of these human cloned melatonin hMT₁ and hMT₂ receptors stably expressed in HEK-293 or CHO cells is presented using a 2-[¹²⁵I]-iodo-melatonin binding assay and a [³⁵S]-GTPγS functional assay. Both reference compounds and new chemically diverse ligands were evaluated. Binding affinities at each receptor were found to be comparable on either HEK-293 or CHO cell membranes. Novel non-selective or selective hMT₁ and hMT₂ ligands are described. The [³⁵S]-GTPγS functional assay was used to define the functional activity of these compounds which included partial, full agonist and/or antagonist activity. None of the compounds acted as an inverse agonist. We report new types of selective antagonists, such as S 25567 and S 26131 for MT₁ and S 24601 for MT₂. These studies brought other new molecular tools such as the selective MT₁ agonist, S 24268, as well as the non-selective antagonist, S 22153. Finally, we also discovered S 25150, the most potent melatonin receptor agonist, so far reported in the literature.