2-(ARYLALKYLAMINO)ADENOSIN-5'-URONAMIDES - A NEW CLASS OF HIGHLY SELECTIVE ADENOSINE-A2 RECEPTOR LIGANDS

The synthesis and receptor-binding profiles at adenosine receptor subtypes for a series of 2-(arylalkylamino)-adenosin-5'-uronamides is described, Halogenated 2-phenethylamino analogues such as 3e show greater than 200-fold selectivity for the A2 receptor subtype on the basis of rat brain receptor binding. The general structure-activity relationship of this series of compounds is discussed both in terms of potency at A2 receptors as well as receptor subtype selectivity. It is possible to introduce a hydrophilic carboxyalkyl substituent to this series such as in CGS 21680A (3h) and still retain good potency and selectivity for A2 receptors. In addition, functional data in a perfused working rat heart model shows that these compounds possess full agonist properties at A2receptors with 3h having a greater than 1500-fold separation between A2 (coronary vosadilatory) and A1 (negative chronotropic) receptor mediated events. © 1990, American Chemical Society. All rights reserved.