8-(3-CHLOROSTYRYL)CAFFEINE (CSC) IS A SELECTIVE ADENOSINE-A2 ANTAGONIST INVITRO AND INVIVO

An adenosine antagonist, 8-(3-chlorostyryl)caffeine (CSC), was shown p reviously to be 520-fold selective for A2a-adenosine receptors in radi oligand binding assays in the rat brain. In reversing agonist effects on adenylate cyclase, CSC was 22-fold selective for A2a receptors in r at pheochromocytoma cells (K(b) 60 nM) vs. A, receptors in rat adipocy tes (K(b) 1.3 muM). Administered i.p. in NIH mice at a dose of 1 mg/kg , CSC shifted the curve for locomotor depression elicited by the A2a-s elective agonist APEC to the right (ED50 value for APEC shifted from 2 0 mug/kg i.p. to 190 mug/kg). CSC had no effect on locomotor depressio n elicited by an ED50 dose of the A1-selective agonist CHA. CSC alone at a dose of 5 mg/kg stimulated locomotor activity by 22% over control values. Coadministration of CSC and the A1-selective antagonist CPX, both at non-stimulatory doses, increased activity by 37% (P < 0.001) o ver CSC alone, suggesting a behavioral synergism of A1- and A2-antagon ist effects in the CNS.