Expression of the early-gene c-fos is an useful method for studying potential sites of action of drugs active in the CNS. Stimulation of adenosine A 2 A receptors by CGS 21680 (5 mg/kg) induced an increase in Fos-like immunoreactivity in the rat nucleus accumbens shell, while in the rostral pole and core CGS 21680 induced Fos-like immunoreactivity only after a high dose. CGS 21680 (5 mg/kg) stimulated c-fos expression also in the lateral septal nucleus and dorso-medial striatum, but not in the dorso-lateral striatum. A similar pattern of Fos-like immunoreactivity was obtained after administration of the A 2 A agonist HENECA (5 mg/kg) which displays higher selectivity for A 2 A receptors than CGS 21680. Administration of the selective A 2 A antagonist SCH 58261 counteracted CGS 21680-induced Fos-like immunoreactivity. Lesions of the dopaminergic mesostriatal projection by 6-hydroxydopamine and stimulation of dopamine D 2 /D 3 receptors by quinpirole, prevented CGS 21680-induced Fos-like immunoreactivity in the nucleus accumbens shell. The present results show that stimulation of A 2 A receptors induces a profile of c-fos expression similar to that of atypical neuroleptics. A 2 A receptor stimulation has been reported to have dopamine antagonistic actions, it is therefore suggested that A 2 A agonists might have antipsychotic activity without producing extrapyramidal side effects.