As it has been reported that the depolarization-induced acetylcholine (ACh) release is modulated by activation of presynaptic A₁-adenosine heteroreceptor in hippocampus and various lines of evidence indicate the involvement of adenylate cyclase system in A₁-adenosine post-receptor mechanism in hippocampus, it was attempted to delineate the role of adenylate cyclase system in the A₁-receptor-mediated control of ACh release in this study. Slices from rat hippocampus were incubated with [³H]-choline and the release of the labelled products was evoked by electrical stimulation (3 Hz, 5 Vcm^-1, 2 ms, rectangular pulses), and the influence of various agents on the evoked tritium-outflow was investigated. N⁶-cyclopentyladenosine (CPA), a specific A₁-adenosine receptor agonist, in concentrations ranging from 0.1 to 10μM, decreased the [³H]-ACh release in a dose-dependent manner without the changes of basal rate of release. 8-cyclopentyl-1,3-dipropylxanthine (DPCPX, 1 ~ 10μM), a selective A₁-receptor antagonist, increased the [³H]-ACh release in a dose-related fashion with slight increase of basal tritium-release. And the CPA effects were significantly inhibited by DPCPX (2μM) pretreatment and the dose-response curve produced by CPA was shifted to the right. The responses to N-ethylmaleimide (NEM, 10 & 30μM), a SH-alkylating agent of G-protein, were characterized by increments of the evoked ACh-release and the basal release, and the CPA effect were completely abolished by NEM pretreatment. Forskolin, a specific adenylate cyclase activator, in concentrations ranging from 0.3 to 10μM, increased the evoked ACh-release in a dose-dependent manner and the CPA effects were inhibited by forskolin. These results indicate that the A₁-adenosine heteroreceptor plays an important role in ACh-release via nucleotide-binding protein Gi in the rat hippocampus and that the adenylate cyclase system might be participated in this process.