High frequency stimulation (HFS) is used to treat a variety of neurological diseases, yet its underlying therapeutic action is not fully elucidated. Previously, we reported that HFS-induced elevation in [K⁺]_e or bath perfusion of raised K⁺_e depressed rat entopeduncular nucleus (EP) neuronal activity via an enhancement of an ionic conductance leading to marked depolarization. Herein, we show that the hyperpolarization-activated (I_h) channel mediates the HFS or K⁺-induced depression of EP neuronal activity. The perfusion of an Ih channel inhibitor, 50 µM ZD7288 or 2 mM CsCl, increased input resistance by 23.5 ± 7% (ZD7288) or 35 ± 10% (CsCl), hyperpolarized cells by 3.4 ± 1.7 mV (ZD7288) or 2.3 ± 0.9 mV (CsCl) and decreased spontaneous action potential (AP) frequency by 51.5 ± 12.5% (ZD7288) or 80 ± 13.5% (CsCl). The I_h sag was absent with either treatment suggesting a block of I_h channel activity. Inhibition of the I_h channel prior to HFS or 6 mM K⁺ perfusion not only prevented the previously observed decrease in AP frequency, but increased neuronal activity. Under voltage-clamp conditions, I_h currents were enhanced in the presence of 6 mM K⁺. Calcium is also involved in the depression of EP neuronal activity, since its removal during raised K⁺_e application prevented this attenuation and blocked the Ih sag. We conclude that enhancement of Ih channel activity initiates the HFS- and K⁺-induced depression of EP neuronal activity. This mechanism could underlie the inhibitory effects of HFS used in deep brain stimulation in output basal ganglia nuclei.