Mechanisms of α-adrenergic potentiation of ventricular arrhythmias in dogs with inherited arrhythmic sudden death

Objective: In German shepherd dogs having inherited arrhythmias and sudden death, pause-dependent arrhythmias are triggered by early afterdepolarizations (EADs) originating from left ventricular (LV) Purkinje fibers (PF). Heterogeneity of LV repolarization provides the arrhythmogenic substrate. To elucidate the mechanisms whereby α-adrenergic stimulation exacerbates these arrhythmias we tested the effects of phenylephrine on both arrhythmogenic trigger and substrate. Methods and results: We used microelectrode techniques to record action potentials from LV and right ventricular (RV) PF and from midmyocardial sections of anteroseptal, anterobasal and posterobasal LV wall of unafflicted and afflicted dogs. EADs occurred spontaneously in 8 of 12 LV PF and in no RV PF from afflicted dogs and in no PF from unafflicted dogs. In LV PF from afflicted dogs, phenylephrine (10⁻⁹–10⁻⁵ M) concentration-dependently decreased membrane potential, induced abnormal automaticity at membrane potentials from −65 to −45 mV in 6 LV PF and potentiated EADs in another 6. To determine the mechanisms of membrane depolarization we studied phenylephrine effects on I_K1 in voltage-clamped single LV and RV PF cells from afflicted dogs. In LV PF, phenylephrine (10⁻⁵ M) reduced I_K1 over the range of −120 to −40 mV and had no effects on RV PF. Regional heterogeneity of LV repolarization was observed in afflicted dogs only. Phenylephrine had no effects on repolarization in either group. Conclusion(s): α-adrenergic stimulation exacerbates arrhythmias in afflicted dogs by increasing the arrhythmogenic trigger while leaving the substrate unchanged. Decrease in I_K1 contributes importantly to α-adrenergic effects on LV PF. [Copyright &y& Elsevier]