Rapid component IKr of the guinea-pig cardiac delayed rectifier K+ current is inhibited by β1-adrenoreceptor activation, via cAMP/protein kinase A-dependent pathways

Objective: The antiarrhythmic potential of betablockers contributes to their beneficial effects in the treatment of cardiac diseases, although the molecular basis of their class 11 antiarrhythmic action has not been clarified yet. Methods: To investigate a putative functional link between beta-adrenoreceptors and the fast component of cardiac delayed rectifier K+ channels (I-Kr), whole-cell patch-clamp L experiments were performed with isolated guinea-pig ventricular myocytes. Tail currents of I-Kr were measured at -40 mV after short (200 ms) test pulses to +40 mV. Results: After application of the unspecific beta-receptor agonist isoproterenol (10 muM) for 12 min, the I-Kr tail current was decreased by 72%, with an IC50 of 1.4 muM. The specific beta(1)-blocker CGP207120A (10 muM) significantly attenuated the isoproterenol effect (net 24% decrease). The specific beta(1)-agonist xamoterol (10 muM), could mimic the isoproterenol effect (58% decrease). Modulators of beta(2)- or beta(3)-adrenoreceptors were far less effective. When isoproterenol or xamoterol were combined with KT5720 (2.5 muM), a specific inhibitor of protein kinase A (PKA), their effects were drastically reduced, indicating that PKA presumably mediates the beta(1)-adrenergic inhibition of I-Kr. Tail current reductions by cAMP, forskolin, PKA catalytic subunit and a combination of PKA holoenzyme and cAMP support an involvement of PKA in the regulation of I-Kr. Conclusions: The functional link between I-Kr and the beta(1)-adrenergic receptor involving PKA may play an important role in arrhythmogenesis and contribute to the antiarrhythmic action of clinically used beta(1)-blockers. (C) 2002 Elsevier Science B.V. All rights reserved.