论文信息 - Effect of bupivacaine on ATP-dependent potassium channels in rat cardiomyocytes.

Effect of bupivacaine on ATP-dependent potassium channels in rat cardiomyocytes.

Bupivacaine induces fatal arrhythmia when accidentally injected i.v. or overdosed, whereas lidocaine is used as an anti-arrhythmic agent. We have suggested recently that the anti-arrhythmic effect of lidocaine may be explained by suppression of ATP-sensitive potassium (KATP) channels. Therefore, it could be argued that different sensitivities of KATP channels to both drugs could be a reason for their different arrhythmic and anti-arrhythmic properties. In this study, we have investigated the direct action of bupivacaine on KATP channels in cardiomyocytes. The effects of bupivacaine on the cardiac KATP channel were investigated using the patch-clamp technique on enzymatically dissociated cardiomyocytes of adult rats. Bupivacaine was applied to the outer side of excised membrane patches using a multiple-barrel perfusion system. Concentration-response curves indicated that bupivacaine blocked the mean current of the KATP channels at a half-maximum inhibiting concentration (IC50) of 29 mumol litre-1, similar to that reported for lidocaine (43 mumol litre-1). Binding of bupivacaine influenced the gating of this channel, but did not reduce the conductance of the open channel. Bupivacaine and lidocaine were equipotent in blocking KATP channels. However, because of its excessive block of the sodium channel in the inactivated state, block of KATP channels by bupivacaine will only enhance its cardiotoxicity.

[1] G. Hempelmann,et al. ATP-dependent potassium channel in rat cardiomyocytes is blocked by lidocaine. Possible impact on the antiarrhythmic action of lidocaine. , 1996, Circulation.

[2] G. Billman. Role of ATP sensitive potassium channel in extracellular potassium accumulation and cardiac arrhythmias during myocardial ischaemia. , 1994, Cardiovascular research.

[3] Z. Bosnjak,et al. Potassium channel openers attenuate atrioventricular block by bupivacaine in isolated hearts. , 1993, Anesthesia and analgesia.

[4] M. Allessie,et al. Electrophysiologic and arrhythmogenic effects of bupivacaine. A study with high-resolution ventricular epicardial mapping in rabbit hearts. , 1992, Anesthesiology.

[5] N. Castle,et al. Bupivacaine inhibits the transient outward K+ current but not the inward rectifier in rat ventricular myocytes. , 1990, The Journal of pharmacology and experimental therapeutics.

[6] I Findlay,et al. Action potential duration and activation of ATP-sensitive potassium current in isolated guinea-pig ventricular myocytes. , 1990, Biochimica et biophysica acta.

[7] L. Hondeghem,et al. Mechanism for Bupivacaine Depression of Cardiac Conduction: Fast Block of Sodium Channels during the Action Potential with Slow Recovery from Block during Diastole , 1985, Anesthesiology.

[8] A. Noma,et al. ATP-regulated K+ channels in cardiac muscle , 1983, Nature.