Comparison of the effects of antiarrhythmic drugs flecainide and verapamil on fKv1.4△N channel currents in Xenopus oocytes
Aim: To study the effects of Na+ channel blocker flecainide and L-type Ca^2+ channel antagonist verapamil on the voltage-gated fKvl.4AN channel, an N-terminal-deleted mutant of the ferret Kvl.4 K+ channel. Methods: fKvl.4hN channels were stably expressed in Xenopus oocytes. The K^+ currents were rec...
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| Published in | Acta pharmacologica Sinica Vol. 34; no. 2; pp. 221 - 230 |
|---|---|
| Main Authors | , , , , , , |
| Format | Journal Article |
| Language | English |
| Published |
Shanghai
Nature Publishing Group
01.02.2013
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| Subjects | |
| Online Access | Get full text |
| ISSN | 1671-4083 1745-7254 |
| DOI | 10.1038/aps.2012.157 |
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| Abstract | Aim: To study the effects of Na+ channel blocker flecainide and L-type Ca^2+ channel antagonist verapamil on the voltage-gated fKvl.4AN channel, an N-terminal-deleted mutant of the ferret Kvl.4 K+ channel. Methods: fKvl.4hN channels were stably expressed in Xenopus oocytes. The K^+ currents were recorded using a two-electrode voltage-clamp technique. The drugs were administered through superfusion. Results: fKvl.4AN currents displayed slow inactivation, with a half-inactivation potential of -41.74 mV and a slow recovery from inactivation (T=1.90 S at -90 mV). Flecainide and verapamil blocked the currents with ICso values of 512.29+56.92 and 260.71+18.50 pmol/L, respectively. The blocking action of the drugs showed opposite voltage-dependence: it was enhanced with depolarization for flecainide, and was attenuated with depolarization for verapamil. Both the drugs exerted state-dependent blockade on fKvl.4AN currents, but verapamil showed a stronger use-dependent blockage compared with flecainide. Flecainide accelerated the C-type inactivation rate without affecting the recovery kinetics and the steady-state activation. Verapamil also accelerated the inactivation kinetics of the currents, but unlike flecainide, it affected both the recovery and the steady-state activation, causing slower recovery of fKvl.4AN channel and a depolarizing shift of the steady-state activation curve. Conclusion: The results demonstrate that widely used antiarrhythmic drugs flecainide and verapamil substantially inhibit fKvl.4hN channels expressed in Xenopus oocytes by binding to the open state of the channels. Therefore, caution should be taken when these drugs are administered in combination with K^+ channel blockers to treat arrhythmia. |
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| AbstractList | Aim: To study the effects of Na+ channel blocker flecainide and L-type Ca^2+ channel antagonist verapamil on the voltage-gated fKvl.4AN channel, an N-terminal-deleted mutant of the ferret Kvl.4 K+ channel. Methods: fKvl.4hN channels were stably expressed in Xenopus oocytes. The K^+ currents were recorded using a two-electrode voltage-clamp technique. The drugs were administered through superfusion. Results: fKvl.4AN currents displayed slow inactivation, with a half-inactivation potential of -41.74 mV and a slow recovery from inactivation (T=1.90 S at -90 mV). Flecainide and verapamil blocked the currents with ICso values of 512.29+56.92 and 260.71+18.50 pmol/L, respectively. The blocking action of the drugs showed opposite voltage-dependence: it was enhanced with depolarization for flecainide, and was attenuated with depolarization for verapamil. Both the drugs exerted state-dependent blockade on fKvl.4AN currents, but verapamil showed a stronger use-dependent blockage compared with flecainide. Flecainide accelerated the C-type inactivation rate without affecting the recovery kinetics and the steady-state activation. Verapamil also accelerated the inactivation kinetics of the currents, but unlike flecainide, it affected both the recovery and the steady-state activation, causing slower recovery of fKvl.4AN channel and a depolarizing shift of the steady-state activation curve. Conclusion: The results demonstrate that widely used antiarrhythmic drugs flecainide and verapamil substantially inhibit fKvl.4hN channels expressed in Xenopus oocytes by binding to the open state of the channels. Therefore, caution should be taken when these drugs are administered in combination with K^+ channel blockers to treat arrhythmia. To study the effects of Na(+) channel blocker flecainide and L-type Ca(2+) channel antagonist verapamil on the voltage-gated fKv1.4ΔN channel, an N-terminal-deleted mutant of the ferret Kv1.4 K(+) channel. fKv1.4ΔN channels were stably expressed in Xenopus oocytes. The K(+) currents were recorded using a two-electrode voltage-clamp technique. The drugs were administered through superfusion. fKv1.4ΔN currents displayed slow inactivation, with a half-inactivation potential of -41.74 mV and a slow recovery from inactivation (τ=1.90 s at -90 mV). Flecainide and verapamil blocked the currents with IC(50) values of 512.29 ± 56.92 and 260.71 ± 18.50 μmol/L, respectively. The blocking action of the drugs showed opposite voltage-dependence: it was enhanced with depolarization for flecainide, and was attenuated with depolarization for verapamil. Both the drugs exerted state-dependent blockade on fKv1.4ΔN currents, but verapamil showed a stronger use-dependent blockage compared with flecainide. Flecainide accelerated the C-type inactivation rate without affecting the recovery kinetics and the steady-state activation. Verapamil also accelerated the inactivation kinetics of the currents, but unlike flecainide, it affected both the recovery and the steady-state activation, causing slower recovery of fKv1.4ΔN channel and a depolarizing shift of the steady-state activation curve. The results demonstrate that widely used antiarrhythmic drugs flecainide and verapamil substantially inhibit fKv1.4ΔN channels expressed in Xenopus oocytes by binding to the open state of the channels. Therefore, caution should be taken when these drugs are administered in combination with K(+) channel blockers to treat arrhythmia. |
| Author | Hui CHEN Dong ZHANG Sheng-ping CHAO Jiang-hua REN Lin XU Xue-jun JIANG Shi-min WANG |
| AuthorAffiliation | Department of Cardiology, Zhongnan Hospital of Wuhan University, Wuhan 430071, China 'Department of Cardiology, RenminHospital of Wuhan University, Wuhan 430073, China |
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| DOI | 10.1038/aps.2012.157 |
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| Notes | Aim: To study the effects of Na+ channel blocker flecainide and L-type Ca^2+ channel antagonist verapamil on the voltage-gated fKvl.4AN channel, an N-terminal-deleted mutant of the ferret Kvl.4 K+ channel. Methods: fKvl.4hN channels were stably expressed in Xenopus oocytes. The K^+ currents were recorded using a two-electrode voltage-clamp technique. The drugs were administered through superfusion. Results: fKvl.4AN currents displayed slow inactivation, with a half-inactivation potential of -41.74 mV and a slow recovery from inactivation (T=1.90 S at -90 mV). Flecainide and verapamil blocked the currents with ICso values of 512.29+56.92 and 260.71+18.50 pmol/L, respectively. The blocking action of the drugs showed opposite voltage-dependence: it was enhanced with depolarization for flecainide, and was attenuated with depolarization for verapamil. Both the drugs exerted state-dependent blockade on fKvl.4AN currents, but verapamil showed a stronger use-dependent blockage compared with flecainide. Flecainide accelerated the C-type inactivation rate without affecting the recovery kinetics and the steady-state activation. Verapamil also accelerated the inactivation kinetics of the currents, but unlike flecainide, it affected both the recovery and the steady-state activation, causing slower recovery of fKvl.4AN channel and a depolarizing shift of the steady-state activation curve. Conclusion: The results demonstrate that widely used antiarrhythmic drugs flecainide and verapamil substantially inhibit fKvl.4hN channels expressed in Xenopus oocytes by binding to the open state of the channels. Therefore, caution should be taken when these drugs are administered in combination with K^+ channel blockers to treat arrhythmia. Kv1.4; fKvl.4△N channel; Xenopus oocytes; antiarrhythmic drugs; flecainide; verapamil; activation; C-type inactivation; Na^+channel blockers; Ca2^+channel antagonists 31-1347/R ObjectType-Article-1 SourceType-Scholarly Journals-1 ObjectType-Feature-2 content type line 14 |
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| Snippet | Aim: To study the effects of Na+ channel blocker flecainide and L-type Ca^2+ channel antagonist verapamil on the voltage-gated fKvl.4AN channel, an... To study the effects of Na(+) channel blocker flecainide and L-type Ca(2+) channel antagonist verapamil on the voltage-gated fKv1.4ΔN channel, an... |
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| SubjectTerms | Antiarrhythmics N通道 抗心律失常 氟 电流 维拉帕米 药物 钙通道阻滞剂 非洲爪蟾卵母细胞 |
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| Title | Comparison of the effects of antiarrhythmic drugs flecainide and verapamil on fKv1.4△N channel currents in Xenopus oocytes |
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