Differential Effects of d, l-Sotalol and d-Sotalol on Isoproterenol-Increased Delayed Rectifier Outward Potassium Current in Guinea Pig Single Ventricular Myocytes

The aim of this study was to compare the effects of d, l-Sotalol and dSotalol on the delayed rectifier K+ outward current in the presence of isoproterenol at different concentrations. Time-dependent delayed rectifier K+ outward currents were measured in isolated guinea pig single myocytes using the whole-cell configuration of the patch-clamp technique. Currents were measured in response to 300 ms depolarizing pulses from a holding potential of -40 mV in three experimental protocols [control, isoproterenol (10^(9)mol/L - 10^(-6) mol/L ), and isoproterenol (10^(-9)mol/L - 10^(-6)mol/L ) plus either d, l-Sotalol (10^(-4) mol/L) or d-Sotalol (10^(-4) mol/L)]. IK tail currents were measured upon repolarization to -40 mV. It was found that Ik was significantly amplified in the presence. of isoproterenol (10^(-9) mol/L- 10^(-6) mol/L) plus d-Sotalol. At 10-8 mol/L isoproterenol, Ik was increased by 92. 7%±17. 1 % (P<0. 05) and 54. 3 %±13. 4 % after d-Sotalol addition (P<0. 05). In contrast, d, l-Sotalol completely conteracted the increase of iK by isoproterenol (<10^(-8) mol/L), and compared to control, Ic was decreased by 35. 6 % ±8. 1% at 10^(-8) mol/L isoproterenol plus d, l-Sotalol (P<0. 05). It is concluded that the β-adrenergic blocking property of d, l-Sotalol but not that of dSotalol maintains the delayed rectifier K+ outward current blockade in the presence of isoproterenol in guinea pig myocytes. This might contribute to a superior antiarrhythmic efficacy as compared to d-Sotalol.

Differential effects of d,l-sotalol and d-sotalol on isoproterenol increased delayed rectifier outward potassium current in guinea pig myocytes

Objective Catecholamines antagonize the clinical efficacy of pure class Ⅲ antiarrhythmic agents in vivo. The antiarrhythmic agent d, l sotalol has β adrenergic blocking properties and class Ⅲ activity. However, its d isomer without β blockade has been shown to exert significant proarrhythmia. To determine the role of β adrenergic blocking properties of d, l sotalol on its antiarrhythmic effect, we compared the effects of d, l sotalol and d sotalol on delayed rectifier K + outward current in the presence of isoproterenol at different concentrations. Methods Time dependent delayed rectifier K + outward currents, I K (I Kr and I Ks ) and tail current (I K tail ) were measured in isolated guinea pig myocytes using the whole cell configuration of the patch clamp technique. Currents were measured in response to 300 ms depolarizing pulses from a holding potential of Department of Cardiology, University Hospital Heidelberg, Germany (Yao XZ, Yannoulis NC, Kiehn J and Brachmann J) 40 mV in three experimental protocols [control, isoproterenol (10 9 -10 6 mol/L), and isoproterenol (10 9 -10 6 mol/L) plus either d, l sotalol (10 4 mol/L) or d sotalol (10 4 mol/L)]. I K tail currents were measured upon repolarization to 40 mV. Results Isoproterenol significantly inreased I K and I K tail in a concentration dependent manner. I K was significantly amplified in the presence of isoproterenol (10 9 -10 6 mol/L) plus d sotalol. At 10 8 mol/L isoproterenol, I K was increased by 92.3%±23.7% before and 54.3%±13.4% after d sotalol. In contrast, d, l sotalol strongly suppressed the effect of isoproterenol on I K, and compared to control, I K was decreased by 35.6%±8.1% at 10 8 mol/L isoproterenol. Conclusions The β adrenergic blocking property of d, l sotalol maintains delayed rectifier K + outward current block in the presence of isoproterenol in guinea pig myocytes. This may result in its supperior antiarrhythmic efficacy compared to d sotalol.

豚鼠左心室不同区域细胞Iks电流对缺血反应的差异

目的:研究缺血时豚鼠左心室心内、外膜细胞及M细胞缓慢激活延迟整流钾通道电流（Iks）的变化特性。方法:利用全细胞膜片钳技术观察豚鼠左心室心内、外膜细胞及M细胞Iks变化,利用不同成分浴槽液模拟细胞正常及缺血环境,观察Iks尾电流锋值的变化情况.结果:缺血时,三层细胞Iks均小于正常状态;指令电压小于0 mV时,三层细胞Iks同步减小,减少率无显著性差异,P>0.05。指令电压≥0mV时,M细胞Iks减少程度明显高于心内、外膜细胞,P<0.05;而心内、外膜细胞减少率无显著性差异,P>0.05。结论:缺血时左心室心内、外膜细胞及M细胞Iks减弱,而M细胞Iks减弱更为明显,这可能会增加心室壁电活动不均一性,诱发心律失常。

Effect of Interleukin-1β on I_A and I_K Currents in Cultured Murine Trigeminal Ganglion Neurons

To investigate the effect of intedeukin-1β （IL-1β） on IA and IK currents in cultured murine trigeminal ganglion （TG） neurons, whole-cell patch clamp technique was used to record the IA and IK currents before and after 20 ng/mL IL-1β perfusion. Our results showed that 20 ng/mL IL-1β inhibited IA currents （18.3±10.7）% （n=6, P〈0.05）. IL-1β at 20 ng/mL had no effect on G-V curve of IA but moved the H-infinity curve V0.5 from -36.6±6. 1 mV to-42.4±5.2 mV （n=5, P〈0.01）. However, 20 ng/mL IL-1β had effect on neither the amplitude nor the G-V curve of IK. IL-1β was found to selectively inhibit IA current in TG neurons and the effect may contribute to hyperalgesia under various inflammatory conditions.

乳酸左氧氟沙星对豚鼠心肌细胞电生理的影响

目的:了解乳酸左氧氟沙星(LVFX)对豚鼠心室肌细胞电生理的影响。方法:经腹腔注射不同剂量的LVFX,记录并分析注药后5～360min豚鼠Ⅱ导联心电图的QT间期,以及校正的QT间期(QTc)。采用全细胞膜片钳技术,记录不同浓度LVFX对体外单个心室肌细胞的延迟整流钾电流(IK)的作用。结果:①LVFX给药量为200mg/kg时,心电图QT间期延长19.38%±3.15%(P<0.05);在50mg/kg和100mg/kg等较低剂量时,QT间期延长不明显(P>0.05)。②LVFX抑制IK电流,且抑制作用呈现电压依赖性和浓度依赖性。结论:LVFX可能通过抑制心肌细胞IK电流引起心脏QT间期延长,临床应谨慎使用。

酚噻嗪对豚鼠心室肌细胞动作电位时程和跨膜离子电流作用的研究

通过观察酚噻嗪对豚鼠单心室肌细胞动作电位时程 (APD)及动作电位形成过程中主要离子通道的作用 ,探讨其诱发长QT间期 (LQT)综合征及室性心律失常的可能机制。采用膜片钳技术中的Nystatin 破膜法观察酚噻嗪对豚鼠心室肌细胞APD的作用 ,采用全细胞技术研究酚噻嗪对心室肌细胞动作电位形成过程中主要离子电流的作用。结果 :①在 5Hz剌激频率时 ,10 0 μmol/L酚噻嗪使APD90 延长 2 5 .8%± 3.8% (n =10 ,P <0 .0 1) ,作用呈部分可逆性 ;②在分别持续 2 5 0ms和 10 0 0ms至不同膜电位水平去极化的实验中 ,酚噻嗪对延迟整流钾电流 (IK)尾电流有明显的抑制作用 ,在 +6 0mV持续 2 5 0ms的去极化时 ,5 0 .6 4 %± 6 .4 6 %的IK尾电流受抑制 (n =7,P <0 .0 5 ) ,这一抑制作用呈浓度依赖性 ,半抑制浓度 (IC50 ) =2 5 .98μmol/L ,Hill常数为 0 .75。当采用IK快速激活成分 (IKr)的特异性阻断剂E 4 0 31阻断IKr后 ,酚噻嗪对IK尾电流的阻断作用消失。 30 0 μmol/L酚噻嗪对IKr的抑制作用仍弱于 0 .5mmol/LE 4 0 31。在 10 0 0ms,至 +2 0mV去极化的情况下 ,酚噻嗪对IK尾电流的IC50 为 2 5 .98μmol/L ,这一抑制作用可部分洗脱。受酚噻嗪抑制的电流与IK中IKr具有相似的通道动力学特性 ;③未发现酚噻嗪对IK稳态电流、IK?

Characterization of a Chinese KCNQ1 mutation （R259H） that shortens repolarization and causes short QT syndrome 2

Objectives To evaluate the association between a KCNQ 1 mutation, R259H, and short QT syndrome （SQTS） and to explore the elec- trophysiological mechanisms underlying their association. Methods We performed genetic screening of SQTS genes in 25 probands and their family members （63 patients）. We used direct sequencing to screen the exons and intron-exon boundaries of candidate genes that en- code ion channels which contribute to the repolarization of the ventricular action potential, including KCNQI, KCNH2, KCNE1, KCNE2, KCNJ2, CACNAlc, CACNB2b and CACNA2D1. In one of the 25 SQTS probands screened, we discovered a KCNQ1 mutation, R259H. We cloned R259H and transiently expressed it in HEK-293 cells; then, currents were recorded using whole cell patch clamp techniques. Results R259H-KCNQ 1 showed significantly increased current density, which was approximately 3-fold larger than that of wild type （WT） after a depolarizing pulse at 1 s. The steady state voltage dependence of the activation and inactivation did not show significant differences between the WT and R259H mutation （P 〉 0.05）, whereas the time constant of deactivation was markedly prolonged in the mutant compared with the WT in terms of the test potentials, which indicated that the deactivation of R259H was markedly slower than that of the WT. These results suggested that the R259H mutation can effectively increase the slowly activated delayed rectifier potassium current （Irs） in phase 3 of the cardiac action potential, which may be an infrequent cause of QT interval shortening. Conclusions R259H is a gain-of-function muta- tion of the KCNQ1 channel that is responsible for SQTS2. This is the first time that the R259H mutation was detected in Chinese people.

豚鼠M细胞缓慢激活型延迟整流钾电流对缺血的反应

目的:研究缺血对豚鼠心室M细胞缓慢激活型延迟整流钾通道电流（Iks）的影响。方法:利用全细胞膜片钳技术观察豚鼠心室M细胞Iks,利用不同成分浴槽液模拟细胞正常及缺血环境,观察Iks尾电流锋值的变化情况。结果:指令电压≥0mV时,缺血组电流显著小于正常组,P<0.05;指令电压小于0mV时,两组间无显著性差异,P>0.05。结论:缺血时M细胞Iks显著减弱,可能会增加心室壁电活动不均一性,促使心律失常的发生.

Effect of Cu^2＋ on K^＋ Current in Acutely Isolated Rat Hippocampal Neurons by Whole Cell Patch Clamp Technique

Using the whole cell patch clamp technique, the effect of Cu^2＋on transient outward K^＋current （/to） and delayed rectifier K^＋ current （Idr） was studied in acutely isolated rat hippocampal neurons.Ito and Idr were increased when the concentration of Cu^2＋ was lower than 2 × 10^-5 and 10^-5 tool/L, respectively, and increased ratio was decreased with increasing Cu^2＋concentration in the bath solutions. When the concentration continued to increase to 5× 10^-5 and 2 × 10^- 5 mol/L, the currents were hardly changed, while the concentration was more than 10^-4 and 5 × 10^-5 mol/L, the currents were inhibited remarkably. Cu^2＋ （10^-5 mol/L） did not affect the activation and inactivation process of Ito. The activation curve of Idr was shifted toward positive potential, but 10^-5 mol/L Cu^2＋did not affect slope factor. According to these results, it was considered that Cu^2＋at low concentration in the bath solution could promote Ito and Idr while at high concentration could inhibit them, and change of amplitude was different with different membrane voltage. Conclusion was drawn： Cu^2＋may be involved in the pathophysiologic mechanism of diseases with neuropathological components.

槲皮素对谷氨酸诱导的PC12细胞损伤的保护作用及对海马CA1锥体神经元钾通道的影响(英文)

槲皮素广泛存在于许多药用植物中,属黄酮类化合物,在临床上常用于心血管疾病的治疗。采用四甲基偶氮唑盐比色法(MTT法)及DAPI染色,研究槲皮素(0.5、1、5、10μmol/L)对谷氨酸(10mmol/L)诱导的PC12细胞损伤作用的影响;并进一步研究槲皮素(0.3、3、30μmol/L)对急性分离的海马CA1锥体神经元离子通道的作用。MTT实验结果显示,槲皮素可提高谷氨酸处理组PC12细胞的存活率,并呈现为浓度和时间依赖性(P<0.05);而槲皮素(5μmol/L)与谷氨酸(10mmol/L)共孵育PC12细胞后,DAPI染色结果表明槲皮素可减弱谷氨酸对PC12细胞的损伤。对电生理结果显示,槲皮素对瞬时外向钾电流(IA)和延迟整流钾电流(IK)有显著的抑制作用(P<0.05),表现为浓度依赖性。以上结果提示,槲皮素可能通过抑制海马锥体神经元的外向钾电流进而对谷氨酸诱导的神经损伤起保护作用,这也说明了槲皮素对缺血样损伤的神经具有保护作用。