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首页> 外文期刊>The Journal of Physiology >Voltage-dependent calcium channels of dog basilar artery.
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Voltage-dependent calcium channels of dog basilar artery.

机译:狗基底动脉的电压依赖性钙通道。

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摘要

Electrophysiological and molecular characteristics of voltage-dependent calcium (Ca(2+)) channels were studied using whole-cell patch clamp, polymerase chain reaction and Western blotting in smooth muscle cells freshly isolated from dog basilar artery. Inward currents evoked by depolarizing steps from a holding potential of -50 or -90 mV in 10 mm barium consisted of low- (LVA) and high-voltage activated (HVA) components. LVA current comprised more than half of total current in 24 (12%) of 203 cells and less than 10% of total current in 52 (26%) cells. The remaining cells (127 cells, 62%) had LVA currents between one tenth and one half of total current. LVA current was rapidly inactivating, slowly deactivating, inhibited by high doses of nimodipine and mibefradil (> 0.3 microM), not affected by omega-agatoxin GVIA (gamma100 nM), omega-conotoxin IVA (1 microM) or SNX-482 (200 nM) and probably carried by T-type Ca(2+) channels based on the presence of messenger ribonucleic acid (mRNA) and protein for Ca(v3.1) and Ca(v3.3) alpha(1) subunits of these channels. LVA currents exhibited window current with a maximum of 13% of the LVA current at -37.4 mV. HVA current was slowly inactivating and rapidly deactivating. It was inhibited by nimodipine (IC(50) = 0.018 microM), mibefradil (IC(50) = 0.39 microM) and omega-conotoxin IV (1 microM). Smooth muscle cells also contained mRNA and protein for L- (Ca(v1.2) and Ca(v1.3)), N- (Ca(v2.2)) and T-type (Ca(v3.1) and Ca(v3.3)) alpha(1) Ca(2+) channel subunits. Confocal microscopy showed Ca(v1.2) and Ca(v1.3) (L-type), Ca(v2.2) (N-type) and Ca(v3.1) and Ca(v3.3) (T-type) protein in smooth muscle cells. Relaxation of intact arteries under isometric tension in vitro to nimodipine (1 microM) and mibefradil (1 microM) but not to omega-agatoxin GVIA (100 nM), omega-conotoxin IVA (1 microM) or SNX-482 (1 microM) confirmed the functional significance of L- and T-type voltage-dependent Ca(2+) channel subtypes but not N-type. These results show that dog basilar artery smooth muscle cells express functional voltage-dependent Ca(2+) channels of multiple types.
机译:电压依赖性钙(Ca(2+))通道的电生理和分子特征是使用全细胞膜片钳,聚合酶链反应和Western印迹法从狗基底动脉新鲜分离的平滑肌细胞中研究的。在10 mm钡中通过从50或-90 mV的保持电位去极化步骤所诱发的流入电流由低(LVA)和高电压激活(HVA)组件组成。 LVA电流在203个单元中的24个(12%)中占总电流的一半以上,而在52个(26%)中则小于10%。其余电池(127个电池,占62%)的LVA电流为总电流的十分之一至一半。 LVA电流迅速失活,缓慢失活,被高剂量尼莫地平和米贝拉地尔(> 0.3 microM)抑制,不受Ω-抗毒素GVIA(γ100nM),Ω-芋螺毒素IVA(1 microM)或SNX-482(200 nM)的影响),并可能由T型Ca(2+)通道根据这些通道的Ca(v3.1)和Ca(v3.3)alpha(1)亚基的信使核糖核酸(mRNA)和蛋白质的存在而携带。 LVA电流表现出窗口电流,在-37.4 mV时最大为LVA电流的13%。 HVA电流缓慢失活并迅速失活。它被尼莫地平(IC(50)= 0.018 microM),米贝地尔(IC(50)= 0.39 microM)和欧米茄伴毒素IV(1 microM)抑制。平滑肌细胞还包含L-(Ca(v1.2)和Ca(v1.3)),N-(Ca(v2.2))和T型(Ca(v3.1)和Ca (v3.3))alpha(1)Ca(2+)通道亚基。共聚焦显微镜显示Ca(v1.2)和Ca(v1.3)(L型),Ca(v2.2)(N型)和Ca(v3.1)和Ca(v3.3)(T-类型)在平滑肌细胞中的蛋白质。在体外等轴测张力下,对尼莫地平(1 microM)和米贝地尔(1 microM)的完整动脉舒张,但对Ω-抗毒素GVIA(100 nM),Ω-芋螺毒素IVA(1 microM)或SNX-482(1 microM)的松弛L和T型电压依赖性Ca(2+)通道亚型而不是N型的功能意义。这些结果表明,狗基底动脉平滑肌细胞表达多种类型的功能性电压依赖的Ca(2+)通道。

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