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首页> 美国卫生研究院文献>The Journal of Physiology >Dihydropyridine-sensitive and omega-conotoxin-sensitive calcium channels in a mammalian neuroblastoma-glioma cell line.
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Dihydropyridine-sensitive and omega-conotoxin-sensitive calcium channels in a mammalian neuroblastoma-glioma cell line.

机译:哺乳动物神经母细胞瘤-神经胶质瘤细胞系中的二氢吡啶敏感和ω-芋螺毒素敏感的钙通道。

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1. Pharmacological and kinetic properties of high-voltage-activated (HVA) Ca2+ channel currents were studied using the whole-cell and perforated patch-clamp methods in a mouse neuroblastoma and rat glioma hybrid cell line, NG108-15, differentiated by dibutyryl cyclic AMP or by prostaglandin E1 and theophylline. 2. The HVA currents were separated into two components by use of two organic Ca2+ channel antagonists, omega-conotoxin GVIA (omega CgTX) and a dihydropyridine (DHP) compound, nifedipine. One current component, IDHP, was blocked by nifedipine (Kd = 8.2 nM) and was resistant to omega CgTX. Conversely, the other component, I omega CgTX, was irreversibly blocked by omega CgTX and was resistant to DHPs. Thus, IDHP could be studied in isolation by a short application of omega CgTX, while I omega CgTX could be studied in the presence of nifedipine. 3. The voltage for half-activation of IDHP was smaller than that of I omega CgTX by 13 mV. IDHP was activated at potentials that were subthreshold for voltage-dependent K+ currents of the cell, whereas I omega CgTX was not. 4. Time courses of activation and deactivation of IDHP were faster than those of I omega CgTX. 5. Voltage-dependent inactivation was small for both IDHP and I omega CgTX at any potential. 6. Ca(2+)-dependent inactivation of IDHP was faster and more prominent than that of I omega CgTX. The time course of the Ca(2+)-dependent inactivation of IDHP, but not I omega CgTX, was slowed as the membrane potential was made more positive between -20 and 30 mV, although amplitude of the current was increased. 7. Alkaline earth metal ions carried the two components of IHVA in the same order: Ba2+ greater than Sr2+ greater than Ca2+. 8. Metal ions blocked the two components of IHVA in the same order of potency: Gd3+ greater than La3+ greater than Cd2+ greater than Cu2+ greater than Mn2+ greater than Ni2+. 9. An alkylating agent, N-ethylmaleimide (NEM, 0.1 mM), selectively augmented IDHP by 30%. 10. During the course of cellular differentiation induced by dibutyryl cyclic AMP, IDHP appeared earlier than I omega CgTX. 11. These results indicate that two classes of Ca2+ channels contribute to the HVA currents of this cell line. The DHP-sensitive channel is more apt to generate Ca2+ spikes and Ca2+ plateau potentials than the omega CgTX-sensitive channel.
机译:1.使用全细胞和穿孔膜片钳方法研究了小鼠神经母细胞瘤和大鼠神经胶质瘤杂交细胞系NG108-15的高电压激活(HVA)Ca2 +通道电流的药理和动力学特性,并以二丁酰环化AMP或由前列腺素E1和茶碱组成。 2.通过使用两种有机Ca2 +通道拮抗剂,ω-芋螺毒素GVIA(omega CgTX)和二氢吡啶(DHP)化合物硝苯地平将HVA电流分为两个部分。一种当前的成分IDHP被硝苯地平(Kd = 8.2 nM)阻断,并且对欧米茄CgTX具有抗性。相反,其他成分IωCgTX被ωCgTX不可逆转地阻断,并且对DHP具有抗性。因此,IDHP可以通过短暂应用omega CgTX进行单独研究,而I omega CgTX可以在硝苯地平存在下进行研究。 3. IDHP的半激活电压比Iomega CgTX的小13 mV。 IDHP在低于电压依赖性细胞K +电流阈值的电势下被激活,而Imega CgTX未被激活。 4. IDHP激活和停用的时程比Iomega CgTX的时程要快。 5.在任何电位下,IDHP和Imega CgTX的电压依赖性失活都很小。 6. IDHP的Ca(2+)依赖性灭活比Iomega CgTX更快和更突出。 Ca(2+)依赖的IDHP失活的时间进程,但IωCgTX的失活时间却变慢,因为膜电位在-20至30 mV之间变得更正,尽管电流幅度增加了。 7.碱土金属离子以相同的顺序携带IHVA的两个成分:Ba2 +大于Sr2 +大于Ca2 +。 8.金属离子以相同的效力顺序阻断了IHVA的两个成分:Gd3 +大于La3 +大于Cd2 +大于Cu2 +大于Mn2 +大于Ni2 +。 9.烷基化剂N-乙基马来酰亚胺(NEM,0.1 mM)使IDHP选择性增加30%。 10.在由二丁酰环AMP诱导的细胞分化过程中,IDHP的出现早于ωCgTX。 11.这些结果表明,两类Ca2 +通道对该细胞系的HVA电流有贡献。与Omega CgTX敏感通道相比,DHP敏感通道更易于产生Ca2 +尖峰和Ca2 +平台电位。

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