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一种哺乳动物神经母细胞瘤-胶质瘤细胞系中的二氢吡啶敏感性和ω-芋螺毒素敏感性钙通道。

Dihydropyridine-sensitive and omega-conotoxin-sensitive calcium channels in a mammalian neuroblastoma-glioma cell line.

作者信息

Kasai H, Neher E

机构信息

Abteilung Membranbiophysik, Max Planck Institut für biophysikalische Chemie, Göttingen, Germany.

出版信息

J Physiol. 1992 Mar;448:161-88. doi: 10.1113/jphysiol.1992.sp019035.

Abstract
  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.
摘要
  1. 运用全细胞膜片钳和穿孔膜片钳技术,在经二丁酰环磷酸腺苷或前列腺素E1与茶碱诱导分化的小鼠神经母细胞瘤和大鼠胶质瘤杂交细胞系NG108 - 15中,研究了高电压激活(HVA)Ca2 +通道电流的药理学和动力学特性。2. 通过使用两种有机Ca2 +通道拮抗剂ω - 芋螺毒素GVIA(ωCgTX)和二氢吡啶(DHP)化合物硝苯地平,将HVA电流分离为两个成分。一个电流成分IDHP被硝苯地平阻断(Kd = 8.2 nM),且对ωCgTX有抗性。相反,另一个成分IωCgTX被ωCgTX不可逆地阻断,且对DHP有抗性。因此,通过短暂施加ωCgTX可单独研究IDHP,而在硝苯地平存在的情况下可研究IωCgTX。3. IDHP的半激活电压比IωCgTX小13 mV。IDHP在低于细胞电压依赖性K +电流阈值的电位下被激活,而IωCgTX则不然。4. IDHP的激活和失活时间进程比IωCgTX快。5. 在任何电位下,IDHP和IωCgTX的电压依赖性失活都很小。6. IDHP的Ca(2 +)依赖性失活比IωCgTX更快且更显著。当膜电位在 - 20至30 mV之间更正时,IDHP的Ca(2 +)依赖性失活时间进程(而非IωCgTX)虽电流幅度增加但减慢。7. 碱土金属离子携带IHVA的两个成分的顺序相同:Ba2 +>Sr2 +>Ca2 +。8. 金属离子以相同的效力顺序阻断IHVA的两个成分:Gd3 +>La3 +>Cd2 +>Cu2 +>Mn2 +>Ni2 +。9. 一种烷基化剂N - 乙基马来酰亚胺(NEM,0.1 mM)选择性地使IDHP增加30%。10. 在由二丁酰环磷酸腺苷诱导的细胞分化过程中,IDHP比IωCgTX更早出现。11. 这些结果表明,两类Ca2 +通道对该细胞系的HVA电流有贡献。DHP敏感通道比ωCgTX敏感通道更易于产生Ca2 +尖峰和Ca2 +平台电位。

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