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NG108 - 15杂交细胞中钙通道类型的多样性及特性

Diversity and properties of calcium channel types in NG108-15 hybrid cells.

作者信息

Lukyanetz E A

机构信息

Royal Free Hospital School of Medicine, London, UK.

出版信息

Neuroscience. 1998 Nov;87(1):265-74. doi: 10.1016/s0306-4522(98)00057-8.

DOI:10.1016/s0306-4522(98)00057-8
PMID:9722156
Abstract

We used an integral of the current-voltage relation as a new evaluation of Ca2+ current component composition in NG108-15 hybrid cells. We determined significant changes in the values and composition of Ca2+ currents during cell differentiation. Only low-voltage-activated Ca2+ currents could be observed in undifferentiated cells; after cell differentiation, high-voltage-activated currents appeared and the total Ca2+ current was increased about 30-fold. By pharmacological and biophysical separation, we determined four main types of Ca2+ channels in differentiated cells: approximately 50%, 20% and 17% of N, T and L types, respectively, and 12% of residual current, which is insensitive to classical blockers of low- and high-voltage-activated currents, with the exception of (omega-conotoxin GVIA. All current components displayed kinetics and pharmacological properties similar to neuronal ones. We also established a significant Ca2+ dependence of omega-conotoxin GVIA to inhibit N-type Ca2+ channels: 10 mM Ca2+ in bath solution reduced the toxin efficacy to block N channels three-fold. The residual component fitted the properties of Q-type Ca2+ channels: it was sensitive to (omega-conotoxin GVIA and very similar to the T-type channel with respect to its kinetics; however, the threshold of its activation was closer to the high-voltage-activated component (- 40 mV). Our results show the functional diversity of Ca2+ channels and demonstrate, for the first time, that presumably the Q type of an alpha1A family, which has biophysical and pharmacological properties distinct from the previously described T, L and N types in these cells, is co-expressed in NG108-15 cells.

摘要

我们使用电流-电压关系的积分作为对NG108-15杂交细胞中Ca2+电流成分组成的一种新的评估方法。我们确定了细胞分化过程中Ca2+电流值和组成的显著变化。在未分化细胞中只能观察到低电压激活的Ca2+电流;细胞分化后,出现了高电压激活电流,并且总Ca2+电流增加了约30倍。通过药理学和生物物理学分离,我们确定了分化细胞中四种主要类型的Ca2+通道:分别约50%、20%和17%的N型、T型和L型,以及12%的残余电流,该残余电流对低电压和高电压激活电流的经典阻滞剂不敏感,但对(ω-芋螺毒素GVIA)除外。所有电流成分均表现出与神经元电流相似的动力学和药理学特性。我们还确定了ω-芋螺毒素GVIA抑制N型Ca2+通道对Ca2+有显著依赖性:浴液中10 mM Ca2+使毒素阻断N通道的效力降低了三倍。残余成分符合Q型Ca2+通道的特性:它对(ω-芋螺毒素GVIA)敏感,并且在动力学方面与T型通道非常相似;然而,其激活阈值更接近高电压激活成分(-40 mV)。我们的结果显示了Ca2+通道的功能多样性,并首次证明在NG108-15细胞中可能共表达了α1A家族的Q型,其生物物理学和药理学特性与这些细胞中先前描述的T型、L型和N型不同。

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