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一种具有细胞周期依赖性的新型内向整流钾电流调控哺乳动物神经母细胞瘤细胞的静息电位。

A novel inward-rectifying K+ current with a cell-cycle dependence governs the resting potential of mammalian neuroblastoma cells.

作者信息

Arcangeli A, Bianchi L, Becchetti A, Faravelli L, Coronnello M, Mini E, Olivotto M, Wanke E

机构信息

Department of General Physiology and Biochemistry, University of Milano, Italy.

出版信息

J Physiol. 1995 Dec 1;489 ( Pt 2)(Pt 2):455-71. doi: 10.1113/jphysiol.1995.sp021065.

Abstract
  1. Human and murine neuroblastoma cell lines were used to investigate, by the whole-cell patch-clamp technique, the properties of a novel inward-rectifying K+ current (IIR) in the adjustment of cell resting potential (Vrest), which was in the range -40 to -20 mV. 2. When elicited from a holding potential of 0 mV, IIR was completely inactivated with time constants ranging from 13 ms at -140 mV to 4.5 s at -50 mV. The steady-state inactivation curve (h(V)) was found to be independent of [Na+]o and [K+]o (2-80 mM) and could be fitted to a Boltzmann curve with a steep slope factor of 5-6, and a V1/2 around Vrest. Divalent ion-free extracellular solutions shifted h(V) to the left by about 28 mV. 3. Peak chord conductance, whose maximal value was approximately proportional to the square root of [K+]o, could be fitted to a Boltzmann curve independently of [K+]o, with a V1/2 value around -48 mV and a slope factor of 18. Extracellular Cs+ and Ba2+ blocked the IIR in a concentration- and voltage-dependent manner, but Ba2+ was less effective than it is on classical inward-rectifier channels. 4. Under control culture conditions the values of Vrest and V1/2 of h(V) varied widely among cells. The knowledge of V1/2 proved crucial or the theoretical prediction of Vrest. After cell synchronization in the G0-G1 phase of the cell cycle, or at the G1-S boundaries, the cells reduced their variability of h(V). The same occurred after cell synchronization in G1 by treatment with retinoic acid. 5. The experimental data could be fitted to a classical model of an inward rectifier, after removing the dependence of conductance activation on (V-EK), and incorporating an inactivation with an intrinsic voltage dependence. Moreover, the model predicts, for this novel inward rectifier and in contrast with the classical inward rectifier, the incapacity of maintaining, in physiological media, a Vrest more negative than -35 to -40 mV, which is an important feature of cancer cells.
摘要
  1. 采用全细胞膜片钳技术,利用人源和鼠源神经母细胞瘤细胞系,研究一种新型内向整流钾电流(IIR)在调节细胞静息电位(Vrest)(范围为-40至-20 mV)方面的特性。2. 当从0 mV的钳制电位诱发时,IIR会随时间完全失活,时间常数范围从-140 mV时的13 ms到-50 mV时的4.5 s。稳态失活曲线(h(V))被发现与[Na+]o和[K+]o(2 - 80 mM)无关,并且可以拟合为具有5 - 6的陡坡因子和Vrest附近的V1/2的玻尔兹曼曲线。无二价离子的细胞外溶液使h(V)向左移动约28 mV。3. 峰值弦电导,其最大值大致与[K+]o的平方根成正比,可独立于[K+]o拟合为玻尔兹曼曲线,V1/2值约为-48 mV,斜率因子为18。细胞外的Cs+和Ba2+以浓度和电压依赖性方式阻断IIR,但Ba2+的作用比其对经典内向整流通道的作用弱。4. 在对照培养条件下,Vrest和h(V)的V1/2值在细胞间差异很大。V1/2的知识被证明对Vrest的理论预测至关重要。在细胞周期的G0 - G1期或G1 - S边界进行细胞同步后,细胞降低了h(V)的变异性。在用视黄酸处理使细胞在G1期同步后也出现了同样的情况。5. 在去除电导激活对(V - EK)的依赖性并纳入具有内在电压依赖性的失活后,实验数据可以拟合为内向整流器的经典模型。此外,该模型预测,对于这种新型内向整流器,与经典内向整流器不同,在生理介质中无法维持比-35至-40 mV更负的Vrest,这是癌细胞的一个重要特征。

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