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CAD细胞中的电压依赖性离子通道:一种表现出诱导分化的儿茶酚胺能神经元系。

Voltage-dependent ion channels in CAD cells: A catecholaminergic neuronal line that exhibits inducible differentiation.

作者信息

Wang H, Oxford G S

机构信息

Curriculum in Oral Biology, School of Dentistry, University of North Carolina, Chapel Hill, North Carolina 27599, USA.

出版信息

J Neurophysiol. 2000 Dec;84(6):2888-95. doi: 10.1152/jn.2000.84.6.2888.

Abstract

Cell lines derived from tumors engineered in the CNS offer promise as models of specific neuronal cell types. CAD cells are an unusual subclone of a murine cell line derived from tyrosine hydroxylase (TH) driven tumorigenesis, which undergoes reversible morphological differentiation on serum deprivation. Using single-cell electrophysiology we have examined the properties of ion channels expressed in CAD cells. Despite relatively low resting potentials, CAD cells can be induced to fire robust action potentials when mildly artificially hyperpolarized. Correspondingly, voltage-dependent sodium and potassium currents were elicited under voltage clamp. Sodium currents are TTX sensitive and exhibit conventional activation and inactivation properties. The potassium currents reflected two pharmacologically distinguishable populations of delayed rectifier type channels while no transient A-type channels were observed. Using barium as a charge carrier, we observed an inactivating current that was completely blocked by nimodipine and thus associated with L-type calcium channels. On differentiation, three changes in functional channel expression occurred; a 4-fold decrease in sodium current density, a 1.5-fold increase in potassium current density, and the induction of a small noninactivating barium current component. The neuronal morphology, excitability properties, and changes in channel function with differentiation make CAD cells an attractive model for study of catecholaminergic neurons.

摘要

源自中枢神经系统工程化肿瘤的细胞系有望成为特定神经元细胞类型的模型。CAD细胞是源自酪氨酸羟化酶(TH)驱动的肿瘤发生的小鼠细胞系的一个特殊亚克隆,在血清剥夺时会经历可逆的形态分化。我们使用单细胞电生理学研究了CAD细胞中表达的离子通道特性。尽管静息电位相对较低,但当轻度人工超极化时,CAD细胞可被诱导产生强烈的动作电位。相应地,在电压钳制下可引出电压依赖性钠电流和钾电流。钠电流对TTX敏感,并表现出传统的激活和失活特性。钾电流反映了两种药理学上可区分的延迟整流型通道群体,未观察到瞬时A型通道。使用钡作为电荷载体,我们观察到一种失活电流,该电流被尼莫地平完全阻断,因此与L型钙通道相关。在分化过程中,功能性通道表达发生了三个变化;钠电流密度降低4倍,钾电流密度增加1.5倍,以及诱导出一个小的非失活钡电流成分。神经元形态、兴奋性特性以及分化过程中通道功能的变化使CAD细胞成为研究儿茶酚胺能神经元的有吸引力的模型。

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