首页> 美国卫生研究院文献>The Journal of Physiology >Na+ channels in cardiac and neuronal cells derived from a mouse embryonal carcinoma cell line.
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Na+ channels in cardiac and neuronal cells derived from a mouse embryonal carcinoma cell line.

机译:源自小鼠胚胎癌细胞系的心脏和神经元细胞中的Na +通道。

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摘要

1. Cells from a pluripotent murine embryonal carcinoma cell line (P19) were differentiated in vitro into cells with neurone- and cardiac-like phenotypes. Cells treated with 0.5 microM retinoic acid developed into neurone-like cells possessing extensive neurites. Dimethyl sulphoxide treatment (0.5%) produced large, spontaneously contracting cell aggregates with many properties of cardiac cells. 2. The neurone- and cardiac-like cells contained voltage-sensitive Na+ channels with properties similar to those of native neuronal and cardiac cells. 3. We used whole-cell patch clamp techniques to measure inward currents from the neurone- and cardiac-like cells. Undifferentiated (untreated) cells had only small inward currents (peak of -0.15 nA in 150 mM external Na+). The peak inward current in the neurone-like and cardiac-like cells was -1.2 nA (in 154 mM external Na+) and -2.8 nA (in only 46 mM Na+), respectively. These large currents were absent when the external solution contained no Na+. 4. Tetrodotoxin (TTX) blocked the Na+ currents in the neurone- and cardiac-like cells in a dose-dependent manner. The Kd for TTX block of the Na+ current in the neurone-like cells was 6.7 nM. The Na+ current in the cardiac-like cells was much more resistant to TTX; the half-blocking concentration was two orders of magnitude higher, 710 nM. 5. The kinetic properties of the Na+ channel currents in the neurone- and cardiac-like cells were similar but developed over somewhat different voltage ranges. The voltage sensitivity of activation was similar in both cell types but the activation mid-point voltage was different: -12 mV in the neuronal cells and -34 mV for cardiac cells. Inactivation of the neuronal Na+ channels had a mid-point near -47 mV and was more sensitive to the membrane voltage than inactivation of the cardiac channels. The mid-point of inactivation for the cardiac Na+ channels was -80 mV.
机译:1.将多能小鼠胚胎癌细胞系(P19)的细胞体外分化为具有神经元和心脏样表型的细胞。用0.5 microM视黄酸处理的细胞发展成为具有大量神经突的神经元样细胞。二甲基亚砜处理(0.5%)可产生大的,自发收缩的细胞聚集体,具有心肌细胞的许多特性。 2.神经元和心脏样细胞包含电压敏感的Na +通道,其性质与天然神经元和心脏细胞相似。 3.我们使用全细胞膜片钳技术来测量神经元和心脏样细胞的内向电流。未分化(未处理)的细胞仅具有较小的内向电流(在150 mM外部Na +中达到-0.15 nA的峰值)。神经元样细胞和心脏样细胞的最大内向电流分别为-1.2 nA(在154 mM的外部Na +中)和-2.8 nA(仅在46 mM的Na +中)。当外部溶液不含Na +时,没有这些大电流。 4.河豚毒素(TTX)以剂量依赖性方式阻断神经元和心脏样细胞中的Na +电流。神经元样细胞中Na +电流的TTX阻滞Kd为6.7 nM。心脏样细胞中的Na +电流对TTX的抵抗力更强。半封闭浓度要高两个数量级,即710 nM。 5.在神经元样细胞和心脏样细胞中,Na +通道电流的动力学特性相似,但在有些不同的电压范围内发展。两种细胞类型的激活电压敏感性相似,但激活中点电压不同:神经元细胞为-12 mV,心脏细胞为-34 mV。神经元Na +通道的失活具有-47 mV的中点,并且比心脏通道的失活对膜电压更敏感。心脏Na +通道失活的中点为-80 mV。

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