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海葵Anthopleura sp.的重组神经毒素对大鼠大脑皮层神经元钠电流的影响。

The effect of recombinant neurotoxins from the sea anemone Anthopleura sp. on sodium currents of rat cerebral cortical neurons.

作者信息

Xiang Hui, Tao Wucheng, Wang Lei, Wang Fang, Xu Anlong

机构信息

School of Life Sciences, Sun Yat-sen (Zhongshan) University, Guangzhou, Guangdong Province 510275, People's Republic of China.

出版信息

Cell Mol Neurobiol. 2008 Dec;28(8):1119-28. doi: 10.1007/s10571-008-9288-8. Epub 2008 Jun 26.

Abstract

We have investigated the action of the recombinant neurotoxins, named Hk7a and Hk2a, whose amino acid sequences differ only in two positions, isolated from the sea anemone Anthopleura sp., on neuronal sodium currents using the whole-cell voltage-clamp techniques. The rat cerebral cortical neurons in primary culture were used for this study. In our experiments, these cells all express tetrodotoxin-sensitive (TTX-S) sodium currents. Under the voltage-clamp condition, application of Hk7a and Hk2a reduced the sodium channel current amplitude and shifted the voltage dependence of activation to more positive potential; while Hk7a produced no significant effect on the voltage at which 50% of the channels were inactivated, Hk2a caused profound hyperpolarizing shift of the voltage-dependent inactivation. Also, both Hk7a and Hk2a increased the time course of recovery from inactivation. In kinetic studies, whereas application of Hk2a slows the time to peak of voltage-gated sodium channel, the time course of fast and slow inactivating component, no significant effect was observed in Hk7a. These results suggested that the difference of key amino acid between Hk7a and Hk2a might contribute to their different action; therefore, they could be used as pharmacological tool to study the structure and function of voltage-gated sodium channel.

摘要

我们使用全细胞电压钳技术,研究了从海葵 Anthopleura sp. 中分离出的名为 Hk7a 和 Hk2a 的重组神经毒素对神经元钠电流的作用,这两种毒素的氨基酸序列仅在两个位置上有所不同。本研究使用了原代培养的大鼠大脑皮质神经元。在我们的实验中,这些细胞均表达对河豚毒素敏感(TTX-S)的钠电流。在电压钳条件下,施加 Hk7a 和 Hk2a 可降低钠通道电流幅度,并使激活的电压依赖性向更正电位移动;虽然 Hk7a 对 50%通道失活时的电压没有显著影响,但 Hk2a 导致电压依赖性失活发生显著的超极化移位。此外,Hk7a 和 Hk2a 均延长了从失活状态恢复的时间进程。在动力学研究中,施加 Hk2a 会减慢电压门控钠通道的峰值时间以及快速和慢速失活成分的时间进程,而 Hk7a 未观察到显著影响。这些结果表明,Hk7a 和 Hk2a 之间关键氨基酸的差异可能导致它们的作用不同;因此,它们可作为药理学工具用于研究电压门控钠通道的结构和功能。

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