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首页> 外文期刊>Neuropharmacology >Multiple structural elements contribute to voltage-dependent facilitation of neuronal alpha 1C (CaV1.2) L-type calcium channels.
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Multiple structural elements contribute to voltage-dependent facilitation of neuronal alpha 1C (CaV1.2) L-type calcium channels.

机译:多个结构元素有助于神经元α1C(CaV1.2)L型钙通道的电压依赖性促进。

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Voltage- and frequency-dependent facilitation of calcium channel activity has been implicated in a number of key physiological processes. Various mechanisms have been proposed to mediate these regulations, including a switch between channel gating modes, voltage-dependent phosphorylation, and a voltage-dependent deinhibition of G-protein block. Studying such modulation on recombinant Ca channels expressed in oocytes, we previously reported that alpha(1C) L-type calcium channel contrast with non-L type Ca channels by its ability to exhibit facilitation by pre-depolarization (Voltage-dependent facilitation of a neuronal alpha(IC) L-type calcium channel, E. Bourinet et al., EMBO Journal, 1994; 13, 5032-5039). To further analyze this effect, we have investigated the molecular determinants which mediate the differences in voltage-dependent facilitation between "facilitable" alpha(1C) and "non facilitable" alpha(1E) calcium channels. We used a series of chimeras which combine the four transmembrane domains of the two channels. Results show that the four domains of alpha(1C) contribute to facilitation, with domain I being most critical. This domain is required but not sufficient alone to generate facilitation. The minimal requirement to observe the effect is the presence of domain I plus one of the three others. We conclude that similarly to activation gating, voltage-dependent facilitation of alpha(1C) is a complex process which involves multiple structural elements were domains I and III play the major role.
机译:钙通道活性的电压和频率依赖性促进作用与许多关键的生理过程有关。已经提出了各种机制来介导这些调节,包括在通道门控模式之间切换,电压依赖性磷酸化和电压依赖性G蛋白嵌段抑制。研究卵母细胞中表达的重组Ca通道的这种调节作用,我们先前曾报道过alpha(1C)L型钙通道与非L型Ca通道的对比在于其通过去极化作用表现出促进作用的能力(神经元的电压依赖性促进作用) α(IC)L型钙通道,E.Bourinet等,EMBO Journal,1994; 13,5032-5039)。为了进一步分析这种影响,我们研究了介导“易”α(1C)和“不易”α(1E)钙通道之间电压依赖性促进的差异的分子决定簇。我们使用了一系列嵌合体,它们结合了两个通道的四个跨膜结构域。结果表明,alpha(1C)的四个域对促进作用做出了贡献,而域I最关键。此域是必需的,但仅此一个域不足以产生便利。观察效果的最低要求是域I加上其他三个域之一。我们得出的结论是,与激活门控类似,电压依赖性的alpha(1C)促进是一个复杂的过程,涉及多个结构元素,其中I和III域起主要作用。

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