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电压门控离子通道中电压传感器的结构、功能及修饰

Structure, function, and modification of the voltage sensor in voltage-gated ion channels.

作者信息

Börjesson Sara I, Elinder Fredrik

机构信息

Department of Clinical and Experimental Medicine, Division of Cell Biology, Linköping University, SE-581 85, Linköping, Sweden.

出版信息

Cell Biochem Biophys. 2008;52(3):149-74. doi: 10.1007/s12013-008-9032-5. Epub 2008 Nov 7.

DOI:10.1007/s12013-008-9032-5
PMID:18989792
Abstract

Voltage-gated ion channels are crucial for both neuronal and cardiac excitability. Decades of research have begun to unravel the intriguing machinery behind voltage sensitivity. Although the details regarding the arrangement and movement in the voltage-sensor domain are still debated, consensus is slowly emerging. There are three competing conceptual models: the helical-screw, the transporter, and the paddle model. In this review we explore the structure of the activated voltage-sensor domain based on the recent X-ray structure of a chimera between Kv1.2 and Kv2.1. We also present a model for the closed state. From this we conclude that upon depolarization the voltage sensor S4 moves approximately 13 A outwards and rotates approximately 180 degrees, thus consistent with the helical-screw model. S4 also moves relative to S3b which is not consistent with the paddle model. One interesting feature of the voltage sensor is that it partially faces the lipid bilayer and therefore can interact both with the membrane itself and with physiological and pharmacological molecules reaching the channel from the membrane. This type of channel modulation is discussed together with other mechanisms for how voltage-sensitivity is modified. Small effects on voltage-sensitivity can have profound effects on excitability. Therefore, medical drugs designed to alter the voltage dependence offer an interesting way to regulate excitability.

摘要

电压门控离子通道对于神经元和心脏的兴奋性都至关重要。数十年的研究已开始揭示电压敏感性背后引人入胜的机制。尽管关于电压传感器结构域的排列和运动的细节仍存在争议,但共识正在慢慢形成。有三种相互竞争的概念模型:螺旋桨模型、转运体模型和桨状模型。在本综述中,我们基于Kv1.2和Kv2.1之间嵌合体的最新X射线结构,探讨激活态电压传感器结构域的结构。我们还提出了一种关闭状态的模型。由此我们得出结论,去极化时电压传感器S4向外移动约13埃并旋转约180度,因此与螺旋桨模型一致。S4相对于S3b也有移动,这与桨状模型不一致。电压传感器的一个有趣特征是它部分面向脂质双层,因此既能与膜本身相互作用,也能与从膜到达通道的生理和药理分子相互作用。这种通道调节类型与电压敏感性改变的其他机制一起进行了讨论。对电压敏感性的微小影响可能对兴奋性产生深远影响。因此,设计用于改变电压依赖性的药物为调节兴奋性提供了一种有趣的方式。

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