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CaV1.2通道的钙依赖性失活可防止钆离子(Gd3+)阻断:钙离子是否会阻断失活通道的孔道?

Ca2+-dependent inactivation of CaV1.2 channels prevents Gd3+ block: does Ca2+ block the pore of inactivated channels?

作者信息

Babich Olga, Matveev Victor, Harris Andrew L, Shirokov Roman

机构信息

Department of Pharmacology and Physiology, University of Medicine and Dentistry of New Jersey, New Jersey Medical School, Newark, NJ 07103, USA.

出版信息

J Gen Physiol. 2007 Jun;129(6):477-83. doi: 10.1085/jgp.200709734.

Abstract

Lanthanide gadolinium (Gd(3+)) blocks Ca(V)1.2 channels at the selectivity filter. Here we investigated whether Gd(3+) block interferes with Ca(2+)-dependent inactivation, which requires Ca(2+) entry through the same site. Using brief pulses to 200 mV that relieve Gd(3+) block but not inactivation, we monitored how the proportions of open and open-blocked channels change during inactivation. We found that blocked channels inactivate much less. This is expected for Gd(3+) block of the Ca(2+) influx that enhances inactivation. However, we also found that the extent of Gd(3+) block did not change when inactivation was reduced by abolition of Ca(2+)/calmodulin interaction, showing that Gd(3+) does not block the inactivated channel. Thus, Gd(3+) block and inactivation are mutually exclusive, suggesting action at a common site. These observations suggest that inactivation causes a change at the selectivity filter that either hides the Gd(3+) site or reduces its affinity, or that Ca(2+) occupies the binding site at the selectivity filter in inactivated channels. The latter possibility is supported by previous findings that the EEQE mutation of the selectivity EEEE locus is void of Ca(2+)-dependent inactivation (Zong Z.Q., J.Y. Zhou, and T. Tanabe. 1994. Biochem. Biophys. Res. Commun. 201:1117-11123), and that Ca(2+)-inactivated channels conduct Na(+) when Ca(2+) is removed from the extracellular medium (Babich O., D. Isaev, and R. Shirokov. 2005. J. Physiol. 565:709-717). Based on these results, we propose that inactivation increases affinity of the selectivity filter for Ca(2+) so that Ca(2+) ion blocks the pore. A minimal model, in which the inactivation "gate" is an increase in affinity of the selectivity filter for permeating ions, successfully simulates the characteristic U-shaped voltage dependence of inactivation in Ca(2+).

摘要

镧系元素钆(Gd(3+))在选择性过滤器处阻断Ca(V)1.2通道。在此,我们研究了Gd(3+)阻断是否会干扰Ca(2+)依赖性失活,而Ca(2+)依赖性失活需要Ca(2+)通过同一部位进入。使用短暂脉冲至200 mV以解除Gd(3+)阻断但不解除失活,我们监测了在失活过程中开放通道和开放-阻断通道的比例如何变化。我们发现被阻断的通道失活程度要小得多。这对于增强失活的Ca(2+)内流的Gd(3+)阻断来说是预期的。然而,我们还发现,当通过消除Ca(2+)/钙调蛋白相互作用降低失活时,Gd(3+)阻断的程度并未改变,这表明Gd(3+)不会阻断失活的通道。因此,Gd(3+)阻断和失活是相互排斥的,提示在共同位点起作用。这些观察结果表明,失活会导致选择性过滤器发生变化,要么隐藏Gd(3+)位点,要么降低其亲和力,要么Ca(2+)占据失活通道中选择性过滤器的结合位点。后一种可能性得到了先前研究结果的支持,即选择性EEEE位点的EEQE突变不存在Ca(2+)依赖性失活(宗Z.Q.、周J.Y.和田边T. 1994.生物化学与生物物理研究通讯201:1117 - 11123),以及当从细胞外介质中去除Ca(2+)时,Ca(2+)失活的通道传导Na(+)(巴比奇O.、伊萨耶夫D.和希罗科夫R. 2005.生理学杂志565:709 - 717)。基于这些结果,我们提出失活会增加选择性过滤器对Ca(2+)的亲和力,从而使Ca(2+)离子阻断孔道。一个最小模型,其中失活 “门” 是选择性过滤器对渗透离子亲和力的增加,成功模拟了Ca(2+)中失活特征性的U形电压依赖性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/034e/2151623/9f1b31329236/jgp1290477f01.jpg

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