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Covalent activation of retinal rod cGMP-gated channels reveals a functional heterogeneity in the ligand binding sites.视网膜视杆细胞环鸟苷酸门控通道的共价激活揭示了配体结合位点的功能异质性。
J Gen Physiol. 1996 Feb;107(2):169-81. doi: 10.1085/jgp.107.2.169.
2
Opening mechanism of a cyclic nucleotide-gated channel based on analysis of single channels locked in each liganded state.基于对锁定在每种配体结合状态的单通道分析的环核苷酸门控通道开放机制
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Specific labeling and permanent activation of the retinal rod cGMP-activated channel by the photoaffinity analog 8-p-azidophenacylthio-cGMP.通过光亲和类似物8-对叠氮苯甲酰硫代环鸟苷酸对视网膜视杆细胞环鸟苷酸激活通道进行特异性标记和永久性激活。
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Activation of retinal rod cGMP-gated channels: what makes for an effective 8-substituted derivative of cGMP?视网膜视杆细胞环鸟苷酸门控通道的激活:何种因素造就有效的环鸟苷酸8-取代衍生物?
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本文引用的文献

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Amplification and kinetics of the activation steps in phototransduction.光转导中激活步骤的放大与动力学
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2
Transduction mechanisms of vertebrate and invertebrate photoreceptors.脊椎动物和无脊椎动物光感受器的转导机制。
J Biol Chem. 1994 May 20;269(20):14329-32.
3
Molecular mechanism of cyclic-nucleotide-gated channel activation.环核苷酸门控通道激活的分子机制。
Nature. 1994 Nov 24;372(6504):369-74. doi: 10.1038/372369a0.
4
Activation of retinal rod cGMP-gated channels: what makes for an effective 8-substituted derivative of cGMP?视网膜视杆细胞环鸟苷酸门控通道的激活:何种因素造就有效的环鸟苷酸8-取代衍生物?
Biochemistry. 1993 Sep 28;32(38):10089-95. doi: 10.1021/bi00089a026.
5
Specific labeling and permanent activation of the retinal rod cGMP-activated channel by the photoaffinity analog 8-p-azidophenacylthio-cGMP.通过光亲和类似物8-对叠氮苯甲酰硫代环鸟苷酸对视网膜视杆细胞环鸟苷酸激活通道进行特异性标记和永久性激活。
Proc Natl Acad Sci U S A. 1993 Jun 1;90(11):5369-73. doi: 10.1073/pnas.90.11.5369.
6
A new subunit of the cyclic nucleotide-gated cation channel in retinal rods.视网膜视杆细胞中环核苷酸门控阳离子通道的一个新亚基。
Nature. 1993 Apr 22;362(6422):764-7. doi: 10.1038/362764a0.
7
Interactions between divalent cations and the gating machinery of cyclic GMP-activated channels in salamander retinal rods.二价阳离子与蝾螈视网膜视杆细胞中环鸟苷酸激活通道门控机制之间的相互作用。
J Gen Physiol. 1993 Jan;101(1):1-25. doi: 10.1085/jgp.101.1.1.
8
Neurotransmitter action: opening of ligand-gated ion channels.神经递质作用:配体门控离子通道的开放。
Cell. 1993 Jan;72 Suppl:31-41. doi: 10.1016/s0092-8674(05)80026-1.
9
Modulation of the cGMP-gated channel of rod photoreceptor cells by calmodulin.钙调蛋白对视杆光感受器细胞中环鸟苷酸门控通道的调节作用。
Nature. 1993 Jan 7;361(6407):76-9. doi: 10.1038/361076a0.
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Cyclic nucleotide gated channels.环核苷酸门控通道
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视网膜视杆细胞环鸟苷酸门控通道的共价激活揭示了配体结合位点的功能异质性。

Covalent activation of retinal rod cGMP-gated channels reveals a functional heterogeneity in the ligand binding sites.

作者信息

Karpen J W, Brown R L

机构信息

Department of Physiology, University of Colorado School of Medicine, Denver 80262, USA.

出版信息

J Gen Physiol. 1996 Feb;107(2):169-81. doi: 10.1085/jgp.107.2.169.

DOI:10.1085/jgp.107.2.169
PMID:8833339
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2219270/
Abstract

Ion channels gated by the binding of multiple ligands play a critical role in synaptic transmission and sensory transduction. It has been difficult to resolve the contribution of individual binding events to channel gating because ligands are continuously binding and unbinding at each site. In examining the allosteric mechanism of retinal rod cGMP-gated channels, we have circumvented this problem by making use of a cGMP derivative, 8-p-azidophenacylthio-cGMP (APT-cGMP), that can be covalently tethered to the binding sites in the presence of long-wavelength UV light. In excised membrane patches, a population of channels was isolated that contained covalently-attached ligands at all but one site. Activation of these channels by cGMP revealed a previously unknown heterogeneity in the ligand-binding sites. The dose-response relations were much shallower than predicted by single-site activation models, but were well described by models in which there are two populations of sites, in roughly equal proportion, that bind cGMP with apparent affinities that differ by a factor of 25. The two apparent affinities, incorporated into a four-site model of the channel, provided an accurate description of the patch's original dose-response relation. A comparison of results on native and expressed channels suggests that the heterogeneity in the native channel arises at least in part from the presence of two different cGMP-binding subunits.

摘要

由多个配体结合所门控的离子通道在突触传递和感觉转导中起着关键作用。由于配体在每个位点持续地结合和解离,所以很难解析单个结合事件对通道门控的贡献。在研究视网膜视杆细胞环鸟苷酸门控通道的变构机制时,我们通过利用一种环鸟苷酸衍生物8-对叠氮苯甲酰硫基环鸟苷酸(APT-cGMP)解决了这个问题,该衍生物在长波长紫外光存在下可共价连接到结合位点。在切除的膜片上,分离出一群通道,除一个位点外,其余位点均含有共价连接的配体。用环鸟苷酸激活这些通道揭示了配体结合位点中一个先前未知的异质性。剂量-反应关系比单一位点激活模型预测的要平缓得多,但用有两类位点的模型能很好地描述,这两类位点比例大致相等,结合环鸟苷酸的表观亲和力相差25倍。将这两种表观亲和力纳入通道的四位点模型,能准确描述膜片最初的剂量-反应关系。对天然通道和表达通道结果的比较表明,天然通道中的异质性至少部分源于两种不同的环鸟苷酸结合亚基的存在。