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来自东方漏斗蛛的新型昆虫选择性毒素对钠通道门控具有独特的钟形电压依赖性调节作用。

Unique bell-shaped voltage-dependent modulation of Na+ channel gating by novel insect-selective toxins from the spider Agelena orientalis.

作者信息

Billen Bert, Vassilevski Alexander, Nikolsky Anton, Debaveye Sarah, Tytgat Jan, Grishin Eugene

机构信息

Laboratory of Toxicology, University of Leuven, KU Leuven, Campus Gasthuisberg O&N2, Herestraat 49, PO Box 922, B-3000 Leuven, Belgium.

出版信息

J Biol Chem. 2010 Jun 11;285(24):18545-54. doi: 10.1074/jbc.M110.125211. Epub 2010 Apr 12.

Abstract

Spider venoms provide a highly valuable source of peptide toxins that act on a wide diversity of membrane-bound receptors and ion channels. In this work, we report isolation, biochemical analysis, and pharmacological characterization of a novel family of spider peptide toxins, designated beta/delta-agatoxins. These toxins consist of 36-38 amino acid residues and originate from the venom of the agelenid funnel-web spider Agelena orientalis. The presented toxins show considerable amino acid sequence similarity to other known toxins such as mu-agatoxins, curtatoxins, and delta-palutoxins-IT from the related spiders Agelenopsis aperta, Hololena curta, and Paracoelotes luctuosus. beta/delta-Agatoxins modulate the insect Na(V) channel (DmNa(V)1/tipE) in a unique manner, with both the activation and inactivation processes being affected. The voltage dependence of activation is shifted toward more hyperpolarized potentials (analogous to site 4 toxins) and a non-inactivating persistent Na(+) current is induced (site 3-like action). Interestingly, both effects take place in a voltage-dependent manner, producing a bell-shaped curve between -80 and 0 mV, and they are absent in mammalian Na(V) channels. To the best of our knowledge, this is the first detailed report of peptide toxins with such a peculiar pharmacological behavior, clearly indicating that traditional classification of toxins according to their binding sites may not be as exclusive as previously assumed.

摘要

蜘蛛毒液是肽毒素的重要来源,这些肽毒素作用于多种膜结合受体和离子通道。在本研究中,我们报告了一种新的蜘蛛肽毒素家族——β/δ-阿加毒素的分离、生化分析及药理学特性。这些毒素由36 - 38个氨基酸残基组成,源自东方漏斗网蜘蛛(Agelena orientalis)的毒液。所呈现的毒素与其他已知毒素,如来自相关蜘蛛美国漏斗网蜘蛛(Agelenopsis aperta)的μ-阿加毒素、曲腹蛛(Hololena curta)的curtatoxins以及黄斑曲腹蛛(Paracoelotes luctuosus)的δ-帕卢毒素-IT,在氨基酸序列上有相当程度的相似性。β/δ-阿加毒素以独特的方式调节昆虫钠通道(DmNa(V)1/tipE),其激活和失活过程均受影响。激活的电压依赖性向更超极化的电位偏移(类似于4位点毒素),并诱导出非失活的持续性钠电流(类似3位点作用)。有趣的是,这两种效应均以电压依赖性方式发生,在- 80至0 mV之间产生钟形曲线,而在哺乳动物钠通道中则不存在。据我们所知,这是关于具有这种特殊药理行为的肽毒素的首次详细报告,清楚地表明根据毒素结合位点进行的传统分类可能不像以前认为的那样具有排他性。

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