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一种害虫防治的新方法——与电压敏感钠通道相互作用的神经毒素组合,以提高选择性和特异性。

A new approach to insect-pest control--combination of neurotoxins interacting with voltage sensitive sodium channels to increase selectivity and specificity.

作者信息

Gordon D

机构信息

CEA, Departement d'Ingenierie et d'Etudes des Proteines, Gif-sur-Yvette, France.

出版信息

Invert Neurosci. 1997 Sep-Dec;3(2-3):103-16. doi: 10.1007/BF02480365.

DOI:10.1007/BF02480365
PMID:9783437
Abstract

Voltage-sensitive sodium channels are responsible for the generation of electrical signals in most excitable tissues and serve as specific targets for many neurotoxins. At least seven distinct classes of neurotoxins have been designated on the basis of physiological activity and competitive binding studies. Although the characterization of the neurotoxin receptor sites was predominantly performed using vertebrate excitable preparations, insect neuronal membranes were shown to possess similar receptor sites. We have demonstrated that the two mutually competing anti-insect excitatory and depressant scorpion toxins, previously suggested to occupy the same receptor site, bind to two distinct receptors on insect sodium channels. The latter provides a new approach to their combined use in insect control strategy. Although the sodium channel receptor sites are topologically separated, there are strong allosteric interactions among them. We have shown that the lipid-soluble sodium channel activators, veratridine and brevetoxin, reveal divergent allosteric modulation on scorpion alpha-toxins binding at homologous receptor sites on mammalian and insect sodium channels. The differences suggest a functionally important structural distinction between these channel subtypes. The differential allosteric modulation may provide a new approach to increase selective activity of pesticides on target organisms by simultaneous application of allosterically interacting drugs, designed on the basis of the selective toxins. Thus, a comparative study of neurotoxin receptor sites on mammalian and invertebrate sodium channels may elucidate the structural features involved in the binding and activity of the various neurotoxins, and may offer new targets and approaches to the development of highly selective pesticides.

摘要

电压敏感性钠通道负责在大多数可兴奋组织中产生电信号,并作为许多神经毒素的特定作用靶点。根据生理活性和竞争性结合研究,至少已确定了七类不同的神经毒素。尽管神经毒素受体位点的表征主要是使用脊椎动物可兴奋制剂进行的,但已证明昆虫神经元膜具有类似的受体位点。我们已经证明,之前认为占据相同受体位点的两种相互竞争的抗昆虫兴奋性和抑制性蝎毒素,实际上结合在昆虫钠通道上的两个不同受体上。这为它们在昆虫控制策略中的联合使用提供了一种新方法。尽管钠通道受体位点在拓扑结构上是分开的,但它们之间存在强烈的变构相互作用。我们已经表明,脂溶性钠通道激活剂藜芦碱和短裸甲藻毒素,对蝎α毒素在哺乳动物和昆虫钠通道同源受体位点上的结合表现出不同的变构调节。这些差异表明这些通道亚型之间在功能上存在重要的结构区别。这种变构调节差异可能通过同时应用基于选择性毒素设计的变构相互作用药物,为提高农药对目标生物体的选择性活性提供一种新方法。因此,对哺乳动物和无脊椎动物钠通道上神经毒素受体位点的比较研究,可能阐明各种神经毒素结合和活性所涉及的结构特征,并可能为开发高选择性农药提供新的靶点和方法。

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Effect of previous scorpion bite(s) on the action of intrathecal bupivacaine: A case control study.既往蝎子蜇伤对鞘内布比卡因作用的影响:一项病例对照研究。
Indian J Anaesth. 2013 May;57(3):236-40. doi: 10.4103/0019-5049.115593.
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Substitutions in the domain III voltage-sensing module enhance the sensitivity of an insect sodium channel to a scorpion beta-toxin.结构域 III 电压感应模块中的取代增强了昆虫钠离子通道对蝎型β-毒素的敏感性。
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Mediators Inflamm. 2010;2010:903295. doi: 10.1155/2010/903295. Epub 2010 Mar 14.
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