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蟑螂钠通道结构域IV的第六个跨膜片段在钠通道阻断剂杀虫剂作用中的角色

Role of the sixth transmembrane segment of domain IV of the cockroach sodium channel in the action of sodium channel blocker insecticides.

作者信息

Silver Kristopher S, Nomura Yoshiko, Salgado Vincent L, Dong Ke

机构信息

Department of Entomology, Genetics and Neuroscience Programs, Michigan State University, East Lansing, MI 48824, USA.

出版信息

Neurotoxicology. 2009 Jul;30(4):613-21. doi: 10.1016/j.neuro.2009.03.009. Epub 2009 Apr 8.

Abstract

Sodium channel blocker insecticides (SCBIs), such as indoxacarb and metaflumizone, are a new class of insecticides with a mechanism of action different from those of other insecticides that target sodium channels. SCBIs block sodium channels in a manner similar to local anesthetics (LAs) such as lidocaine. Several residues, particularly F1579 and Y1586, in the sixth transmembrane segment (S6) of domain IV (IV) of rat Na(v)1.4 sodium channels are required for the action of LAs and SCBIs and may form part of overlapping receptor sites. However, the binding site for SCBIs in insect sodium channels remains undefined. We used site-directed mutagenesis, the Xenopus laevis oocyte expression system, and the two-electrode voltage clamp technique to study the effects on SCBI activity of mutating F1817 and Y1824 (analogous to those residues identified in mammalian sodium channels) to alanine, in the voltage-sensitive sodium channel of the German cockroach, Blattella germanica. The mutant channels showed no effect or a marked increase in channel sensitivity to both DCJW (the active metabolite of indoxacarb) and metaflumizone. Thus, it appeared that although the F1817 residue plays a role in the action of SCBIs and that both residues are involved in LA activity in mammalian sodium channels, neither F1817 nor Y1824 are integral determinants of SCBI binding on insect sodium channels. Our results suggest that the receptor site of SCBIs on insect sodium channels may be significantly different from that on mammalian sodium channels.

摘要

钠通道阻断剂杀虫剂(SCBIs),如茚虫威和氰氟虫腙,是一类新型杀虫剂,其作用机制不同于其他靶向钠通道的杀虫剂。SCBIs阻断钠通道的方式类似于利多卡因等局部麻醉剂(LAs)。大鼠Na(v)1.4钠通道结构域IV(IV)的第六跨膜片段(S6)中的几个残基,特别是F1579和Y1586,是LAs和SCBIs发挥作用所必需的,可能构成重叠受体位点的一部分。然而,昆虫钠通道中SCBIs的结合位点仍未明确。我们使用定点诱变、非洲爪蟾卵母细胞表达系统和双电极电压钳技术,研究了在德国小蠊(Blattella germanica)的电压敏感钠通道中,将F1817和Y1824(类似于在哺乳动物钠通道中鉴定出的那些残基)突变为丙氨酸对SCBI活性的影响。突变通道对DCJW(茚虫威的活性代谢物)和氰氟虫腙的通道敏感性没有影响或显著增加。因此,尽管F1817残基在SCBIs的作用中发挥作用,并且这两个残基都参与哺乳动物钠通道中的LA活性,但F1817和Y1824都不是昆虫钠通道上SCBI结合的完整决定因素。我们的结果表明,昆虫钠通道上SCBIs的受体位点可能与哺乳动物钠通道上的受体位点有显著差异。

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