Chen Mengli, Du Yuzhe, Nomura Yoshiko, Zhu Guonian, Zhorov Boris S, Dong Ke
Institute of Pesticide and Environmental Toxicology, Zhejiang University, Hangzhou 310029, China; Department of Entomology, Genetics and Neuroscience Programs, Michigan State University, East Lansing, MI48824, USA.
Department of Entomology, Genetics and Neuroscience Programs, Michigan State University, East Lansing, MI48824, USA.
Neurotoxicology. 2017 May;60:197-206. doi: 10.1016/j.neuro.2016.06.009. Epub 2016 Jun 18.
Pyrethroid insecticides exert toxic effects by prolonging the opening of voltage-gated sodium channels. More than 20 sodium channel mutations from arthropod pests and disease vectors have been confirmed to confer pyrethroid resistance. These mutations have been valuable in elucidating the molecular interaction between pyrethroids and sodium channels, including identification of two pyrethroid receptor sites. Previously, two alanine to valine substitutions, one in the pore helix IIIP1 and the other in the linker-helix connecting S4 and S5 in domain III (IIIL45), were found in Drosophila melanogaster mutants that are resistant to DDT and deltamethrin (a type II pyrethroid with an α-cyano group at the phenylbenzyl alcohol position, which is lacking in type I pyrethroids), but their role in target-site-mediated insecticide resistance has not been functionally confirmed. In this study, we functionally examined the two mutations in cockroach sodium channels expressed in Xenopus laevis oocytes. Both mutations caused depolarizing shifts in the voltage dependence of activation, conferred DDT resistance and also resistance to two Type I pyrethroids by almost abolishing the tail currents induced by Type I pyrethroids. In contrast, neither mutation reduced the amplitude of tail currents induced by the Type II pyrethroids, deltamethrin or cypermethrin. However, both mutations accelerated the decay of Type II pyrethroid-induced tail currents, which normally decay extremely slowly. These results provided new insight into the molecular basis of different actions of Type I and Type II pyrethroids on sodium channels. Computer modeling predicts that both mutations may allosterically affect pyrethroid binding.
拟除虫菊酯类杀虫剂通过延长电压门控钠通道的开放时间来发挥毒性作用。已证实节肢动物害虫和病媒中的20多种钠通道突变可导致拟除虫菊酯抗性。这些突变对于阐明拟除虫菊酯与钠通道之间的分子相互作用非常有价值,包括确定两个拟除虫菊酯受体位点。此前,在对滴滴涕和溴氰菊酯(一种II型拟除虫菊酯,在苯苄醇位置有一个α-氰基,I型拟除虫菊酯中没有)具有抗性的黑腹果蝇突变体中,发现了两个丙氨酸到缬氨酸的替换,一个在孔螺旋IIIP1中,另一个在结构域III中连接S4和S5的连接螺旋(IIIL45)中,但它们在靶标位点介导的杀虫剂抗性中的作用尚未得到功能上的证实。在本研究中,我们在非洲爪蟾卵母细胞中表达的蟑螂钠通道上对这两个突变进行了功能研究。这两个突变均导致激活电压依赖性的去极化偏移,赋予了对滴滴涕的抗性以及对两种I型拟除虫菊酯的抗性,几乎消除了I型拟除虫菊酯诱导的尾电流。相比之下,这两个突变均未降低II型拟除虫菊酯溴氰菊酯或氯氰菊酯诱导的尾电流幅度。然而,这两个突变均加速了II型拟除虫菊酯诱导的尾电流的衰减,而正常情况下其衰减极其缓慢。这些结果为I型和II型拟除虫菊酯对钠通道不同作用的分子基础提供了新的见解。计算机模拟预测这两个突变可能通过变构作用影响拟除虫菊酯的结合。