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An insecticide resistance-breaking mosquitocide targeting inward rectifier potassium channels in vectors of Zika virus and malaria

机译:针对寨卡病毒和疟疾媒介中向内整流钾通道的杀虫剂抗性灭蚊剂

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摘要

Insecticide resistance is a growing threat to mosquito control programs around the world, thus creating the need to discover novel target sites and target-specific compounds for insecticide development. Emerging evidence suggests that mosquito inward rectifier potassium (Kir) channels represent viable molecular targets for developing insecticides with new mechanisms of action. Here we describe the discovery and characterization of VU041, a submicromolar-affinity inhibitor of Anopheles (An.) gambiae and Aedes (Ae.) aegypti Kir1 channels that incapacitates adult female mosquitoes from representative insecticide-susceptible and -resistant strains of An. gambiae (G3 and Akron, respectively) and Ae. aegypti (Liverpool and Puerto Rico, respectively) following topical application. VU041 is selective for mosquito Kir channels over several mammalian orthologs, with the exception of Kir2.1, and is not lethal to honey bees. Medicinal chemistry was used to develop an analog, termed VU730, which retains activity toward mosquito Kir1 but is not active against Kir2.1 or other mammalian Kir channels. Thus, VU041 and VU730 are promising chemical scaffolds for developing new classes of insecticides to combat insecticide-resistant mosquitoes and the transmission of mosquito-borne diseases, such as Zika virus, without harmful effects on humans and beneficial insects.
机译:杀虫剂抗药性对世界各地的蚊子控制计划构成越来越大的威胁,因此需要发现新的目标部位和特定于目标的化合物以开发杀虫剂。新兴证据表明,蚊子内向整流钾通道代表了开发具有新作用机理的杀虫剂的可行分子靶标。在这里,我们描述了VU041的发现和特性,VU041是冈比亚按蚊(An。)和伊蚊(Aees)埃及伊蚊(Ayespti Kir1)的亚微摩尔亲和性抑制剂,它使代表性的易受杀虫剂耐药的An。冈比亚(分别为G3和Akron)和Ae。 aegypti(分别为利物浦和波多黎各)进行局部应用。除了Kir2.1以外,VU041对几种哺乳动物直系同源物的蚊子Kir通道具有选择性,并且对蜜蜂没有致死性。药物化学用于开发类似物,称为VU730,该类似物保留了对蚊Kir1的活性,但对Kir2.1或其他哺乳动物Kir通道没有活性。因此,VU041和VU730是有前途的化学支架,可用于开发新型杀虫剂,以对抗具有抗杀虫剂作用的蚊子和Zika病毒等蚊媒疾病的传播,而又不会对人类和有益昆虫产生有害影响。

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