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G3’MTMD3 in the insect GABA receptor subunit, RDL, confers resistance to broflanilide and fluralaner

生物 蛋白质亚单位 昆虫 抗性(生态学) 受体 遗传学 计算生物学 细胞生物学 生态学 基因
作者
Yichi Zhang,Qiu‐Tang Huang,Cheng‐Wang Sheng,Genyan Liu,Kexin Zhang,Zhong‐Qiang Jia,Tao Tang,Xin Mao,Andrew K. Jones,Zhaojun Han,Chunqing Zhao
出处
期刊:PLOS Genetics 卷期号:19 (6): e1010814-e1010814 被引量:5
标识
DOI:10.1371/journal.pgen.1010814
摘要

Meta-diamides (e.g. broflanilide) and isoxazolines (e.g. fluralaner) are novel insecticides that target the resistant to dieldrin (RDL) subunit of insect γ-aminobutyric acid receptors (GABARs). In this study, we used in silico analysis to identify residues that are critical for the interaction between RDL and these insecticides. Substitution of glycine at the third position (G3’) in the third transmembrane domain (TMD3) with methionine (G3’M TMD3 ), which is present in vertebrate GABARs, had the strongest effect on fluralaner binding. This was confirmed by expression of RDL from the rice stem borer, Chilo suppressalis ( Cs RDL) in oocytes of the African clawed frog, Xenopus laevis , where the G3’M TMD3 mutation almost abolished the antagonistic action of fluralaner. Subsequently, G3’M TMD3 was introduced into the Rdl gene of the fruit fly, Drosophila melanogaster , using the CRISPR/Cas9 system. Larvae of heterozygous lines bearing G3’M TMD3 did not show significant resistance to avermectin, fipronil, broflanilide, and fluralaner. However, larvae homozygous for G3’M TMD3 were highly resistant to broflanilide and fluralaner whilst still being sensitive to fipronil and avermectin. Also, homozygous lines showed severely impaired locomotivity and did not survive to the pupal stage, indicating a significant fitness cost associated with G3’M TMD3 . Moreover, the M3’G TMD3 mutation in the mouse Mus musculus α1β2 GABAR increased sensitivity to fluralaner. Taken together, these results provide convincing in vitro and in vivo evidence for both broflanilide and fluralaner acting on the same amino acid site, as well as insights into potential mechanisms leading to target-site resistance to these insecticides. In addition, our findings could guide further modification of isoxazolines to achieve higher selectivity for the control of insect pests with minimal effects on mammals.

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