Identification and functional characterization of CYP3002B2, a cytochrome P450 associated with amitraz and flumethrin resistance in the major bee parasite Varroa destructor

IF 4.2 1区 农林科学 Q2 BIOCHEMISTRY & MOLECULAR BIOLOGY
Konstantinos Mavridis , Dimitra Tsakireli , Spyridon Vlogiannitis , Jason Charamis , Inga Siden-Kiamos , Angelina Fathia Osabutey , Victoria Soroker , John Vontas
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引用次数: 0

Abstract

Beekeeping worldwide is increasingly threatened by the parasitic mite Varroa destructor, whose management relies heavily on synthetic acaricides such as amitraz and flumethrin. However, the growing incidence of acaricide resistance in V. destructor presents a significant global challenge to apiculture. In this study, we investigated the mechanisms underlying resistance to these compounds in a V. destructor population exhibiting reduced susceptibility to both amitraz and flumethrin. Specifically, bioassays revealed that the resistant population (IL-R) displayed 35.0 % mortality in response to amitraz and 39.5 % mortality to flumethrin, in contrast to >90 % mortality observed in the susceptible IL-L and ATH-S populations. The resistance phenotype was not strongly associated with any of the known target site mutations; the putative amitraz resistance mutation F290L in the Octβ2R gene, and the pyrethroid resistant mutation L925V in the vgsc gene, were found at low frequencies (8.6 % and 13.6 % respectively). Transcriptomic analysis, comparing gene expression levels between the resistant population and two susceptible populations, revealed that resistance is associated with the overexpression of several cuticle genes and the cytochrome P450 gene CYP3002B2. CYP3002B2 was functionally expressed in E. coli, exhibiting catalytic activity against multiple model substrates and effectively metabolizing both amitraz and flumethrin. The predominant product of amitraz metabolism is likely an inactive, hydroxylated form of the insecticide, rather than any of the known activated/toxic metabolites of amitraz. These findings are crucial for evidence-based V. destructor management, as CYP3002B2 is the first detoxification enzyme shown to metabolize two major acaricides from different modes of action classes.

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来源期刊
CiteScore
7.00
自引率
8.50%
发文量
238
审稿时长
4.2 months
期刊介绍: Pesticide Biochemistry and Physiology publishes original scientific articles pertaining to the mode of action of plant protection agents such as insecticides, fungicides, herbicides, and similar compounds, including nonlethal pest control agents, biosynthesis of pheromones, hormones, and plant resistance agents. Manuscripts may include a biochemical, physiological, or molecular study for an understanding of comparative toxicology or selective toxicity of both target and nontarget organisms. Particular interest will be given to studies on the molecular biology of pest control, toxicology, and pesticide resistance. Research Areas Emphasized Include the Biochemistry and Physiology of: • Comparative toxicity • Mode of action • Pathophysiology • Plant growth regulators • Resistance • Other effects of pesticides on both parasites and hosts.
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