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Discovery of piperonyl-tethered sulfoximines as novel low bee-toxicity aphicides targeting Amelα1/ratβ2 complex.

Authors :
Han, Qing
Zhou, Yuxin
Zi, Yunjiang
Zhang, Rulei
Feng, Tianyu
Zou, Renxuan
Zhu, Wenya
Wang, Yinliang
Duan, Hongxia
Source :
International Journal of Biological Macromolecules. Dec2023:Part 2, Vol. 253, pN.PAG-N.PAG. 1p.
Publication Year :
2023

Abstract

Nicotinic acetylcholine receptor (nAChR) is recognized as a significant insecticide target for neonicotinoids and some agonists. In this study, the nAChR α1 subunit from Apis mellifera was first found to be narrowly tuned to different bee toxicity insecticides, namely, sulfoxaflor (SFX) and flupyradifurone (FPF). Hence, novel sulfoximine derivatives 7a-h were rationally designed and synthesized by introducing a benzo[ d ][1,3]dioxole moiety into a unique sulfoximine skeleton based on the binding cavity characteristics of Amelα1/ratβ2. The two electrode voltage clamp responses of 7a-h were obviously lower than that of SFX, indicating their potentially low bee toxicity. Besides, representative compounds 7b and 7g exhibited low bee toxicity (LD 50 > 11.0 μg/bee at 48 h) revealed by acute contact toxicity bioassays. Molecular modelling results indicated that Ile152, Ala151, and Val160 from honeybee subunit Amelα1 and Lys144 and Trp80 from aphid subunit Mpα1 may be crucial for bee toxicity and aphicidal activity, respectively. These results clarify the toxic mechanism of agonist insecticides on nontargeted pollinators and reveal novel scaffold sulfoximine aphicidal candidates with low bee toxicity. These results will provide a new perspective on the rational design and highly effective development of novel eco-friendly insecticides based on the structure of the nAChR subunit. [Display omitted] • nAChR α1 subunit from Apis mellifera was related to bee toxicity of sulfoxaflor. • Novel low bee-toxicity sulfoximine aphicides were discovered by targeting Amelα1/ratβ2 complex. • Some residues were critical for aphicidal activity and bee toxicity, respectively. [ABSTRACT FROM AUTHOR]

Details

Language :
English
ISSN :
01418130
Volume :
253
Database :
Academic Search Index
Journal :
International Journal of Biological Macromolecules
Publication Type :
Academic Journal
Accession number :
173694843
Full Text :
https://doi.org/10.1016/j.ijbiomac.2023.126719