Vacuolar H+-ATPase subunit a was identified as the target protein of the oomycete inhibitor fluopicolide

Author:

Dai TanORCID,Yang Jikun,Zhao Chuang,Zhang Can,Wang ZhiwenORCID,Peng Qin,Liu Pengfei,Miao Jianqiang,Liu Xili

Abstract

Approximately 240 fungicides are currently in use. However, only a few direct targets have been identified, which limits the development of fungicides and rapid resistance monitoring. Fluopicolide, which is an excellent oomycete inhibitor, is classified as delocalization of spectrin-like proteins inhibitors by FRAC. In the current study, aPcα-actininknockout had no effect on the sensitivity ofPhytophthora capsicito fluopicolide. The vacuolar H+-ATPase subunit a (PcVHA-a) was identified using a BSA-seq and DARTS assay. Four kinds of point mutations in PcVHA-a that cause fluopicolide resistance inP.capsiciwere confirmed using site-directed mutagenesis. The results of MST, molecular docking, and a DARTS assay indicated that PcVHA-a could bind fluopicolide. Sequence analysis and a molecular docking assay proved the specificity of fluopicolide to oomycetes or fish. Our results suggest that PcVHA-a is the target of fluopicolide, and H+-ATPase could be used as a novel target for the development of new fungicides.

Publisher

Cold Spring Harbor Laboratory

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