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用新型二氮杂硼烷抑制 C-4 甲基固醇氧化酶以靶向真菌植物病原体。

Inhibiting C-4 Methyl Sterol Oxidase with Novel Diazaborines to Target Fungal Plant Pathogens.

机构信息

Department of Molecular Genetics, University of Toronto, Toronto, Ontario M5G 1M1, Canada.

5Metis, Inc., 5 Laboratory Drive, Ste. 2175, Durham, North Carolina 27709, United States.

出版信息

ACS Chem Biol. 2022 Jun 17;17(6):1343-1350. doi: 10.1021/acschembio.2c00257. Epub 2022 May 18.

Abstract

With resistance to current agricultural fungicides rising, a great need has emerged for new antifungals with unexploited targets. In response, we report a novel series of diazaborines with potent activity against representative fungal plant pathogens. To identify their mode of action, we selected for resistant isolates using the model fungus . Whole-genome sequencing of independent diazaborine-resistant lineages identified a recurring mutation in which encodes a C-4 methyl sterol oxidase required for ergosterol biosynthesis in fungi. Haploinsufficiency and allele-swap experiments provided additional genetic evidence for Erg25 as the most biologically relevant target of our diazaborines. Confirming Erg25 as putative target, sterol profiling of compound-treated yeast revealed marked accumulation of the Erg25 substrate, 4,4-dimethylzymosterol and depletion of both its immediate product, zymosterol, as well as ergosterol. Encouraged by these mechanistic insights, the potential utility of targeting Erg25 with a diazaborine was demonstrated in soybean-rust and grape-rot models of fungal plant disease.

摘要

由于当前农业杀菌剂的耐药性不断上升,因此迫切需要具有未开发靶点的新型抗真菌药物。有鉴于此,我们报告了一系列新型的重氮硼烷,它们对代表性的真菌植物病原体具有很强的活性。为了确定它们的作用模式,我们使用模型真菌 选择了具有抗性的分离株。对独立的重氮硼烷抗性谱系进行全基因组测序,鉴定出 中一个反复出现的突变,该基因编码一种 C-4 甲基甾醇氧化酶,该酶是真菌中麦角固醇生物合成所必需的。杂合不足和等位基因交换实验为 Erg25 作为我们的重氮硼烷最具生物学相关性的靶标提供了额外的遗传证据。甾醇分析证实 Erg25 是潜在的靶标,化合物处理酵母的甾醇谱显示 Erg25 底物 4,4-二甲基酵母甾醇的明显积累,以及其直接产物麦角固醇和麦角固醇的耗尽。基于这些机制上的见解,在真菌植物病害的大豆锈病和葡萄腐烂模型中,用重氮硼烷靶向 Erg25 的潜在效用得到了证明。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6e16/9208374/875dbd856b6d/cb2c00257_0001.jpg

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