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甾醇 3-酮还原酶敏感性在灰葡萄孢菌和其他植物病原菌对杀真菌剂 Fenhexamid 易感性中的作用。

Role of sterol 3-ketoreductase sensitivity in susceptibility to the fungicide fenhexamid in Botrytis cinerea and other phytopathogenic fungi.

机构信息

INRA, UR 1290 BIOGER-CPP, Thiverval-Grignon, France.

出版信息

Pest Manag Sci. 2013 May;69(5):642-51. doi: 10.1002/ps.3418. Epub 2012 Nov 9.

Abstract

BACKGROUND

The narrow-spectrum fungicide fenhexamid was introduced into French vineyards in 2000 to control grey mould caused by a complex of two cryptic species: Botrytis cinerea, the predominant species sensitive to fenhexamid, and Botrytis pseudocinerea, naturally resistant. Fenhexamid was suggested to inhibit the 3-ketoreductase involved at C-4 demethylation steps during ergosterol biosynthesis, as revealed by its effects on the B. cinerea sterol profile. Resistance monitoring studies have hitherto identified two B. cinerea fenhexamid-resistant phenotypes, both resulting from mutations in the erg27 gene encoding 3-ketoreductase.

RESULTS

The role of 3-ketoreductase sensitivity in fungal susceptibility to fenhexamid was investigated by studying sterol profiles and microsomal 3-ketoreductase in various fungal strains. Fenhexamid does inhibit B. cinerea 3-ketoreductase activity. Erg27 mutations causing amino acid substitutions in or near the transmembrane domain strongly decrease the affinity of fenhexamid for 3-ketoreductase. Fenhexamid has very low affinities for 3-ketoreductase in inherently resistant species, whether closely related to B. cinerea, like B. pseudocinerea, or more distantly related, like Nectria haematococca.

CONCLUSION

erg27 mutation and erg27 polymorphism may therefore contribute to the unfavourable binding of fenhexamid to its target, 3-ketoreductase, explaining the acquisition of fenhexamid resistance in B. cinerea and the narrow spectrum of this fungicide.

摘要

背景

窄谱杀菌剂烯肟菌胺于 2000 年引入法国葡萄园,用于防治由两个隐种复合体引起的灰霉病:对烯肟菌胺敏感的优势种 Botrytis cinerea 和天然抗药性的 Botrytis pseudocinerea。烯肟菌胺被认为通过其对 B. cinerea 甾醇谱的影响,抑制甾醇生物合成中 C-4 去甲基化步骤涉及的 3-酮还原酶。迄今为止,抗性监测研究已经确定了两种 B. cinerea 对烯肟菌胺具有抗药性的表型,这两种表型都源于编码 3-酮还原酶的 erg27 基因的突变。

结果

通过研究各种真菌菌株的甾醇谱和微粒体 3-酮还原酶,研究了 3-酮还原酶敏感性在真菌对烯肟菌胺敏感性中的作用。烯肟菌胺确实抑制了 B. cinerea 的 3-酮还原酶活性。导致跨膜域中或附近氨基酸取代的 erg27 突变强烈降低了烯肟菌胺与 3-酮还原酶的亲和力。烯肟菌胺对固有抗性物种的 3-酮还原酶亲和力非常低,无论是与 B. cinerea 密切相关的 Botrytis pseudocinerea,还是更远缘的 Nectria haematococca。

结论

因此,erg27 突变和 erg27 多态性可能导致烯肟菌胺与其靶标 3-酮还原酶的结合不良,从而解释了 B. cinerea 对烯肟菌胺的抗性获得以及该杀菌剂的狭窄谱。

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