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农杆菌介导的无脊椎动物病原体绿僵菌中一个非核糖体肽合成酶基因的破坏揭示了一种肽类孢子因子。

Agrobacterium-mediated disruption of a nonribosomal peptide synthetase gene in the invertebrate pathogen Metarhizium anisopliae reveals a peptide spore factor.

作者信息

Moon Yong-Sun, Donzelli Bruno G G, Krasnoff Stuart B, McLane Heather, Griggs Mike H, Cooke Peter, Vandenberg John D, Gibson Donna M, Churchill Alice C L

机构信息

Boyce Thompson Institute for Plant Research, Ithaca, New York 14853, USA.

出版信息

Appl Environ Microbiol. 2008 Jul;74(14):4366-80. doi: 10.1128/AEM.00285-08. Epub 2008 May 23.

Abstract

Numerous secondary metabolites have been isolated from the insect pathogenic fungus Metarhizium anisopliae, but the roles of these compounds as virulence factors in disease development are poorly understood. We targeted for disruption by Agrobacterium tumefaciens-mediated transformation a putative nonribosomal peptide synthetase (NPS) gene, MaNPS1. Four of six gene disruption mutants identified were examined further. Chemical analyses showed the presence of serinocyclins, cyclic heptapeptides, in the extracts of conidia of control strains, whereas the compounds were undetectable in DeltaManps1 mutants treated identically or in other developmental stages, suggesting that MaNPS1 encodes a serinocyclin synthetase. Production of the cyclic depsipeptide destruxins, M. anisopliae metabolites also predicted to be synthesized by an NPS, was similar in DeltaManps1 mutant and control strains, indicating that MaNPS1 does not contribute to destruxin biosynthesis. Surprisingly, a MaNPS1 fragment detected DNA polymorphisms that correlated with relative destruxin levels produced in vitro, and MaNPS1 was expressed concurrently with in vitro destruxin production. DeltaManps1 mutants exhibited in vitro development and responses to external stresses comparable to control strains. No detectable differences in pathogenicity of the DeltaManps1 mutants were observed in bioassays against beet armyworm and Colorado potato beetle in comparison to control strains. This is the first report of targeted disruption of a secondary metabolite gene in M. anisopliae, which revealed a novel cyclic peptide spore factor.

摘要

人们已从昆虫病原真菌绿僵菌中分离出许多次生代谢产物,但对于这些化合物作为致病因子在疾病发展过程中的作用却知之甚少。我们通过根癌农杆菌介导的转化,靶向破坏了一个假定的非核糖体肽合成酶(NPS)基因MaNPS1。对鉴定出的6个基因破坏突变体中的4个进行了进一步研究。化学分析表明,对照菌株分生孢子提取物中存在丝氨酸环肽(一种环状七肽),而在经过相同处理的ΔManps1突变体或其他发育阶段中未检测到这些化合物,这表明MaNPS1编码一种丝氨酸环肽合成酶。环缩肽类毒素(也是预测由NPS合成的绿僵菌代谢产物)在ΔManps1突变体和对照菌株中的产生情况相似,这表明MaNPS1对类毒素生物合成没有贡献。令人惊讶的是,一个MaNPS1片段检测到与体外产生的相对类毒素水平相关的DNA多态性,并且MaNPS1与体外类毒素产生同时表达。ΔManps1突变体在体外的发育以及对外部压力的反应与对照菌株相当。与对照菌株相比,在针对甜菜夜蛾和科罗拉多马铃薯甲虫的生物测定中,未观察到ΔManps1突变体在致病性上有可检测到的差异。这是关于绿僵菌次生代谢产物基因靶向破坏的首次报道,该报道揭示了一种新型的环状肽孢子因子。

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