Small NRPS-like enzymes in Aspergillus sections Flavi and Circumdati selectively form substituted pyrazinone metabolites.

IF 2.1 Q3 MYCOLOGY Frontiers in fungal biology Pub Date : 2022-10-26 eCollection Date: 2022-01-01 DOI:10.3389/ffunb.2022.1029195
Matthew D Lebar, Brian M Mack, Carol H Carter-Wientjes, Qijian Wei, Christopher P Mattison, Jeffrey W Cary
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Abstract

Aspergillus fungi produce mycotoxins that are detrimental to human and animal health. Two sections of aspergilli are of particular importance to cereal food crops such as corn and barley. Aspergillus section Flavi species like A. flavus and A. parasiticus produce aflatoxins, while section Circumdati species like A. ochraceus and A. sclerotiorum produce ochratoxin A. Mitigating these toxins in food and feed is a critical and ongoing worldwide effort. We have previously investigated biosynthetic gene clusters in Aspergillus flavus that are linked to fungal virulence in corn. We found that one such cluster, asa, is responsible for the production of aspergillic acid, an iron-binding, hydroxamic acid-containing pyrazinone metabolite. Furthermore, we found that the asa gene cluster is present in many other aflatoxin- and ochratoxin-producing aspergilli. The core gene in the asa cluster encodes the small nonribosomal peptide synthetase-like (NRPS-like) protein AsaC. We have swapped the asaC ortholog from A. sclerotiorum into A. flavus, replacing its native copy, and have also cloned both asaC orthologs into Saccharomyces cerevisiae. We show that AsaC orthologs in section Flavi and section Circumdati, while only containing adenylation-thiolation-reductase (ATR) domains, can selectively biosynthesize distinct pyrazinone natural products: deoxyaspergillic acid and flavacol, respectively. Because pyrazinone natural products and the gene clusters responsible for their production are implicated in a variety of important microbe-host interactions, uncovering the function and selectivity of the enzymes involved could lead to strategies that ultimately benefit human health.

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曲霉菌切片中的小NRPS样酶Flavi和Circodati选择性地形成取代的吡嗪酮代谢产物。
曲霉产生的真菌毒素对人类和动物健康有害。曲霉菌病的两个部分对玉米和大麦等谷类食品作物特别重要。黄曲霉和寄生曲霉等曲霉菌类产生黄曲霉毒素,而赭曲霉和核盘菌等环孢菌类产生赭曲霉毒素A。减轻食品和饲料中的这些毒素是一项关键的、正在进行的全球努力。我们之前已经研究了黄曲霉中与玉米真菌毒力有关的生物合成基因簇。我们发现其中一个簇asa负责产生曲霉菌病,曲霉菌病是一种铁结合的含异羟肟酸的吡嗪酮代谢产物。此外,我们发现asa基因簇存在于许多其他产生黄曲霉毒素和赭曲霉毒素的曲霉菌中。asa簇中的核心基因编码小的非核糖体肽合成酶样(NRPS样)蛋白AsaC。我们已经将核盘菌的asaC直向同源物替换为黄曲霉,取代了其天然拷贝,还将两种asaC直序同源物克隆到酿酒酵母中。我们发现,Flavi部分和Circodati部分的AsaC直链同源物,虽然只含有腺苷化硫基化还原酶(ATR)结构域,但可以选择性地生物合成不同的吡嗪酮天然产物:脱氧曲霉菌酸和黄曲霉醇。由于吡嗪酮天然产物及其产生的基因簇与各种重要的微生物-宿主相互作用有关,揭示相关酶的功能和选择性可能会导致最终有益于人类健康的策略。
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2.70
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0.00%
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审稿时长
13 weeks
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