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干酪成熟真菌罗克福青霉中铁载体粪产碱菌素生物合成的分子基础。

Molecular basis for the biosynthesis of the siderophore coprogen in the cheese-ripening fungus Penicillium roqueforti.

作者信息

González Kathia, Montanares Mariana, Gallardo Matías, Gil-Durán Carlos, Forero Abel M, Rodríguez Jaime, Jiménez Carlos, Vaca Inmaculada, Chávez Renato

机构信息

Departamento de Biología, Facultad de Química y Biología, Universidad de Santiago de Chile (USACH), Alameda 3363, Estación Central, Santiago, Chile.

Departamento de Química, Facultad de Ciencias, Universidad de Chile, Las Palmeras 3425, Ñuñoa, Santiago, Chile.

出版信息

Biol Res. 2025 Jul 21;58(1):51. doi: 10.1186/s40659-025-00633-2.

Abstract

BACKGROUND

Iron is an essential nutrient for microorganisms, including fungi, which have evolved strategies to acquire it. The most common strategy is the secretion of siderophores, low-molecular-weight compounds with a high affinity for ferric ions, which are involved in cellular iron uptake. Penicillium roqueforti, the fungus responsible for the ripening of blue-veined cheeses, produces coprogen, a hydroxamate-type siderophore. However, to date, the molecular basis for its biosynthesis remains elusive.

RESULTS

In this study, we identified and characterized a biosynthetic gene cluster (BGC) responsible for coprogen biosynthesis in P. roqueforti, named the cop BGC. This BGC contains seven genes, three of which (copA, copB and copE) encode enzymes directly involved in coprogen biosynthesis from precursors molecules. Using CRISPR-Cas9, we targeted these three genes and analyzed the resulting mutants by Liquid Chromatography/High-Resolution Mass Spectrometry (LC/HRMS). Our results confirmed that all three genes are necessary for coprogen biosynthesis. Phenotypically, the mutants displayed growth differences under iron-deficient conditions, which correlated with their ability to either synthesize or fail to synthesize coprogen B and dimerumic acid, intermediates in the coprogen pathway with siderophore activity.

CONCLUSIONS

The results obtained in this work provide important insights into the molecular basis of coprogen biosynthesis in P. roqueforti, enhancing the understanding of how siderophores enable this fungus to thrive in iron-deficient environments.

摘要

背景

铁是包括真菌在内的微生物必需的营养素,这些微生物已经进化出获取铁的策略。最常见的策略是分泌铁载体,即对铁离子具有高亲和力的低分子量化合物,其参与细胞对铁的摄取。负责蓝纹奶酪成熟的真菌罗克福特青霉会产生粪卟啉原,一种异羟肟酸型铁载体。然而,迄今为止,其生物合成的分子基础仍然不清楚。

结果

在本研究中,我们鉴定并表征了罗克福特青霉中负责粪卟啉原生物合成的生物合成基因簇(BGC),命名为cop BGC。该BGC包含七个基因,其中三个基因(copA、copB和copE)编码直接参与从前体分子合成粪卟啉原的酶。使用CRISPR-Cas9,我们靶向这三个基因,并通过液相色谱/高分辨率质谱(LC/HRMS)分析产生的突变体。我们的结果证实,这三个基因对于粪卟啉原的生物合成都是必需的。从表型上看,突变体在缺铁条件下表现出生长差异,这与其合成或无法合成粪卟啉原B和二聚酸的能力相关,粪卟啉原B和二聚酸是粪卟啉原途径中具有铁载体活性的中间体。

结论

本研究获得的结果为罗克福特青霉中粪卟啉原生物合成的分子基础提供了重要见解,增强了对铁载体如何使这种真菌在缺铁环境中茁壮成长的理解。

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