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空肠弯曲菌对谷氨酸和岩藻糖丰富存在的意外差异代谢反应。

Unexpected differential metabolic responses of Campylobacter jejuni to the abundant presence of glutamate and fucose.

机构信息

Bioinformatics Group, Wageningen University, 6708PB, Wageningen, The Netherlands.

King Abdulaziz University, Jeddah, 21589, Kingdom of Saudi Arabia.

出版信息

Metabolomics. 2018 Oct 23;14(11):144. doi: 10.1007/s11306-018-1438-5.

Abstract

INTRODUCTION

Campylobacter jejuni is the leading cause of foodborne bacterial enteritis in humans, and yet little is known in regard to how genetic diversity and metabolic capabilities among isolates affect their metabolic phenotype and pathogenicity.

OBJECTIVES

For instance, the C. jejuni 11168 strain can utilize both L-fucose and L-glutamate as a carbon source, which provides the strain with a competitive advantage in some environments and in this study we set out to assess the metabolic response of C. jejuni 11168 to the presence of L-fucose and L-glutamate in the growth medium.

METHODS

To achieve this, untargeted hydrophilic liquid chromatography coupled to mass spectrometry was used to obtain metabolite profiles of supernatant extracts obtained at three different time points up to 24 h.

RESULTS

This study identified both the depletion and the production and subsequent release of a multitude of expected and unexpected metabolites during the growth of C. jejuni 11168 under three different conditions. A large set of standards allowed identification of a number of metabolites. Further mass spectrometry fragmentation analysis allowed the additional annotation of substrate-specific metabolites. The results show that C. jejuni 11168 upon L-fucose addition indeed produces degradation products of the fucose pathway. Furthermore, methionine was faster depleted from the medium, consistent with previously-observed methionine auxotrophy.

CONCLUSIONS

Moreover, a multitude of not previously annotated metabolites in C. jejuni were found to be increased specifically upon L-fucose addition. These metabolites may well play a role in the pathogenicity of this C. jejuni strain.

摘要

简介

空肠弯曲菌是人类食源性细菌性肠炎的主要致病菌,但我们对于分离株的遗传多样性和代谢能力如何影响其代谢表型和致病性知之甚少。

目的

例如,C. jejuni 11168 株可以同时利用 L-岩藻糖和 L-谷氨酸作为碳源,这使该菌株在某些环境中具有竞争优势。在本研究中,我们评估了 C. jejuni 11168 对生长培养基中 L-岩藻糖和 L-谷氨酸存在的代谢反应。

方法

为此,我们使用非靶向亲水液相色谱-质谱联用技术,在 24 小时内的三个不同时间点获得上清液提取物的代谢谱。

结果

本研究在三种不同条件下,鉴定了 C. jejuni 11168 生长过程中预期和意外的多种代谢物的消耗和产生以及随后的释放。大量的标准品允许鉴定出许多代谢物。进一步的质谱碎裂分析允许对底物特异性代谢物进行额外注释。结果表明,C. jejuni 11168 确实在添加 L-岩藻糖后产生了岩藻糖途径的降解产物。此外,培养基中的蛋氨酸更快耗尽,这与先前观察到的蛋氨酸营养缺陷一致。

结论

此外,发现大量以前未注释的 C. jejuni 代谢物在添加 L-岩藻糖后特异性增加。这些代谢物可能在该 C. jejuni 菌株的致病性中发挥作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e33f/6208705/1ec09ac92235/11306_2018_1438_Fig1_HTML.jpg

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