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多组学分析揭示粪便样本物流对代谢物和微生物组成的影响。

Multi-Omics Analysis Unravels the Impact of Stool Sample Logistics on Metabolites and Microbial Composition.

作者信息

Krause Jannike L, Engelmann Beatrice, Lallinger David J D, Rolle-Kampczyk Ulrike, von Bergen Martin, Chang Hyun-Dong

机构信息

German Rheumatism Research Center Berlin, A Leibniz Institute-DRFZ, Schwiete Laboratory for Microbiota and Inflammation, 10117 Berlin, Germany.

Helmholtz-Centre for Environmental Research-UFZ, Department of Molecular Toxicology, 04318 Leipzig, Germany.

出版信息

Microorganisms. 2024 Sep 30;12(10):1998. doi: 10.3390/microorganisms12101998.

Abstract

Human health and the human microbiome are inevitably intertwined, increasing their relevance in clinical research. However, the collection, transportation and storage of faecal samples may introduce bias due to methodological differences, especially since postal shipping is a common practise in large-scale clinical cohort studies. Using four different Omics layer, we determined the structural (16S rRNA sequencing, cytometric microbiota profiling) and functional integrity (SCFAs, global metabolome) of the microbiota in relation to different easy-to-handle conditions. These conditions were storage at -20 °C, -20 °C as glycerol stock, 4 °C and room temperature with and without oxygen exposure for a maximum of one week. Storage time affected the microbiota on all Omics levels. However, the magnitude was donor-dependent, highlighting the need for purpose-optimized sample collection in clinical multi-donor studies. The effects of oxygen exposure were negligible for all analyses. At ambient temperature, SCFA and compositional profiles were stable for 24 h and 48 h, respectively, while at 4 °C, SCFA profiles were maintained for 48 h. The global metabolome was highly susceptible, already changing at 24 h in non-frozen conditions. Thus, faecal microbiota was best preserved on all levels when transported as a native sample frozen within 24 h, leading to the least biased outcomes in the analysis. We conclude that the immediate freezing of native stool samples for transportation to the lab is best suited for planned multi-Omics analyses that include metabolomics to extend standard sequencing approaches.

摘要

人类健康与人类微生物组不可避免地相互交织,这增加了它们在临床研究中的相关性。然而,粪便样本的采集、运输和储存可能会因方法上的差异而引入偏差,特别是在大规模临床队列研究中邮政运输是常见做法的情况下。我们使用四种不同的组学层面,确定了微生物群在不同易于处理条件下的结构(16S rRNA测序、流式细胞术微生物群分析)和功能完整性(短链脂肪酸、全局代谢组)。这些条件包括在-20°C、作为甘油原液在-20°C、4°C以及室温下储存,有或没有氧气暴露,最长储存一周。储存时间在所有组学水平上都会影响微生物群。然而,影响程度因供体而异,这突出了在临床多供体研究中进行有针对性的样本采集优化的必要性。对于所有分析而言,氧气暴露的影响可忽略不计。在环境温度下,短链脂肪酸和组成谱分别在24小时和48小时内保持稳定,而在4°C时,短链脂肪酸谱可维持48小时。全局代谢组高度敏感,在非冷冻条件下仅24小时就会发生变化。因此,粪便微生物群在作为天然样本在24小时内冷冻运输时,在所有层面上保存得最好,从而在分析中产生的偏差最小。我们得出结论,将天然粪便样本立即冷冻以便运输到实验室最适合于包括代谢组学在内的计划多组学分析,以扩展标准测序方法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/644c/11509235/bf021e4e0809/microorganisms-12-01998-g001.jpg

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