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高通量鉴定肠道微生物组依赖性代谢物。

High-throughput identification of gut microbiome-dependent metabolites.

机构信息

Department of Biochemistry, Duke University School of Medicine, Durham, NC, USA.

Duke Microbiome Center, Duke University School of Medicine, Durham, NC, USA.

出版信息

Nat Protoc. 2024 Jul;19(7):2180-2205. doi: 10.1038/s41596-024-00980-6. Epub 2024 May 13.

DOI:10.1038/s41596-024-00980-6
PMID:38740909
Abstract

A significant hurdle that has limited progress in microbiome science has been identifying and studying the diverse set of metabolites produced by gut microbes. Gut microbial metabolism produces thousands of difficult-to-identify metabolites, which present a challenge to study their roles in host biology. In recent years, mass spectrometry-based metabolomics has become one of the core technologies for identifying small metabolites. However, metabolomics expertise, ranging from sample preparation to instrument use and data analysis, is often lacking in academic labs. Most targeted metabolomics methods provide high levels of sensitivity and quantification, while they are limited to a panel of predefined molecules that may not be informative to microbiome-focused studies. Here we have developed a gut microbe-focused and wide-spectrum metabolomic protocol using liquid chromatography-mass spectrometry and bioinformatic analysis. This protocol enables users to carry out experiments from sample collection to data analysis, only requiring access to a liquid chromatography-mass spectrometry instrument, which is often available at local core facilities. By applying this protocol to samples containing human gut microbial metabolites, spanning from culture supernatant to human biospecimens, our approach enables high-confidence identification of >800 metabolites that can serve as candidate mediators of microbe-host interactions. We expect this protocol will lower the barrier to tracking gut bacterial metabolism in vitro and in mammalian hosts, propelling hypothesis-driven mechanistic studies and accelerating our understanding of the gut microbiome at the chemical level.

摘要

在微生物组科学中,一个重要的障碍是鉴定和研究肠道微生物产生的多样化代谢物。肠道微生物代谢产生了数千种难以识别的代谢物,这给研究它们在宿主生物学中的作用带来了挑战。近年来,基于质谱的代谢组学已成为鉴定小分子代谢物的核心技术之一。然而,学术实验室通常缺乏代谢组学方面的专业知识,包括从样品制备到仪器使用和数据分析等方面。大多数靶向代谢组学方法提供了高灵敏度和定量水平,但它们仅限于一组预先定义的分子,这些分子可能对以微生物组为重点的研究没有信息价值。在这里,我们开发了一种使用液相色谱-质谱联用和生物信息学分析的肠道微生物组聚焦和广谱代谢组学方案。该方案使用户能够从样品采集到数据分析进行实验,只需要能够使用液相色谱-质谱联用仪器,而这种仪器通常在当地核心设施中都可以获得。通过将该方案应用于包含人类肠道微生物代谢物的样本,从培养上清液到人类生物样本,我们的方法能够高度置信地鉴定出 800 多种代谢物,这些代谢物可以作为微生物-宿主相互作用的候选介质。我们预计该方案将降低在体外和哺乳动物宿主中追踪肠道细菌代谢的障碍,推动以假说为驱动的机制研究,并加速我们对肠道微生物组在化学水平上的理解。

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