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预测人类肠道细菌厌氧利用胆碱的广泛分布基因簇的表征与检测

Characterization and detection of a widely distributed gene cluster that predicts anaerobic choline utilization by human gut bacteria.

作者信息

Martínez-del Campo Ana, Bodea Smaranda, Hamer Hilary A, Marks Jonathan A, Haiser Henry J, Turnbaugh Peter J, Balskus Emily P

机构信息

Department of Chemistry and Chemical Biology, Harvard University, Cambridge, Massachusetts, USA.

Novartis Institutes for Biomedical Research, Cambridge, Massachusetts, USA.

出版信息

mBio. 2015 Apr 14;6(2):e00042-15. doi: 10.1128/mBio.00042-15.

Abstract

UNLABELLED

Elucidation of the molecular mechanisms underlying the human gut microbiota's effects on health and disease has been complicated by difficulties in linking metabolic functions associated with the gut community as a whole to individual microorganisms and activities. Anaerobic microbial choline metabolism, a disease-associated metabolic pathway, exemplifies this challenge, as the specific human gut microorganisms responsible for this transformation have not yet been clearly identified. In this study, we established the link between a bacterial gene cluster, the choline utilization (cut) cluster, and anaerobic choline metabolism in human gut isolates by combining transcriptional, biochemical, bioinformatic, and cultivation-based approaches. Quantitative reverse transcription-PCR analysis and in vitro biochemical characterization of two cut gene products linked the entire cluster to growth on choline and supported a model for this pathway. Analyses of sequenced bacterial genomes revealed that the cut cluster is present in many human gut bacteria, is predictive of choline utilization in sequenced isolates, and is widely but discontinuously distributed across multiple bacterial phyla. Given that bacterial phylogeny is a poor marker for choline utilization, we were prompted to develop a degenerate PCR-based method for detecting the key functional gene choline TMA-lyase (cutC) in genomic and metagenomic DNA. Using this tool, we found that new choline-metabolizing gut isolates universally possessed cutC. We also demonstrated that this gene is widespread in stool metagenomic data sets. Overall, this work represents a crucial step toward understanding anaerobic choline metabolism in the human gut microbiota and underscores the importance of examining this microbial community from a function-oriented perspective.

IMPORTANCE

Anaerobic choline utilization is a bacterial metabolic activity that occurs in the human gut and is linked to multiple diseases. While bacterial genes responsible for choline fermentation (the cut gene cluster) have been recently identified, there has been no characterization of these genes in human gut isolates and microbial communities. In this work, we use multiple approaches to demonstrate that the pathway encoded by the cut genes is present and functional in a diverse range of human gut bacteria and is also widespread in stool metagenomes. We also developed a PCR-based strategy to detect a key functional gene (cutC) involved in this pathway and applied it to characterize newly isolated choline-utilizing strains. Both our analyses of the cut gene cluster and this molecular tool will aid efforts to further understand the role of choline metabolism in the human gut microbiota and its link to disease.

摘要

未标记

将与整个肠道群落相关的代谢功能与单个微生物及活性联系起来存在困难,这使得阐明人类肠道微生物群对健康和疾病影响的分子机制变得复杂。厌氧微生物胆碱代谢是一种与疾病相关的代谢途径,它体现了这一挑战,因为负责这种转化的特定人类肠道微生物尚未被明确鉴定。在本研究中,我们通过结合转录、生化、生物信息学和基于培养的方法,在人类肠道分离株中建立了细菌基因簇——胆碱利用(cut)簇与厌氧胆碱代谢之间的联系。对两种cut基因产物的定量逆转录 - PCR分析和体外生化特性分析将整个簇与胆碱上的生长联系起来,并支持了该途径的模型。对已测序细菌基因组的分析表明,cut簇存在于许多人类肠道细菌中,可预测已测序分离株中的胆碱利用情况,并且广泛但不连续地分布于多个细菌门中。鉴于细菌系统发育对于胆碱利用来说并不是一个很好的标记,我们促使开发一种基于简并PCR的方法来检测基因组和宏基因组DNA中的关键功能基因胆碱TMA裂解酶(cutC)。使用这个工具,我们发现新的利用胆碱的肠道分离株普遍拥有cutC。我们还证明了该基因在粪便宏基因组数据集中广泛存在。总体而言,这项工作是朝着理解人类肠道微生物群中厌氧胆碱代谢迈出的关键一步,并强调了从功能导向的角度研究这个微生物群落的重要性。

重要性

厌氧胆碱利用是一种在人类肠道中发生的细菌代谢活动,与多种疾病相关。虽然最近已经鉴定出负责胆碱发酵的细菌基因(cut基因簇),但尚未对人类肠道分离株和微生物群落中的这些基因进行表征。在这项工作中,我们使用多种方法证明cut基因编码的途径在多种人类肠道细菌中存在且具有功能,并且在粪便宏基因组中也广泛存在。我们还开发了一种基于PCR的策略来检测参与该途径的关键功能基因(cutC),并将其应用于表征新分离的利用胆碱的菌株。我们对cut基因簇的分析和这个分子工具都将有助于进一步了解胆碱代谢在人类肠道微生物群中的作用及其与疾病的联系。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0077/4453576/706aba55ba21/mbo0021522670002.jpg

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