Gut microbial structural variations as determinants of human bile acid metabolism

Wang, Daoming; Doestzada, Marwah; Lianmin, Chen; Andreu‐Sánchez, Sergio; Munckhof, Inge C.L. van den; Augustijn, Hannah E.; Koehorst, Martijn; Bloks, Vincent W.; Riksen, Niels P.; Rutten, Joseph Henricus Wilhelmus; Netea, Mihai G.; Zhernakova, Alexandra; Kuipers, Folkert; Fu, Jingyuan

doi:10.1101/2021.02.28.432952

Cited by 3 publications

(2 citation statements)

References 47 publications

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“…The diversity and composition of the gut microbiome have been studied for over a decade, but their precise roles in influencing host physiology and maintaining tissue homeostasis are still under intense investigation. [32,33] In this study, we found that ampicillin-induced gut dysbiosis led to unbalanced Firmicutes/Bacteroidetes ratios and reduced production of secondary bile acids. Bile acids are synthesized from cholesterol in the liver and further metabolized by the gut microbiota into secondary bile acids to exert biological functions.…”

Section: Discussionmentioning

confidence: 62%

Antibiotic‐Induced Gut Microbiota Dysbiosis Modulates Host Transcriptome and m⁶A Epitranscriptome via Bile Acid Metabolism

Yang,

Zheng,

Fan

et al. 2024

Advanced Science

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Gut microbiota can influence host gene expression and physiology through metabolites. Besides, the presence or absence of gut microbiome can reprogram host transcriptome and epitranscriptome as represented by N6‐methyladenosine (m6A), the most abundant mammalian mRNA modification. However, which and how gut microbiota‐derived metabolites reprogram host transcriptome and m6A epitranscriptome remain poorly understood. Here, investigation is conducted into how gut microbiota‐derived metabolites impact host transcriptome and m6A epitranscriptome using multiple mouse models and multi‐omics approaches. Various antibiotics‐induced dysbiotic mice are established, followed by fecal microbiota transplantation (FMT) into germ‐free mice, and the results show that bile acid metabolism is significantly altered along with the abundance change in bile acid‐producing microbiota. Unbalanced gut microbiota and bile acids drastically change the host transcriptome and the m6A epitranscriptome in multiple tissues. Mechanistically, the expression of m6A writer proteins is regulated in animals treated with antibiotics and in cultured cells treated with bile acids, indicating a direct link between bile acid metabolism and m6A biology. Collectively, these results demonstrate that antibiotic‐induced gut dysbiosis regulates the landscape of host transcriptome and m6A epitranscriptome via bile acid metabolism pathway. This work provides novel insights into the interplay between microbial metabolites and host gene expression.

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Section: Discussionmentioning

confidence: 62%

Antibiotic‐Induced Gut Microbiota Dysbiosis Modulates Host Transcriptome and m⁶A Epitranscriptome via Bile Acid Metabolism

Yang,

Zheng,

Fan

et al. 2024

Advanced Science

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“…Next, we explored associations between the abundance of crAss-like phages and structural variants (SVs) in bacterial genomes (Wang et al, 2021; Zeevi et al, 2019). Based on the collection of samples from the three independent cohorts LLD, 300OB and IBD, we detected 7,999 deletion structural variants (dSVs, genome segments absent in 25% to 75% samples) and 3,559 variable structural variants (vSVs, genome segments absent in < 25% samples).…”

Section: Resultsmentioning

confidence: 99%

Discovery, diversity and functional associations of crAss-like phages in human gut metagenomes from four Dutch cohorts

Gulyaeva

Garmaeva

et al. 2021

Preprint

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The crAss-like phages are a diverse group of related viruses that includes one of the most abundant viruses of the human gut. To explore their diversity and functional role in human population and clinical cohorts, we analyzed gut metagenomic data collected from more than 2000 individuals from the Netherlands. We discovered 125 novel species-level and 32 novel genus-level clusters of crAss-like phages, all belonging to five previously recognized groups associated with the human gut. Analysis of their genomic features revealed that closely related crAss-like phages can possess strikingly divergent regions responsible for transcription, presumably acquired through recombination. Prediction of crAss-like phage hosts pointed primarily to bacteria of the phylum Bacteroidetes, consistent with previous reports. Finally, we explored the temporal stability of crAss-like phages over a 4-year period and identified associations between the abundance of crAss-like phages and several human phenotypes, including depletion of crAss-like phages in inflammatory bowel disease patients.

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Multiomics reveals gut dysbiosis contributes to fatty acid dysmetabolism in early phase of acute myocardial infarction

Fan,

Ying,

Huangfu

et al. 2024

Preprint

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Background:Acute myocardial infarction (AMI) remains a major cause of death, with limited understanding of its early risk stratification. While late-stage AMI has recognized associations with gut microbiome disturbances, the connection to eAMI is less explored.Methods:Using metabolomics and metagenomics, we analyzed 56 samples, comprising 30 eAMI patients (within 12 hours of onset) and 26 age- and gender-matched healthy controls, to discern the influence of gut microbes and their metabolites.Results:We found the eAMI plasma is dominated by increased long-chain fatty acids (LCFAs), 14 of which provide differentiating power of eAMI patients from HCs. Multiomics analysis reveals up to 70% of the variance in LCFAs of eAMI patients can be explained by altered gut microbiome. Higher-resolution profiling of gut bacterial species demonstrated that bacterial structural variations are mechanistically linked to LCFAs dysregulation. Byin silicomolecular docking andin vitrothrombogenic assay in isolated human platelets, we highlighted that eAMI-associated LCFAs contribute to platelet aggregation, a driving factor for AMI initiation.Conclusions:LCFAs hold significant potential as early biomarkers of AMI and gut microbiome contributes to altered LCFAs in eAMI. Further studies are imperative to expand upon these observations to better leverage LCFAs as a potential biomarker for eAMI and as a therapeutic target for inhibition of platelet aggregation in eAMI.

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Gut microbial structural variations as determinants of human bile acid metabolism

Cited by 3 publications

References 47 publications

Antibiotic‐Induced Gut Microbiota Dysbiosis Modulates Host Transcriptome and m⁶A Epitranscriptome via Bile Acid Metabolism

Antibiotic‐Induced Gut Microbiota Dysbiosis Modulates Host Transcriptome and m⁶A Epitranscriptome via Bile Acid Metabolism

Discovery, diversity and functional associations of crAss-like phages in human gut metagenomes from four Dutch cohorts

Multiomics reveals gut dysbiosis contributes to fatty acid dysmetabolism in early phase of acute myocardial infarction

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Gut microbial structural variations as determinants of human bile acid metabolism

Cited by 3 publications

References 47 publications

Antibiotic‐Induced Gut Microbiota Dysbiosis Modulates Host Transcriptome and m6A Epitranscriptome via Bile Acid Metabolism

Antibiotic‐Induced Gut Microbiota Dysbiosis Modulates Host Transcriptome and m6A Epitranscriptome via Bile Acid Metabolism

Discovery, diversity and functional associations of crAss-like phages in human gut metagenomes from four Dutch cohorts

Multiomics reveals gut dysbiosis contributes to fatty acid dysmetabolism in early phase of acute myocardial infarction

Contact Info

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Resources

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Antibiotic‐Induced Gut Microbiota Dysbiosis Modulates Host Transcriptome and m⁶A Epitranscriptome via Bile Acid Metabolism

Antibiotic‐Induced Gut Microbiota Dysbiosis Modulates Host Transcriptome and m⁶A Epitranscriptome via Bile Acid Metabolism