Literature DB >> 33590776

The contribution of gut bacterial metabolites in the human immune signaling pathway of non-communicable diseases.

F Hosseinkhani1, A Heinken2, I Thiele2, P W Lindenburg1,3, A C Harms1, T Hankemeier1.   

Abstract

The interaction disorder between gut microbiota and its host has been documented in different non-communicable diseases (NCDs) such as metabolic syndrome, neurodegenerative disease, and autoimmune disease. The majority of these altered interactions arise through metabolic cross-talk between gut microbiota and host immune system, inducing a low-grade chronic inflammation that characterizes all NCDs. In this review, we discuss the contribution of bacterial metabolites to immune signaling pathways involved in NCDs. We then review recent advances that aid to rationally design microbial therapeutics. A deeper understanding of these intersections between host and gut microbiota metabolism using metabolomics-based system biology platform promises to reveal the fundamental mechanisms that drive metabolic predispositions to disease and suggest new avenues to use microbial therapeutic opportunities for NCDs treatment and prevention. Abbreviations: NCDs: non-communicable disease, IBD: inflammatory bowel disease, IL: interleukin, T2D: type 2 diabetes, SCFAs: short-chain fatty acids, HDAC: histone deacetylases, GPCR: G-protein coupled receptors, 5-HT: 5-hydroxytryptamine receptor signaling, DCs: dendritic cells, IECs: intestinal epithelial cells, T-reg: T regulatory cell, NF-κB: nuclear factor κB, TNF-α: tumor necrosis factor alpha, Th: T helper cell, CNS: central nervous system, ECs: enterochromaffin cells, NSAIDs: non-steroidal anti-inflammatory drugs, AhR: aryl hydrocarbon receptor, IDO: indoleamine 2,3-dioxygenase, QUIN: quinolinic acid, PC: phosphatidylcholine, TMA: trimethylamine, TMAO: trimethylamine N-oxide, CVD: cardiovascular disease, NASH: nonalcoholic steatohepatitis, BAs: bile acids, FXR: farnesoid X receptor, CDCA: chenodeoxycholic acid, DCA: deoxycholic acid, LCA: lithocholic acid, UDCA: ursodeoxycholic acid, CB: cannabinoid receptor, COBRA: constraint-based reconstruction and analysis.

Entities:  

Keywords:  Bacterial metabolites; gut microbiota; immune signaling; metabolomics; non-communicable diseases; system biology

Mesh:

Substances:

Year:  2021        PMID: 33590776      PMCID: PMC7899087          DOI: 10.1080/19490976.2021.1882927

Source DB:  PubMed          Journal:  Gut Microbes        ISSN: 1949-0976


  151 in total

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Review 2.  GPCR-Mediated Signaling of Metabolites.

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Review 7.  Gut Microbiota Regulation of Tryptophan Metabolism in Health and Disease.

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Journal:  Cell Host Microbe       Date:  2018-06-13       Impact factor: 21.023

8.  Gut bacterial phospholipase Ds support disease-associated metabolism by generating choline.

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Review 4.  The role of intestinal microbiota and its metabolites in intestinal and extraintestinal organ injury induced by intestinal ischemia reperfusion injury.

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Review 5.  Metabolomics: The Key to Unraveling the Role of the Microbiome in Visceral Pain Neurotransmission.

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Review 6.  Anthocyanins in Chronic Diseases: The Power of Purple.

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Review 7.  The Role of Bifidobacteria in Predictive and Preventive Medicine: A Focus on Eczema and Hypercholesterolemia.

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Review 9.  The Role of the Intestinal Microbiota in Nonalcoholic Steatohepatitis.

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10.  Towards Standards for Human Fecal Sample Preparation in Targeted and Untargeted LC-HRMS Studies.

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