Decrease in acetyl-CoA pathway utilizing butyrate-producing bacteria is a key pathogenic feature of alcohol-induced functional gut microbial dysbiosis and development of liver disease in mice

Emerging research evidence has established the critical role of the gut-liver axis in the development of alcohol-associated liver disease (ALD). The present study employed 16S rRNA gene and whole genome shotgun (WGS) metagenomic analysis in combination with a revised microbial dataset to comprehensi...

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Autores principales: Singhal, Richa, Donde, Hridgandh, Ghare, Smita, Stocke, Kendall, Zhang, Jingwein, Vadhanam, Manicka, Reddy, Sreelatha, Gobejishvili, Leila, Chilton, Paula, Joshi-Barve, Swati, Feng, Wenke, McClain, Craig, Hoffman, Kristi, Petrosino, Joseph, Vital, Marius, Barve, Shirish
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Taylor & Francis 2021
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8354657/
https://www.ncbi.nlm.nih.gov/pubmed/34369304
http://dx.doi.org/10.1080/19490976.2021.1946367
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author Singhal, Richa
Donde, Hridgandh
Ghare, Smita
Stocke, Kendall
Zhang, Jingwein
Vadhanam, Manicka
Reddy, Sreelatha
Gobejishvili, Leila
Chilton, Paula
Joshi-Barve, Swati
Feng, Wenke
McClain, Craig
Hoffman, Kristi
Petrosino, Joseph
Vital, Marius
Barve, Shirish
author_facet Singhal, Richa
Donde, Hridgandh
Ghare, Smita
Stocke, Kendall
Zhang, Jingwein
Vadhanam, Manicka
Reddy, Sreelatha
Gobejishvili, Leila
Chilton, Paula
Joshi-Barve, Swati
Feng, Wenke
McClain, Craig
Hoffman, Kristi
Petrosino, Joseph
Vital, Marius
Barve, Shirish
author_sort Singhal, Richa
collection PubMed
description Emerging research evidence has established the critical role of the gut-liver axis in the development of alcohol-associated liver disease (ALD). The present study employed 16S rRNA gene and whole genome shotgun (WGS) metagenomic analysis in combination with a revised microbial dataset to comprehensively detail the butyrate-producing microbial communities and the associated butyrate metabolic pathways affected by chronic ethanol feeding. Specifically, the data demonstrated that a decrease in several butyrate-producing bacterial genera belonging to distinct families within the Firmicutes phyla was a significant component of ethanol-induced dysbiosis. WGS analysis of total bacterial genomes encompassing butyrate synthesizing pathways provided the functional characteristics of the microbiome associated with butyrate synthesis. The data revealed that in control mice microbiome, the acetyl-coenzyme A (CoA) butyrate synthesizing pathway was the most prevalent and was significantly and maximally decreased by chronic ethanol feeding. Further WGS analysis i) validated the ethanol-induced decrease in the acetyl-CoA pathway by identifying the decrease in two critical genes but – (butyryl-CoA: acetate CoA transferase) and buk – (butyrate kinase) that encode the terminal condensing enzymes required for converting butyryl-CoA to butyrate and ii) detection of specific taxa of butyrate-producing bacteria containing but and buk genes. Notably, the administration of tributyrin (Tb) – a butyrate prodrug - significantly prevented ethanol-induced decrease in butyrate-producing bacteria, hepatic steatosis, inflammation, and injury. Taken together, our findings strongly suggest that the loss of butyrate-producing bacteria using the acetyl-CoA pathway is a significant pathogenic feature of ethanol-induced microbial dysbiosis and ALD and can be targeted for therapy.
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spelling pubmed-83546572021-08-13 Decrease in acetyl-CoA pathway utilizing butyrate-producing bacteria is a key pathogenic feature of alcohol-induced functional gut microbial dysbiosis and development of liver disease in mice Singhal, Richa Donde, Hridgandh Ghare, Smita Stocke, Kendall Zhang, Jingwein Vadhanam, Manicka Reddy, Sreelatha Gobejishvili, Leila Chilton, Paula Joshi-Barve, Swati Feng, Wenke McClain, Craig Hoffman, Kristi Petrosino, Joseph Vital, Marius Barve, Shirish Gut Microbes Research Paper Emerging research evidence has established the critical role of the gut-liver axis in the development of alcohol-associated liver disease (ALD). The present study employed 16S rRNA gene and whole genome shotgun (WGS) metagenomic analysis in combination with a revised microbial dataset to comprehensively detail the butyrate-producing microbial communities and the associated butyrate metabolic pathways affected by chronic ethanol feeding. Specifically, the data demonstrated that a decrease in several butyrate-producing bacterial genera belonging to distinct families within the Firmicutes phyla was a significant component of ethanol-induced dysbiosis. WGS analysis of total bacterial genomes encompassing butyrate synthesizing pathways provided the functional characteristics of the microbiome associated with butyrate synthesis. The data revealed that in control mice microbiome, the acetyl-coenzyme A (CoA) butyrate synthesizing pathway was the most prevalent and was significantly and maximally decreased by chronic ethanol feeding. Further WGS analysis i) validated the ethanol-induced decrease in the acetyl-CoA pathway by identifying the decrease in two critical genes but – (butyryl-CoA: acetate CoA transferase) and buk – (butyrate kinase) that encode the terminal condensing enzymes required for converting butyryl-CoA to butyrate and ii) detection of specific taxa of butyrate-producing bacteria containing but and buk genes. Notably, the administration of tributyrin (Tb) – a butyrate prodrug - significantly prevented ethanol-induced decrease in butyrate-producing bacteria, hepatic steatosis, inflammation, and injury. Taken together, our findings strongly suggest that the loss of butyrate-producing bacteria using the acetyl-CoA pathway is a significant pathogenic feature of ethanol-induced microbial dysbiosis and ALD and can be targeted for therapy. Taylor & Francis 2021-08-07 /pmc/articles/PMC8354657/ /pubmed/34369304 http://dx.doi.org/10.1080/19490976.2021.1946367 Text en © 2021 The Author(s). Published with license by Taylor & Francis Group, LLC. https://creativecommons.org/licenses/by/4.0/This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/ (https://creativecommons.org/licenses/by/4.0/) ), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Paper
Singhal, Richa
Donde, Hridgandh
Ghare, Smita
Stocke, Kendall
Zhang, Jingwein
Vadhanam, Manicka
Reddy, Sreelatha
Gobejishvili, Leila
Chilton, Paula
Joshi-Barve, Swati
Feng, Wenke
McClain, Craig
Hoffman, Kristi
Petrosino, Joseph
Vital, Marius
Barve, Shirish
Decrease in acetyl-CoA pathway utilizing butyrate-producing bacteria is a key pathogenic feature of alcohol-induced functional gut microbial dysbiosis and development of liver disease in mice
title Decrease in acetyl-CoA pathway utilizing butyrate-producing bacteria is a key pathogenic feature of alcohol-induced functional gut microbial dysbiosis and development of liver disease in mice
title_full Decrease in acetyl-CoA pathway utilizing butyrate-producing bacteria is a key pathogenic feature of alcohol-induced functional gut microbial dysbiosis and development of liver disease in mice
title_fullStr Decrease in acetyl-CoA pathway utilizing butyrate-producing bacteria is a key pathogenic feature of alcohol-induced functional gut microbial dysbiosis and development of liver disease in mice
title_full_unstemmed Decrease in acetyl-CoA pathway utilizing butyrate-producing bacteria is a key pathogenic feature of alcohol-induced functional gut microbial dysbiosis and development of liver disease in mice
title_short Decrease in acetyl-CoA pathway utilizing butyrate-producing bacteria is a key pathogenic feature of alcohol-induced functional gut microbial dysbiosis and development of liver disease in mice
title_sort decrease in acetyl-coa pathway utilizing butyrate-producing bacteria is a key pathogenic feature of alcohol-induced functional gut microbial dysbiosis and development of liver disease in mice
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8354657/
https://www.ncbi.nlm.nih.gov/pubmed/34369304
http://dx.doi.org/10.1080/19490976.2021.1946367
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