Article (Périodiques scientifiques)
Comparative Genomic Analysis of the Human Gut Microbiome Reveals a Broad Distribution of Metabolic Pathways for the Degradation of Host-Synthetized Mucin Glycans and Utilization of Mucin-Derived Monosaccharides
RAVCHEEV, Dmitry; THIELE, Ines
2017In Frontiers in Genetics, 8, p. 111
Peer reviewed vérifié par ORBi
 

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The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest. The reviewer WY and handling Editor declared their shared affiliation.


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Détails



Mots-clés :
human gut microbiome; comparative genomics; mucin glycans; carbohydrate utilization; metabolism reconstruction
Résumé :
[en] The colonic mucus layer is a dynamic and complex structure formed by secreted and transmembrane mucins, which are high-molecular-weight and heavily glycosylated proteins. Colonic mucus consists of a loose outer layer and a dense epithelium-attached layer. The outer layer is inhabited by various representatives of the human gut microbiota (HGM). Glycans of the colonic mucus can be used by the HGM as a source of carbon and energy when dietary fibers are not sufficiently available. Both commensals and pathogens can utilize mucin glycans. Commensals are mostly involved in the cleavage of glycans, while pathogens mostly utilize monosaccharides released by commensals. This HGM-derived degradation of the mucus layer increases pathogen susceptibility and causes many other health disorders. Here, we analyzed 397 individual HGM genomes to identify pathways for the cleavage of host-synthetized mucin glycans to monosaccharides as well as for the catabolism of the derived monosaccharides. Our key results are as follows: (i) Genes for the cleavage of mucin glycans were found in 86% of the analyzed genomes, which significantly higher than a previous estimation. (ii) Genes for the catabolism of derived monosaccharides were found in 89% of the analyzed genomes. (iii) Comparative genomic analysis identified four alternative forms of the monosaccharide-catabolizing enzymes and four alternative forms of monosaccharide transporters. (iv) Eighty-five percent of the analyzed genomes may be involved in potential feeding pathways for the monosaccharides derived from cleaved mucin glycans. (v) The analyzed genomes demonstrated different abilities to degrade known mucin glycans. Generally, the ability to degrade at least one type of mucin glycan was predicted for 81% of the analyzed genomes. (vi) Eighty-two percent of the analyzed genomes can form mutualistic pairs that are able to degrade mucin glycans and are not degradable by any of the paired organisms alone. Taken together, these findings provide further insight into the inter-microbial communications of the HGM as well as into host-HGM interactions.
Disciplines :
Microbiologie
Biochimie, biophysique & biologie moléculaire
Auteur, co-auteur :
RAVCHEEV, Dmitry ;  University of Luxembourg > Luxembourg Centre for Systems Biomedicine (LCSB)
THIELE, Ines ;  University of Luxembourg > Luxembourg Centre for Systems Biomedicine (LCSB)
Co-auteurs externes :
no
Langue du document :
Anglais
Titre :
Comparative Genomic Analysis of the Human Gut Microbiome Reveals a Broad Distribution of Metabolic Pathways for the Degradation of Host-Synthetized Mucin Glycans and Utilization of Mucin-Derived Monosaccharides
Date de publication/diffusion :
29 août 2017
Titre du périodique :
Frontiers in Genetics
eISSN :
1664-8021
Maison d'édition :
Frontiers, Lausanne, Suisse
Volume/Tome :
8
Pagination :
111
Peer reviewed :
Peer reviewed vérifié par ORBi
Focus Area :
Computational Sciences
Intitulé du projet de recherche :
Genome-based analysis of the human gut microbiome: in silico reconstruction of metabolic and regulatory pathways
Organisme subsidiant :
National Research Fund Luxembourg
Disponible sur ORBilu :
depuis le 12 septembre 2017

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