Cross-Feeding and Enzymatic Catabolism for Ma ItalicKeyboard shortcut Ctrl plus Innan-Oligosaccharide Utilization by the Butyrate-Producing Gut Bacterium Roseburia hominis A2-183

MICROORGANISMS(2022)

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摘要
beta-Mannan is abundant in the human diet and in hemicellulose derived from softwood. Linear or galactose-substituted beta-mannan-oligosaccharides (MOS/GMOSs) derived from beta-mannan are considered emerging prebiotics that could stimulate health-associated gut microbiota. However, the underlying mechanisms are not yet resolved. Therefore, this study investigated the cross-feeding and metabolic interactions between Bifidobacterium adolescentis ATCC 15703, an acetate producer, and Roseburia hominis A2-183 DSMZ 16839, a butyrate producer, during utilization of MOS/GMOSs. Cocultivation studies suggest that both strains coexist due to differential MOS/GMOS utilization, along with the cross-feeding of acetate from B. adolescentis E194a to R. hominis A2-183. The data suggest that R. hominis A2-183 efficiently utilizes MOS/GMOS in mono- and cocultivation. Notably, we observed the transcriptional upregulation of certain genes within a dedicated MOS/GMOS utilization locus (RhMosUL), and an exo-oligomannosidase (RhMan113A) gene located distally in the R. hominis A2-183 genome. Significantly, biochemical analysis of beta-1,4 mannan-oligosaccharide phosphorylase (RhMOP130A), alpha-galactosidase (RhGal36A), and exo-oligomannosidase (RhMan113A) suggested their potential synergistic role in the initial utilization of MOS/GMOSs. Thus, our results enhance the understanding of MOS/GMOS utilization by potential health-promoting human gut microbiota and highlight the role of cross-feeding and metabolic interactions between two secondary mannan degraders inhabiting the same ecological niche in the gut.
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beta-mannan-oligosaccharides,Roseburia hominis,Bifidobacterium adolescentis,cocultivation,cross-feeding,butyrate production,differential gene expression,beta-1,4 mannan-oligosaccharide phosphorylase,alpha-galactosidase,exo-oligomannosidase
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