Literature DB >> 21883787

Arabinoxylans and inulin differentially modulate the mucosal and luminal gut microbiota and mucin-degradation in humanized rats.

Pieter Van den Abbeele1, Philippe Gérard, Sylvie Rabot, Aurélia Bruneau, Sahar El Aidy, Muriel Derrien, Michiel Kleerebezem, Erwin G Zoetendal, Hauke Smidt, Willy Verstraete, Tom Van de Wiele, Sam Possemiers.   

Abstract

The endogenous gut microbiota affects the host in many ways. Prebiotics should favour beneficial intestinal microbes and thus improve host health. In this study, we investigated how a novel class of potential prebiotic long-chain arabinoxylans (LC-AX) and the well-established prebiotic inulin (IN) modulate the gut microbiota of humanized rats. Six weeks after axenic rats were inoculated with a human faecal microbiota, their colonic microbiota was similar to this inoculum (∼ 70%), whereas their caecal microbiota was enriched with Verrucomicrobia and Firmicutes concomitant with lower abundance of Bacteroidetes. Moreover, different Bifidobacterium species colonized the lumen (B. adolescentis) and mucus (B. longum and B. bifidum). Both LC-AX and IN increased SCFA levels and induced a shift from acetate towards health-promoting propionate and butyrate respectively. By applying a high-resolution phylogenetic micro-array (HITChip) at the site of fermentation (caecum), IN and LC-AX were shown to stimulate bacterial groups with known butyrate-producers (Roseburia intestinalis, Eubacterium rectale, Anaerostipes caccae) and bifidobacteria (B. longum) respectively. Prebiotic administration also resulted in lower caecal abundances of the mucin-degrading Akkermansia muciniphila and potentially more mucin production by the host. Both factors might explain the increased caecal mucin levels for LC-AX (threefold) and IN (sixfold). These mucins were degraded along the colon, resulting in high faecal abundances of Akkermansia muciniphila for LC-AX and especially IN-treated rats. Finally, the microbial changes caused an adaptation period for the host with less weight gain, after which the host fine-tuned the interaction with this altered microbiota. Our results demonstrate that next to IN, LC-AX are promising prebiotic compounds by stimulating production of health-promoting metabolites by specific microbes in the proximal regions. Further, prebiotic supplementation shifted mucin degradation to distal regions, where mucin-degraders may produce beneficial metabolites (e.g. propionate by Akkermansia muciniphila), so that prebiotics may potentially improve gut health along the entire length of the intestine.
© 2011 Society for Applied Microbiology and Blackwell Publishing Ltd.

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Year:  2011        PMID: 21883787     DOI: 10.1111/j.1462-2920.2011.02533.x

Source DB:  PubMed          Journal:  Environ Microbiol        ISSN: 1462-2912            Impact factor:   5.491


  71 in total

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Authors:  Audrey Rivière; Mérilie Gagnon; Stefan Weckx; Denis Roy; Luc De Vuyst
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2.  Gut microbiota: Inulin regulates endothelial function: a prebiotic smoking gun?

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Review 4.  Linking dietary patterns with gut microbial composition and function.

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Review 5.  The prebiotic potential of brewers' spent grain on livestock's health: a review.

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6.  Butyrate-producing Clostridium cluster XIVa species specifically colonize mucins in an in vitro gut model.

Authors:  Pieter Van den Abbeele; Clara Belzer; Margot Goossens; Michiel Kleerebezem; Willem M De Vos; Olivier Thas; Rosemarie De Weirdt; Frederiek-Maarten Kerckhof; Tom Van de Wiele
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7.  Synergetic responses of intestinal microbiota and epithelium to dietary inulin supplementation in pigs.

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Review 9.  Microbiota and metabolic diseases.

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10.  Beneficial effects of protease preparations derived from Aspergillus on the colonic luminal environment in rats consuming a high-fat diet.

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Journal:  Biomed Rep       Date:  2015-07-15
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