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      Specific substrate-driven changes in human faecal microbiota composition contrast with functional redundancy in short-chain fatty acid production

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          Abstract

          The diet provides carbohydrates that are non-digestible in the upper gut and are major carbon and energy sources for the microbial community in the lower intestine, supporting a complex metabolic network. Fermentation produces the short-chain fatty acids (SCFAs) acetate, propionate and butyrate, which have health-promoting effects for the human host. Here we investigated microbial community changes and SCFA production during in vitro batch incubations of 15 different non-digestible carbohydrates, at two initial pH values with faecal microbiota from three different human donors. To investigate temporal stability and reproducibility, a further experiment was performed 1 year later with four of the carbohydrates. The lower pH (5.5) led to higher butyrate and the higher pH (6.5) to more propionate production. The strongest propionigenic effect was found with rhamnose, followed by galactomannans, whereas fructans and several α- and β-glucans led to higher butyrate production. 16S ribosomal RNA gene-based quantitative PCR analysis of 22 different microbial groups together with 454 sequencing revealed significant stimulation of specific bacteria in response to particular carbohydrates. Some changes were ascribed to metabolite cross-feeding, for example, utilisation by Eubacterium hallii of 1,2-propanediol produced from fermentation of rhamnose by Blautia spp. Despite marked inter-individual differences in microbiota composition, SCFA production was surprisingly reproducible for different carbohydrates, indicating a level of functional redundancy. Interestingly, butyrate formation was influenced not only by the overall % butyrate-producing bacteria in the community but also by the initial pH, consistent with a pH-dependent shift in the stoichiometry of butyrate production.

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          Author and article information

          Journal
          ISME J
          ISME J
          The ISME Journal
          Nature Publishing Group
          1751-7362
          1751-7370
          February 2018
          01 December 2017
          : 12
          : 2
          : 610-622
          Affiliations
          [1 ] The Rowett Institute, University of Aberdeen , Foresterhill, Aberdeen, UK
          [2 ] Institute of Molecular, Cell and Systems Biology, College of Medical, Veterinary and Life Sciences, University of Glasgow , Glasgow, UK
          [3 ] Biomathematics and Statistics Scotland , Foresterhill, Aberdeen, UK
          [4 ] Department of Food Chemistry and Phytochemistry, Karlsruhe Institute of Technology (KIT) , Adenauerring 20A, Karlsruhe, Germany
          [5 ] Scottish Universities Environmental Research Centre, University of Glasgow, Rankine Avenue , East Kilbride, UK
          Author notes
          [* ] The Rowett Institute, University of Aberdeen, Foresterhill , Aberdeen AB25 2ZD, UK. E-mail: p.louis@ 123456abdn.ac.uk
          Author information
          http://orcid.org/0000-0002-9900-5682
          http://orcid.org/0000-0003-2115-2399
          Article
          PMC5776475 PMC5776475 5776475 ismej2017196
          10.1038/ismej.2017.196
          5776475
          29192904
          16b9dac1-fc54-41c3-870e-462a37855aba
          Copyright © 2018 International Society for Microbial Ecology
          History
          : 19 May 2017
          : 03 October 2017
          : 09 October 2017
          Categories
          Original Article

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