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Multi-omics signatures in new-onset diabetes predict metabolic response to dietary inulin: findings from an observational study followed by an interventional trial

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Autor
Ďásková, NikolaORCiD Profile - 0000-0002-8038-8361Scopus Profile - 57208670001
Modos, Istvan
Krbcová, Magdaléna
Kuzma, Marek
Pelantová, Helena
Hradecký, Jaromír
Heczková, Marie
Bratová, Monika
Videňská, Petra
Šplíchalová, Petra
Králová, Maria
Heniková, MarinaORCiD Profile - 0000-0002-3253-0853
Potočková, Jana
Ouřadová, Anna
Landberg, Rikard
Kühn, Tilman
Cahová, Monika
Gojda, JanORCiD Profile - 0000-0002-7995-5947WoS Profile - F-8909-2017Scopus Profile - 54388050200

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Datum vydání
2023
Publikováno v
Nutrition & Diabetes [online]
Ročník / Číslo vydání
13 (1)
ISBN / ISSN
ISSN: 2044-4052
Metadata
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Kolekce
  • 1. lékařská fakulta

Tato publikace má vydavatelskou verzi s DOI 10.1038/s41387-023-00235-5

Abstrakt
AIM: The metabolic performance of the gut microbiota contributes to the onset of type 2 diabetes. However, targeted dietary interventions are limited by the highly variable inter-individual response. We hypothesized (1) that the composition of the complex gut microbiome and metabolome (MIME) differ across metabolic spectra (lean-obese-diabetes); (2) that specific MIME patterns could explain the differential responses to dietary inulin; and (3) that the response can be predicted based on baseline MIME signature and clinical characteristics. METHOD: Forty-nine patients with newly diagnosed pre/diabetes (DM), 66 metabolically healthy overweight/obese (OB), and 32 healthy lean (LH) volunteers were compared in a cross-sectional case-control study integrating clinical variables, dietary intake, gut microbiome, and fecal/serum metabolomes (16 S rRNA sequencing, metabolomics profiling). Subsequently, 27 DM were recruited for a predictive study: 3 months of dietary inulin (10 g/day) intervention. RESULTS: MIME composition was different between groups. While the DM and LH groups represented opposite poles of the abundance spectrum, OB was closer to DM. Inulin supplementation was associated with an overall improvement in glycemic indices, though the response was very variable, with a shift in microbiome composition toward a more favorable profile and increased serum butyric and propionic acid concentrations. The improved glycemic outcomes of inulin treatment were dependent on better baseline glycemic status and variables related to the gut microbiota, including the abundance of certain bacterial taxa (i.e., Blautia, Eubacterium halii group, Lachnoclostridium, Ruminiclostridium, Dialister, or Phascolarctobacterium), serum concentrations of branched-chain amino acid derivatives and asparagine, and fecal concentrations of indole and several other volatile organic compounds. CONCLUSION: We demonstrated that obesity is a stronger determinant of different MIME patterns than impaired glucose metabolism. The large inter-individual variability in the metabolic effects of dietary inulin was explained by differences in baseline glycemic status and MIME signatures. These could be further validated to personalize nutritional interventions in patients with newly diagnosed diabetes.
Klíčová slova
chain fatty-acids, gut microbiota, insulin-secretion, fermentation, metagenome, increases, capacity, dilution, obesity, fiber
Trvalý odkaz
https://hdl.handle.net/20.500.14178/1877
Zobraz publikaci v dalších systémech
WOS:000975357800002
SCOPUS:2-s2.0-85153555484
PUBMED:37085526
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