4.8 Article

Western-type diet influences mortality from necrotising pancreatitis and demonstrates a central role for butyrate

Journal

GUT
Volume 70, Issue 5, Pages 915-927

Publisher

BMJ PUBLISHING GROUP
DOI: 10.1136/gutjnl-2019-320430

Keywords

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Funding

  1. NIH [R01-GM062344-18]
  2. AMC Executive Board

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The gut microbiota plays a central role in necrotising pancreatitis, with a Western-type diet leading to increased mortality and bacterial dissemination. Butyrate supplementation can reverse these effects, while antibiotic decontamination reduces mortality but increases Gram-positive dissemination. Patients with acute pancreatitis show depleted butyrate producers, indicating a potential role of butyrate in disease progression.
Objective The gut microbiota are the main source of infections in necrotising pancreatitis. We investigated the effect of disruption of the intestinal microbiota by a Western-type diet on mortality and bacterial dissemination in necrotising pancreatitis and its reversal by butyrate supplementation. Design C57BL/6 mice were fed either standard chow or a Western-type diet for 4 weeks and were then subjected to taurocholate-induced necrotising pancreatitis. Blood and pancreas were collected for bacteriology and immune analysis. The cecum microbiota composition of mice was analysed using 16S rRNA gene amplicon sequencing and cecal content metabolites were analysed by targeted (ie, butyrate) and untargeted metabolomics. Prevention of necrotising pancreatitis in this model was compared between faecal microbiota transplantation (FMT) from healthy mice, antibiotic decontamination against Gram-negative bacteria and oral or systemic butyrate administration. Additionally, the faecal microbiota of patients with pancreatitis and healthy subjects were analysed. Results Mortality, systemic inflammation and bacterial dissemination were increased in mice fed Western diet and their gut microbiota were characterised by a loss of diversity, a bloom of Escherichia coli and an altered metabolic profile with butyrate depletion. While antibiotic decontamination decreased mortality, Gram-positive dissemination was increased. Both oral and systemic butyrate supplementation decreased mortality, bacterial dissemination, and reversed the microbiota alterations. Paradoxically, mortality and bacterial dissemination were increased with FMT administration. Finally, patients with acute pancreatitis demonstrated an increase in Proteobacteria and a decrease of butyrate producers compared with healthy subjects. Conclusion Butyrate depletion and its repletion appear to play a central role in disease progression towards necrotising pancreatitis.

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