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Dietary supplementation with inulin-propionate ester or inulin improves insulin sensitivity in adults with overweight and obesity with distinct effects on the gut microbiota, plasma metabolome and systemic inflammatory responses: a randomised cross-over trial

菊粉 丙酸盐 肠道菌群 代谢组 内科学 内分泌学 胰岛素 胰岛素抵抗 纤维素 化学 医学 食品科学 生物化学 代谢物
作者
Edward S. Chambers,Claire Byrne,Douglas J. Morrison,Kevin G. Murphy,Tom Preston,Catriona Tedford,Isabel García‐Pérez,Sofia Fountana,José Iván Serrano-Contreras,Elaine Holmes,Catherine J. Reynolds,Jordie F Roberts,Rosemary J. Boyton,Daniel M. Altmann,Julie A. K. McDonald,Julian R. Marchesi,Arne N. Akbar,Natalie E. Riddell,Gareth A. Wallis,Gary Frost
出处
期刊:Gut [BMJ]
卷期号:68 (8): 1430-1438 被引量:280
标识
DOI:10.1136/gutjnl-2019-318424
摘要

Objective To investigate the underlying mechanisms behind changes in glucose homeostasis with delivery of propionate to the human colon by comprehensive and coordinated analysis of gut bacterial composition, plasma metabolome and immune responses. Design Twelve non-diabetic adults with overweight and obesity received 20 g/day of inulin-propionate ester (IPE), designed to selectively deliver propionate to the colon, a high-fermentable fibre control (inulin) and a low-fermentable fibre control (cellulose) in a randomised, double-blind, placebo-controlled, cross-over design. Outcome measurements of metabolic responses, inflammatory markers and gut bacterial composition were analysed at the end of each 42-day supplementation period. Results Both IPE and inulin supplementation improved insulin resistance compared with cellulose supplementation, measured by homeostatic model assessment 2 (mean±SEM 1.23±0.17 IPE vs 1.59±0.17 cellulose, p=0.001; 1.17±0.15 inulin vs 1.59±0.17 cellulose, p=0.009), with no differences between IPE and inulin (p=0.272). Fasting insulin was only associated positively with plasma tyrosine and negatively with plasma glycine following inulin supplementation. IPE supplementation decreased proinflammatory interleukin-8 levels compared with cellulose, while inulin had no impact on the systemic inflammatory markers studied. Inulin promoted changes in gut bacterial populations at the class level (increased Actinobacteria and decreased Clostridia) and order level (decreased Clostridiales) compared with cellulose, with small differences at the species level observed between IPE and cellulose. Conclusion These data demonstrate a distinctive physiological impact of raising colonic propionate delivery in humans, as improvements in insulin sensitivity promoted by IPE and inulin were accompanied with different effects on the plasma metabolome, gut bacterial populations and markers of systemic inflammation.

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