Hostname: page-component-8448b6f56d-qsmjn Total loading time: 0 Render date: 2024-04-19T23:00:07.251Z Has data issue: false hasContentIssue false
  • English
  • Français

Targeted delivery of propionate to the human colon prevents body weight and intra-abdominal adipose tissue gain in overweight adults

Published online by Cambridge University Press:  20 May 2014

E. S. Chambers ,
A. Viardot ,
A. Psichas ,
D. J. Morrison ,
K. G. Murphy ,
S. E. K. Zac-Varghese ,
K. MacDougall ,
T. Preston ,
M. C. Tedford  and
J. D. Bell
...Show all authors
E. S. Chambers
Affiliation:
Nutrition and Dietetic Research Group, University of Glasgow, G75 0QF, UK
A. Viardot
Affiliation:
Nutrition and Dietetic Research Group, University of Glasgow, G75 0QF, UK
A. Psichas
Affiliation:
Nutrition and Dietetic Research Group, University of Glasgow, G75 0QF, UK
D. J. Morrison
Affiliation:
Scottish Universities Environmental Research Centre, University of Glasgow, G75 0QF, UK
K. G. Murphy
Affiliation:
Section of Investigative Medicine, Imperial College London, W12 0NN, UK
S. E. K. Zac-Varghese
Affiliation:
Section of Investigative Medicine, Imperial College London, W12 0NN, UK
K. MacDougall
Affiliation:
School of Science, University of the West of Scotland, Paisley PA1 2BE, UK
T. Preston
Affiliation:
Scottish Universities Environmental Research Centre, University of Glasgow, G75 0QF, UK
M. C. Tedford
Affiliation:
School of Science, University of the West of Scotland, Paisley PA1 2BE, UK
J. D. Bell
Affiliation:
MRC Clinical Science Centre, Imperial College London, W12 0NN, UK
E. L. Thomas
Affiliation:
MRC Clinical Science Centre, Imperial College London, W12 0NN, UK
S. Mt-Isa
Affiliation:
Imperial Clinical Trials Unit, Imperial College London, W2 1NY, UK
D. Ashby
Affiliation:
Imperial Clinical Trials Unit, Imperial College London, W2 1NY, UK
W. S. Dhillo
Affiliation:
Section of Investigative Medicine, Imperial College London, W12 0NN, UK
S. R. Bloom
Affiliation:
Section of Investigative Medicine, Imperial College London, W12 0NN, UK
W. G. Morley
Affiliation:
Leatherhead Food Research, Leatherhead KT22 7RY, UK
S. Clegg
Affiliation:
Leatherhead Food Research, Leatherhead KT22 7RY, UK
G. Frost
Affiliation:
Nutrition and Dietetic Research Group, University of Glasgow, G75 0QF, UK
Rights & Permissions [Opens in a new window]

Abstract

An abstract is not available for this content. As you have access to this content, full HTML content is provided on this page. A PDF of this content is also available in through the ‘Save PDF’ action button.
Type
Abstract
Information
Proceedings of the Nutrition Society , Volume 73 , Issue OCE1: Winter Meeting, 11–12 December 2013, Diet, gut microbiology and human health , 2014 , E22
Copyright
Copyright © The Authors 2014 

The colonic microbiota ferment available carbohydrates, producing short chain fatty acids (SCFAs), which trigger the release of the anorectic gut hormones peptide YY (PYY) and glucagon like peptide-1 (GLP-1) by stimulating the free fatty acid receptors (FFAR) 2 and 3 on the enteroendocrine L cells( Reference Tolhurst, Heffron and Lam 1 ). We have developed a novel inulin propionate ester that targets delivery of gram quantities of the SCFA propionate to the human colon and which significantly increases PYY and GLP-1 secretion and reduces food intake following acute ingestion at a dose of 10 g (unpublished observation). We hypothesised that long-term supplementation with propionate ester would prevent weight gain in overweight adults.

Forty nine men and women aged 40–65 years, with a body mass index (BMI) of 25–40 kg/m2 were recruited and randomly assigned to receive either 10 g/day inulin control (n = 24) or 10 g/day propionate ester (n = 25) for 24-weeks. Body composition data, assessed using magnetic resonance imaging, was collected from 17 subjects in the propionate ester group and 15 subjects in the control group.

AT, adipose tissue. **P < 0.01 within-group, ***P < 0.001 within-group, †P < 0.05 between groups.

Significantly fewer subjects gained ⩾3% (P = 0.036) and >5% (P = 0.033) of their baseline body weight following propionate ester supplementation. Weight loss after 24 weeks was greater in the propionate ester group, but this effect was not significantly different between groups (−1.02 kg [95% CI, −2.10 to 0.04] propionate ester vs. 0.38 kg [95% CI, −0.95 to 1.72] control; P = 0.099). The change in the distribution of intra-abdominal adipose tissue (AT) was significantly lower in the propionate ester group compared with control supplementation (P = 0.027). Furthermore, internal AT (P = 0.002) was significantly increased within the control group, but not in the propionate ester group.

In conclusion, this investigation provides the first direct evidence that colonic propionate can prevent body weight and intra-abdominal AT gain in humans. Dietary strategies that promote colonic propionate production may play a role in weight management over the life-course.

This work was supported by the Biotechnology & Biological Sciences Research Council (BB/H004971/1). The clinical trial (NCT00750438) was conducted in accordance with the Declaration of Helsinki.

References

1. Tolhurst, G, Heffron, H, Lam, YS, et al. (2011) Diabetes 61, 364371.Google Scholar