Two microbiota subtypes identified in irritable bowel syndrome with distinct responses to the low FODMAP diet

Kevin Vervier; Stephen Moss; Nitin Kumar; Anne Adoum; Meg Barne; Hilary Browne; Arthur Kaser; Christopher J. Kiely; B. Anne Neville; Nina Powell; Tim Raine; Mark D. Stares; Ana Zhu; Juan De La Revilla Negro; Trevor D. Lawley; Miles Parkes

doi:10.1136/gutjnl-2021-325177

Two microbiota subtypes identified in irritable bowel syndrome with distinct responses to the low FODMAP diet

Kevin Vervier
, Stephen Moss
, Nitin Kumar
, Anne Adoum
, Meg Barne
, Hilary Browne
, Arthur Kaser
, Christopher J. Kiely
, B. Anne Neville
, Nina Powell
, Tim Raine
, Mark D. Stares
, Ana Zhu
, Juan De La Revilla Negro
, Trevor D. Lawley
, Miles Parkes

Research output: Contribution to journal › Article › peer-review

Abstract

Objective: Reducing FODMAPs (fermentable oligosaccharides, disaccharides, monosaccharides and polyols) can be clinically beneficial in IBS but the mechanism is incompletely understood. We aimed to detect microbial signatures that might predict response to the low FODMAP diet and assess whether microbiota compositional and functional shifts could provide insights into its mode of action. Design: We used metagenomics to determine high-resolution taxonomic and functional profiles of the stool microbiota from IBS cases and household controls (n=56 pairs) on their usual diet. Clinical response and microbiota changes were studied in 41 pairs after 4 weeks on a low FODMAP diet. Results: Unsupervised analysis of baseline IBS cases pre-diet identified two distinct microbiota profiles, which we refer to as IBS^P (pathogenic-like) and IBS^H (health-like) subtypes. IBS^P microbiomes were enriched in Firmicutes and genes for amino acid and carbohydrate metabolism, but depleted in Bacteroidetes species. IBS^H microbiomes were similar to controls. On the low FODMAP diet, IBS^H and control microbiota were unaffected, but the IBS^P signature shifted towards a health-associated microbiome with an increase in Bacteroidetes (p=0.009), a decrease in Firmicutes species (p=0.004) and normalisation of primary metabolic genes. The clinical response to the low FODMAP diet was greater in IBS^P subjects compared with IBS^H (p=0.02). Conclusion: 50% of IBS cases manifested a 'pathogenic' gut microbial signature. This shifted towards the healthy profile on the low FODMAP diet; and IBS^P cases showed an enhanced clinical responsiveness to the dietary therapy. The effectiveness of FODMAP reduction in IBS^P may result from the alterations in gut microbiota and metabolites produced. Microbiota signatures could be useful as biomarkers to guide IBS treatment; and investigating IBS^P species and metabolic pathways might yield insights regarding IBS pathogenic mechanisms.

Original language	English
Pages (from-to)	1821-1830
Number of pages	10
Journal	Gut
Volume	71
Issue number	9
DOIs	https://doi.org/10.1136/gutjnl-2021-325177
Publication status	Published - 2022
Externally published	Yes

Access to Document

10.1136/gutjnl-2021-325177

Cite this

Vervier, K., Moss, S., Kumar, N., Adoum, A., Barne, M., Browne, H., Kaser, A., Kiely, C. J., Neville, B. A., Powell, N., Raine, T., Stares, M. D., Zhu, A., Negro, J. D. L. R., Lawley, T. D., & Parkes, M. (2022). Two microbiota subtypes identified in irritable bowel syndrome with distinct responses to the low FODMAP diet. Gut, 71(9), 1821-1830. https://doi.org/10.1136/gutjnl-2021-325177

@article{9133b1d328874c43bf2fc52775d9ff9c,

title = "Two microbiota subtypes identified in irritable bowel syndrome with distinct responses to the low FODMAP diet",

abstract = "Objective: Reducing FODMAPs (fermentable oligosaccharides, disaccharides, monosaccharides and polyols) can be clinically beneficial in IBS but the mechanism is incompletely understood. We aimed to detect microbial signatures that might predict response to the low FODMAP diet and assess whether microbiota compositional and functional shifts could provide insights into its mode of action. Design: We used metagenomics to determine high-resolution taxonomic and functional profiles of the stool microbiota from IBS cases and household controls (n=56 pairs) on their usual diet. Clinical response and microbiota changes were studied in 41 pairs after 4 weeks on a low FODMAP diet. Results: Unsupervised analysis of baseline IBS cases pre-diet identified two distinct microbiota profiles, which we refer to as IBSP (pathogenic-like) and IBSH (health-like) subtypes. IBSP microbiomes were enriched in Firmicutes and genes for amino acid and carbohydrate metabolism, but depleted in Bacteroidetes species. IBSH microbiomes were similar to controls. On the low FODMAP diet, IBSH and control microbiota were unaffected, but the IBSP signature shifted towards a health-associated microbiome with an increase in Bacteroidetes (p=0.009), a decrease in Firmicutes species (p=0.004) and normalisation of primary metabolic genes. The clinical response to the low FODMAP diet was greater in IBSP subjects compared with IBSH (p=0.02). Conclusion: 50\% of IBS cases manifested a 'pathogenic' gut microbial signature. This shifted towards the healthy profile on the low FODMAP diet; and IBSP cases showed an enhanced clinical responsiveness to the dietary therapy. The effectiveness of FODMAP reduction in IBSP may result from the alterations in gut microbiota and metabolites produced. Microbiota signatures could be useful as biomarkers to guide IBS treatment; and investigating IBSP species and metabolic pathways might yield insights regarding IBS pathogenic mechanisms.",

author = "Kevin Vervier and Stephen Moss and Nitin Kumar and Anne Adoum and Meg Barne and Hilary Browne and Arthur Kaser and Kiely, \{Christopher J.\} and Neville, \{B. Anne\} and Nina Powell and Tim Raine and Stares, \{Mark D.\} and Ana Zhu and Negro, \{Juan De La Revilla\} and Lawley, \{Trevor D.\} and Miles Parkes",

note = "Publisher Copyright: {\textcopyright} 2022 Author(s) (or their employer(s)).",

year = "2022",

doi = "10.1136/gutjnl-2021-325177",

language = "English",

volume = "71",

pages = "1821--1830",

journal = "Gut",

issn = "0017-5749",

publisher = "BMJ Publishing Group",

number = "9",

}

Vervier, K, Moss, S, Kumar, N, Adoum, A, Barne, M, Browne, H, Kaser, A, Kiely, CJ, Neville, BA, Powell, N, Raine, T, Stares, MD, Zhu, A, Negro, JDLR, Lawley, TD & Parkes, M 2022, 'Two microbiota subtypes identified in irritable bowel syndrome with distinct responses to the low FODMAP diet', Gut, vol. 71, no. 9, pp. 1821-1830. https://doi.org/10.1136/gutjnl-2021-325177

TY - JOUR

T1 - Two microbiota subtypes identified in irritable bowel syndrome with distinct responses to the low FODMAP diet

AU - Vervier, Kevin

AU - Moss, Stephen

AU - Kumar, Nitin

AU - Adoum, Anne

AU - Barne, Meg

AU - Browne, Hilary

AU - Kaser, Arthur

AU - Kiely, Christopher J.

AU - Neville, B. Anne

AU - Powell, Nina

AU - Raine, Tim

AU - Stares, Mark D.

AU - Zhu, Ana

AU - Negro, Juan De La Revilla

AU - Lawley, Trevor D.

AU - Parkes, Miles

PY - 2022

Y1 - 2022

N2 - Objective: Reducing FODMAPs (fermentable oligosaccharides, disaccharides, monosaccharides and polyols) can be clinically beneficial in IBS but the mechanism is incompletely understood. We aimed to detect microbial signatures that might predict response to the low FODMAP diet and assess whether microbiota compositional and functional shifts could provide insights into its mode of action. Design: We used metagenomics to determine high-resolution taxonomic and functional profiles of the stool microbiota from IBS cases and household controls (n=56 pairs) on their usual diet. Clinical response and microbiota changes were studied in 41 pairs after 4 weeks on a low FODMAP diet. Results: Unsupervised analysis of baseline IBS cases pre-diet identified two distinct microbiota profiles, which we refer to as IBSP (pathogenic-like) and IBSH (health-like) subtypes. IBSP microbiomes were enriched in Firmicutes and genes for amino acid and carbohydrate metabolism, but depleted in Bacteroidetes species. IBSH microbiomes were similar to controls. On the low FODMAP diet, IBSH and control microbiota were unaffected, but the IBSP signature shifted towards a health-associated microbiome with an increase in Bacteroidetes (p=0.009), a decrease in Firmicutes species (p=0.004) and normalisation of primary metabolic genes. The clinical response to the low FODMAP diet was greater in IBSP subjects compared with IBSH (p=0.02). Conclusion: 50% of IBS cases manifested a 'pathogenic' gut microbial signature. This shifted towards the healthy profile on the low FODMAP diet; and IBSP cases showed an enhanced clinical responsiveness to the dietary therapy. The effectiveness of FODMAP reduction in IBSP may result from the alterations in gut microbiota and metabolites produced. Microbiota signatures could be useful as biomarkers to guide IBS treatment; and investigating IBSP species and metabolic pathways might yield insights regarding IBS pathogenic mechanisms.

AB - Objective: Reducing FODMAPs (fermentable oligosaccharides, disaccharides, monosaccharides and polyols) can be clinically beneficial in IBS but the mechanism is incompletely understood. We aimed to detect microbial signatures that might predict response to the low FODMAP diet and assess whether microbiota compositional and functional shifts could provide insights into its mode of action. Design: We used metagenomics to determine high-resolution taxonomic and functional profiles of the stool microbiota from IBS cases and household controls (n=56 pairs) on their usual diet. Clinical response and microbiota changes were studied in 41 pairs after 4 weeks on a low FODMAP diet. Results: Unsupervised analysis of baseline IBS cases pre-diet identified two distinct microbiota profiles, which we refer to as IBSP (pathogenic-like) and IBSH (health-like) subtypes. IBSP microbiomes were enriched in Firmicutes and genes for amino acid and carbohydrate metabolism, but depleted in Bacteroidetes species. IBSH microbiomes were similar to controls. On the low FODMAP diet, IBSH and control microbiota were unaffected, but the IBSP signature shifted towards a health-associated microbiome with an increase in Bacteroidetes (p=0.009), a decrease in Firmicutes species (p=0.004) and normalisation of primary metabolic genes. The clinical response to the low FODMAP diet was greater in IBSP subjects compared with IBSH (p=0.02). Conclusion: 50% of IBS cases manifested a 'pathogenic' gut microbial signature. This shifted towards the healthy profile on the low FODMAP diet; and IBSP cases showed an enhanced clinical responsiveness to the dietary therapy. The effectiveness of FODMAP reduction in IBSP may result from the alterations in gut microbiota and metabolites produced. Microbiota signatures could be useful as biomarkers to guide IBS treatment; and investigating IBSP species and metabolic pathways might yield insights regarding IBS pathogenic mechanisms.

UR - https://www.scopus.com/pages/publications/85136339240

U2 - 10.1136/gutjnl-2021-325177

DO - 10.1136/gutjnl-2021-325177

M3 - Article

C2 - 34810234

AN - SCOPUS:85136339240

SN - 0017-5749

VL - 71

SP - 1821

EP - 1830

JO - Gut

JF - Gut

IS - 9

ER -

Two microbiota subtypes identified in irritable bowel syndrome with distinct responses to the low FODMAP diet

Abstract

Access to Document

Other files and links

Fingerprint

Cite this