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Longitudinal multi-omics reveals subset-specific mechanisms underlying irritable bowel syndrome

Longitudinal multi-omics reveals subset-specific mechanisms underlying irritable bowel syndrome
Longitudinal multi-omics reveals subset-specific mechanisms underlying irritable bowel syndrome

The gut microbiome has been implicated in multiple human chronic gastrointestinal (GI) disorders. Determining its mechanistic role in disease has been difficult due to apparent disconnects between animal and human studies and lack of an integrated multi-omics view of disease-specific physiological changes. We integrated longitudinal multi-omics data from the gut microbiome, metabolome, host epigenome, and transcriptome in the context of irritable bowel syndrome (IBS) host physiology. We identified IBS subtype-specific and symptom-related variation in microbial composition and function. A subset of identified changes in microbial metabolites correspond to host physiological mechanisms that are relevant to IBS. By integrating multiple data layers, we identified purine metabolism as a novel host-microbial metabolic pathway in IBS with translational potential. Our study highlights the importance of longitudinal sampling and integrating complementary multi-omics data to identify functional mechanisms that can serve as therapeutic targets in a comprehensive treatment strategy for chronic GI diseases. Video Abstract: [Figure presented]. Integrated and longitudinal multiomic analyses of patients with irritable bowel syndrome reveals a role for the gut microbiota in modulating purine metabolism and influencing host gastrointestinal function.

physiology, functional bowel disorders, diet, symptom severity, secretion, nucleosides, bile acids, short chain fatti acids
0092-8674
1460-1473.e17
Mars, Ruben A.T.
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Yang, Yi
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Ward, Tonya
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Houtti, Mo
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Priya, Sambhawa
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Lekatz, Heather R.
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Tang, Xiaojia
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Sun, Zhifu
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Kalari, Krishna R.
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Korem, Tal
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Bhattarai, Yogesh
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Zheng, Tenghao
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Bar, Noam
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Frost, Gary
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Johnson, Abigail J.
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Treuren, Will van
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Han, Shuo
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Ordog, Tamas
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Grover, Madhusudan
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Sonnenburg, Justin
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D’Amato, Mauro
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Camilleri, Michael
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Elinav, Eran
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Segal, Eran
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Blekhman, Ran
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Farrugia, Gianrico
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Swann, Jonathan R.
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Knights, Dan
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Kashyap, Purna C.
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Mars, Ruben A.T.
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Yang, Yi
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Ward, Tonya
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Houtti, Mo
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Priya, Sambhawa
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Lekatz, Heather R.
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Tang, Xiaojia
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Sun, Zhifu
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Kalari, Krishna R.
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Korem, Tal
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Bhattarai, Yogesh
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Zheng, Tenghao
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Bar, Noam
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Frost, Gary
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Johnson, Abigail J.
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Treuren, Will van
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Han, Shuo
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Ordog, Tamas
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Grover, Madhusudan
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Sonnenburg, Justin
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D’Amato, Mauro
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Camilleri, Michael
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Elinav, Eran
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Segal, Eran
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Blekhman, Ran
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Farrugia, Gianrico
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Swann, Jonathan R.
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Knights, Dan
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Kashyap, Purna C.
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Mars, Ruben A.T., Yang, Yi, Ward, Tonya, Houtti, Mo, Priya, Sambhawa, Lekatz, Heather R., Tang, Xiaojia, Sun, Zhifu, Kalari, Krishna R., Korem, Tal, Bhattarai, Yogesh, Zheng, Tenghao, Bar, Noam, Frost, Gary, Johnson, Abigail J., Treuren, Will van, Han, Shuo, Ordog, Tamas, Grover, Madhusudan, Sonnenburg, Justin, D’Amato, Mauro, Camilleri, Michael, Elinav, Eran, Segal, Eran, Blekhman, Ran, Farrugia, Gianrico, Swann, Jonathan R., Knights, Dan and Kashyap, Purna C. (2020) Longitudinal multi-omics reveals subset-specific mechanisms underlying irritable bowel syndrome. Cell, 182 (6), 1460-1473.e17. (doi:10.1016/j.cell.2020.08.007).

Record type: Article

Abstract

The gut microbiome has been implicated in multiple human chronic gastrointestinal (GI) disorders. Determining its mechanistic role in disease has been difficult due to apparent disconnects between animal and human studies and lack of an integrated multi-omics view of disease-specific physiological changes. We integrated longitudinal multi-omics data from the gut microbiome, metabolome, host epigenome, and transcriptome in the context of irritable bowel syndrome (IBS) host physiology. We identified IBS subtype-specific and symptom-related variation in microbial composition and function. A subset of identified changes in microbial metabolites correspond to host physiological mechanisms that are relevant to IBS. By integrating multiple data layers, we identified purine metabolism as a novel host-microbial metabolic pathway in IBS with translational potential. Our study highlights the importance of longitudinal sampling and integrating complementary multi-omics data to identify functional mechanisms that can serve as therapeutic targets in a comprehensive treatment strategy for chronic GI diseases. Video Abstract: [Figure presented]. Integrated and longitudinal multiomic analyses of patients with irritable bowel syndrome reveals a role for the gut microbiota in modulating purine metabolism and influencing host gastrointestinal function.

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Accepted/In Press date: 31 July 2020
e-pub ahead of print date: 10 September 2020
Published date: 17 September 2020
Additional Information: Funding Information: The authors would like to thank Lyndsay Busby for secretarial assistance and J.M. Nielsen for help with figures. This work was supported by NIH grant DK114007 (P.C.K.); the Center for Individualized Medicine, Mayo Clinic , Rochester, MN (P.C.K.); the Minnesota Partnership for Biotechnology and Medical Genomics (P.C.K. and D.K.); the STRATiGRAD PhD training program of Imperial College London ( https://www.imperial.ac.uk/stratigrad/ ) (Y.Y.); Société des Produits Nestle (J.R.S.); Imperial College NIHR BRC (J.R.S.); and NIH grant R35-GM128716 (R.B.). Publisher Copyright: © 2020 Elsevier Inc.
Keywords: physiology, functional bowel disorders, diet, symptom severity, secretion, nucleosides, bile acids, short chain fatti acids

Identifiers

Local EPrints ID: 443952
URI: http://eprints.soton.ac.uk/id/eprint/443952
DOI: doi:10.1016/j.cell.2020.08.007
ISSN: 0092-8674
PURE UUID: a3b54431-4ffe-4aff-a227-363c7dc0e6a6
ORCID for Jonathan R. Swann: ORCID iD orcid.org/0000-0002-6485-4529

Catalogue record

Date deposited: 17 Sep 2020 16:41
Last modified: 17 Mar 2024 05:54

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Contributors

Author: Ruben A.T. Mars
Author: Yi Yang
Author: Tonya Ward
Author: Mo Houtti
Author: Sambhawa Priya
Author: Heather R. Lekatz
Author: Xiaojia Tang
Author: Zhifu Sun
Author: Krishna R. Kalari
Author: Tal Korem
Author: Yogesh Bhattarai
Author: Tenghao Zheng
Author: Noam Bar
Author: Gary Frost
Author: Abigail J. Johnson
Author: Will van Treuren
Author: Shuo Han
Author: Tamas Ordog
Author: Madhusudan Grover
Author: Justin Sonnenburg
Author: Mauro D’Amato
Author: Michael Camilleri
Author: Eran Elinav
Author: Eran Segal
Author: Ran Blekhman
Author: Gianrico Farrugia
Author: Jonathan R. Swann ORCID iD
Author: Dan Knights
Author: Purna C. Kashyap

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