Linking microbial genes to plasma and stool metabolites uncovers host-microbial interactions underlying ulcerative colitis disease course

Melanie Schirmer; Martin Stražar; Julian Avila-Pacheco; Daniel F. Rojas-Tapias; Eric M. Brown; Emily Temple; Amy Deik; Kevin Bullock; Sarah Jeanfavre; Kerry Pierce; Shen Jin; Rachele Invernizzi; Marie Madlen Pust; Zach Costliow; David R. Mack; Anne M. Griffiths; Thomas Walters; Brendan M. Boyle; Subra Kugathasan; Hera Vlamakis; Jeffrey Hyams; Lee Denson; Clary B. Clish; Ramnik J. Xavier

doi:10.1016/j.chom.2023.12.013

Linking microbial genes to plasma and stool metabolites uncovers host-microbial interactions underlying ulcerative colitis disease course

Melanie Schirmer
, Martin Stražar
, Julian Avila-Pacheco
, Daniel F. Rojas-Tapias
, Eric M. Brown
, Emily Temple
, Amy Deik
, Kevin Bullock
, Sarah Jeanfavre
, Kerry Pierce
, Shen Jin
, Rachele Invernizzi
, Marie Madlen Pust
, Zach Costliow
, David R. Mack
, Anne M. Griffiths
, Thomas Walters
, Brendan M. Boyle
, Subra Kugathasan
, Hera Vlamakis

Jeffrey Hyams, Lee Denson, Clary B. Clish, Ramnik J. Xavier

Professur für Translational Microbiome Data Integration

The Broad Institute of MIT and Harvard
Massachusetts General Hospital
Technische Universität München
University of Ottawa
Hospital for Sick Children and University of Toronto
Center for Microbial Pathogenesis
Emory University School of Medicine
Connecticut Children's Medical Center
Cincinnati Children’s Hospital Medical Center
Massachusetts Institute of Technology

Publikation: Beitrag in Fachzeitschrift › Artikel › Begutachtung

56 Zitate (Scopus)

Abstract

Understanding the role of the microbiome in inflammatory diseases requires the identification of microbial effector molecules. We established an approach to link disease-associated microbes to microbial metabolites by integrating paired metagenomics, stool and plasma metabolomics, and culturomics. We identified host-microbial interactions correlated with disease activity, inflammation, and the clinical course of ulcerative colitis (UC) in the Predicting Response to Standardized Colitis Therapy (PROTECT) pediatric inception cohort. In severe disease, metabolite changes included increased dipeptides and tauro-conjugated bile acids (BAs) and decreased amino-acid-conjugated BAs in stool, whereas in plasma polyamines (N-acetylputrescine and N1-acetylspermidine) increased. Using patient samples and Veillonella parvula as a model, we uncovered nitrate- and lactate-dependent metabolic pathways, experimentally linking V. parvula expansion to immunomodulatory tryptophan metabolite production. Additionally, V. parvula metabolizes immunosuppressive thiopurine drugs through xdhA xanthine dehydrogenase, potentially impairing the therapeutic response. Our findings demonstrate that the microbiome contributes to disease-associated metabolite changes, underscoring the importance of these interactions in disease pathology and treatment.

Originalsprache	Englisch
Seiten (von - bis)	209-226.e7
Fachzeitschrift	Cell Host and Microbe
Jahrgang	32
Ausgabenummer	2
DOIs	https://doi.org/10.1016/j.chom.2023.12.013
Publikationsstatus	Veröffentlicht - 14 Feb. 2024

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10.1016/j.chom.2023.12.013

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Schirmer, M., Stražar, M., Avila-Pacheco, J., Rojas-Tapias, D. F., Brown, E. M., Temple, E., Deik, A., Bullock, K., Jeanfavre, S., Pierce, K., Jin, S., Invernizzi, R., Pust, M. M., Costliow, Z., Mack, D. R., Griffiths, A. M., Walters, T., Boyle, B. M., Kugathasan, S., ... Xavier, R. J. (2024). Linking microbial genes to plasma and stool metabolites uncovers host-microbial interactions underlying ulcerative colitis disease course. Cell Host and Microbe, 32(2), 209-226.e7. https://doi.org/10.1016/j.chom.2023.12.013

@article{2062701e771a48ee84547f26dd621820,

title = "Linking microbial genes to plasma and stool metabolites uncovers host-microbial interactions underlying ulcerative colitis disease course",

abstract = "Understanding the role of the microbiome in inflammatory diseases requires the identification of microbial effector molecules. We established an approach to link disease-associated microbes to microbial metabolites by integrating paired metagenomics, stool and plasma metabolomics, and culturomics. We identified host-microbial interactions correlated with disease activity, inflammation, and the clinical course of ulcerative colitis (UC) in the Predicting Response to Standardized Colitis Therapy (PROTECT) pediatric inception cohort. In severe disease, metabolite changes included increased dipeptides and tauro-conjugated bile acids (BAs) and decreased amino-acid-conjugated BAs in stool, whereas in plasma polyamines (N-acetylputrescine and N1-acetylspermidine) increased. Using patient samples and Veillonella parvula as a model, we uncovered nitrate- and lactate-dependent metabolic pathways, experimentally linking V. parvula expansion to immunomodulatory tryptophan metabolite production. Additionally, V. parvula metabolizes immunosuppressive thiopurine drugs through xdhA xanthine dehydrogenase, potentially impairing the therapeutic response. Our findings demonstrate that the microbiome contributes to disease-associated metabolite changes, underscoring the importance of these interactions in disease pathology and treatment.",

keywords = "Veillonella parvula, culturomics, metabolomics, metagenomics, microbiome, multiomics data integration, nitrate respiration, thiopurines, tryptophan metabolism, ulcerative colitis",

author = "Melanie Schirmer and Martin Stra{\v z}ar and Julian Avila-Pacheco and Rojas-Tapias, \{Daniel F.\} and Brown, \{Eric M.\} and Emily Temple and Amy Deik and Kevin Bullock and Sarah Jeanfavre and Kerry Pierce and Shen Jin and Rachele Invernizzi and Pust, \{Marie Madlen\} and Zach Costliow and Mack, \{David R.\} and Griffiths, \{Anne M.\} and Thomas Walters and Boyle, \{Brendan M.\} and Subra Kugathasan and Hera Vlamakis and Jeffrey Hyams and Lee Denson and Clish, \{Clary B.\} and Xavier, \{Ramnik J.\}",

note = "Publisher Copyright: {\textcopyright} 2023 Elsevier Inc.",

year = "2024",

month = feb,

day = "14",

doi = "10.1016/j.chom.2023.12.013",

language = "English",

volume = "32",

pages = "209--226.e7",

journal = "Cell Host and Microbe",

issn = "1931-3128",

publisher = "Cell Press",

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Schirmer, M, Stražar, M, Avila-Pacheco, J, Rojas-Tapias, DF, Brown, EM, Temple, E, Deik, A, Bullock, K, Jeanfavre, S, Pierce, K, Jin, S, Invernizzi, R, Pust, MM, Costliow, Z, Mack, DR, Griffiths, AM, Walters, T, Boyle, BM, Kugathasan, S, Vlamakis, H, Hyams, J, Denson, L, Clish, CB & Xavier, RJ 2024, 'Linking microbial genes to plasma and stool metabolites uncovers host-microbial interactions underlying ulcerative colitis disease course', Cell Host and Microbe, Jg. 32, Nr. 2, S. 209-226.e7. https://doi.org/10.1016/j.chom.2023.12.013

TY - JOUR

T1 - Linking microbial genes to plasma and stool metabolites uncovers host-microbial interactions underlying ulcerative colitis disease course

AU - Schirmer, Melanie

AU - Stražar, Martin

AU - Avila-Pacheco, Julian

AU - Rojas-Tapias, Daniel F.

AU - Brown, Eric M.

AU - Temple, Emily

AU - Deik, Amy

AU - Bullock, Kevin

AU - Jeanfavre, Sarah

AU - Pierce, Kerry

AU - Jin, Shen

AU - Invernizzi, Rachele

AU - Pust, Marie Madlen

AU - Costliow, Zach

AU - Mack, David R.

AU - Griffiths, Anne M.

AU - Walters, Thomas

AU - Boyle, Brendan M.

AU - Kugathasan, Subra

AU - Vlamakis, Hera

AU - Hyams, Jeffrey

AU - Denson, Lee

AU - Clish, Clary B.

AU - Xavier, Ramnik J.

PY - 2024/2/14

Y1 - 2024/2/14

N2 - Understanding the role of the microbiome in inflammatory diseases requires the identification of microbial effector molecules. We established an approach to link disease-associated microbes to microbial metabolites by integrating paired metagenomics, stool and plasma metabolomics, and culturomics. We identified host-microbial interactions correlated with disease activity, inflammation, and the clinical course of ulcerative colitis (UC) in the Predicting Response to Standardized Colitis Therapy (PROTECT) pediatric inception cohort. In severe disease, metabolite changes included increased dipeptides and tauro-conjugated bile acids (BAs) and decreased amino-acid-conjugated BAs in stool, whereas in plasma polyamines (N-acetylputrescine and N1-acetylspermidine) increased. Using patient samples and Veillonella parvula as a model, we uncovered nitrate- and lactate-dependent metabolic pathways, experimentally linking V. parvula expansion to immunomodulatory tryptophan metabolite production. Additionally, V. parvula metabolizes immunosuppressive thiopurine drugs through xdhA xanthine dehydrogenase, potentially impairing the therapeutic response. Our findings demonstrate that the microbiome contributes to disease-associated metabolite changes, underscoring the importance of these interactions in disease pathology and treatment.

AB - Understanding the role of the microbiome in inflammatory diseases requires the identification of microbial effector molecules. We established an approach to link disease-associated microbes to microbial metabolites by integrating paired metagenomics, stool and plasma metabolomics, and culturomics. We identified host-microbial interactions correlated with disease activity, inflammation, and the clinical course of ulcerative colitis (UC) in the Predicting Response to Standardized Colitis Therapy (PROTECT) pediatric inception cohort. In severe disease, metabolite changes included increased dipeptides and tauro-conjugated bile acids (BAs) and decreased amino-acid-conjugated BAs in stool, whereas in plasma polyamines (N-acetylputrescine and N1-acetylspermidine) increased. Using patient samples and Veillonella parvula as a model, we uncovered nitrate- and lactate-dependent metabolic pathways, experimentally linking V. parvula expansion to immunomodulatory tryptophan metabolite production. Additionally, V. parvula metabolizes immunosuppressive thiopurine drugs through xdhA xanthine dehydrogenase, potentially impairing the therapeutic response. Our findings demonstrate that the microbiome contributes to disease-associated metabolite changes, underscoring the importance of these interactions in disease pathology and treatment.

KW - Veillonella parvula

KW - culturomics

KW - metabolomics

KW - metagenomics

KW - microbiome

KW - multiomics data integration

KW - nitrate respiration

KW - thiopurines

KW - tryptophan metabolism

KW - ulcerative colitis

UR - https://www.scopus.com/pages/publications/85185218409

U2 - 10.1016/j.chom.2023.12.013

DO - 10.1016/j.chom.2023.12.013

M3 - Article

C2 - 38215740

AN - SCOPUS:85185218409

SN - 1931-3128

VL - 32

SP - 209-226.e7

JO - Cell Host and Microbe

JF - Cell Host and Microbe

IS - 2

ER -

Linking microbial genes to plasma and stool metabolites uncovers host-microbial interactions underlying ulcerative colitis disease course

Abstract

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