Multi-Compartment Profiling of Bacterial and Host Metabolites Identifies Intestinal Dysbiosis and Its Functional Consequences in the Critically Ill Child

OBJECTIVES: Adverse physiology and antibiotic exposure devastate the intestinal microbiome in critical illness. Time and cost implications limit the immediate clinical potential of microbial sequencing to identify or treat intestinal dysbiosis. Here, we examined whether metabolic profiling is a feas...

Descripción completa

Detalles Bibliográficos
Autores principales: Wijeyesekera, Anisha, Wagner, Josef, De Goffau, Marcus, Thurston, Sarah, Rodrigues Sabino, Adilson, Zaher, Sara, White, Deborah, Ridout, Jenna, Peters, Mark J., Ramnarayan, Padmanabhan, Branco, Ricardo G., Torok, M. Estee, Valla, Frederic, Meyer, Rosan, Klein, Nigel, Frost, Gary, Parkhill, Julian, Holmes, Elaine, Pathan, Nazima
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Lippincott Williams & Wilkins 2019
Materias:
Online Clinical Investigations
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6699985/
https://www.ncbi.nlm.nih.gov/pubmed/31169619
http://dx.doi.org/10.1097/CCM.0000000000003841
_version_ 1783444778323542016
author Wijeyesekera, Anisha
Wagner, Josef
De Goffau, Marcus
Thurston, Sarah
Rodrigues Sabino, Adilson
Zaher, Sara
White, Deborah
Ridout, Jenna
Peters, Mark J.
Ramnarayan, Padmanabhan
Branco, Ricardo G.
Torok, M. Estee
Valla, Frederic
Meyer, Rosan
Klein, Nigel
Frost, Gary
Parkhill, Julian
Holmes, Elaine
Pathan, Nazima
author_facet Wijeyesekera, Anisha
Wagner, Josef
De Goffau, Marcus
Thurston, Sarah
Rodrigues Sabino, Adilson
Zaher, Sara
White, Deborah
Ridout, Jenna
Peters, Mark J.
Ramnarayan, Padmanabhan
Branco, Ricardo G.
Torok, M. Estee
Valla, Frederic
Meyer, Rosan
Klein, Nigel
Frost, Gary
Parkhill, Julian
Holmes, Elaine
Pathan, Nazima
author_sort Wijeyesekera, Anisha
collection PubMed
description OBJECTIVES: Adverse physiology and antibiotic exposure devastate the intestinal microbiome in critical illness. Time and cost implications limit the immediate clinical potential of microbial sequencing to identify or treat intestinal dysbiosis. Here, we examined whether metabolic profiling is a feasible method of monitoring intestinal dysbiosis in critically ill children. DESIGN: Prospective multicenter cohort study. SETTING: Three U.K.-based PICUs. PATIENTS: Mechanically ventilated critically ill (n = 60) and age-matched healthy children (n = 55). INTERVENTIONS: Collection of urine and fecal samples in children admitted to the PICU. A single fecal and urine sample was collected in healthy controls. MEASUREMENTS AND MAIN RESULTS: Untargeted and targeted metabolic profiling using 1H-nuclear magnetic resonance spectroscopy and liquid chromatography-mass spectrometry or urine and fecal samples. This was integrated with analysis of fecal bacterial 16S ribosomal RNA profiles and clinical disease severity indicators. We observed separation of global urinary and fecal metabolic profiles in critically ill compared with healthy children. Urinary excretion of mammalian-microbial co-metabolites hippurate, 4-cresol sulphate, and formate were reduced in critical illness compared with healthy children. Reduced fecal excretion of short-chain fatty acids (including butyrate, propionate, and acetate) were observed in the patient cohort, demonstrating that these metabolites also distinguished between critical illness and health. Dysregulation of intestinal bile metabolism was evidenced by increased primary and reduced secondary fecal bile acid excretion. Fecal butyrate correlated with days free of intensive care at 30 days (r = 0.38; p = 0.03), while urinary formate correlated inversely with vasopressor requirement (r = –0.2; p = 0.037). CONCLUSIONS: Disruption to the functional activity of the intestinal microbiome may result in worsening organ failure in the critically ill child. Profiling of bacterial metabolites in fecal and urine samples may support identification and treatment of intestinal dysbiosis in critical illness.
format Online
Article
Text
id pubmed-6699985
institution National Center for Biotechnology Information
language English
publishDate 2019
publisher Lippincott Williams & Wilkins
record_format MEDLINE/PubMed
spelling pubmed-66999852019-09-01 Multi-Compartment Profiling of Bacterial and Host Metabolites Identifies Intestinal Dysbiosis and Its Functional Consequences in the Critically Ill Child Wijeyesekera, Anisha Wagner, Josef De Goffau, Marcus Thurston, Sarah Rodrigues Sabino, Adilson Zaher, Sara White, Deborah Ridout, Jenna Peters, Mark J. Ramnarayan, Padmanabhan Branco, Ricardo G. Torok, M. Estee Valla, Frederic Meyer, Rosan Klein, Nigel Frost, Gary Parkhill, Julian Holmes, Elaine Pathan, Nazima Crit Care Med Online Clinical Investigations OBJECTIVES: Adverse physiology and antibiotic exposure devastate the intestinal microbiome in critical illness. Time and cost implications limit the immediate clinical potential of microbial sequencing to identify or treat intestinal dysbiosis. Here, we examined whether metabolic profiling is a feasible method of monitoring intestinal dysbiosis in critically ill children. DESIGN: Prospective multicenter cohort study. SETTING: Three U.K.-based PICUs. PATIENTS: Mechanically ventilated critically ill (n = 60) and age-matched healthy children (n = 55). INTERVENTIONS: Collection of urine and fecal samples in children admitted to the PICU. A single fecal and urine sample was collected in healthy controls. MEASUREMENTS AND MAIN RESULTS: Untargeted and targeted metabolic profiling using 1H-nuclear magnetic resonance spectroscopy and liquid chromatography-mass spectrometry or urine and fecal samples. This was integrated with analysis of fecal bacterial 16S ribosomal RNA profiles and clinical disease severity indicators. We observed separation of global urinary and fecal metabolic profiles in critically ill compared with healthy children. Urinary excretion of mammalian-microbial co-metabolites hippurate, 4-cresol sulphate, and formate were reduced in critical illness compared with healthy children. Reduced fecal excretion of short-chain fatty acids (including butyrate, propionate, and acetate) were observed in the patient cohort, demonstrating that these metabolites also distinguished between critical illness and health. Dysregulation of intestinal bile metabolism was evidenced by increased primary and reduced secondary fecal bile acid excretion. Fecal butyrate correlated with days free of intensive care at 30 days (r = 0.38; p = 0.03), while urinary formate correlated inversely with vasopressor requirement (r = –0.2; p = 0.037). CONCLUSIONS: Disruption to the functional activity of the intestinal microbiome may result in worsening organ failure in the critically ill child. Profiling of bacterial metabolites in fecal and urine samples may support identification and treatment of intestinal dysbiosis in critical illness. Lippincott Williams & Wilkins 2019-09 2019-08-15 /pmc/articles/PMC6699985/ /pubmed/31169619 http://dx.doi.org/10.1097/CCM.0000000000003841 Text en Copyright © 2019 The Author(s). Published by Wolters Kluwer Health, Inc. on behalf of the Society of Critical Care Medicine and Wolters Kluwer Health, Inc. This is an open access article distributed under the Creative Commons Attribution License 4.0 (CCBY) (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Online Clinical Investigations
Wijeyesekera, Anisha
Wagner, Josef
De Goffau, Marcus
Thurston, Sarah
Rodrigues Sabino, Adilson
Zaher, Sara
White, Deborah
Ridout, Jenna
Peters, Mark J.
Ramnarayan, Padmanabhan
Branco, Ricardo G.
Torok, M. Estee
Valla, Frederic
Meyer, Rosan
Klein, Nigel
Frost, Gary
Parkhill, Julian
Holmes, Elaine
Pathan, Nazima
Multi-Compartment Profiling of Bacterial and Host Metabolites Identifies Intestinal Dysbiosis and Its Functional Consequences in the Critically Ill Child
title Multi-Compartment Profiling of Bacterial and Host Metabolites Identifies Intestinal Dysbiosis and Its Functional Consequences in the Critically Ill Child
title_full Multi-Compartment Profiling of Bacterial and Host Metabolites Identifies Intestinal Dysbiosis and Its Functional Consequences in the Critically Ill Child
title_fullStr Multi-Compartment Profiling of Bacterial and Host Metabolites Identifies Intestinal Dysbiosis and Its Functional Consequences in the Critically Ill Child
title_full_unstemmed Multi-Compartment Profiling of Bacterial and Host Metabolites Identifies Intestinal Dysbiosis and Its Functional Consequences in the Critically Ill Child
title_short Multi-Compartment Profiling of Bacterial and Host Metabolites Identifies Intestinal Dysbiosis and Its Functional Consequences in the Critically Ill Child
title_sort multi-compartment profiling of bacterial and host metabolites identifies intestinal dysbiosis and its functional consequences in the critically ill child
topic Online Clinical Investigations
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6699985/
https://www.ncbi.nlm.nih.gov/pubmed/31169619
http://dx.doi.org/10.1097/CCM.0000000000003841
work_keys_str_mv AT wijeyesekeraanisha multicompartmentprofilingofbacterialandhostmetabolitesidentifiesintestinaldysbiosisanditsfunctionalconsequencesinthecriticallyillchild
AT wagnerjosef multicompartmentprofilingofbacterialandhostmetabolitesidentifiesintestinaldysbiosisanditsfunctionalconsequencesinthecriticallyillchild
AT degoffaumarcus multicompartmentprofilingofbacterialandhostmetabolitesidentifiesintestinaldysbiosisanditsfunctionalconsequencesinthecriticallyillchild
AT thurstonsarah multicompartmentprofilingofbacterialandhostmetabolitesidentifiesintestinaldysbiosisanditsfunctionalconsequencesinthecriticallyillchild
AT rodriguessabinoadilson multicompartmentprofilingofbacterialandhostmetabolitesidentifiesintestinaldysbiosisanditsfunctionalconsequencesinthecriticallyillchild
AT zahersara multicompartmentprofilingofbacterialandhostmetabolitesidentifiesintestinaldysbiosisanditsfunctionalconsequencesinthecriticallyillchild
AT whitedeborah multicompartmentprofilingofbacterialandhostmetabolitesidentifiesintestinaldysbiosisanditsfunctionalconsequencesinthecriticallyillchild
AT ridoutjenna multicompartmentprofilingofbacterialandhostmetabolitesidentifiesintestinaldysbiosisanditsfunctionalconsequencesinthecriticallyillchild
AT petersmarkj multicompartmentprofilingofbacterialandhostmetabolitesidentifiesintestinaldysbiosisanditsfunctionalconsequencesinthecriticallyillchild
AT ramnarayanpadmanabhan multicompartmentprofilingofbacterialandhostmetabolitesidentifiesintestinaldysbiosisanditsfunctionalconsequencesinthecriticallyillchild
AT brancoricardog multicompartmentprofilingofbacterialandhostmetabolitesidentifiesintestinaldysbiosisanditsfunctionalconsequencesinthecriticallyillchild
AT torokmestee multicompartmentprofilingofbacterialandhostmetabolitesidentifiesintestinaldysbiosisanditsfunctionalconsequencesinthecriticallyillchild
AT vallafrederic multicompartmentprofilingofbacterialandhostmetabolitesidentifiesintestinaldysbiosisanditsfunctionalconsequencesinthecriticallyillchild
AT meyerrosan multicompartmentprofilingofbacterialandhostmetabolitesidentifiesintestinaldysbiosisanditsfunctionalconsequencesinthecriticallyillchild
AT kleinnigel multicompartmentprofilingofbacterialandhostmetabolitesidentifiesintestinaldysbiosisanditsfunctionalconsequencesinthecriticallyillchild
AT frostgary multicompartmentprofilingofbacterialandhostmetabolitesidentifiesintestinaldysbiosisanditsfunctionalconsequencesinthecriticallyillchild
AT parkhilljulian multicompartmentprofilingofbacterialandhostmetabolitesidentifiesintestinaldysbiosisanditsfunctionalconsequencesinthecriticallyillchild
AT holmeselaine multicompartmentprofilingofbacterialandhostmetabolitesidentifiesintestinaldysbiosisanditsfunctionalconsequencesinthecriticallyillchild
AT pathannazima multicompartmentprofilingofbacterialandhostmetabolitesidentifiesintestinaldysbiosisanditsfunctionalconsequencesinthecriticallyillchild

Ejemplares similares