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Urinary Leukotriene E(4) and Prostaglandin D(2) Metabolites Increase in Adult and Childhood Severe Asthma Characterized by Type 2 Inflammation. A Clinical Observational Study

Rationale: New approaches are needed to guide personalized treatment of asthma. Objectives: To test if urinary eicosanoid metabolites can direct asthma phenotyping. Methods: Urinary metabolites of prostaglandins (PGs), cysteinyl leukotrienes (CysLTs), and isoprostanes were quantified in the U-BIOPRE...

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Autores principales: Kolmert, Johan, Gómez, Cristina, Balgoma, David, Sjödin, Marcus, Bood, Johan, Konradsen, Jon R., Ericsson, Magnus, Thörngren, John-Olof, James, Anna, Mikus, Maria, Sousa, Ana R., Riley, John H., Bates, Stewart, Bakke, Per S., Pandis, Ioannis, Caruso, Massimo, Chanez, Pascal, Fowler, Stephen J., Geiser, Thomas, Howarth, Peter, Horváth, Ildikó, Krug, Norbert, Montuschi, Paolo, Sanak, Marek, Behndig, Annelie, Shaw, Dominick E., Knowles, Richard G., Holweg, Cécile T. J., Wheelock, Åsa M., Dahlén, Barbro, Nordlund, Björn, Alving, Kjell, Hedlin, Gunilla, Chung, Kian Fan, Adcock, Ian M., Sterk, Peter J., Djukanovic, Ratko, Dahlén, Sven-Erik
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Thoracic Society 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7781128/
https://www.ncbi.nlm.nih.gov/pubmed/32667261
http://dx.doi.org/10.1164/rccm.201909-1869OC
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author Kolmert, Johan
Gómez, Cristina
Balgoma, David
Sjödin, Marcus
Bood, Johan
Konradsen, Jon R.
Ericsson, Magnus
Thörngren, John-Olof
James, Anna
Mikus, Maria
Sousa, Ana R.
Riley, John H.
Bates, Stewart
Bakke, Per S.
Pandis, Ioannis
Caruso, Massimo
Chanez, Pascal
Fowler, Stephen J.
Geiser, Thomas
Howarth, Peter
Horváth, Ildikó
Krug, Norbert
Montuschi, Paolo
Sanak, Marek
Behndig, Annelie
Shaw, Dominick E.
Knowles, Richard G.
Holweg, Cécile T. J.
Wheelock, Åsa M.
Dahlén, Barbro
Nordlund, Björn
Alving, Kjell
Hedlin, Gunilla
Chung, Kian Fan
Adcock, Ian M.
Sterk, Peter J.
Djukanovic, Ratko
Dahlén, Sven-Erik
author_facet Kolmert, Johan
Gómez, Cristina
Balgoma, David
Sjödin, Marcus
Bood, Johan
Konradsen, Jon R.
Ericsson, Magnus
Thörngren, John-Olof
James, Anna
Mikus, Maria
Sousa, Ana R.
Riley, John H.
Bates, Stewart
Bakke, Per S.
Pandis, Ioannis
Caruso, Massimo
Chanez, Pascal
Fowler, Stephen J.
Geiser, Thomas
Howarth, Peter
Horváth, Ildikó
Krug, Norbert
Montuschi, Paolo
Sanak, Marek
Behndig, Annelie
Shaw, Dominick E.
Knowles, Richard G.
Holweg, Cécile T. J.
Wheelock, Åsa M.
Dahlén, Barbro
Nordlund, Björn
Alving, Kjell
Hedlin, Gunilla
Chung, Kian Fan
Adcock, Ian M.
Sterk, Peter J.
Djukanovic, Ratko
Dahlén, Sven-Erik
author_sort Kolmert, Johan
collection PubMed
description Rationale: New approaches are needed to guide personalized treatment of asthma. Objectives: To test if urinary eicosanoid metabolites can direct asthma phenotyping. Methods: Urinary metabolites of prostaglandins (PGs), cysteinyl leukotrienes (CysLTs), and isoprostanes were quantified in the U-BIOPRED (Unbiased Biomarkers for the Prediction of Respiratory Diseases Outcomes) study including 86 adults with mild-to-moderate asthma (MMA), 411 with severe asthma (SA), and 100 healthy control participants. Validation was performed internally in 302 participants with SA followed up after 12–18 months and externally in 95 adolescents with asthma. Measurement and Main Results: Metabolite concentrations in healthy control participants were unrelated to age, body mass index, and sex, except for the PGE(2) pathway. Eicosanoid concentrations were generally greater in participants with MMA relative to healthy control participants, with further elevations in participants with SA. However, PGE(2) metabolite concentrations were either the same or lower in male nonsmokers with asthma than in healthy control participants. Metabolite concentrations were unchanged in those with asthma who adhered to oral corticosteroid treatment as documented by urinary prednisolone detection, whereas those with SA treated with omalizumab had lower concentrations of LTE(4) and the PGD(2) metabolite 2,3-dinor-11β-PGF(2α). High concentrations of LTE(4) and PGD(2) metabolites were associated with lower lung function and increased amounts of exhaled nitric oxide and eosinophil markers in blood, sputum, and urine in U-BIOPRED participants and in adolescents with asthma. These type 2 (T2) asthma associations were reproduced in the follow-up visit of the U-BIOPRED study and were found to be as sensitive to detect T2 inflammation as the established biomarkers. Conclusions: Monitoring of urinary eicosanoids can identify T2 asthma and introduces a new noninvasive approach for molecular phenotyping of adult and adolescent asthma. Clinical trial registered with www.clinicaltrials.gov (NCT 01976767).
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spelling pubmed-77811282021-01-15 Urinary Leukotriene E(4) and Prostaglandin D(2) Metabolites Increase in Adult and Childhood Severe Asthma Characterized by Type 2 Inflammation. A Clinical Observational Study Kolmert, Johan Gómez, Cristina Balgoma, David Sjödin, Marcus Bood, Johan Konradsen, Jon R. Ericsson, Magnus Thörngren, John-Olof James, Anna Mikus, Maria Sousa, Ana R. Riley, John H. Bates, Stewart Bakke, Per S. Pandis, Ioannis Caruso, Massimo Chanez, Pascal Fowler, Stephen J. Geiser, Thomas Howarth, Peter Horváth, Ildikó Krug, Norbert Montuschi, Paolo Sanak, Marek Behndig, Annelie Shaw, Dominick E. Knowles, Richard G. Holweg, Cécile T. J. Wheelock, Åsa M. Dahlén, Barbro Nordlund, Björn Alving, Kjell Hedlin, Gunilla Chung, Kian Fan Adcock, Ian M. Sterk, Peter J. Djukanovic, Ratko Dahlén, Sven-Erik Am J Respir Crit Care Med Original Articles Rationale: New approaches are needed to guide personalized treatment of asthma. Objectives: To test if urinary eicosanoid metabolites can direct asthma phenotyping. Methods: Urinary metabolites of prostaglandins (PGs), cysteinyl leukotrienes (CysLTs), and isoprostanes were quantified in the U-BIOPRED (Unbiased Biomarkers for the Prediction of Respiratory Diseases Outcomes) study including 86 adults with mild-to-moderate asthma (MMA), 411 with severe asthma (SA), and 100 healthy control participants. Validation was performed internally in 302 participants with SA followed up after 12–18 months and externally in 95 adolescents with asthma. Measurement and Main Results: Metabolite concentrations in healthy control participants were unrelated to age, body mass index, and sex, except for the PGE(2) pathway. Eicosanoid concentrations were generally greater in participants with MMA relative to healthy control participants, with further elevations in participants with SA. However, PGE(2) metabolite concentrations were either the same or lower in male nonsmokers with asthma than in healthy control participants. Metabolite concentrations were unchanged in those with asthma who adhered to oral corticosteroid treatment as documented by urinary prednisolone detection, whereas those with SA treated with omalizumab had lower concentrations of LTE(4) and the PGD(2) metabolite 2,3-dinor-11β-PGF(2α). High concentrations of LTE(4) and PGD(2) metabolites were associated with lower lung function and increased amounts of exhaled nitric oxide and eosinophil markers in blood, sputum, and urine in U-BIOPRED participants and in adolescents with asthma. These type 2 (T2) asthma associations were reproduced in the follow-up visit of the U-BIOPRED study and were found to be as sensitive to detect T2 inflammation as the established biomarkers. Conclusions: Monitoring of urinary eicosanoids can identify T2 asthma and introduces a new noninvasive approach for molecular phenotyping of adult and adolescent asthma. Clinical trial registered with www.clinicaltrials.gov (NCT 01976767). American Thoracic Society 2021-01-01 2021-01-01 /pmc/articles/PMC7781128/ /pubmed/32667261 http://dx.doi.org/10.1164/rccm.201909-1869OC Text en Copyright © 2021 by the American Thoracic Society https://creativecommons.org/licenses/by-nc-nd/4.0/This article is open access and distributed under the terms of the Creative Commons Attribution Non-Commercial No Derivatives License 4.0 (http://creativecommons.org/licenses/by-nc-nd/4.0/ (https://creativecommons.org/licenses/by-nc-nd/4.0/) ). For commercial usage and reprints, please contact Diane Gern (dgern@thoracic.org).
spellingShingle Original Articles
Kolmert, Johan
Gómez, Cristina
Balgoma, David
Sjödin, Marcus
Bood, Johan
Konradsen, Jon R.
Ericsson, Magnus
Thörngren, John-Olof
James, Anna
Mikus, Maria
Sousa, Ana R.
Riley, John H.
Bates, Stewart
Bakke, Per S.
Pandis, Ioannis
Caruso, Massimo
Chanez, Pascal
Fowler, Stephen J.
Geiser, Thomas
Howarth, Peter
Horváth, Ildikó
Krug, Norbert
Montuschi, Paolo
Sanak, Marek
Behndig, Annelie
Shaw, Dominick E.
Knowles, Richard G.
Holweg, Cécile T. J.
Wheelock, Åsa M.
Dahlén, Barbro
Nordlund, Björn
Alving, Kjell
Hedlin, Gunilla
Chung, Kian Fan
Adcock, Ian M.
Sterk, Peter J.
Djukanovic, Ratko
Dahlén, Sven-Erik
Urinary Leukotriene E(4) and Prostaglandin D(2) Metabolites Increase in Adult and Childhood Severe Asthma Characterized by Type 2 Inflammation. A Clinical Observational Study
title Urinary Leukotriene E(4) and Prostaglandin D(2) Metabolites Increase in Adult and Childhood Severe Asthma Characterized by Type 2 Inflammation. A Clinical Observational Study
title_full Urinary Leukotriene E(4) and Prostaglandin D(2) Metabolites Increase in Adult and Childhood Severe Asthma Characterized by Type 2 Inflammation. A Clinical Observational Study
title_fullStr Urinary Leukotriene E(4) and Prostaglandin D(2) Metabolites Increase in Adult and Childhood Severe Asthma Characterized by Type 2 Inflammation. A Clinical Observational Study
title_full_unstemmed Urinary Leukotriene E(4) and Prostaglandin D(2) Metabolites Increase in Adult and Childhood Severe Asthma Characterized by Type 2 Inflammation. A Clinical Observational Study
title_short Urinary Leukotriene E(4) and Prostaglandin D(2) Metabolites Increase in Adult and Childhood Severe Asthma Characterized by Type 2 Inflammation. A Clinical Observational Study
title_sort urinary leukotriene e(4) and prostaglandin d(2) metabolites increase in adult and childhood severe asthma characterized by type 2 inflammation. a clinical observational study
topic Original Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7781128/
https://www.ncbi.nlm.nih.gov/pubmed/32667261
http://dx.doi.org/10.1164/rccm.201909-1869OC
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