Increased Ornithine-Derived Polyamines Cause Airway Hyperresponsiveness in a Mouse Model of Asthma
Up-regulation of arginase contributes to airways hyperresponsiveness (AHR) in asthma by reducing L-arginine bioavailability for the nitric oxide (NO) synthase isozymes. The product of arginase activity, L-ornithine, can be metabolized into polyamines by ornithine decarboxylase. We tested the hypothe...
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| Published in | American journal of respiratory cell and molecular biology Vol. 48; no. 6; pp. 694 - 702 |
|---|---|
| Main Authors | , , , , , |
| Format | Journal Article |
| Language | English |
| Published |
United States
American Thoracic Society
01.06.2013
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| Subjects | |
| Online Access | Get full text |
| ISSN | 1044-1549 1535-4989 1535-4989 |
| DOI | 10.1165/rcmb.2012-0323OC |
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| Abstract | Up-regulation of arginase contributes to airways hyperresponsiveness (AHR) in asthma by reducing L-arginine bioavailability for the nitric oxide (NO) synthase isozymes. The product of arginase activity, L-ornithine, can be metabolized into polyamines by ornithine decarboxylase. We tested the hypothesis that increases in L-ornithine-derived polyamines contribute to AHR in mouse models of allergic airways inflammation. After measuring significantly increased polyamine levels in sputum samples from human subjects with asthma after allergen challenge, we used acute and subacute ovalbumin sensitization and challenge mouse models of allergic airways inflammation and naive mice to investigate the relationship of AHR to methacholine and polyamines in the lung. We found that spermine levels were elevated significantly in lungs from the acute model, which exhibits robust AHR, but not in the subacute murine model of asthma, which does not develop AHR. Intratracheal administration of spermine significantly augmented airways responsiveness to methacholine in both naive mice and mice with subacute airways inflammation, and reduced nitrite/nitrate levels in lung homogenates, suggesting that the AHR developed as a consequence of inhibition of constitutive NO production in the airways. Chronic inhibition of polyamine synthesis using an ornithine decarboxylase inhibitor significantly reduced polyamine levels, restored nitrite/nitrate levels to normal, and abrogated the AHR to methacholine in the acute model of allergic airways inflammation. We demonstrate that spermine increases airways responsiveness to methacholine, likely through inhibition of constitutive NO synthesis. Thus, inhibition of polyamine production may represent a new therapeutic target to treat airway obstruction in allergic asthma. |
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| AbstractList | Up-regulation of arginase contributes to airways hyperresponsiveness (AHR) in asthma by reducing L-arginine bioavailability for the nitric oxide (NO) synthase isozymes. The product of arginase activity, L-ornithine, can be metabolized into polyamines by ornithine decarboxylase. We tested the hypothesis that increases in L-ornithine-derived polyamines contribute to AHR in mouse models of allergic airways inflammation. After measuring significantly increased polyamine levels in sputum samples from human subjects with asthma after allergen challenge, we used acute and subacute ovalbumin sensitization and challenge mouse models of allergic airways inflammation and naive mice to investigate the relationship of AHR to methacholine and polyamines in the lung. We found that spermine levels were elevated significantly in lungs from the acute model, which exhibits robust AHR, but not in the subacute murine model of asthma, which does not develop AHR. Intratracheal administration of spermine significantly augmented airways responsiveness to methacholine in both naive mice and mice with subacute airways inflammation, and reduced nitrite/nitrate levels in lung homogenates, suggesting that the AHR developed as a consequence of inhibition of constitutive NO production in the airways. Chronic inhibition of polyamine synthesis using an ornithine decarboxylase inhibitor significantly reduced polyamine levels, restored nitrite/nitrate levels to normal, and abrogated the AHR to methacholine in the acute model of allergic airways inflammation. We demonstrate that spermine increases airways responsiveness to methacholine, likely through inhibition of constitutive NO synthesis. Thus, inhibition of polyamine production may represent a new therapeutic target to treat airway obstruction in allergic asthma.Up-regulation of arginase contributes to airways hyperresponsiveness (AHR) in asthma by reducing L-arginine bioavailability for the nitric oxide (NO) synthase isozymes. The product of arginase activity, L-ornithine, can be metabolized into polyamines by ornithine decarboxylase. We tested the hypothesis that increases in L-ornithine-derived polyamines contribute to AHR in mouse models of allergic airways inflammation. After measuring significantly increased polyamine levels in sputum samples from human subjects with asthma after allergen challenge, we used acute and subacute ovalbumin sensitization and challenge mouse models of allergic airways inflammation and naive mice to investigate the relationship of AHR to methacholine and polyamines in the lung. We found that spermine levels were elevated significantly in lungs from the acute model, which exhibits robust AHR, but not in the subacute murine model of asthma, which does not develop AHR. Intratracheal administration of spermine significantly augmented airways responsiveness to methacholine in both naive mice and mice with subacute airways inflammation, and reduced nitrite/nitrate levels in lung homogenates, suggesting that the AHR developed as a consequence of inhibition of constitutive NO production in the airways. Chronic inhibition of polyamine synthesis using an ornithine decarboxylase inhibitor significantly reduced polyamine levels, restored nitrite/nitrate levels to normal, and abrogated the AHR to methacholine in the acute model of allergic airways inflammation. We demonstrate that spermine increases airways responsiveness to methacholine, likely through inhibition of constitutive NO synthesis. Thus, inhibition of polyamine production may represent a new therapeutic target to treat airway obstruction in allergic asthma. Up-regulation of arginase contributes to airways hyperresponsiveness (AHR) in asthma by reducing L-arginine bioavailability for the nitric oxide (NO) synthase isozymes. The product of arginase activity, L-ornithine, can be metabolized into polyamines by ornithine decarboxylase. We tested the hypothesis that increases in L-ornithine-derived polyamines contribute to AHR in mouse models of allergic airways inflammation. After measuring significantly increased polyamine levels in sputum samples from human subjects with asthma after allergen challenge, we used acute and subacute ovalbumin sensitization and challenge mouse models of allergic airways inflammation and naive mice to investigate the relationship of AHR to methacholine and polyamines in the lung. We found that spermine levels were elevated significantly in lungs from the acute model, which exhibits robust AHR, but not in the subacute murine model of asthma, which does not develop AHR. Intratracheal administration of spermine significantly augmented airways responsiveness to methacholine in both naive mice and mice with subacute airways inflammation, and reduced nitrite/nitrate levels in lung homogenates, suggesting that the AHR developed as a consequence of inhibition of constitutive NO production in the airways. Chronic inhibition of polyamine synthesis using an ornithine decarboxylase inhibitor significantly reduced polyamine levels, restored nitrite/nitrate levels to normal, and abrogated the AHR to methacholine in the acute model of allergic airways inflammation. We demonstrate that spermine increases airways responsiveness to methacholine, likely through inhibition of constitutive NO synthesis. Thus, inhibition of polyamine production may represent a new therapeutic target to treat airway obstruction in allergic asthma. |
| Author | Gauvreau, Gail M. Scott, Jeremy A. North, Michelle L. Grasemann, Hartmut Khanna, Nivedita Inman, Mark D. |
| Author_xml | – sequence: 1 givenname: Michelle L. surname: North fullname: North, Michelle L. organization: Institute of Medical Science, Faculty of Medicine, and, Divisions of Occupational and Respiratory Medicine, Department and Faculty of Medicine, University of Toronto, Toronto, Ontario, Canada, Gage Occupational and Environmental Health Unit, University of Toronto and St. Michael’s Hospital, Toronto, Ontario, Canada, Keenan Research Centre in the Li Ka Shing Knowledge Institute of St. Michael’s Hospital, Toronto, Ontario, Canada – sequence: 2 givenname: Hartmut surname: Grasemann fullname: Grasemann, Hartmut organization: Institute of Medical Science, Faculty of Medicine, and, Program in Physiology and Experimental Medicine, Research Institute, The Hospital for Sick Children, and Division of Respiratory Medicine, Department of Paediatrics, University of Toronto, Toronto, Ontario, Canada – sequence: 3 givenname: Nivedita surname: Khanna fullname: Khanna, Nivedita organization: Divisions of Occupational and Respiratory Medicine, Department and Faculty of Medicine, University of Toronto, Toronto, Ontario, Canada, Gage Occupational and Environmental Health Unit, University of Toronto and St. Michael’s Hospital, Toronto, Ontario, Canada, Keenan Research Centre in the Li Ka Shing Knowledge Institute of St. Michael’s Hospital, Toronto, Ontario, Canada – sequence: 4 givenname: Mark D. surname: Inman fullname: Inman, Mark D. organization: Division of Respirology, Department of Medicine, McMaster University, Hamilton, Ontario, Canada – sequence: 5 givenname: Gail M. surname: Gauvreau fullname: Gauvreau, Gail M. organization: Division of Respirology, Department of Medicine, McMaster University, Hamilton, Ontario, Canada – sequence: 6 givenname: Jeremy A. surname: Scott fullname: Scott, Jeremy A. organization: Institute of Medical Science, Faculty of Medicine, and, Divisions of Occupational and Respiratory Medicine, Department and Faculty of Medicine, University of Toronto, Toronto, Ontario, Canada, Gage Occupational and Environmental Health Unit, University of Toronto and St. Michael’s Hospital, Toronto, Ontario, Canada, Keenan Research Centre in the Li Ka Shing Knowledge Institute of St. Michael’s Hospital, Toronto, Ontario, Canada, Division of Occupational and Environmental Health, Dalla Lana School of Public Health, Faculty of Medicine, University of Toronto, Toronto, Ontario, Canada; and |
| BackLink | https://www.ncbi.nlm.nih.gov/pubmed/23470627$$D View this record in MEDLINE/PubMed |
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| SubjectTerms | Adolescent Adult Animals Asthma - drug therapy Asthma - immunology Asthma - metabolism Asthma - pathology Disease Models, Animal Eflornithine - pharmacology Female Humans Hypersensitivity - drug therapy Hypersensitivity - immunology Hypersensitivity - metabolism Hypersensitivity - pathology Inflammation - immunology Inflammation - metabolism Inflammation - pathology Lung - drug effects Lung - immunology Lung - metabolism Lung - pathology Male Methacholine Chloride - metabolism Methacholine Chloride - pharmacology Mice Middle Aged Nitrates - metabolism Nitric Oxide - metabolism Nitric Oxide Synthase - immunology Nitric Oxide Synthase - metabolism Ornithine - metabolism Ornithine Decarboxylase - metabolism Ornithine Decarboxylase Inhibitors Ovalbumin - adverse effects Ovalbumin - immunology Polyamines - antagonists & inhibitors Polyamines - metabolism Spermine - administration & dosage Spermine - adverse effects Spermine - pharmacology Sputum - metabolism Young Adult |
| Title | Increased Ornithine-Derived Polyamines Cause Airway Hyperresponsiveness in a Mouse Model of Asthma |
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