TY - JOUR
T1 - Activity of the cyclooxygenase 2-prostaglandin-E prostanoid receptor pathway in mice exposed to house dust mite aeroallergens, and impact of exogenous prostaglandin E2
AU - Herrerias, Aida
AU - Torres, Rosa
AU - Serra, Mariona
AU - Marco, Alberto
AU - Pujols, Laura
AU - Picado, César
AU - De Mora, Fernando
N1 - Copyright:
Copyright 2010 Elsevier B.V., All rights reserved.
PY - 2009/10/30
Y1 - 2009/10/30
N2 - Background. Prostaglandin E2(PGE2), experimentally administered to asthma patients or assayed in murine models, improves allergen-driven airway inflammation. The mechanisms are unknown, but fluctuations of the endogenous cyclooxygenase (COX)-2/prostaglandin/E prostanoid (EP) receptor pathway activity likely contribute to the clinical outcome. We analyzed the activity of the pathway in mice sensitized to aeroallergens, and then studied its modulation under exogenous PGE2. Methods. Mice were exposed to house dust mite (HDM) aeroallergens, a model that enable us to mimic the development of allergic asthma in humans, and were then treated with either subcutaneous PGE2or the selective EP1/3 receptor agonist sulprostone. Simultaneously with airway responsiveness and inflammation, lung COX-2 and EP receptor mRNA expression were assessed. Levels of PGE2, PGI 2, PGD2were also determined in bronchoalveolar lavage fluid. Results. HDM-induced airway hyperreactivity and inflammation were accompanied by increased COX-2 mRNA production. In parallel, airway PGE 2and PGI2, but not PGD2, were upregulated, and the EP2 receptor showed overexpression. Subcutaneous PGE2attenuated aeroallergen-driven airway eosinophilic inflammation and reduced endogenous PGE2and PGI2production. Sulprostone had neither an effect on airway responsiveness or inflammation nor diminished allergen-induced COX-2 and PGE2overexpression. Finally, lung EP2 receptor levels remained high in mice treated with PGE2, but not in those treated with sulprostone. Conclusion. The lung COX-2/PGE2/EP2 receptor pathway is upregulated in HDM-exposed mice, possibly as an effort to attenuate allergen-induced airway inflammation. Exogenous PGE2downregulates its endogenous counterpart but maintains EP2 overexpression, a phenomenon that might be required for administered PGE2to exert its protective effect.
AB - Background. Prostaglandin E2(PGE2), experimentally administered to asthma patients or assayed in murine models, improves allergen-driven airway inflammation. The mechanisms are unknown, but fluctuations of the endogenous cyclooxygenase (COX)-2/prostaglandin/E prostanoid (EP) receptor pathway activity likely contribute to the clinical outcome. We analyzed the activity of the pathway in mice sensitized to aeroallergens, and then studied its modulation under exogenous PGE2. Methods. Mice were exposed to house dust mite (HDM) aeroallergens, a model that enable us to mimic the development of allergic asthma in humans, and were then treated with either subcutaneous PGE2or the selective EP1/3 receptor agonist sulprostone. Simultaneously with airway responsiveness and inflammation, lung COX-2 and EP receptor mRNA expression were assessed. Levels of PGE2, PGI 2, PGD2were also determined in bronchoalveolar lavage fluid. Results. HDM-induced airway hyperreactivity and inflammation were accompanied by increased COX-2 mRNA production. In parallel, airway PGE 2and PGI2, but not PGD2, were upregulated, and the EP2 receptor showed overexpression. Subcutaneous PGE2attenuated aeroallergen-driven airway eosinophilic inflammation and reduced endogenous PGE2and PGI2production. Sulprostone had neither an effect on airway responsiveness or inflammation nor diminished allergen-induced COX-2 and PGE2overexpression. Finally, lung EP2 receptor levels remained high in mice treated with PGE2, but not in those treated with sulprostone. Conclusion. The lung COX-2/PGE2/EP2 receptor pathway is upregulated in HDM-exposed mice, possibly as an effort to attenuate allergen-induced airway inflammation. Exogenous PGE2downregulates its endogenous counterpart but maintains EP2 overexpression, a phenomenon that might be required for administered PGE2to exert its protective effect.
UR - http://www.scopus.com/inward/record.url?scp=72749116493&partnerID=8YFLogxK
U2 - 10.1186/1476-9255-6-30
DO - 10.1186/1476-9255-6-30
M3 - Article
SN - 1476-9255
VL - 6
SP - 30
EP - 38
JO - Journal of Inflammation
JF - Journal of Inflammation
ER -