Elevated circulating adenosine level potentiates antigen-induced immediate bronchospasm and bronchoconstrictor mediator release in sensitized guinea pigs - 09/09/11
Abstract |
Background: Adenosine causes bronchoconstriction in asthmatic patients, and it is also accepted that adenosine influences histamine release from activated human mast cells and basophils in vitro. Objective: In this study we tested the hypothesis that adenosine potentiates both the airway narrowing and the release of bronchoconstrictor mediators induced by ovalbumin challenge in sensitized guinea pigs. Methods: After ovalbumin sensitization, 4 groups were studied: control group, adenosine group (ADO), ovalbumin group (OA), and adenosine plus ovalbumin group (ADO + OA). Changes in airway resistance were assessed from continuously recorded pulmonary insufflation pressure (PIP). The concentration of histamine, PGD2 , and thromboxane B2 were determined from bronchoalveolar lavage fluids. Results: Adenosine alone (6 mg/kg intravenously) did not influence baseline values of PIP and the mediator concentrations; however, ovalbumin (10 mg/kg intravenously) increased both the PIP and the levels of the measured mediators compared with the control and ADO groups. When ovalbumin challenge was preceded by adenosine administration, both PIP and mediator levels were significantly enhanced compared with values obtained after simple ovalbumin provocation (ADO + OA vs OA: P < .05). Conclusion: These results suggest that adenosine potentiates the airway narrowing induced by ovalbumin challenge and that this effect may develop through facilitation of the release of bronchoconstrictor mediators during the immediate airway response. (J Allergy Clin Immunol 1998;102:687-91.)
Le texte complet de cet article est disponible en PDF.Keywords : Adenosine, antigen challenge, histamine, PGD2, thromboxane B2, prostaglandins, asthma, guinea pigs
Abbreviations : BAL:, cAMP:, HR:, IP3 :, MABP:, PIP:, TXB2 :
Plan
From a the Department of Pathophysiology, National “Korányi” Institute for TB and Pulmonology, and b the Second Department of Physiology, Semmelweis Medical University, Budapest. |
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Supported by the Hungarian National Scientific Research Funds (OTKA T016270, OTKA F0170 50, and ETT T-06 146/96). |
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Reprint requests: Éva Huszár, PhD, Department of Pathophysiology, National “Korányi” Institute for TB and Pulmonology, Budapest, Pihenö u. 1, 1529-Hungary. |
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0091-6749/98 $5.00 + 0 1/1/91948 |
Vol 102 - N° 4
P. 687-691 - octobre 1998 Retour au numéroBienvenue sur EM-consulte, la référence des professionnels de santé.
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