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George T. De Sanctis, James A. MacLean, Shixin Qin, Walter W. Wolyniec, Hartmut Grasemann, Chandri N. Yandava, Aiping Jiao, Thomas Noonan, Joan Stein-Streilein, Francis H.Y. Green, Jeffrey M. Drazen
J Clin Invest. 1999;
103(4):507
doi:10.1172/JCI4017
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W
e examined the role of the interleukin-8 (IL-8) receptor in a murine model of allergen-induced pulmonary inflammation using mice with a targeted deletion of the murine IL-8 receptor homologue (IL-8r–/–). Wild-type (Wt) and IL-8r–/– mice were systemically immunized to ovalbumin (OVA) and were exposed with either single or multiple challenge of aerosolized phosphate-buffered saline (OVA/PBS) or OVA (OVA/OVA). Analysis of cells recovered from bronchoalveolar lavage (BAL) revealed a diminished recruitment of neutrophils to the airway lumen after single challenge in IL-8r–/– mice compared with Wt mice, whereas multiply challenged IL-8r–/– mice had increased B cells and fewer neutrophils compared with Wt mice. Both Wt and IL-8r–/– OVA/OVA mice recruited similar numbers of eosinophils to the BAL fluid and exhibited comparable degrees of pulmonary inflammation histologically. Both total and OVA-specific IgE levels were greater in multiply challenged IL-8r–/– OVA/OVA mice than in Wt mice. Both the IL-8r–/– OVA/OVA and OVA/PBS mice were significantly less responsive to methacholine than their respective Wt groups, but both Wt and IL-8r mice showed similar degrees of enhancement after multiple allergen challenge. The data demonstrate that the IL-8r modulates IgE production, airway responsiveness, and the composition of the cells (B cells and neutrophils) recruited to the airway lumen in response to antigen.
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