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Short ragweed allergen induces eosinophilic lung disease in HLA-DQ transgenic mice
Svetlana P. Chapoval, … , Amy G. Andrews, Chella S. David
Svetlana P. Chapoval, … , Amy G. Andrews, Chella S. David
Published June 15, 1999
Citation Information: J Clin Invest. 1999;103(12):1707-1717. https://doi.org/10.1172/JCI6175.
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Article

Short ragweed allergen induces eosinophilic lung disease in HLA-DQ transgenic mice

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Abstract

The human leukocyte antigen (HLA) restriction of the IgE response to different allergens in humans has been a subject of numerous published studies. However, the role and contribution of specific HLA class II molecules in the pathogenesis of allergic airway inflammation are unknown and difficult to assess. HLA-DQ6 and HLA-DQ8 transgenic mice lacking endogenous mouse class II gene expression were actively immunized and later challenged intranasally with short ragweed (SRW) allergenic extract. The HLA-DQ transgenic mice developed pulmonary eosinophilia and lung tissue damage. We also found an increase in total protein (TP) level and IL-5 production in bronchoalveolar lavage (BAL) fluid and an increase in SRW-specific Th2-type immunoglobulins (IgG1, IgG2b) and total serum IgE levels. Under similar treatment, DQ-negative full-sib control mice were normal. The allergic response could be significantly inhibited or abrogated in HLA-DQ mice by systemic treatment with anti-DQ mAb. The in vivo responses of HLA-DQ6 and HLA-DQ8 mice showed differences in terms of levels of eosinophilia, BAL protein, IL-5 concentration, and lung hyperreactivity to inhaled methacholine. These findings demonstrate the crucial role for specific HLA-DQ molecules in SRW-specific CD4+ T-cell activation and resulting recruitment of eosinophils into the airways.

Authors

Svetlana P. Chapoval, Gerald H. Nabozny, Eric V. Marietta, Ernie L. Raymond, Christopher J. Krco, Amy G. Andrews, Chella S. David

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Figure 5

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Immunostaining of lung tissue for mouse eosinophil MBP. H-2Aβ0, HLA-DQ6,...
Immunostaining of lung tissue for mouse eosinophil MBP. H-2Aβ0, HLA-DQ6, or HLA-DQ8 mice were immunized, boosted, and challenged intranasally with SRW allergenic extract as described in Methods. PBS-treated, PBS-challenged mice served as a control for this study. (a) Lung of PSB-treated HLA-DQ6 mouse with a few eosinophils in lung tissue (×10). (b) Lung of SRW-sensitized and -challenged H-2Aβ0 mouse (×10). Severe perivascular and peribronchial concentration of eosinophils in SRW-treated HLA-DQ6 (c) and HLA-DQ8 (d) mice (×10). (e–h) High-power magnification of lungs from HLA-DQ mice (×40). Eosinophil migration from blood vessel to airway mucosa and epithelium in HLA-DQ6 (e) and HLA-DQ8 (f) transgenic mice, and their granule release (f and g). Positive staining of infiltrating macrophages for MBP (h) as a result of its uptake from degranulating eosinophils. Arrow, blood vessel; arrowhead, bronchiole; m, macrophages.

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ISSN: 0021-9738 (print), 1558-8238 (online)

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