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Am J Physiol Lung Cell Mol Physiol 283: L1110-L1116, 2002. First published June 28, 2002; doi:10.1152/ajplung.00107.2002
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Vol. 283, Issue 5, L1110-L1116, November 2002

Bleomycin-induced lung fibrosis in IL-4-overexpressing and knockout mice

Gabriel Izbicki1, Reuven Or2, Thomas G. Christensen3, Michael J. Segel1, Alan Fine4, Ronald H. Goldstein4, and Raphael Breuer1,3,4

1 Lung Cellular and Molecular Biology Laboratory, Institute of Pulmonology, 2 Bone Marrow Transplantation Department, Hadassah University Hospital and The Hebrew University-Hadassah Medical School, 91120 Jerusalem, Israel; and 3 Mallory Institute of Pathology, Department of Pathology and 4 Pulmonary Center, Boston University School of Medicine and Boston Veterans Administration Medical Center, Boston, Massachusetts 02118

The role of IL-4 in the development of lung fibrosis is as yet unclear. Bleomycin (Bleo) or saline (Sal) was injected intratracheally into three groups of C57BL/6J mice: transgenic animals that overexpressed IL-4 (IL-4 TG, n = 14), mice with a targeted knockout mutation of the IL-4 gene (IL-4 KO, n = 11), and wild-type (WT, n = 13) mice. At 14 days, lung fibrosis was evaluated by hydroxyproline measurement and by quantitative image analysis of fibrosis fraction and alveolar wall area fraction. Bronchoalveolar lavage cell counts in all Bleo-treated groups demonstrated an increased percentage of lymphocytes with a corresponding decrease in the percentage of macrophages. Comparing Bleo- to Sal-treated controls within each group of mice showed increases in all lung fibrosis parameters in IL-4 KO and WT, but not in any of the parameters in IL-4 TG mice. The severity of Bleo-induced fibrotic response was decreased in overexpressed IL-4 TG compared with IL-4 KO mice. These data negate a critical profibrotic role for IL-4 in Bleo-induced lung fibrosis.

interstitial lung disease; computer-assisted morphometry; C57BL/6J; transgenic mice


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