Abrogation of IL-4 receptor-α-dependent alternatively activated macrophages is sufficient to confer resistance against pulmonary cryptococcosis despite an ongoing Th2 response

In the murine model of pulmonary infection with Cryptococcus neoformans, IL-4 receptor α (IL-4Rα)-dependent polyfunctional Th2 cells induce disease progression associated with alternative activation of lung macrophages. To characterize the effector role of IL-4Rα-dependent alternatively activated ma...

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Published in:International immunology 2013-08, Vol.25 (8), p.459-470
Main Authors: Müller, Uwe, Stenzel, Werner, Piehler, Daniel, Grahnert, Andreas, Protschka, Martina, Köhler, Gabriele, Frey, Oliver, Held, Josephin, Richter, Tina, Eschke, Maria, Kamradt, Thomas, Brombacher, Frank, Alber, Gottfried
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container_issue 8
container_start_page 459
container_title International immunology
container_volume 25
creator Müller, Uwe
Stenzel, Werner
Piehler, Daniel
Grahnert, Andreas
Protschka, Martina
Köhler, Gabriele
Frey, Oliver
Held, Josephin
Richter, Tina
Eschke, Maria
Kamradt, Thomas
Brombacher, Frank
Alber, Gottfried
description In the murine model of pulmonary infection with Cryptococcus neoformans, IL-4 receptor α (IL-4Rα)-dependent polyfunctional Th2 cells induce disease progression associated with alternative activation of lung macrophages. To characterize the effector role of IL-4Rα-dependent alternatively activated macrophages (aaMph), we intra-nasally infected mice with genetically ablated IL-4Rα expression on macrophages (LysMCreIL-4Rα–/lox mice) and IL-4Rα–/lox littermates. LysMCreIL-4Rα–/lox mice were significantly more resistant to pulmonary cryptococcosis with higher survival rates and lower lung burden than non-deficient heterozygous littermates. Infected LysMCreIL-4Rα–/lox mice had reduced but detectable numbers of aaMph expressing arginase-1, chitinase-like enzyme (YM1) and CD206. Similar pulmonary expression of inducible nitric oxide synthase was found in LysMCreIL-4Rα–/lox and IL-4Rα–/lox control mice, but macrophages from LysMCreIL-4Rα–/lox mice showed a higher potential to produce nitric oxide. In contrast to the differences in the macrophage phenotype, pulmonary Th2 responses were similar in infected LysMCreIL-4Rα–/lox and IL-4Rα–/lox mice with each mouse strain harboring polyfunctional Th2 cells. Consistently, type 2 pulmonary allergic inflammation associated with eosinophil recruitment and epithelial mucus production was present in lungs of both LysMCreIL-4Rα–/lox and IL-4Rα–/lox mice. Our results demonstrate that, despite residual IL-4Rα-independent alternative macrophage activation and ongoing Th2-dependent allergic inflammation, abrogation of IL-4Rα-dependent aaMph is sufficient to confer resistance in pulmonary cryptococcosis. This is even evident on a relatively resistant heterozygous IL-4Rα+/– background indicating a key contribution of macrophage IL-4Rα expression to susceptibility in allergic bronchopulmonary mycosis.
doi_str_mv 10.1093/intimm/dxt003
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title Abrogation of IL-4 receptor-α-dependent alternatively activated macrophages is sufficient to confer resistance against pulmonary cryptococcosis despite an ongoing Th2 response
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