Paul J. Justice scite author profile

. Intrinsic AHR in IL-5 transgenic mice is dependent on CD4 ϩ cells and CD49d-mediated signaling. Am J Physiol Lung Cell Mol Physiol 281: L653-L659, 2001.-Overexpression of interleukin (IL)-5 by the airway epithelium in mice using the rat CC10 promoter (NJ.1726 line) leads to several histopathologies characteristic of human asthma, including airway hyperreactivity (AHR). We investigated the contribution of B and T cells, as well as CD4 expression, to the development of AHR in IL-5 transgenic mice. NJ.1726 mice on a T cell or CD4 knockout background, but not on a B cell knockout background, lost intrinsic AHR. These effects occurred without decreases in IL-5 or eosinophils. We further investigated the contribution of ␣ 4-integrin signaling to the development of AHR in IL-5 transgenic mice through the administration of anti-CD49d (␣ 4-integrin) antibody (PS/2). Administration of PS/2 resulted in immediate (16-h) inhibition of AHR. The inhibition of AHR was not associated with a decrease in airway eosinophils. These studies demonstrate that, despite the presence of increased levels of IL-5 and eosinophils in the lungs of NJ.1726 mice, CD4 ϩ cells and ␣4-integrin signaling are necessary for the intrinsic AHR that develops in IL-5 transgenic mice.

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Gq Signaling Is Required for Allergen-Induced Pulmonary Eosinophilia

Borchers

Justice

Ansay

et al. 2002

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The complexity and magnitude of interactions leading to the selective infiltration of eosinophils in response to inhaled allergens are formidable obstacles to a larger understanding of the pulmonary pathology associated with allergic asthma. This study uses knockout mice to demonstrate a novel function for the heterotrimeric G protein, Gq, in the regulation of pulmonary eosinophil recruitment. In the absence of Gq signaling, eosinophils failed to accumulate in the lungs following allergen challenge. These studies demonstrate that the inhibition of eosinophil accumulation in the airways is attributed to the failure of hemopoietically derived cells to elaborate GM-CSF in the airways. The data suggest that activation of a Gq-coupled receptor(s) on resident leukocytes in the lung elicits expression of GM-CSF, which, in turn, is required for allergen-induced pulmonary eosinophilia, identifying a novel pathway of eosinophil-associated effector functions leading to pulmonary pathology in diseases such as asthma.

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Paul J. Justice

Differential Modulation of Allergic Eye Disease by Chronic and AcuteAscarisInfection

Intrinsic AHR in IL-5 transgenic mice is dependent on CD4⁺cells and CD49d-mediated signaling

Gq Signaling Is Required for Allergen-Induced Pulmonary Eosinophilia

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Paul J. Justice

Differential Modulation of Allergic Eye Disease by Chronic and AcuteAscarisInfection

Intrinsic AHR in IL-5 transgenic mice is dependent on CD4+cells and CD49d-mediated signaling

Gq Signaling Is Required for Allergen-Induced Pulmonary Eosinophilia

Contact Info

Product

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Intrinsic AHR in IL-5 transgenic mice is dependent on CD4⁺cells and CD49d-mediated signaling