A.L.P. de Siqueira scite author profile

The potent spasmogenic properties of IL-13 have identified this molecule as a potential regulator of airways hyperreactivity (AHR) in asthma. Although IL-13 is thought to primarily signal through the IL-13Rα1-IL-4Rα complex, the cellular and molecular components employed by this cytokine to induce AHR in the allergic lung have not been identified. By transferring OVA-specific CD4+ T cells that were wild type (IL-13+/+ T cells) or deficient in IL-13 (IL-13−/− T cells) to nonsensitized mice that were then challenged with OVA aerosol, we show that T cell-derived IL-13 plays a key role in regulating AHR, mucus hypersecretion, eotaxin production, and eosinophilia in the allergic lung. Moreover, IL-13+/+ T cells induce these features (except mucus production) of allergic disease independently of the IL-4Rα chain. By contrast, IL-13+/+ T cells did not induce disease in STAT6-deficient mice. This shows that IL-13 employs a novel component of the IL-13 receptor signaling system that involves STAT6, independently of the IL-4Rα chain, to modulate pathogenesis. We show that this novel pathway for IL-13 signaling is dependent on T cell activation in the lung and is critically linked to downstream effector pathways regulated by eotaxin and STAT6.

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Prevention of lung eosinophilic inflammation by oral tolerance

Russo

Jancar

Siqueira

et al. 1998

Immunology Letters

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A new murine model of pulmonary eosinophilic hypersensitivity: Contribution to experimental asthma

Siqueira¹,

Russo²,

Steil³

et al. 1997

Journal of Allergy and Clinical Immunology

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A novel murine model of late‐phase reaction of immediate hypersensitivity

Facincone

Siqueira

Jancar

et al. 1997

Mediators of Inflammation

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We describe here a novel experimental model of late-phase reaction of immediate hypersensitivity developed in mice. It consists of introducing small fragments of heat-coagulated hen egg white into the subcutaneous tissue of mice. After 14 days, animals challenged with purified ovalbumin into the footpad presented an immediate swelling of the paw peaking at 30 min, followed by two peaks of swelling at 6 and 24 h. Histological examination of the paws showed a massive eosinophil infiltration (more than 800 cells/5 microscopic fields). This intense infiltration persisted for more than 14 days after the challenge. Furthermore, in mice immunized with coagulated egg white the delayed swelling of the paws and eosinophilic infiltration were significantly higher than in mice immunized with the classical protocol of ovalbumin in alumen adjuvant. Transfer of lymph node cells obtained from mice implanted with heat-coagulated hen egg white induced footpad swelling and eosinophil infiltration in response to ovalbumin. High levels of ovalbuminspecific IgG1 but not of IgE were detected in the serum of these animals. The advantages of this model for the experimental study of late-phase reaction per se and its relevance to the study of allergic diseases such as asthma are discussed.

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Oral tolerance prevents the development of experimental asthma

Russo¹,

Jancar²,

Siqueira³

et al. 1997

Immunology Letters

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A.L.P. de Siqueira

IL-13 Induces Airways Hyperreactivity Independently of the IL-4Rα Chain in the Allergic Lung

Prevention of lung eosinophilic inflammation by oral tolerance

A new murine model of pulmonary eosinophilic hypersensitivity: Contribution to experimental asthma

A novel murine model of late‐phase reaction of immediate hypersensitivity

Oral tolerance prevents the development of experimental asthma

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