Attenuation of IgE Affinity for FcϵRI Radically Reduces the Allergic Response in Vitro and in Vivo

Attenuation of IgE Affinity for FcϵRI Radically Reduces the Allergic Response in Vitro and in Vivo

The high affinity of IgE for its receptor, FcϵRI (Ka ∼ 1010m–1), is responsible for the persistence of mast cell sensitization. Cross-linking of FcϵRI-bound IgE by multivalent allergen leads to cellular activation and release of pro-inflammatory mediators responsible for the symptoms of allergic dis...

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Veröffentlicht in:The Journal of biological chemistry 2008-10, Vol.283 (44), p.29882-29887
Hauptverfasser: Hunt, James, Bracher, Marguerite G., Shi, Jianguo, Fleury, Sébastien, Dombrowicz, David, Gould, Hannah J., Sutton, Brian J., Beavil, Andrew J.
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Mechanisms of Signal Transduction
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container_end_page 29887
container_issue 44
container_start_page 29882
container_title The Journal of biological chemistry
container_volume 283
creator Hunt, James
Bracher, Marguerite G.
Shi, Jianguo
Fleury, Sébastien
Dombrowicz, David
Gould, Hannah J.
Sutton, Brian J.
Beavil, Andrew J.
description The high affinity of IgE for its receptor, FcϵRI (Ka ∼ 1010m–1), is responsible for the persistence of mast cell sensitization. Cross-linking of FcϵRI-bound IgE by multivalent allergen leads to cellular activation and release of pro-inflammatory mediators responsible for the symptoms of allergic disease. We previously demonstrated that limiting the IgE-FcϵRI interaction to just one of the two Cϵ3 domains in IgE-Fc, which together constitute the high affinity binding site, results in 1000-fold reduced affinity. Such attenuation, effected by a small molecule binding to part of the IgE:FcϵRI interface or a distant allosteric site, rather than complete blocking of the interaction, may represent a viable approach to the treatment of allergic disease. However, the degree to which the interaction would need to be disrupted is unclear, because the importance of high affinity for immediate hypersensitivity has never been investigated. We have incorporated into human IgE a mutation, R334S, previously characterized in IgE-Fc, which reduces its affinity for FcϵRI ∼50-fold. We have compared the ability of wild type and R334S IgE to stimulate allergen-induced mast cell activation in vitro and in vivo. We confirmed the expected difference in affinity between wild type and mutant IgE for FcϵRI (∼50-fold) and found that, in vitro, mast cell degranulation was reduced proportionately. The effect in vivo was also marked, with a 75% reduction in the passive cutaneous anaphylaxis response. We have therefore demonstrated that the high affinity of IgE for FcϵRI is critical to the allergic response, and that even moderate attenuation of this affinity has a substantial effect in vivo.
doi_str_mv 10.1074/jbc.M804742200
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Cross-linking of FcϵRI-bound IgE by multivalent allergen leads to cellular activation and release of pro-inflammatory mediators responsible for the symptoms of allergic disease. We previously demonstrated that limiting the IgE-FcϵRI interaction to just one of the two Cϵ3 domains in IgE-Fc, which together constitute the high affinity binding site, results in 1000-fold reduced affinity. Such attenuation, effected by a small molecule binding to part of the IgE:FcϵRI interface or a distant allosteric site, rather than complete blocking of the interaction, may represent a viable approach to the treatment of allergic disease. However, the degree to which the interaction would need to be disrupted is unclear, because the importance of high affinity for immediate hypersensitivity has never been investigated. We have incorporated into human IgE a mutation, R334S, previously characterized in IgE-Fc, which reduces its affinity for FcϵRI ∼50-fold. We have compared the ability of wild type and R334S IgE to stimulate allergen-induced mast cell activation in vitro and in vivo. We confirmed the expected difference in affinity between wild type and mutant IgE for FcϵRI (∼50-fold) and found that, in vitro, mast cell degranulation was reduced proportionately. The effect in vivo was also marked, with a 75% reduction in the passive cutaneous anaphylaxis response. 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title Attenuation of IgE Affinity for FcϵRI Radically Reduces the Allergic Response in Vitro and in Vivo
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