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膜免疫球蛋白E以抗原非依赖的方式结合并激活FcεRI。

Membrane IgE binds and activates Fc epsilon RI in an antigen-independent manner.

作者信息

Vangelista Luca, Soprana Elisa, Cesco-Gaspere Michela, Mandiola Paola, Di Lullo Giulia, Fucci Rita N, Codazzi Franca, Palini Alessio, Paganelli Giovanni, Burrone Oscar R, Siccardi Antonio G

机构信息

Department of Biology and Genetics, University of Milan, Milan, Italy.

出版信息

J Immunol. 2005 May 1;174(9):5602-11. doi: 10.4049/jimmunol.174.9.5602.

Abstract

Interaction of secretory IgE with FcepsilonRI is the prerequisite for allergen-driven cellular responses, fundamental events in immediate and chronic allergic manifestations. Previous studies reported the binding of soluble FcepsilonRIalpha to membrane IgE exposed on B cells. In this study, the functional interaction between human membrane IgE and human FcepsilonRI is presented. Four different IgE versions were expressed in mouse B cell lines, namely: a truncation at the Cepsilon2-Cepsilon3 junction of membrane IgE isoform long, membrane IgE isoform long (without Igalpha/Igbeta BCR accessory proteins), and both epsilonBCRs (containing membrane IgE isoforms short and long). All membrane IgE versions activated a rat basophilic leukemia cell line transfected with human FcepsilonRI, as detected by measuring the release of both preformed and newly synthesized mediators. The interaction led also to Ca(2+) responses in the basophil cell line, while membrane IgE-FcepsilonRI complexes were detected by immunoprecipitation. FcepsilonRI activation by membrane IgE occurs in an Ag-independent manner. Noteworthily, human peripheral blood basophils and monocytes also were activated upon contact with cells bearing membrane IgE. In humans, the presence of FcepsilonRI in several cellular entities suggests a possible membrane IgE-FcepsilonRI-driven cell-cell dialogue, with likely implications for IgE homeostasis in physiology and pathology.

摘要

分泌型IgE与FcepsilonRI的相互作用是变应原驱动的细胞反应的前提条件,是速发型和慢性过敏表现中的基本事件。先前的研究报道了可溶性FcepsilonRIα与B细胞表面暴露的膜IgE的结合。在本研究中,展示了人膜IgE与人FcepsilonRI之间的功能相互作用。在小鼠B细胞系中表达了四种不同的IgE变体,即:膜IgE长异构体在Cepsilon2-Cepsilon3连接处的截短形式、膜IgE长异构体(无Igalpha/Igbeta BCR辅助蛋白)以及两种epsilonBCR(包含膜IgE短异构体和长异构体)。通过测量预先形成的和新合成的介质的释放来检测,所有膜IgE变体均激活了转染了人FcepsilonRI的大鼠嗜碱性白血病细胞系。这种相互作用还导致嗜碱性粒细胞系中的Ca(2+)反应,同时通过免疫沉淀检测到膜IgE-FcepsilonRI复合物。膜IgE对FcepsilonRI的激活以不依赖抗原的方式发生。值得注意的是,人外周血嗜碱性粒细胞和单核细胞在与携带膜IgE的细胞接触时也被激活。在人类中,几种细胞实体中存在FcepsilonRI表明可能存在膜IgE-FcepsilonRI驱动的细胞间对话,这可能对生理和病理状态下的IgE稳态产生影响。

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