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重组变应原分子:研究效应细胞活化的工具

Recombinant allergen molecules: tools to study effector cell activation.

作者信息

Valenta R, Kraft D

机构信息

Department of Pathophysiology, Vienna General Hospital, University of Vienna, Austria.

出版信息

Immunol Rev. 2001 Feb;179:119-27. doi: 10.1034/j.1600-065x.2001.790112.x.

Abstract

The IgE antibody-mediated activation of allergic effector cells is the key pathomechanism underlying the immediate symptoms of Type I allergy, a genetically determined hypersensitivity disease affecting 25% of the population. In recent years important environmental allergens and their epitopes have become available as structurally defined recombinant molecules. In addition, corresponding human monoclonal IgE and IgG antibodies have been isolated. This review summarizes data obtained regarding the three-dimensional structure of allergens, their IgE epitopes and the recognition of allergens by IgE and IgG antibodies. In particular, we discuss results of recent in vitro and in vivo studies with defined allergen molecules, their epitopes and the corresponding antibodies which support the hypothesis that the density and geometrical arrangement of IgE epitopes on a particular allergen molecule may profoundly affect effector cell activation. If the structural requirements for effector cell activation can be delineated, it may be envisaged that, based on this knowledge, allergens can be converted into hypoallergenic immunogens by reorientation of IgE epitopes. Such allergen derivatives may be used for allergen-specific immunotherapy with reduced risk of inducing anaphylactic side effects.

摘要

IgE抗体介导的过敏效应细胞激活是I型过敏即时症状的关键发病机制,I型过敏是一种影响25%人口的遗传性超敏疾病。近年来,重要的环境过敏原及其表位已作为结构明确的重组分子出现。此外,相应的人源单克隆IgE和IgG抗体也已分离出来。本综述总结了关于过敏原三维结构、其IgE表位以及IgE和IgG抗体对过敏原识别的相关数据。特别是,我们讨论了近期针对特定过敏原分子、其表位及相应抗体的体外和体内研究结果,这些结果支持这样一种假说,即特定过敏原分子上IgE表位的密度和几何排列可能会深刻影响效应细胞的激活。如果能够确定效应细胞激活的结构要求,那么可以设想,基于这一知识,通过重新排列IgE表位,过敏原可转化为低变应原性免疫原。此类过敏原衍生物可用于过敏原特异性免疫治疗,降低诱发过敏副作用的风险。

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