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一种单克隆抗IgE抗体无过敏反应性的分子基础。

Molecular basis for nonanaphylactogenicity of a monoclonal anti-IgE antibody.

作者信息

Rudolf M P, Zuercher A W, Nechansky A, Ruf C, Vogel M, Miescher S M, Stadler B M, Kricek F

机构信息

Institute of Immunology and Allergology, Inselspital, University of Bern, Bern, Switzerland.

出版信息

J Immunol. 2000 Jul 15;165(2):813-9. doi: 10.4049/jimmunol.165.2.813.

DOI:10.4049/jimmunol.165.2.813
PMID:10878355
Abstract

IgE Abs mediate allergic responses by binding to specific high affinity receptors (FcepsilonRI) on mast cells and basophils. Therefore, the IgE/FcepsilonRI interaction is a target for clinical intervention in allergic disease. An anti-IgE mAb, termed BSW17, is nonanaphylactogenic, although recognizing IgE bound to FcepsilonRI, and interferes with binding of IgE to FcepsilonRI. Thus, BSW17 represents a candidate Ab for treatment of IgE-mediated disorders. By panning BSW17 against random peptide libraries displayed on phages, we defined mimotopes that mimic the conformational epitope recognized on human IgE. Two types of mimotopes, one within the Cepsilon3 and one within the Cepsilon4 domain, were identified, indicating that this mAb may recognize either a large conformational epitope or eventually two distinct epitopes on IgE. On the basis of alignments of the two mimotopes with the human IgE sequence, we postulate that binding of BSW17 to the Cepsilon3 region predominantly blocks binding of IgE to FcepsilonRI, leading to neutralization of IgE. Moreover, binding of BSW17 to the Cepsilon4 region may explain how BSW17 recognizes FcepsilonRI-bound IgE, and binding to this region may also interfere with degranulation of IgE sensitized cells (basophils and mast cells). As a practical application of these findings, mimotope peptides coupled to a carrier protein may be used for the development of a peptide-based anti-allergy vaccine by induction of anti-IgE Abs similar to the current approach of using humanized nonanaphylactogenic anti-IgE Abs as a passive vaccine.

摘要

IgE抗体通过与肥大细胞和嗜碱性粒细胞上的特异性高亲和力受体(FcepsilonRI)结合来介导过敏反应。因此,IgE/FcepsilonRI相互作用是过敏性疾病临床干预的一个靶点。一种名为BSW17的抗IgE单克隆抗体虽然能识别与FcepsilonRI结合的IgE,但不会引起过敏反应,并且能干扰IgE与FcepsilonRI的结合。因此,BSW17是治疗IgE介导疾病的候选抗体。通过用BSW17筛选噬菌体展示的随机肽库,我们确定了模拟人IgE上识别的构象表位的模拟表位。鉴定出两种类型的模拟表位,一种在Cepsilon3内,一种在Cepsilon4域内,这表明该单克隆抗体可能识别IgE上的一个大的构象表位或最终两个不同的表位。根据这两种模拟表位与人类IgE序列的比对,我们推测BSW17与Cepsilon3区域的结合主要阻断IgE与FcepsilonRI的结合,从而导致IgE的中和。此外,BSW17与Cepsilon4区域的结合可能解释了BSW17如何识别与FcepsilonRI结合的IgE,并且与该区域的结合也可能干扰IgE致敏细胞(嗜碱性粒细胞和肥大细胞)的脱颗粒。作为这些发现的实际应用,与载体蛋白偶联的模拟表位肽可用于开发基于肽的抗过敏疫苗,通过诱导类似于目前使用人源化无过敏反应抗IgE抗体作为被动疫苗的方法产生抗IgE抗体。

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