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以内源性凝集素(IgE结合蛋白)的差异识别为特征的异质性IgE糖型。

Heterogeneous IgE glycoforms characterized by differential recognition of an endogenous lectin (IgE-binding protein).

作者信息

Robertson M W, Liu F T

机构信息

Department of Molecular and Experimental Medicine, Research Institute of Scripps Clinic, La Jolla, CA 92037.

出版信息

J Immunol. 1991 Nov 1;147(9):3024-30.

PMID:1919004
Abstract

IgE is highly glycosylated, but the function of the oligosaccharide side chains is largely unknown. The previous discovery of an animal lectin, IgE-binding protein (epsilon BP), affords an opportunity to study potential carbohydrate-dependent effector functions of IgE. epsilon BP is a beta-galactoside-specific lectin with binding affinity for IgE and is now known to be equivalent to carbohydrate-binding protein 35 and the Mac-2 Ag; thus, it may have multiple functions in addition to IgE binding. We have previously shown that rat r epsilon BP recognizes sialidase-treated human myeloma IgE to a much greater extent than the untreated IgE. In contrast, human epsilon BP binds essentially equivalently to a monoclonal murine IgE with or without sialidase pretreatment. To validate a possible role for epsilon BP in the IgE system, we investigated the pattern of recognition of epsilon BP for various polyclonal human IgE samples. We show that polyclonal IgE derived from four individuals with hyper-IgE syndrome or atopic dermatitis recognizes epsilon BP and that there is individual variation in the proportion of IgE recognized by epsilon BP, ranging from greater than 60% for one sample to almost undetectable levels in another. We conclude that epsilon BP does indeed recognize polyclonal IgE and that this recognition is modulated by sialylation of IgE oligosaccharides. Furthermore, there exist different IgE glycoforms, varying in the degree of sialylation, and these are distributed in a distinct manner in different individuals.

摘要

免疫球蛋白E(IgE)高度糖基化,但其寡糖侧链的功能在很大程度上尚不清楚。先前发现的一种动物凝集素,即IgE结合蛋白(εBP),为研究IgE潜在的碳水化合物依赖性效应功能提供了一个机会。εBP是一种对β-半乳糖苷具有特异性的凝集素,对IgE具有结合亲和力,现在已知它等同于碳水化合物结合蛋白35和Mac-2抗原;因此,它可能除了IgE结合外还具有多种功能。我们先前已经表明,大鼠的εBP对经唾液酸酶处理的人骨髓瘤IgE的识别程度比未经处理的IgE要高得多。相比之下,人εBP对经或未经唾液酸酶预处理的单克隆鼠IgE的结合基本相同。为了验证εBP在IgE系统中可能发挥的作用,我们研究了εBP对各种多克隆人IgE样本的识别模式。我们发现,来自四名高IgE综合征患者或特应性皮炎患者的多克隆IgE能够识别εBP,并且εBP识别的IgE比例存在个体差异,从一个样本中的大于60%到另一个样本中的几乎检测不到的水平不等。我们得出结论,εBP确实能够识别多克隆IgE,并且这种识别受到IgE寡糖唾液酸化的调节。此外,存在不同的IgE糖型,其唾液酸化程度不同,并且在不同个体中以不同的方式分布。

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