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基于金黄色葡萄球菌蛋白A的免疫球蛋白A(IgA)和IgE特异性体外筛选结合蛋白(亲合体)在葡萄球菌表面的展示

Staphylococcal surface display of immunoglobulin A (IgA)- and IgE-specific in vitro-selected binding proteins (affibodies) based on Staphylococcus aureus protein A.

作者信息

Gunneriusson E, Samuelson P, Ringdahl J, Grönlund H, Nygren P A, Ståhl S

机构信息

Department of Biotechnology, Royal Institute of Technology (KTH), S-100 44 Stockholm, Sweden.

出版信息

Appl Environ Microbiol. 1999 Sep;65(9):4134-40. doi: 10.1128/AEM.65.9.4134-4140.1999.

Abstract

An expression system designed for cell surface display of hybrid proteins on Staphylococcus carnosus has been evaluated for the display of Staphylococcus aureus protein A (SpA) domains, normally binding to immunoglobulin G (IgG) Fc but here engineered by combinatorial protein chemistry to yield SpA domains, denoted affibodies, with new binding specificities. Such affibodies, with human IgA or IgE binding activity, have previously been selected from a phage library, based on an SpA domain. In this study, these affibodies have been genetically introduced in monomeric or dimeric forms into chimeric proteins expressed on the surface of S. carnosus by using translocation signals from a Staphylococcus hyicus lipase construct together with surface-anchoring regions of SpA. The recombinant surface proteins, containing the IgA- or IgE-specific affibodies, were demonstrated to be expressed as full-length proteins, localized and properly exposed at the cell surface of S. carnosus. Furthermore, these chimeric receptors were found to be functional, since recombinant S. carnosus cells were shown to have gained IgA and IgE binding capacity, respectively. In addition, a positive effect in terms of IgA and IgE reactivity was observed when dimeric versions of the affibodies were present. Potential applications for recombinant bacteria with redirected binding specificity in their surface proteins are discussed.

摘要

一种设计用于在肉葡萄球菌上进行杂合蛋白细胞表面展示的表达系统,已被用于展示金黄色葡萄球菌蛋白A(SpA)结构域。SpA结构域通常与免疫球蛋白G(IgG)的Fc段结合,但在此通过组合蛋白质化学方法进行改造,以产生具有新结合特异性的SpA结构域,即亲和体。此前已基于SpA结构域从噬菌体文库中筛选出具有人IgA或IgE结合活性的此类亲和体。在本研究中,利用来自猪葡萄球菌脂肪酶构建体的转运信号以及SpA的表面锚定区域,将这些亲和体以单体或二聚体形式基因导入到肉葡萄球菌表面表达的嵌合蛋白中。含有IgA或IgE特异性亲和体的重组表面蛋白被证明以全长蛋白形式表达,定位于肉葡萄球菌细胞表面并正确暴露。此外,这些嵌合受体被发现具有功能,因为重组肉葡萄球菌细胞分别显示出获得了IgA和IgE结合能力。此外,当存在亲和体的二聚体形式时,在IgA和IgE反应性方面观察到了积极效果。讨论了表面蛋白具有重新定向结合特异性的重组细菌的潜在应用。

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