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由葡萄球菌蛋白A和链球菌蛋白G改造而成的嵌合IgG结合受体。

Chimeric IgG-binding receptors engineered from staphylococcal protein A and streptococcal protein G.

作者信息

Eliasson M, Olsson A, Palmcrantz E, Wiberg K, Inganäs M, Guss B, Lindberg M, Uhlén M

机构信息

Department of Biochemistry, Royal Institute of Technology, Stockholm, Sweden.

出版信息

J Biol Chem. 1988 Mar 25;263(9):4323-7.

PMID:2964447
Abstract

Chimeric Fc receptors, consisting of the IgG-binding domains of both staphylococcal protein A and streptococcal protein G, were constructed. An efficient bacterial expression system was used to produce the recombinant proteins, which vary in size and number of IgG-binding domains. The purified receptors were analyzed by immunodiffusion and a competitive enzyme-linked immunosorbent assay to establish the relative binding strength to various polyclonal and monoclonal immunoglobulins from different species. The results demonstrate that protein A and protein G have complementary binding patterns and that the chimeric receptors retain the binding capacities of both the parental constituents. This suggests that these novel chimeric receptors might be versatile reagents for immunochemical assays.

摘要

构建了由葡萄球菌蛋白A和链球菌蛋白G的IgG结合结构域组成的嵌合Fc受体。使用高效的细菌表达系统来生产重组蛋白,这些重组蛋白在IgG结合结构域的大小和数量上有所不同。通过免疫扩散和竞争性酶联免疫吸附测定法对纯化的受体进行分析,以确定其与来自不同物种的各种多克隆和单克隆免疫球蛋白的相对结合强度。结果表明,蛋白A和蛋白G具有互补的结合模式,并且嵌合受体保留了两种亲本成分的结合能力。这表明这些新型嵌合受体可能是免疫化学分析的通用试剂。

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