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一种基于葡萄球菌蛋白A的合成IgG结合结构域。

A synthetic IgG-binding domain based on staphylococcal protein A.

作者信息

Nilsson B, Moks T, Jansson B, Abrahmsén L, Elmblad A, Holmgren E, Henrichson C, Jones T A, Uhlén M

机构信息

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

出版信息

Protein Eng. 1987 Feb-Mar;1(2):107-13. doi: 10.1093/protein/1.2.107.

Abstract

A synthetic IgG-binding domain based on staphylococcal protein A was designed with the aid of sequence comparisons and computer graphic analysis. A strategy, utilizing non-palindromic restriction sites, was used to overcome the difficulties of introducing site-specific changes into the repetitive gene. A single mutagenized gene fragment was polymerized to different multiplicities, and the different gene products were expressed in Escherichia coli. Using this scheme, protein A-like proteins composed of different numbers of IgG-binding domains were produced. These domains were changed to lack asparagine--glycine dipeptide sequences as well as methionine residues and are thus, in contrast to native protein A, resistant to treatment with hydroxylamine and cyanogen bromide.

摘要

基于葡萄球菌蛋白A设计了一种合成IgG结合结构域,借助序列比较和计算机图形分析完成。采用一种利用非回文限制酶切位点的策略,以克服将位点特异性变化引入重复基因的困难。将单个诱变基因片段聚合成不同的拷贝数,并在大肠杆菌中表达不同的基因产物。利用该方案,产生了由不同数量IgG结合结构域组成的类蛋白A蛋白。这些结构域经改造后缺少天冬酰胺-甘氨酸二肽序列以及甲硫氨酸残基,因此与天然蛋白A不同,对羟胺和溴化氰处理具有抗性。

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