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两种具有共同独特型特异性的人IgM抗γ球蛋白(Lay/Pom)可变区的完整氨基酸序列。

Complete amino acid sequence of the variable domains of two human IgM anti-gamma globulins (Lay/Pom) with shared idiotypic specificities.

作者信息

Capra J D, Klapper D G

出版信息

Scand J Immunol. 1976;5(6-7):677-84. doi: 10.1111/j.1365-3083.1976.tb03017.x.

Abstract

On the basis of extensive shared idiotypic specificities, two human IgM anti-gamma-globulins (Lay/Pom) were selected for complete amino acid sequence analysis of their variable domains. Previous studies on the variable regions of the heavy chains of these proteins had shown but eight amino acid differences, only one of which was within a complementarity-determining hypervariable region. The complete amino acid sequence of the variable regions of the light chains of these two proteins is the subject of this report. Protein Lay is a typical VchiI protein with only five 'framework' differences when compared with protein Roy. Protein Pom is best classified as a VchiII, but in the 'framework' there are 16 differences between it and protein Ti. Although there are extensive differences in the first hypervariable region, the second and third light-chain hypervariable regions have an identical sequence. The finding of two identical light-chain and two identical heavy-chain hypervariable regions in these two proteins, which were selected on the basis of their combining specificities and their idiotypic cross-reactions, strongly implicates hypervariable regions in the constitution of the idiotypic determinants and the antibody combining site. Additionally, the finding of identical hypervariable regions in light chains of different V-region subgroups fulfills a prediction of the gene-interaction concept of antibody variability.

摘要

基于广泛的共同独特型特异性,选择了两种人IgM抗γ球蛋白(Lay/Pom)对其可变区进行完整的氨基酸序列分析。此前对这些蛋白质重链可变区的研究仅显示出八个氨基酸差异,其中只有一个位于互补决定高变区内。本报告的主题是这两种蛋白质轻链可变区的完整氨基酸序列。与Roy蛋白相比,Lay蛋白是一种典型的VchiI蛋白,仅有五个“框架”差异。Pom蛋白最好归类为VchiII,但它与Ti蛋白在“框架”上有16个差异。尽管在第一个高变区存在广泛差异,但第二和第三轻链高变区具有相同的序列。在这两种基于结合特异性和独特型交叉反应而选择的蛋白质中发现两个相同的轻链高变区和两个相同的重链高变区,有力地表明高变区参与了独特型决定簇和抗体结合位点的构成。此外,在不同V区亚组的轻链中发现相同的高变区,证实了抗体变异性基因相互作用概念的一个预测。

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