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具有抗γ球蛋白活性的人单克隆IgM κ轻链之间的序列相似性和交叉独特型特异性。

Sequence similarities and cross-idiotypic specificity of L chains among human monoclonal IgM kappa with anti-gamma-globulin activity.

作者信息

Goñi F, Chen P P, Pons-Estel B, Carson D A, Frangione B

出版信息

J Immunol. 1985 Dec;135(6):4073-9.

PMID:2415598
Abstract

The complete amino acid sequence of five light chain variable (V) regions of human monoclonal IgM kappa rheumatoid factors (RF) was determined, and their cross-reactive idiotypes (CRI) were characterized with antibodies induced by immunization with synthetic peptides PSL2 and PSL3, corresponding to the second and third complementarity-determining regions (CDR) of the SIE light chain. Together with two additional RF studied previously, all seven RF belong to the V kappa IIIb sub-subgroup. The region encoded by the V kappa gene segment (positions 1 to 95) in all seven proteins was virtually identical in primary structure, whereas the sequence from positions 96 to 108 defined the usage of the J kappa 1 gene in three proteins and the J kappa 2 gene in four of them. Position 96 contributed by the recombination of the V kappa and J kappa gene segments showed the presence of four different amino acid residues. Both anti-PSL2 and anti-PSL3 bind efficiently to all separated L chains when analyzed by the Western blot technique, and the binding was inhibited specifically by the corresponding peptides. The results reveal that the majority of human IgM-RF light chains are derived from a single germ line V kappa gene or a family of closely related V kappa III germ line genes, and express two "primary structure-dependent" CRI, which are largely dependent on the amino acid sequence of the second and third light chain CDR.

摘要

测定了人单克隆IgMκ类风湿因子(RF)5个轻链可变(V)区的完整氨基酸序列,并用对应于SIE轻链第二和第三互补决定区(CDR)的合成肽PSL2和PSL3免疫诱导产生的抗体对其交叉反应性独特型(CRI)进行了表征。连同之前研究的另外两种RF,所有7种RF都属于VκIIIb亚亚组。所有7种蛋白质中由Vκ基因片段编码的区域(第1至95位)在一级结构上几乎相同,而第96至108位的序列确定了3种蛋白质中Jκ1基因的使用情况以及另外4种蛋白质中Jκ2基因的使用情况。由Vκ和Jκ基因片段重组产生的第96位显示存在4种不同的氨基酸残基。通过蛋白质印迹技术分析时,抗PSL2和抗PSL3均能有效结合所有分离的轻链,且相应肽段能特异性抑制这种结合。结果表明,大多数人IgM-RF轻链源自单个种系Vκ基因或一个密切相关的VκIII种系基因家族,并表达两种“一级结构依赖性”CRI,这在很大程度上取决于轻链第二和第三CDR的氨基酸序列。

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