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小鼠狼疮中IgM和IgG抗DNA抗体的体细胞多样化及亲和力成熟

Somatic diversification and affinity maturation of IgM and IgG anti-DNA antibodies in murine lupus.

作者信息

Hirose S, Wakiya M, Kawano-Nishi Y, Yi J, Sanokawa R, Taki S, Shimamura T, Kishimoto T, Tsurui H, Nishimura H

机构信息

Department of Pathology, Juntendo University School of Medicine, Tokyo, Japan.

出版信息

Eur J Immunol. 1993 Nov;23(11):2813-20. doi: 10.1002/eji.1830231114.

DOI:10.1002/eji.1830231114
PMID:8223857
Abstract

Molecular events occurring during the process of generation of pathogenic immunoglobulin (Ig)G anti-DNA antibodies in systemic lupus erythematosus (SLE) were studied using a newly established method. We analyzed the Ig variable (V) region gene sequence and DNA-binding activity of IgM and IgG anti-DNA monoclonal antibodies (mAb) from individual SLE-prone (NZB x NZW) F1 mice. The first event appeared to be clonal selection and expansion of IgM anti-DNA clones, in which several clones had intraclonal V gene mutations. Although the number of mutations was small, the mutated IgM clones were associated with an increase in DNA-binding activity. The somatic mutations located in complementarity-determining regions (CDR) and in framework regions (FR) of V genes were apparently related to changes in DNA-binding activity. IgG anti-DNA clones that progressively increased in number with aging had numerous somatic mutations in the V region genes and there was a pair of clones which showed an intraclonal accumulation of mutations, in association with increase in the DNA-binding activity. All these findings show that somatic mutations associated with affinity maturation of the V region begin immediately before isotype-switching from IgM to IgG of the clones that have been selected and expanded, in an antigen-driven manner and/or by other forces. We propose that further accumulations of intraclonal somatic hypermutation, in association with selection and expansion of high affinity IgG clones, may lead to formation of highly pathogenic anti-DNA antibodies.

摘要

利用一种新建立的方法,研究了系统性红斑狼疮(SLE)中致病性免疫球蛋白(Ig)G抗DNA抗体产生过程中发生的分子事件。我们分析了来自易患SLE的(NZB×NZW)F1小鼠个体的IgM和IgG抗DNA单克隆抗体(mAb)的Ig可变(V)区基因序列和DNA结合活性。第一个事件似乎是IgM抗DNA克隆的克隆选择和扩增,其中几个克隆存在克隆内V基因的突变。虽然突变数量较少,但突变的IgM克隆与DNA结合活性的增加有关。位于V基因互补决定区(CDR)和框架区(FR)的体细胞突变显然与DNA结合活性的变化有关。随着年龄增长数量逐渐增加的IgG抗DNA克隆在V区基因中有大量体细胞突变,并且有一对克隆显示出克隆内突变的积累,同时DNA结合活性增加。所有这些发现表明,与V区亲和力成熟相关的体细胞突变在已被选择和扩增的克隆从IgM向IgG进行同种型转换之前立即开始,以抗原驱动的方式和/或其他力量。我们提出,克隆内体细胞超突变的进一步积累,与高亲和力IgG克隆的选择和扩增相关,可能导致高致病性抗DNA抗体的形成。

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