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重链可变区、轻链可变区以及重链互补决定区3对人单克隆类风湿因子的单反应性和多反应性及亲和力的影响。

Heavy chain variable region, light chain variable region, and heavy chain CDR3 influences on the mono- and polyreactivity and on the affinity of human monoclonal rheumatoid factors.

作者信息

Crouzier R, Martin T, Pasquali J L

机构信息

Laboratory of Immunopathology, University Hospitals of Strasbourg, France.

出版信息

J Immunol. 1995 May 1;154(9):4526-35.

PMID:7722307
Abstract

Monoreactive high affinity pathologic autoantibodies were supposed previously to derive through somatic mutation from polyreactive low affinity autoantibodies that are encoded by a small set of unmutated V region genes in fetal and neonatal B cells. However, recent data exploring the physiologically expressed Ab repertoire and the importance of the stochastically generated heavy chain CDR3 (H-CDR3) in autoreactivity suggest that this scheme is incomplete. Here we analyzed via gene-swapping experiments and site-directed mutagenesis the relative contributions of the mutations in the light chain variable region (VL) and the heavy chain variable region (VH) domains and of the H-CDR3 in the autoreactivity of two IgM rheumatoid factors (RF), one a polyreactive low affinity Ab, the other a monoreactive high affinity Ab. These two RFs derived from the same V kappa III (humkv325) and VH1 (51p1) genes, but differed from each other by a few mutations and by the structure of the H-CDR3. The analysis of the reactivity patterns of different combinations of wild-type and in vitro engineered hybrid gene products clearly demonstrates the main influence of the H-CDR3 in the autoAb activity profiles. The results directly demonstrate the previously proposed hypothesis, namely, that the H-CDR3 plays a critical role in distinguishing poly- from monospecific RF. However, the data also indicate that self polyreactivity is a very fragile property and is dependent upon the primary structure of the VH segment.

摘要

以前认为,单反应性高亲和力病理性自身抗体是由胎儿和新生儿B细胞中一小部分未突变的V区基因编码的多反应性低亲和力自身抗体通过体细胞突变产生的。然而,最近探索生理表达的抗体库以及随机产生的重链互补决定区3(H-CDR3)在自身反应性中的重要性的数据表明,这一模式并不完整。在这里,我们通过基因交换实验和定点诱变分析了轻链可变区(VL)和重链可变区(VH)结构域中的突变以及H-CDR3对两种IgM类风湿因子(RF)自身反应性的相对贡献,其中一种是多反应性低亲和力抗体,另一种是单反应性高亲和力抗体。这两种RF源自相同的VκIII(humkv325)和VH1(51p1)基因,但彼此之间存在一些突变差异以及H-CDR3结构的不同。对野生型和体外工程化杂交基因产物不同组合的反应模式分析清楚地证明了H-CDR3对自身抗体活性谱的主要影响。结果直接证明了先前提出的假设,即H-CDR3在区分多特异性和单特异性RF中起关键作用。然而,数据也表明自身多反应性是一种非常脆弱的特性,并且依赖于VH区段的一级结构。

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