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天然自身抗体体细胞选择的证据。

Evidence for somatic selection of natural autoantibodies.

作者信息

Martin T, Duffy S F, Carson D A, Kipps T J

机构信息

Institut de Chimiebiologique, Faculté de Médecine, Strasburg, France.

出版信息

J Exp Med. 1992 Apr 1;175(4):983-91. doi: 10.1084/jem.175.4.983.

Abstract

Natural autoantibodies are primarily immunoglobulin M (IgM) antibodies that bind to a variety of self-antigens, including self-IgG. Accounting for a large proportion of the early B cell repertoire, such polyspecific autoantibodies are speculated to contribute to the homeostasis and/or competence of the primary humoral immune system. Recent studies indicate that the leukemia cells from most patients with chronic lymphocytic leukemia (CLL) also express such IgM autoantibodies. Similarly, the leukemia cells from many CLL patients react with murine monoclonal antibodies (mAbs) specific for crossreactive idiotypes (CRIs) associated with human IgM autoantibodies. In particular, leukemic cells frequently react with G6, a mAb specific for an Ig heavy chain (H chain)-associated CRI, and/or with 17.109, a mAb that defines a kappa light chain (L chain)-associated CRI. Generated against IgM rheumatoid factor (RF) paraproteins, G6 and 17.109 each recognize a major CRI that is present in many IgM RF paraproteins. Furthermore, over 90% of the IgM paraproteins found to bear both H and L chain-associated CRIs also are found to have RF activity. Molecular characterization of these CRIs demonstrates that each is a serologic marker for expression of a highly conserved Ig V gene. As such, the frequent production of IgM polyspecific autoantibodies in CLL simply may reflect the frequent use of such highly conserved autoantibody-encoding Ig V genes with little or no somatic mutation. To test this hypothesis, we generated murine transfectomas to pair the 17.109-reactive kappa L chain of SMI, a 17.109/G6-reactive CLL population, with the Ig H chain of SMI or other G6-reactive leukemia cells or tonsillar lymphocytes. Cotransfection of vectors encoding the Ig H and L chains of SMI generated transfectomas that produce IgM kappa RF autoantibodies reactive with human IgG1 and IgG4. In contrast to G6/17.109-reactive IgM kappa RF Waldenstrom's paraproteins, the SMI IgM kappa also reacts with several other self-antigens, including myoglobin, actin, and ssDNA. However, cotransfection of the SMI L chain with a vector encoding any one of 10 different G6-reactive Ig H chains generated transfectomas that produce IgM kappa antibodies without detectable polyspecific autoantibody activity. These results indicate that polyspecific antiself-reactivity of G6/17.019-reactive Ig is dependent on the somatically generated Ig third complementarity determining region. Collectively, these studies imply that selection may be responsible for the frequent expression of polyspecific autoantibodies in CLL and early B cell ontogeny.

摘要

天然自身抗体主要是免疫球蛋白M(IgM)抗体,可与多种自身抗原结合,包括自身IgG。这类多特异性自身抗体在早期B细胞库中占很大比例,据推测有助于初级体液免疫系统的稳态和/或功能。最近的研究表明,大多数慢性淋巴细胞白血病(CLL)患者的白血病细胞也表达此类IgM自身抗体。同样,许多CLL患者的白血病细胞可与针对与人IgM自身抗体相关的交叉反应性独特型(CRI)的鼠单克隆抗体(mAb)发生反应。特别是,白血病细胞常与G6(一种针对Ig重链(H链)相关CRI的mAb)和/或17.109(一种定义κ轻链(L链)相关CRI的mAb)发生反应。G6和17.109是针对IgM类风湿因子(RF)副蛋白产生的,它们各自识别许多IgM RF副蛋白中存在的主要CRI。此外,发现同时带有H链和L链相关CRI的IgM副蛋白中,超过90%也具有RF活性。对这些CRI的分子特征分析表明,每个CRI都是高度保守的Ig V基因表达的血清学标志物。因此,CLL中IgM多特异性自身抗体的频繁产生可能仅仅反映了此类高度保守的自身抗体编码Ig V基因的频繁使用,几乎没有或没有体细胞突变。为了验证这一假设,我们构建了鼠转染瘤,将SMI(一个17.109/G6反应性CLL群体)的17.109反应性κ轻链与SMI或其他G6反应性白血病细胞或扁桃体淋巴细胞的Ig H链配对。共转染编码SMI的Ig H链和L链的载体产生了能产生与人类IgG1和IgG4反应的IgMκRF自身抗体的转染瘤。与G6/17.109反应性IgMκRF瓦尔登斯特伦副蛋白不同,SMI IgMκ也与其他几种自身抗原反应,包括肌红蛋白、肌动蛋白和单链DNA。然而,将SMI轻链与编码10种不同G6反应性Ig H链中的任何一种的载体共转染,产生了能产生无明显多特异性自身抗体活性的IgMκ抗体的转染瘤。这些结果表明,G6/17.019反应性Ig的多特异性抗自身反应性取决于体细胞产生的Ig第三互补决定区。总的来说,这些研究表明选择可能是CLL和早期B细胞发育过程中多特异性自身抗体频繁表达的原因。

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