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重链互补决定区3(CDR3)长度受限是狼疮易感的补体缺陷小鼠中随机分离出的6种疾病相关VH J558 + IgM自身抗体的特征。

Restricted CDR3 length of the heavy chain is characteristic of six randomly isolated disease-associated VH J558+ IgM autoantibodies in lupus prone motheaten mice.

作者信息

Lipsanen V, Walter B, Emara M, Siminovitch K, Lam J, Kaushik A

机构信息

Department of Pathobiology, University of Guelph, Ontario, Canada.

出版信息

Int Immunol. 1997 May;9(5):655-64. doi: 10.1093/intimm/9.5.655.

Abstract

To investigate the origin of disease-associated IgM autoantibodies (AAb), we compared the genetic and structural characteristics of IgM AAb from autoimmune prone motheaten (mev) mice with natural autoantibodies (NAAb) from normal background C57/BL6 strain. Six hybridoma-derived IgM molecules each were obtained both from mev mice, at the terminal stage of systemic autoimmune disease, and from mitogen-stimulated C57/BL6 mice. These were randomly selected for VH J558 gene expression (aberrantly expressed in mev mice). The variable regions of the IgM molecules, both from autoimmune and normal mice, were encoded by unmutated germline VH genes. Disease-associated AAb from mev mice were predominantly encoded by the J558 subfamily 186.2, whereas five J558 subfamilies were utilized in NAAb originating from normal mice. Junctional diversity as a result of N or P nucleotide insertions and D-D fusions was noted among IgMs originating from both mev (mostly B-1 lymphocytes) and C57BL/6 (mostly B-2 lymphocytes) mice. Interestingly, all six J558+ IgMs from mev mice showed a restricted CDR3 length of 10 amino acids, with similar hydrophobicity indices. Four unique V-D-J rearrangements were observed among these IgMs. None of the IgMs were polyreactive and three of the six were subsequently observed to express monospecific autoreactivity with synthetic peptides (residues 81-92 and 37-53) representing segments of the T cell CD4-accessory molecule. Three IgM antibodies had hydrophilic arginine residues in their CDR3 heavy chain region. By contrast, all six J558+ IgMs from C57/BL6 mice had variable CDR3 length, distinct VDJ rearrangements and a local negative charge in the CDR3 region. Four of these IgMs demonstrated polyreactivity with multiple conserved autoantigens and, hence, were classified as NAAb. These findings provide evidence for either positive or impaired negative selection of B-1 lymphocytes secreting disease-associated IgM AAb in mev mice. This likely results from a reduced threshold of responsiveness to autoantigens due to PTP1C deficiency, which is targeted at the CDR3 length of the variable region of the heavy chain. In addition, characteristic differences in the size and hydrophobicity pattern of the CDR3 of the heavy chain allow structural distinction between monospecific disease-associated IgM AAb and the polyreactive IgM NAAb.

摘要

为了研究疾病相关IgM自身抗体(AAb)的起源,我们比较了自身免疫易感的肌无力(mev)小鼠的IgM AAb与正常背景C57/BL6品系的天然自身抗体(NAAb)的遗传和结构特征。分别从处于系统性自身免疫疾病终末期的mev小鼠以及丝裂原刺激的C57/BL6小鼠中各获得了6个杂交瘤来源的IgM分子。这些分子是随机选取用于VH J558基因表达的(在mev小鼠中异常表达)。来自自身免疫小鼠和正常小鼠的IgM分子的可变区均由未突变的种系VH基因编码。来自mev小鼠的疾病相关AAb主要由J558亚家族186.2编码,而来自正常小鼠的NAAb则利用了5个J558亚家族。在源自mev小鼠(主要是B-1淋巴细胞)和C57BL/6小鼠(主要是B-2淋巴细胞)的IgM中均发现了由于N或P核苷酸插入以及D-D融合导致的连接多样性。有趣的是,来自mev小鼠的所有6个J558 + IgM均显示出受限的10个氨基酸的CDR3长度,具有相似的疏水性指数。在这些IgM中观察到4种独特的V-D-J重排。没有一种IgM具有多反应性,并且随后观察到6种中的3种与代表T细胞CD4辅助分子片段的合成肽(残基81-92和37-53)表现出单特异性自身反应性。三种IgM抗体在其CDR3重链区域具有亲水性精氨酸残基。相比之下,来自C57/BL6小鼠的所有6个J558 + IgM均具有可变的CDR3长度、独特的VDJ重排以及CDR3区域的局部负电荷。其中4种IgM与多种保守自身抗原表现出多反应性,因此被归类为NAAb。这些发现为mev小鼠中分泌疾病相关IgM AAb的B-1淋巴细胞的阳性选择或阴性选择受损提供了证据。这可能是由于PTP1C缺陷导致对自身抗原的反应阈值降低所致,该缺陷针对重链可变区的CDR3长度。此外,重链CDR3的大小和疏水性模式的特征差异使得单特异性疾病相关IgM AAb与多反应性IgM NAAb在结构上得以区分。

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