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一种携带独特型D23的多特异性鼠抗DNA单克隆抗体形成肾小球免疫沉积物。天然自身抗体的致病作用?

An idiotype D23-bearing polyspecific, murine anti-DNA monoclonal antibody forms glomerular immune deposits. Pathogenic role of natural autoantibodies?

作者信息

Gilbert D, Brard F, Margaritte C, Delpech A, Tron F

机构信息

Pathologie Lymphocytaire et Génétique Moléculaire (Institut Fédératif de Recherche Multidisciplinaire sur les Peptides), Faculté de Medécine et de Pharmacie and CHU Charles Nicolle, Rouen, France.

出版信息

Mol Immunol. 1995 May;32(7):477-86. doi: 10.1016/0161-5890(95)00003-w.

Abstract

Identification of the immunochemical and structural properties of pathogenic anti-DNA antibodies is a major goal for understanding their origins and the mechanisms whereby they induce tissue lesions. Herein, we report on the production of an IgG2a,k anti-DNA monoclonal antibody (4B1), derived from a 12-month-old (NZB x NZW)F1 lupus mouse, able to form glomerular immune deposits. mAb 4B1 is a polyspecific antibody able to bind to ssDNA, actin, tubulin, cardiolipin and to laminin as shown by solid phase ELISAs. Indirect immunofluorescence labeling of HEp-2 cells gave a cytoplasmic staining pattern similar to that obtained with anti-cytoskeleton antibodies. Western blot analysis demonstrated that mAb 4B1 bore idiotype D23, previously shown to be characteristic of natural antibodies derived from normal mice. After injecting the 4B1-secreting hybridoma intraperitoneally into normal (NZW x BALB/c)F1 mice, glomerular immune deposits were observed along the capillary wall. These deposits contained mainly IgM, IgG2a and mAb 4B1, as demonstrated by direct immunofluorescence using a biotinylated-rat anti-4B1 idiotype mAb and kidney eluate analysis. Nucleotide sequence analysis of the VH and VL genes showed that mAb 4B1 is encoded by VH Q52, DSP2.9 and JH2 genes with minimal mutations and by VK8 very similar to the canonic D23 light chain, and JK1 germline genes. No arginine residues were observed in the VH CDR and both chains lacked N-segment addition. Thus, no structural characteristics deduced from the primary structure of mAb 4B1 could explain its pathogenic potential. However, the immunochemical and structural properties suggest that autoantibodies closely related to natural autoantibodies may be pathogenic.

摘要

鉴定致病性抗DNA抗体的免疫化学和结构特性是理解其起源以及它们诱导组织损伤机制的主要目标。在此,我们报告了一种源自12月龄(NZB×NZW)F1狼疮小鼠的IgG2a,k抗DNA单克隆抗体(4B1)的产生,该抗体能够形成肾小球免疫沉积物。如固相ELISA所示,单克隆抗体4B1是一种多特异性抗体,能够结合单链DNA、肌动蛋白、微管蛋白、心磷脂和层粘连蛋白。对HEp-2细胞进行间接免疫荧光标记得到的细胞质染色模式与用抗细胞骨架抗体得到的模式相似。蛋白质印迹分析表明,单克隆抗体4B1具有独特型D23,先前已证明其是源自正常小鼠的天然抗体的特征。将分泌4B1的杂交瘤腹腔注射到正常(NZW×BALB/c)F1小鼠中后,沿毛细血管壁观察到肾小球免疫沉积物。如使用生物素化大鼠抗4B1独特型单克隆抗体的直接免疫荧光和肾脏洗脱液分析所示,这些沉积物主要包含IgM型、IgG2a型和单克隆抗体4B1。VH和VL基因的核苷酸序列分析表明,单克隆抗体4B1由具有最小突变的VH Q52、DSP2.9和JH2基因以及与典型D23轻链非常相似的VK8和JK1种系基因编码。在VH互补决定区未观察到精氨酸残基,并且两条链均缺乏N段添加。因此,从单克隆抗体4B1的一级结构推导的结构特征无法解释其致病潜力。然而,免疫化学和结构特性表明,与天然自身抗体密切相关的自身抗体可能具有致病性。

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