首页> 美国卫生研究院文献>Clinical and Experimental Immunology >Detection of nucleosome–IgG immune complexes in ascites from mice transplanted with anti-DNA antibody-secreting hybridomas and in plasmas from MRL-lpr/lpr mice
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Detection of nucleosome–IgG immune complexes in ascites from mice transplanted with anti-DNA antibody-secreting hybridomas and in plasmas from MRL-lpr/lpr mice

机译:检测分泌抗DNA抗体的杂交瘤小鼠腹水和MRL-lpr / lpr小鼠血浆中核小体-IgG免疫复合物

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摘要

Autoantibodies directed against chromatin components characterize lupus diseases. Immune complexes made of these autoantibodies bound to nucleosomes released from dead cells could play some pathogenic role. The aims of this study were to investigate if nucleosome–IgG complexes could contaminate IgG anti-DNA MoAb preparations, and if such complexes circulate in lupus diseases. A new method was set up using preformed nucleosome–IgG complexes. Complexes were adsorbed onto microplate through Fc binding and nucleosomal DNA was detected by internal incorporation of labelled nucleotide. Using this method, high amounts of complexes were found in ascites from mice transplanted with anti-DNA antibody-secreting hybridomas. In some ascites, nucleosome was found to be strongly associated with the MoAb, confirming that nucleosome–IgG complexes could contaminate monoclonal autoantibody preparations. In MRL-lpr/lpr mice, nucleosome–IgG complexes were detected at 16–24 weeks of age at a time when kidney lesions are rapidly worsening, raising the question of their pathogenic significance.
机译:针对染色质成分的自身抗体是狼疮疾病的特征。由这些自身抗体制成的免疫复合物与从死细胞释放的核小体结合,可以发挥某些致病作用。这项研究的目的是研究核小体-IgG复合物是否会污染IgG抗DNA MoAb制剂,以及这种复合物是否在狼疮疾病中传播。使用预先形成的核小体-IgG复合物建立了一种新方法。通过Fc结合将复合物吸附到微板上,并通过内部掺入标记的核苷酸来检测核小体DNA。使用这种方法,在移植有抗DNA抗体分泌型杂交瘤的小鼠腹水中发现了大量的复合物。在某些腹水中,发现核小体与MoAb密切相关,这证明核小体-IgG复合物可能污染单克隆自身抗体的制备。在MRL-lpr / lpr小鼠中,当肾脏病变迅速恶化时,在16-24周龄时检测到核小体-IgG复合物,这提出了其致病意义的问题。

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