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在系统性红斑狼疮患者的循环免疫复合物中,与 RNA 相关的自身抗体比抗 dsDNA 抗体更丰富。

Autoantibodies associated with RNA are more enriched than anti-dsDNA antibodies in circulating immune complexes in SLE.

机构信息

Department of Immunology, Genetics and Pathology, Rudbeck Laboratory, Uppsala University, Uppsala, Sweden.

出版信息

Lupus. 2012 May;21(6):586-95. doi: 10.1177/0961203311434938. Epub 2012 Feb 2.

Abstract

To what extent different autoantibodies accumulate in systemic lupus erythematosus (SLE) immune complexes (ICs), and whether such accumulation is associated with disease activity has been investigated. ICs were isolated from SLE sera by both polyethylene glycol (PEG) precipitation and C1q-binding. Autoantibody specificities were determined using a lineblot assay quantified by densitometry. To compare the relative levels of autoantibodies, levels were normalized to the total levels of IgG measured by ELISA in sera and parallel ICs. Samples were investigated both in a cross-sectional design as well as in a paired design with samples obtained during both active and inactive SLE. All investigated autoantibody specificities except anti-dsDNA were enriched in circulating ICs as compared with parallel sera. The group of antibodies against RNA-associated antigens (anti-RNP/Sm, anti-Sm, anti-SSA/Ro60, anti-SSA/Ro52, anti-SSB/La) all exhibited higher median enrichment than the DNA-associated (anti-dsDNA, anti-histones, anti-nucleosomes) or cytoplasmic (anti-ribosomal P) antigens. In particular autoantibodies against RNP/Sm and SSA/Ro52 had the highest degree of enrichment in SLE PEG precipitates. These findings were corroborated by analysis of autoantibody content in C1q-bound ICs. There was no difference in degree of IC accumulation of the investigated autoantibodies during active and inactive SLE. Our findings demonstrate a difference in enrichment between autoantibodies against RNA- and DNA-associated autoantigens in isolated SLE IC, suggesting that the RNA-associated autoantibodies are more prone to form circulating ICs in SLE, in contrast to antibodies against DNA-associated autoantigens such as dsDNA. These finding have implications in understanding mechanisms of differential autoantibody accumulation in target organs in SLE.

摘要

已经研究了系统性红斑狼疮 (SLE) 免疫复合物 (IC) 中不同自身抗体的积累程度,以及这种积累是否与疾病活动度相关。通过聚乙二醇 (PEG) 沉淀和 C1q 结合从 SLE 血清中分离 IC。使用线印迹分析通过密度计定量确定自身抗体特异性。为了比较自身抗体的相对水平,将水平标准化为通过 ELISA 在血清和平行 IC 中测量的 IgG 的总水平。使用横断面设计和具有在 SLE 活动期和非活动期获得的样品的配对设计来研究样品。与平行血清相比,除抗 dsDNA 外,所有研究的自身抗体特异性均在循环 IC 中富集。针对 RNA 相关抗原的抗体组(抗 RNP/Sm、抗 Sm、抗 SSA/Ro60、抗 SSA/Ro52、抗 SSB/La)的中位富集程度均高于 DNA 相关(抗 dsDNA、抗组蛋白、抗核小体)或细胞质(抗核糖体 P)抗原。特别是针对 RNP/Sm 和 SSA/Ro52 的自身抗体在 SLE PEG 沉淀中具有最高的富集度。通过分析 C1q 结合的 IC 中的自身抗体含量证实了这些发现。在 SLE 活动期和非活动期,研究的自身抗体在 IC 中的积累程度没有差异。我们的发现表明,在分离的 SLE IC 中,针对 RNA 和 DNA 相关自身抗原的自身抗体的富集程度存在差异,这表明与 dsDNA 等针对 DNA 相关自身抗原的抗体相比,针对 RNA 相关自身抗原的抗体更容易在 SLE 中形成循环 IC。这些发现对理解 SLE 中靶器官中差异自身抗体积累的机制具有影响。

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