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抗 RNP 抗体与干扰素基因特征相关,但与 SLE 中的补体水平降低无关。

Anti-RNP antibodies are associated with the interferon gene signature but not decreased complement levels in SLE.

机构信息

AMPEL BioSolutions LLC, Charlottesville, Virginia, USA.

RILITE Foundation, Charlottesville, Virginia, USA.

出版信息

Ann Rheum Dis. 2022 May;81(5):632-643. doi: 10.1136/annrheumdis-2021-221662. Epub 2022 Feb 3.

Abstract

OBJECTIVES

The goals of these studies were to elucidate the inter-relationships of specific anti-nuclear antibody (ANA), complement, and the interferon gene signature (IGS) in the pathogenesis of systemic lupus erythematosus (SLE).

METHODS

Data from the Illuminate trials were analysed for antibodies to dsDNA as well as RNA-binding proteins (RBP), levels of C3, C4 and various IGS. Statistical hypothesis testing, linear regression analyses and classification and regression trees analysis were employed to assess relationships between the laboratory features of SLE.

RESULTS

Inter-relationships of ANAs, complement and the IGS differed between patients of African Ancestry (AA) and European Ancestry (EA); anti-RNP and multiple autoantibodies were more common in AA patients and, although both related to the presence of the IGS, relationships between autoantibodies and complement differed. Whereas, anti-dsDNA had an inverse relationship to C3 and C4, levels of anti-RNP were not related to these markers. The IGS was only correlated with anti-dsDNA in EA SLE and complement was more correlated to the IGS in AA SLE. Finally, autoantibodies occurred in the presence and absence of the IGS, whereas the IGS was infrequent in anti-dsDNA/anti-RBP-negative SLE patients.

CONCLUSION

There is a complex relationship between autoantibodies and the IGS, with anti-RNP associated in AA and both anti-dsDNA and RNP associated in EA. Moreover, there was a difference in the relationship between anti-dsDNA, but not anti-RBP, with complement levels. The lack of a relationship of anti-RNP with C3 and C4 suggests that anti-RNP immune complexes (ICs) may drive the IGS without complement fixation, whereas anti-dsDNA ICs involve complement consumption.

摘要

目的

本研究旨在阐明抗核抗体(ANA)、补体和干扰素基因特征(IGS)在系统性红斑狼疮(SLE)发病机制中的相互关系。

方法

对 Illuminate 试验的数据进行分析,以评估 dsDNA 抗体以及 RNA 结合蛋白(RBP)、C3、C4 和各种 IGS 的水平。采用统计假设检验、线性回归分析以及分类和回归树分析来评估 SLE 实验室特征之间的关系。

结果

ANA、补体和 IGS 之间的相互关系在非裔美国人群(AA)和欧洲裔美国人(EA)中存在差异;抗 RNP 和多种自身抗体在 AA 患者中更为常见,尽管它们都与 IGS 的存在相关,但自身抗体与补体之间的关系不同。虽然抗 dsDNA 与 C3 和 C4 呈负相关,但抗 RNP 水平与这些标志物无关。IGS 仅与 EA 中的抗 dsDNA 相关,而补体与 AA 中的 IGS 更为相关。最后,自身抗体在 IGS 存在或缺失的情况下均会出现,而 IGS 在抗 dsDNA/抗 RBP 阴性的 SLE 患者中并不常见。

结论

自身抗体和 IGS 之间存在复杂的关系,抗 RNP 在 AA 中相关,而抗 dsDNA 和 RNP 在 EA 中均相关。此外,抗 dsDNA 与补体水平之间的关系存在差异,但抗 RBP 则不然。抗 RNP 与 C3 和 C4 之间缺乏关系表明,抗 RNP 免疫复合物(ICs)可能在不固定补体的情况下驱动 IGS,而抗 dsDNA ICs 则涉及补体消耗。

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