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HLA-DR 和 HLA-DQ 转基因小鼠对 Smith D 自身抗原的不同反应:HLA-DR3 转基因小鼠的优势反应伴有针对小核核糖核蛋白、双链 DNA 和核抗原自身抗体的多样化。

Differential responses to Smith D autoantigen by mice with HLA-DR and HLA-DQ transgenes: dominant responses by HLA-DR3 transgenic mice with diversification of autoantibodies to small nuclear ribonucleoprotein, double-stranded DNA, and nuclear antigens.

机构信息

Division of Rheumatology and Immunology, Department of Medicine, University of Virginia School of Medicine, Charlottesville, VA 22908, USA.

出版信息

J Immunol. 2010 Jan 15;184(2):1085-91. doi: 10.4049/jimmunol.0902670. Epub 2009 Dec 9.

Abstract

Anti-Smith (Sm) D autoantibodies are specific for systemic lupus erythematosus. In this investigation, the influence of HLA-D genes on immune responses to SmD was investigated. Mice with HLA-DR3, HLA-DR4, HLA-DQ0601, HLA-DQ0604, or HLA-DQ8 transgenes were immunized with recombinant SmD1, and their Ab responses were analyzed. Analysis by ELISA showed that all strains responded well to SmD. However, when synthetic SmD peptides were used as substrate, DR3 mice had the highest Ab response followed by DQ8, DQ0604, DQ0601, and DR4. A similar trend was observed in Western blot analysis using WEHI 7.1 cell lysate as the substrate, with the exception that DR4 mice did not generate detectable amounts of Abs. Only sera from DR3 and DQ0604 mice immunoprecipitated A-ribonucleoprotein (RNP), SmB, and SmD. Intermolecular epitope spreading to A-RNP and SmB was evident in DR3 and DQ0604 mice, as sera depleted of anti-SmD Abs were reactive with these proteins. DR3 mice also generated an immune response to C-RNP. Anti-nuclear Abs were detected in the majority of the DR3 mice, whereas moderate reactivities were seen in DQ0604 and DQ8 mice. Interestingly, only DR3 mice mounted an anti-dsDNA Ab response. Approximately half of the anti-dsDNA Abs were cross-reactive with SmD. Ab responses correlated with the strength of the T cell responses. Thus, HLA-DR3 appears to be the dominant HLA-D gene that determines the magnitude and quality of the anti-SmD immune response. In addition, our findings provide insights into the origin of the anti-dsDNA Abs often detected in patients with systemic lupus erythematosus.

摘要

抗-Smith (Sm) D 自身抗体是系统性红斑狼疮的特异性抗体。在本研究中,我们研究了 HLA-D 基因对 SmD 免疫反应的影响。用重组 SmD1 免疫 HLA-DR3、HLA-DR4、HLA-DQ0601、HLA-DQ0604 或 HLA-DQ8 转基因小鼠,并分析其 Ab 反应。ELISA 分析表明,所有品系对 SmD 均有良好的反应。然而,当使用合成 SmD 肽作为底物时,DR3 小鼠的 Ab 反应最高,其次是 DQ8、DQ0604、DQ0601 和 DR4。用 WEHI 7.1 细胞裂解物作为底物的 Western blot 分析也观察到类似的趋势,只是 DR4 小鼠未产生可检测量的 Ab。只有来自 DR3 和 DQ0604 小鼠的血清可免疫沉淀 A-核糖核蛋白 (RNP)、SmB 和 SmD。DR3 和 DQ0604 小鼠中存在分子间表位扩展至 A-RNP 和 SmB,因为耗尽抗 SmD Ab 的血清与这些蛋白反应。DR3 小鼠还对 C-RNP 产生免疫反应。在大多数 DR3 小鼠中检测到抗核 Ab,而在 DQ0604 和 DQ8 小鼠中观察到中等反应性。有趣的是,只有 DR3 小鼠产生抗 dsDNA Ab 反应。大约一半的抗 dsDNA Ab 与 SmD 交叉反应。Ab 反应与 T 细胞反应的强度相关。因此,HLA-DR3 似乎是决定抗 SmD 免疫反应强度和质量的主要 HLA-D 基因。此外,我们的研究结果为系统性红斑狼疮患者中经常检测到的抗 dsDNA Ab 的起源提供了见解。

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