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抗原组织对狼疮自身抗体产生的影响。

Influence of antigen organization on the development of lupus autoantibodies.

作者信息

Fatenejad S, Bennett M, Moslehi J, Craft J

机构信息

Yale University School of Medicine, New Haven, Connecticut 06520-8031, USA.

出版信息

Arthritis Rheum. 1998 Apr;41(4):603-12. doi: 10.1002/1529-0131(199804)41:4<603::AID-ART7>3.0.CO;2-E.

Abstract

OBJECTIVE

To investigate the reason for grouping of antibodies against small nuclear RNP (snRNP) particles, which are major autoantigens in systemic lupus erythematosus (SLE).

METHODS

Mice were immunized with biochemically purified native snRNP particles or recombinant proteins, followed by assessment of antibody and T cell responses. Since mouse (self) snRNPs are not immunogenic in mice, a eukaryotic expression vector was constructed to induce high-level expression of the human U1 snRNP-associated A protein in murine cells. Native chimeric (mouse/human) snRNP particles were used to immunize normal mice of both H-2k and H-2b backgrounds. We also disrupted the native snRNPs by digestion with ribonuclease and used this mixture of proteins to immunize mice.

RESULTS

Immunization with native chimeric snRNPs resulted in the development of antibodies against a set of snRNP-associated proteins, a response which was accompanied by breakdown in T cell tolerance to mouse snRNPs in mice immunized with chimeric snRNPs. We also demonstrated that the ordered production of these antibodies was due to the fact that snRNP-associated proteins are grouped together in snRNP particles, since disruption of the particles resulted in development of antibodies in a random order, distinct from antibodies seen with intact particles.

CONCLUSION

Our findings directly demonstrate that the pattern of development of antibodies to native snRNPs is similar to that which is commonly observed in SLE, and that disruption of the particles results in disappearance of this ordered pattern. These results suggest that the autoimmune response to snRNPs, and possibly to other autoantigens, in lupus is a specific reaction similar to that seen in a typical immune response to foreign immunogens.

摘要

目的

研究针对小核核糖核蛋白(snRNP)颗粒抗体分组的原因,snRNP颗粒是系统性红斑狼疮(SLE)中的主要自身抗原。

方法

用生物化学方法纯化的天然snRNP颗粒或重组蛋白免疫小鼠,随后评估抗体和T细胞反应。由于小鼠(自身)snRNPs在小鼠中无免疫原性,构建了真核表达载体以诱导人U1 snRNP相关A蛋白在鼠细胞中的高水平表达。用天然嵌合(小鼠/人)snRNP颗粒免疫H-2k和H-2b背景的正常小鼠。我们还用核糖核酸酶消化破坏天然snRNPs,并使用这种蛋白质混合物免疫小鼠。

结果

用天然嵌合snRNPs免疫导致产生针对一组snRNP相关蛋白的抗体,在用嵌合snRNPs免疫的小鼠中,这种反应伴随着对小鼠snRNPs的T细胞耐受性的破坏。我们还证明,这些抗体的有序产生是由于snRNP相关蛋白在snRNP颗粒中聚集在一起,因为颗粒的破坏导致抗体以随机顺序产生,这与完整颗粒产生的抗体不同。

结论

我们的研究结果直接表明,针对天然snRNPs的抗体产生模式与SLE中常见的模式相似,并且颗粒的破坏导致这种有序模式消失。这些结果表明,狼疮中对snRNPs以及可能对其他自身抗原的自身免疫反应是一种类似于对外来免疫原的典型免疫反应的特异性反应。

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