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类风湿关节炎中IgA和绒毛野豌豆结合性T细胞亚群的鉴定与特征分析

Identification and characterization of IgA and Vicia villosa-binding T cell subsets in rheumatoid arthritis.

作者信息

Fortune F, Kingston J, Barnes C S, Lehner T

机构信息

Department of Immunology, United Medical School, Guy's Hospital, London, England.

出版信息

Clin Exp Immunol. 1990 Feb;79(2):202-8. doi: 10.1111/j.1365-2249.1990.tb05179.x.

Abstract

Autoimmunity may be due to augmentation of immune responses by human CD8 cells which bind the lectin Vicia villosa (VV). We have investigated T cells in rheumatoid arthritis (RA) by double immunofluorescence flow cytometry, in order to assess VV-binding CD8 and CD4 cells from the peripheral blood and synovial fluid. A significant increase in CD8+VV adherent (P less than 0.0001) and CD4+VV adherent cells (P less than 0.001) was found in synovial fluid, as compared with peripheral blood from patients with RA. A significant increase in VV-binding CD8+ or CD4+ cells was, however, not found in the blood of patients with RA, as compared with controls. We suggest that the lack of VV-binding T cells separated from blood, in contrast to those from synovial fluid, may be due to an inhibiting agent expressing N-acetyl D-galactosamine. Indeed, IgA1 is rich in N-acetyl D-galactosamine, it inhibits VV binding to T cells and is significantly bound to CD8 cells (P less than 0.001). The IgA1 was then characterized and in about half the patients J chains and secretory component was found, suggesting that the IgA1 is of the polymeric and secretory variety. IgA bound to the T cells engaged the Fc alpha receptors and a significant decrease in the Fc alpha receptors was found in CD8 cells (P less than 0.0001) and CD4 cells (P less than 0.01). Desorption studies were then carried out on CD8 and CD4 cells which showed that a loss of cell-bound IgA1 was associated with an increase in VV binding. Conversely, adsorption of IgA to T cells was associated with a loss in VV binding. The results suggest that the failure of VV binding to CD8+ and CD4+ cells from peripheral blood of patients with RA can be ascribed to cell-bound IgA1. Cytophilic IgA1 may inhibit the function of CD8+VV binding cells, thereby preventing augmentation of the systemic immune response, consistent with the lack of extra-articular disease in these patients with RA.

摘要

自身免疫可能是由于与凝集素野豌豆(VV)结合的人类CD8细胞增强了免疫反应所致。我们通过双免疫荧光流式细胞术研究了类风湿关节炎(RA)中的T细胞,以评估外周血和滑液中与VV结合的CD8和CD4细胞。与RA患者的外周血相比,滑液中CD8 + VV黏附细胞(P小于0.0001)和CD4 + VV黏附细胞(P小于0.001)显著增加。然而,与对照组相比,RA患者血液中与VV结合的CD8 +或CD4 +细胞未发现显著增加。我们认为,与滑液中的T细胞相比,从血液中分离出的缺乏与VV结合的T细胞可能是由于一种表达N - 乙酰 - D - 半乳糖胺的抑制剂所致。事实上,IgA1富含N - 乙酰 - D - 半乳糖胺,它抑制VV与T细胞的结合,并且与CD8细胞有显著结合(P小于0.001)。然后对IgA1进行了表征,在大约一半的患者中发现了J链和分泌成分,这表明IgA1是多聚体和分泌型的。与T细胞结合的IgA与Fcα受体结合,并且在CD8细胞(P小于0.0001)和CD4细胞(P小于0.01)中发现Fcα受体显著减少。然后对CD8和CD4细胞进行了解吸研究,结果表明细胞结合的IgA1的丢失与VV结合的增加有关。相反,IgA吸附到T细胞上与VV结合的减少有关。结果表明,RA患者外周血中VV与CD8 +和CD4 +细胞结合失败可归因于细胞结合的IgA1。亲细胞性IgA1可能抑制CD8 + VV结合细胞的功能,从而阻止全身免疫反应的增强,这与这些RA患者缺乏关节外疾病是一致的。

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