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系统性硬化症中循环辅助记忆T细胞的早期表型激活:与疾病活动的相关性

Early phenotypic activation of circulating helper memory T cells in scleroderma: correlation with disease activity.

作者信息

Fiocco U, Rosada M, Cozzi L, Ortolani C, De Silvestro G, Ruffatti A, Cozzi E, Gallo C, Todesco S

机构信息

Division of Rheumatology, University of Padova, Italy.

出版信息

Ann Rheum Dis. 1993 Apr;52(4):272-7. doi: 10.1136/ard.52.4.272.

Abstract

OBJECTIVES

The differential expression of several accessory/activation molecules (CD26, CD29, CD45RA, CD25, MLR4, HLA-DR) on peripheral blood CD4+ and CD8+ T lymphocytes in patients with scleroderma was compared with that in controls and patients with other connective systemic diseases to look for evidence of the involvement of T cells in the disease process of scleroderma.

METHODS

The two colour expression of surface molecules by circulating T cells was analysed with a panel of monoclonal antibodies and flow cytometry in 17 patients with scleroderma, 10 patients with systemic lupus erythematosus, and five patients with rheumatoid arthritis, and the results compared with those for 10 normal controls. The two colour T CD4+ phenotype was further compared between patients with active and quiescent disease in these patients with scleroderma. The coexpression of surface molecules by CD4+ T cells was also analysed by three colour flow cytometry in eight patients with scleroderma.

RESULTS

Patients with scleroderma showed increased CD4+CD26+ and CD4+CD25+ percentages and absolute numbers and decreased CD8+CD29+ percentages compared with controls. Moreover, a significant correlation between the higher CD4+CD26+ T cell percentage and absolute cell numbers with disease activity was observed. Most of the CD4+ peripheral blood T cells from patients with scleroderma showed the CD26+CD45RA- phenotype by three colour flow cytometry analysis.

CONCLUSIONS

The distinctive pattern of early helper memory T cell activation in these patients with rapidly evolving scleroderma supports the role of a T cell mediated mechanism in the progression of scleroderma.

摘要

目的

比较硬皮病患者外周血CD4+和CD8+T淋巴细胞上几种辅助/激活分子(CD26、CD29、CD45RA、CD25、MLR4、HLA-DR)的差异表达与对照组及其他结缔组织系统性疾病患者,以寻找T细胞参与硬皮病疾病进程的证据。

方法

用一组单克隆抗体和流式细胞术分析17例硬皮病患者、10例系统性红斑狼疮患者和5例类风湿关节炎患者循环T细胞表面分子的双色表达,并将结果与10例正常对照者的结果进行比较。在这些硬皮病患者中,还比较了活动期和静止期患者的CD4+T细胞双色表型。用三色流式细胞术分析了8例硬皮病患者CD4+T细胞表面分子的共表达情况。

结果

与对照组相比,硬皮病患者CD4+CD26+和CD4+CD25+的百分比和绝对数量增加,CD8+CD29+的百分比降低。此外,观察到较高的CD4+CD26+T细胞百分比和绝对细胞数量与疾病活动之间存在显著相关性。通过三色流式细胞术分析,硬皮病患者外周血中大多数CD4+T细胞表现为CD26+CD45RA-表型。

结论

这些快速进展的硬皮病患者早期辅助性记忆T细胞激活的独特模式支持T细胞介导机制在硬皮病进展中的作用。

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