活动性系统性红斑狼疮患者中CD4+、CD25- T细胞对CD4+、CD25高表达、CD127 -/低表达调节性T细胞抑制功能的敏感性降低。

Reduced CD4+,CD25- T cell sensitivity to the suppressive function of CD4+,CD25high,CD127 -/low regulatory T cells in patients with active systemic lupus erythematosus.

作者信息

Venigalla Ram Kumar Chowdary, Tretter Theresa, Krienke Stefan, Max Regina, Eckstein Volker, Blank Norbert, Fiehn Christoph, Ho Anthony Dick, Lorenz Hanns-Martin

机构信息

University of Heidelberg, Heidelberg, Germany.

出版信息

Arthritis Rheum. 2008 Jul;58(7):2120-30. doi: 10.1002/art.23556.

DOI:10.1002/art.23556

PMID:18576316

Abstract

OBJECTIVE

CD4+,CD25high regulatory T (Treg) cells play a crucial role in the maintenance of self tolerance and prevention of organ-specific autoimmunity. The presence of many in vivo-preactivated CD4+,CD25++ T cells in patients with systemic lupus erythematosus (SLE) poses a difficulty in discriminating CD25++ activated T cells from CD25high Treg cells. To overcome this problem, we analyzed the phenotype and function of CD4+,CD25high,CD127(-/low) natural Treg (nTreg) cells isolated from the peripheral blood of patients with SLE.

METHODS

CD4+,CD25high,CD127(-/low) nTreg cells and CD4+,CD25- responder T (Tresp) cells from patients with SLE and normal donors were separated by fluorescence-activated cell sorting. Cell proliferation was quantified by 3H-thymidine incorporation, and immunophenotyping of the cells was done using FACScan.

RESULTS

Comparable percentages of CD4+,CD25high,FoxP3+ T cells were observed in patients with SLE and normal donors. Proliferation of SLE nTreg cells sorted into the subset CD4+,CD25high,CD127(-/low) was significantly decreased compared with that of SLE nTreg cells sorted into the subset CD4+,CD25high (mean +/- SEM 2,223 +/- 351 counts per minute versus 9,104 +/- 1,720 cpm, respectively), while in normal donors, these values were 802 +/- 177 cpm and 2,028 +/- 548 cpm, respectively, confirming that effector cell contamination was reduced. Notably, the suppressive activity of nTreg cells was intact in all groups. However, CD4+,CD25- Tresp cells isolated from patients with active SLE were significantly less sensitive than those from patients with inactive SLE to the suppressive function of autologous or normal donor CD4+,CD25high,CD127(-/low) nTreg cells. Furthermore, a significant inverse correlation was observed between the extent of T cell regulation in suppressor assays and the level of lupus disease activity.

CONCLUSION

This study is the first to show that, in human SLE, impaired sensitivity of Tresp cells to the suppressive effects of a comparably functional, highly purified nTreg cell population leads to a defective suppression of T cell proliferation in active SLE. Studies aiming to define the mechanisms leading to Tresp cell resistance might help in the development of highly specific, alternative immunotherapeutic tools for the control of systemic autoimmune diseases such as SLE.

摘要

目的

CD4+、CD25高表达调节性T（Treg）细胞在维持自身耐受及预防器官特异性自身免疫中起关键作用。系统性红斑狼疮（SLE）患者体内存在许多预激活的CD4+、CD25++ T细胞，这给区分CD25++激活T细胞与CD25高表达Treg细胞带来困难。为克服这一问题，我们分析了从SLE患者外周血中分离出的CD4+、CD25高表达、CD127（- /低）天然Treg（nTreg）细胞的表型和功能。

方法

通过荧光激活细胞分选法分离SLE患者及正常供者的CD4+、CD25高表达、CD127（- /低）nTreg细胞和CD4+、CD25 -反应性T（Tresp）细胞。通过3H -胸苷掺入法对细胞增殖进行定量，并使用FACScan对细胞进行免疫表型分析。

结果

SLE患者和正常供者中CD4+、CD25高表达、FoxP3+ T细胞的百分比相当。与分选到CD4+、CD25高表达亚群的SLE nTreg细胞相比，分选到CD4+、CD25高表达、CD127（- /低）亚群的SLE nTreg细胞增殖显著降低（分别为平均±标准误2,223±351次/分钟和9,104±1,720次/分钟），而在正常供者中，这些值分别为每次802±177次/分钟和2,028±548次/分钟，证实效应细胞污染减少。值得注意的是，所有组中nTreg细胞的抑制活性均保持完整。然而，从活动期SLE患者中分离出的CD4+、CD25 - Tresp细胞对自体或正常供者CD4+、CD25高表达、CD127（- /低）nTreg细胞抑制功能的敏感性明显低于非活动期SLE患者来源的细胞。此外，在抑制试验中T细胞调节程度与狼疮疾病活动水平之间观察到显著的负相关。