系统性红斑狼疮患者抗原呈递细胞功能缺陷

Defective antigen-presenting cell function in patients with systemic lupus erythematosus.

作者信息

Tsokos G C, Kovacs B, Sfikakis P P, Theocharis S, Vogelgesang S, Via C S

机构信息

Walter Reed Army Medical Center, Washington, DC 20307-5100, USA.

出版信息

Arthritis Rheum. 1996 Apr;39(4):600-9. doi: 10.1002/art.1780390409.

DOI:10.1002/art.1780390409

PMID:8630108

Abstract

OBJECTIVE

Patients with systemic lupus erythematosus (SLE) who exhibit defective in vitro responses to recall antigens and normal responses to alloantigens have been shown to have an abnormality in antigen-presenting cell (APC) function. This study was undertaken to further characterize this defect in APC function in lupus patients.

METHODS

Mononuclear cells (MNC) from the peripheral blood of patients with SLE and from normal individuals were cultured in the presence of either recall antigen tetanus toxoid (TT), anti-CD3 (OKT3) monoclonal antibody, or alloantigens, and proliferative or interleukin-2 responses were assessed. Cell surface expression of B7-1 was assessed by flow cytometry.

RESULTS

MNC from all normal individuals and from 7 patients with SLE responded to both TT and alloantigen and were designated +/+. Twelve SLE patients did not respond to TT but did respond to alloantigen stimulation and were designated -/+. In both normal subjects and SLE patients, the ability to respond to OKT3 correlated strongly with the ability to respond to recall antigen. A defect in APC costimulatory function was suggested by data demonstrating that interferon-gamma-induced expression of B7-1 was significantly reduced in SLE patients compared with controls. Neither controls nor SLE patients expressed detectable amounts of surface B7-1 molecule on resting APC. Defective recall and anti-CD3-stimulated responses could be enhanced in SLE patients in the presence of B7/BBl-transfected P815 murine mastocytoma cells underscoring an SLE-associated defect in costimulatory activity. However, nontransfected P815 cells were also able to enhance responses to OKT3 in -/+ patients; blocking experiments showed that this was mediated through an IgG Fc receptor-dependent mechanism.

CONCLUSION

These data indicate that SLE-associated defects in APC function in vitro can be accounted for by abnormalities in APC surface membrane molecules such as B7, IgG Fc receptors, and possibly others.

摘要

目的

系统性红斑狼疮（SLE）患者对回忆抗原的体外反应存在缺陷，但对同种异体抗原反应正常，这已表明其抗原呈递细胞（APC）功能存在异常。本研究旨在进一步明确狼疮患者APC功能的这一缺陷。

方法

将SLE患者和正常个体外周血中的单核细胞（MNC）在回忆抗原破伤风类毒素（TT）、抗CD3（OKT3）单克隆抗体或同种异体抗原存在的情况下进行培养，并评估增殖或白细胞介素-2反应。通过流式细胞术评估B7-1的细胞表面表达。

结果

所有正常个体和7例SLE患者的MNC对TT和同种异体抗原均有反应，被指定为+/+。12例SLE患者对TT无反应，但对同种异体抗原刺激有反应，被指定为-/+。在正常受试者和SLE患者中，对OKT3的反应能力与对回忆抗原的反应能力密切相关。数据表明，与对照组相比，SLE患者中干扰素-γ诱导的B7-1表达显著降低，提示APC共刺激功能存在缺陷。静止的APC上，对照组和SLE患者均未表达可检测量的表面B7-1分子。在存在B7/BBl转染的P815小鼠肥大细胞瘤细胞的情况下，SLE患者中缺陷的回忆反应和抗CD3刺激反应可得到增强，这突出了SLE相关的共刺激活性缺陷。然而，未转染的P815细胞也能够增强-/+患者对OKT3的反应；阻断实验表明，这是通过IgG Fc受体依赖性机制介导的。