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通过细胞因子分泌流式细胞术鉴定耶尔森菌诱导的反应性关节炎患者中的免疫显性CD4 + T细胞表位。

Identification of immunodominant CD4+ T cell epitopes in patients with Yersinia-induced reactive arthritis by cytometric cytokine secretion assay.

作者信息

Thiel Andreas, Wu Peihua, Lanowska Malgorzata, Dong Jun, Radbruch Andreas, Sieper Joachim

机构信息

Deutsches Rheuma-Forschungszentrum, Berlin, Germany.

出版信息

Arthritis Rheum. 2006 Nov;54(11):3583-90. doi: 10.1002/art.22183.

DOI:10.1002/art.22183
PMID:17075864
Abstract

OBJECTIVE

In reactive arthritis (ReA), a bacteria-specific T cell response to the triggering microbe is detected in synovial fluid. So far, direct characterization of bacteria-specific T cells and identification of the immunodominant fine specificities remain difficult due to the lack of appropriate techniques. The aim of the present study was to directly determine the fine specificity of CD4+ T cells specific to ReA-associated bacteria-derived protein.

METHODS

In 2 patients with Yersinia-induced ReA, live Yersinia Hsp60-specific CD4+ T cells were directly isolated from synovial fluid after stimulation with Yersinia-derived protein Hsp60 using a cytometric cytokine secretion assay. Generated short-term T cell lines were then tested in vitro for their peptide epitope specificity. Also, direct cross-reactivity of one line with Chlamydia- and human-derived Hsp60 was assessed.

RESULTS

Generated short-term CD4+ T cell lines were highly antigen-specific and revealed single immunodominant peptide epitopes that were confirmed by direct testing with single peptides in both peripheral blood and synovial fluid cells. Yersinia Hsp60-specific T cells of one patient cross-reacted directly with human Hsp60.

CONCLUSION

Our results demonstrate the feasibility of direct assessment of live, potentially pathogenic, antigen-specific interferon-gamma+ CD4+ T cells taken from inflammatory lesions of patients with rheumatic diseases such as ReA. This might have implications not only regarding pathogenesis, but also in the design of new immunotherapies.

摘要

目的

在反应性关节炎(ReA)中,在滑液中检测到针对引发微生物的细菌特异性T细胞反应。到目前为止,由于缺乏合适的技术,对细菌特异性T细胞进行直接表征以及鉴定免疫显性精细特异性仍然很困难。本研究的目的是直接确定ReA相关细菌衍生蛋白特异性CD4 + T细胞的精细特异性。

方法

在2例耶尔森菌诱导的ReA患者中,使用细胞因子分泌流式细胞术检测法,在用耶尔森菌衍生蛋白Hsp60刺激后,直接从滑液中分离出活的耶尔森菌热休克蛋白60(Hsp60)特异性CD4 + T细胞。然后在体外测试所产生的短期T细胞系的肽表位特异性。此外,评估了其中一个细胞系与衣原体和人源Hsp60的直接交叉反应性。

结果

所产生的短期CD4 + T细胞系具有高度抗原特异性,并揭示了单一免疫显性肽表位,这通过在外周血和滑液细胞中用单一肽进行直接测试得到证实。一名患者的耶尔森菌Hsp60特异性T细胞与人Hsp60直接发生交叉反应。

结论

我们的结果证明了直接评估取自ReA等风湿性疾病患者炎症病变的活的、潜在致病性的、抗原特异性干扰素-γ+ CD4 + T细胞具有可行性。这不仅可能对发病机制有影响,而且对新免疫疗法的设计也有影响。

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