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从沙眼衣原体蛋白质组中鉴定与HLA - B27相关疾病可能相关的HLA - B27限制性肽段。

Identification of HLA-B27-restricted peptides from the Chlamydia trachomatis proteome with possible relevance to HLA-B27-associated diseases.

作者信息

Kuon W, Holzhütter H G, Appel H, Grolms M, Kollnberger S, Traeder A, Henklein P, Weiss E, Thiel A, Lauster R, Bowness P, Radbruch A, Kloetzel P M, Sieper J

机构信息

Medical Department I, Klinikum Benjamin Franklin, Freie Universität Berlin, Berlin, Germany.

出版信息

J Immunol. 2001 Oct 15;167(8):4738-46. doi: 10.4049/jimmunol.167.8.4738.

Abstract

The association of HLA-B27 with ankylosing spondylitis and reactive arthritis is the strongest one known between an MHC class I Ag and a disease. We have searched the proteome of the bacterium Chlamydia trachomatis for HLA-B27 binding peptides that are stimulatory for CD8(+) cells both in a model of HLA-B27 transgenic mice and in patients. This was done by combining two biomathematical computer programs, the first of which predicts HLA-B27 peptide binding epitopes, and the second the probability of HLA-B27 peptide generation by the proteasome system. After preselection, immunodominant peptides were identified by Ag-specific flow cytometry. Using this approach we have identified for the first time nine peptides derived from different C. trachomatis proteins that are stimulatory for CD8(+) T cells. Eight of these nine murine-derived peptides were recognized by cytotoxic T cells. The same strategy was used to identify B27-restricted chlamydial peptides in three patients with reactive arthritis. Eleven peptides were found to be stimulatory for patient-derived CD8(+) T cells, of which eight overlapped those found in mice. Additionally, we applied the tetramer technology, showing that a B27/chlamydial peptide containing one of the chlamydial peptides stained CD8(+) T cells in patients with Chlamydia-induced arthritis. This comprehensive approach offers the possibility of clarifying the pathogenesis of B27-associated diseases.

摘要

HLA - B27与强直性脊柱炎和反应性关节炎之间的关联是已知的MHC I类抗原与疾病之间最强的关联。我们在沙眼衣原体的蛋白质组中搜索了HLA - B27结合肽,这些肽在HLA - B27转基因小鼠模型和患者体内对CD8(+)细胞均具有刺激作用。这是通过结合两个生物数学计算机程序来完成的,第一个程序预测HLA - B27肽结合表位,第二个程序预测蛋白酶体系统产生HLA - B27肽的可能性。预选后,通过抗原特异性流式细胞术鉴定免疫显性肽。使用这种方法,我们首次鉴定出了9种源自不同沙眼衣原体蛋白的对CD8(+) T细胞具有刺激作用的肽。这9种源自小鼠的肽中有8种能被细胞毒性T细胞识别。我们采用相同的策略在3例反应性关节炎患者中鉴定出B27限制性衣原体肽。发现有11种肽对患者来源的CD8(+) T细胞具有刺激作用,其中8种与在小鼠中发现的肽重叠。此外,我们应用四聚体技术,结果显示一种包含衣原体肽之一的B27/衣原体肽能使衣原体诱导的关节炎患者的CD8(+) T细胞染色。这种综合方法为阐明B27相关疾病的发病机制提供了可能性。

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