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T cell receptor (TCR) V gene usage in patients with systemic necrotizing vasculitis.

机译:系统性坏死性血管炎患者使用T细胞受体(TCR)V基因。

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摘要

Wegener's granulomatosis (WG) and polyarteritis nodosa (PAN) are systemic necrotizing vasculitides of unknown etiology. These disorders run a fatal course if untreated. T lymphocytes are implicated in the pathogenesis of WG, since they have been found to infiltrate affected organs, and sIL-2R correlates with disease activity. To elucidate further the role of T cells in necrotizing vasculitis, we have used a panel of 12 TCR V-specific MoAbs to investigate the number of cells expressing certain V alpha and V beta gene segments in the CD4+ and CD8+ subsets of altogether 11 patients with WG or PAN. In the group of patients, we found abnormal expansions of T cells using particular TCR V alpha or V beta gene products. These T cell expansions were more numerous, of a dramatically higher magnitude, and frequently more often found in the CD4 subset, compared with T cell expansions identified in healthy individuals. In long-term studies of the T cell expansions for up to 18 months, a heterogeneous pattern was revealed, with no obvious correlation to clinical features such as disease activity or treatment. Studies of TCR V gene usage in this group of patients may help in understanding the pathogenesis of necrotizing vasculitis, and in the identification of unknown antigens, and may open the possibility to a highly selective immunotherapy by targeting disease-mediating T cells.
机译:韦格纳肉芽肿病(WG)和结节性多发性动脉炎(PAN)是病因不明的全身性坏死性血管炎。如果不加以治疗,这些疾病会致命。 T淋巴细胞与WG的发病机制有关,因为已经发现T淋巴细胞能够浸润受影响的器官,并且sIL-2R与疾病活动相关。为了进一步阐明T细胞在坏死性血管炎中的作用,我们使用了12组TCR V特异性MoAb来研究总共11例患有CD的患者的CD4 +和CD8 +亚型中表达某些V alpha和V beta基因区段的细胞数量。 WG或PAN。在该组患者中,我们发现使用特定的TCR V alpha或V beta基因产物导致T细胞异常扩增。与健康个体中发现的T细胞扩增相比,这些T细胞扩增数量更多,数量更高,并且在CD4亚群中更为常见。在长达18个月的T细胞扩增的长期研究中,发现了一种异质模式,与诸如疾病活动或治疗等临床特征没有明显的相关性。对这组患者使用TCR V基因的研究可能有助于了解坏死性血管炎的发病机理,并鉴定未知抗原,并可能通过靶向介导疾病的T细胞为高度选择性的免疫疗法打开可能性。

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