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胸腺瘤改变血液中的T细胞亚群组成:胸腺瘤相关自身免疫性疾病的一种潜在机制。

Thymomas alter the T-cell subset composition in the blood: a potential mechanism for thymoma-associated autoimmune disease.

作者信息

Hoffacker V, Schultz A, Tiesinga J J, Gold R, Schalke B, Nix W, Kiefer R, Müller-Hermelink H K, Marx A

机构信息

Institute of Pathology, University of Würzburg, Würzburg, Germany.

出版信息

Blood. 2000 Dec 1;96(12):3872-9.

PMID:11090072
Abstract

Thymomas are the only tumors that are proven to generate mature T cells from immature precursors. It is unknown, however, whether intratumorous thymopoiesis has an impact on the peripheral T-cell pool and might thus be related to the high frequency of thymoma-associated myasthenia gravis. This study shows, using fluorescence-activated cell sorting-based analyses and T-cell proliferation assays, that thymopoiesis and T-cell function in thymomas correspond with immunologic alterations in the blood. Specifically, the proportion of circulating CD45RA(+)CD8(+) T cells is significantly increased in patients with thymoma compared with normal controls, in accordance with intratumorous T-cell development that is abnormally skewed toward the CD8(+) phenotype. Moreover, it is primarily the proportion of circulating CD45RA(+)CD8(+) T cells that decreases after thymectomy. The results also demonstrate that T cells reactive toward recombinant autoantigens are distributed equally between thymomas and blood, whereas T-cell responses to foreign antigen (ie, tetanus toxoid) are seen only among circulating T cells and not among thymoma-derived T cells. These functional studies support the hypothesis that thymopoiesis occurring within thymomas alters the peripheral T-cell repertoire. Because many thymomas are enriched with autoantigen-specific T cells, a disturbance of circulating T-cell subset composition by export of intratumorous T cells may contribute to paraneoplastic autoimmune disease arising in patients with thymoma. (Blood. 2000;96:3872-3879)

摘要

胸腺瘤是唯一被证实在体内能从未成熟前体细胞生成成熟T细胞的肿瘤。然而,瘤内胸腺生成是否会对外周T细胞库产生影响,进而可能与胸腺瘤相关重症肌无力的高发病率有关,目前尚不清楚。本研究通过基于荧光激活细胞分选的分析和T细胞增殖试验表明,胸腺瘤中的胸腺生成和T细胞功能与血液中的免疫改变相对应。具体而言,与正常对照组相比,胸腺瘤患者循环中CD45RA(+)CD8(+)T细胞的比例显著增加,这与瘤内T细胞发育异常偏向CD8(+)表型一致。此外,胸腺切除术后主要是循环中CD45RA(+)CD8(+)T细胞的比例下降。结果还表明,对重组自身抗原产生反应的T细胞在胸腺瘤和血液中分布均匀,而对外源抗原(即破伤风类毒素)的T细胞反应仅见于循环T细胞,而不见于胸腺瘤来源的T细胞。这些功能研究支持了这样一种假说,即胸腺瘤内发生的胸腺生成会改变外周T细胞库。由于许多胸腺瘤富含自身抗原特异性T细胞,瘤内T细胞输出导致的循环T细胞亚群组成紊乱可能促成胸腺瘤患者发生副肿瘤性自身免疫疾病。(《血液》。2000年;96:3872 - 3879)

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