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微结节型胸腺瘤:一种上皮性肿瘤,具有异常趋化因子表达,为淋巴瘤的发展奠定基础。

Micronodular thymoma: an epithelial tumour with abnormal chemokine expression setting the stage for lymphoma development.

作者信息

Ströbel Philipp, Marino Mirella, Feuchtenberger Martin, Rouzière Anne-Sophie, Tony Hans Peter, Wulbrand Ulrich, Förster Reinhold, Zettl Andreas, Lee Harris Nancy, Kreipe Hans, Laeng R Hubert, Müller-Hermelink Hans Konrad, Marx Alexander

机构信息

Institute of Pathology, University of Würzburg, Germany.

出版信息

J Pathol. 2005 Sep;207(1):72-82. doi: 10.1002/path.1808.

DOI:10.1002/path.1808
PMID:15965907
Abstract

The aetiology of primary B-cell lymphomas of the thymus is enigmatic. Although thymic follicular lymphoid hyperplasia (TFH) is commonly associated with myasthenia gravis (MG), lymphoma is not a complication of this condition. The present paper reports a high frequency of monoclonal B-cell populations (6 of 18 cases; 33%) in micronodular thymoma (MNT), a peculiar thymic epithelial neoplasm with a B-cell-rich stroma, while B cells were consistently polyclonal in TFH (25 cases) and other types of thymomas (15 cases) (p < 0.001). An intratumoural lymphoma could be identified in three of the six monoclonal MNTs. Sequencing of the monoclonal IgH chain revealed partially overlapping VDJ gene usage in MNT and thymic mucosa-associated lymphoid tissue (MALT) lymphomas. The neoplastic epithelium of MNTs, but not of TFH and other types of thymoma, expressed high levels of dendritic cell, T-cell, and B-cell chemoattractants, such as CCL18, CCR6, and CCL20. It is concluded that abnormal chemokine expression in an epithelial tumour, MNT, can promote the recruitment of MALT, the emergence of monoclonal B cells, and, eventually, the subsequent development of mediastinal lymphomas. More generally, the concept that expression of a 'high-risk' spectrum of chemokines due to local or genetic factors may interfere with B-cell homeostasis and may contribute to MALT lymphoma development in chronic inflammatory states is proposed.

摘要

胸腺原发性B细胞淋巴瘤的病因尚不清楚。虽然胸腺滤泡性淋巴样增生(TFH)通常与重症肌无力(MG)相关,但淋巴瘤并非此病的并发症。本文报告了微结节性胸腺瘤(MNT)中高频出现单克隆B细胞群体(18例中有6例;33%),MNT是一种特殊的胸腺上皮肿瘤,其基质富含B细胞,而TFH(25例)和其他类型胸腺瘤(15例)中的B细胞始终为多克隆性(p<0.001)。在6例单克隆MNT中有3例可识别出肿瘤内淋巴瘤。单克隆IgH链测序显示MNT和胸腺黏膜相关淋巴组织(MALT)淋巴瘤中VDJ基因使用存在部分重叠。MNT的肿瘤上皮而非TFH和其他类型胸腺瘤的肿瘤上皮表达高水平的树突状细胞、T细胞和B细胞趋化因子,如CCL18、CCR6和CCL20。结论是上皮性肿瘤MNT中异常的趋化因子表达可促进MALT的募集、单克隆B细胞的出现,并最终导致纵隔淋巴瘤的后续发展。更一般地说,提出了由于局部或遗传因素导致“高危”趋化因子谱表达可能干扰B细胞稳态并可能在慢性炎症状态下促进MALT淋巴瘤发生的概念。

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