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从显微操作的单细胞中扩增TCRβ基因重排:霍奇金病中围绕霍奇金和里德-斯腾伯格细胞形成玫瑰花结的T细胞是多克隆的。

Amplification of TCRbeta gene rearrangements from micromanipulated single cells: T cells rosetting around Hodgkin and Reed-Sternberg cells in Hodgkin's disease are polyclonal.

作者信息

Roers A, Montesinos-Rongen M, Hansmann M L, Rajewsky K, Küppers R

机构信息

Institute for Genetics, University of Cologne, Germany.

出版信息

Eur J Immunol. 1998 Aug;28(8):2424-31. doi: 10.1002/(SICI)1521-4141(199808)28:08<2424::AID-IMMU2424>3.0.CO;2-R.

Abstract

Despite accounting for only a minor fraction of all cells in Hodgkin's lymphoma tissue, the Hodgkin and Reed-Sternberg (HRS) cells represent the malignant tumor cell clone in Hodgkin's disease (HD). By far the most abundant cell type in the tumor tissue are CD4+ T cells. Some of them intimately associate with HRS cells forming rosettes around them. This study addresses the question whether the rosetting phenomenon reflects a specific interaction between T and HRS cells by asking whether the rosettes are composed of T cells expressing a restricted TCR repertoire. Single rosetting T cells were micromanipulated from frozen sections of tumor tissue in two cases of nodular sclerosing HD and one case of lymphocyte predominant HD. TCR Vbeta gene rearrangements were amplified from these single cells by PCR. Of 83 potentially functional Vbeta gene rearrangements obtained altogether from the three cases, 81 were found to be clonally unrelated. Furthermore, they did not show signs of selection of the receptor chains for recognition of common epitopes: The usage of Vbeta and Jbeta gene segments as well as the distribution of complementarity-determining region (CDR) 3 lengths was similar to what was seen in a collection of 60 Vbeta gene rearrangements from blood of healthy donors and no recurrent CDR3 amino acid motifs were found. These data suggest that the HRS cells attract CD4+ T cells nonspecifically.

摘要

尽管霍奇金淋巴瘤组织中的霍奇金和里德-斯腾伯格(HRS)细胞仅占所有细胞的一小部分,但它们代表了霍奇金病(HD)中的恶性肿瘤细胞克隆。肿瘤组织中迄今为止最丰富的细胞类型是CD4 + T细胞。其中一些细胞与HRS细胞紧密结合,在其周围形成玫瑰花结。本研究通过询问玫瑰花结是否由表达受限TCR库的T细胞组成,来探讨玫瑰花结现象是否反映了T细胞与HRS细胞之间的特异性相互作用。从两例结节硬化型HD和一例淋巴细胞为主型HD的肿瘤组织冰冻切片中,通过显微操作分离出单个形成玫瑰花结的T细胞。通过PCR从这些单个细胞中扩增TCR Vβ基因重排。从这三例中总共获得的83个潜在功能性Vβ基因重排中,发现81个在克隆上不相关。此外,它们没有显示出为识别共同表位而选择受体链的迹象:Vβ和Jβ基因片段的使用以及互补决定区(CDR)3长度的分布与从健康供体血液中收集的60个Vβ基因重排中所见相似,并且未发现重复的CDR3氨基酸基序。这些数据表明,HRS细胞非特异性地吸引CD4 + T细胞。

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