分子生物学在人类淋巴瘤诊断中的贡献。

Diagnostic immunology Pub Date : 1986-01-01
P Vezzoni, G Cairo, M R Pozzi, L Bardella, L Schiaffonati, R Giardini, F Rilke, D Delia, I Biunno
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引用次数: 0

摘要

本文研究了25例未选择的人淋巴瘤以及正常和非肿瘤淋巴样组织中T细胞受体(TCR) β与基因免疫球蛋白重链位点的关系。将我们的印迹与Jurkat 2 (TCR β链基因特异性克隆)杂交,在由50-95% t细胞组成的非肿瘤组织中没有显示出额外的条带。相反,在6例t细胞淋巴瘤中,有6例检测到重排的条带。11例b细胞淋巴瘤未检测到TCR β基因重排,这表明免疫球蛋白重链基因的种系结构发生了改变。我们的研究结果表明,TCR β链基因重排是人类t细胞肿瘤的一个很好的标记,并补充了免疫球蛋白基因探针的分析。第8个样本没有任何重排:如文中所述,该组包括临床缓解的霍奇金病t淋巴母细胞淋巴瘤和来源不明的恶性肿瘤病例。我们的结论是,使用特异性的TCR β和IgH基因的DNA探针分析可以帮助病理学家诊断和分类人类淋巴瘤。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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The contribution of molecular biology in the diagnosis of human lymphomas.

The relationship between T cell receptor (TCR) beta and gene immunoglobulin heavy chain locus was investigated in 25 cases of unselected human lymphomas as well as in normal and non-neoplastic lymphoid tissues. Hybridizing our blots with Jurkat 2, a clone specific for the beta chain gene of TCR, did not demonstrate extra bands in non-neoplastic tissues composed of 50-95% T-cells. On the contrary, rearranged bands were detected in six out of six cases of T-cell lymphomas. No TCR beta gene rearrangements were detected in 11 B-cell lymphomas, which in turn presented modification of the immunoglobulin heavy chain gene germline configuration. Our results suggest that TCR beta chain gene rearrangements are a good marker for human T-cell neoplasias in humans and complement the analysis with immunoglobulin genes probes. Eighth samples were devoid of any rearrangements: this group comprises cases of Hodgkin's disease T-lymphoblastic lymphomas in clinical remission and malignancies of unknown origin, as discussed in the text. We conclude that the analysis using DNA probes specific for TCR beta and IgH genes can be of aid to the pathologist in the diagnosis and classification of human lymphomas.

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