Division of Hematopathology, Mayo Clinic, Rochester, Minnesota.
Cytometry B Clin Cytom. 2020 Jan;98(1):99-107. doi: 10.1002/cyto.b.21782. Epub 2019 Apr 11.
The diagnosis of T-cell neoplasms is often challenging, due to overlapping features with reactive T-cells and limitations of currently available T-cell clonality assays. The description of an antibody specific for one of two mutually exclusive T-cell receptor (TCR) β-chain constant regions (TRBC1) provide an opportunity to facilitate the detection of clonal TCRαβ T-cells based on TRBC-restriction.
Twenty patients with mature T-cell neoplasms and 44 patients without evidence of T-cell neoplasia were studied. Peripheral blood (51), bone marrow (10), and lymph node (3) specimens were evaluated by 9-color flow cytometry including TRBC1 (CD2/CD3/CD4/CD5/CD7/CD8/CD45/TCRγδ/TRBC1 and/or CD2/CD3/CD4/CD5/CD7/CD8/CD26/CD45/TRBC1). Monophasic TRBC1 expression on any immunophenotypically distinct CD4-positive or CD8-positive/TCRγδ-negative T-cell subset was considered indicative of clonality.
Monophasic (clonal) TRBC1 expression was identified on immunophenotypically abnormal T-cells from all 20 patients with T-cell malignancies (100% sensitivity), including 17 cases with either >97% or <3% TRBC1-positive events, and three cases with monophasic homogenous TRBC1-dim expression. All immunophenotypically distinct CD4-positive and CD8-positive/TCRγδ-negative T-cell subsets from 44 patients without T-cell malignancies showed the expected mixture of TRBC1-positive and TRBC-1-negative subpopulations (non-clonal), except for seven patients (16%) with very small CD8-positive T-cell subsets exhibiting a monophasic (clonal) pattern.
Inclusion of a single anti-TRBC1 antibody into a diagnostic T-cell flow cytometry panel facilitates the rapid identification of T-cell neoplasms, in addition to small monotypic CD8-positive subsets of uncertain significance. © 2019 International Clinical Cytometry Society.
T 细胞肿瘤的诊断常常具有挑战性,这是因为其与反应性 T 细胞具有重叠特征,并且目前可用的 T 细胞克隆性检测存在局限性。描述一种针对两个相互排斥的 T 细胞受体(TCR)β链恒定区(TRBC1)之一的抗体,为基于 TRBC 限制来检测克隆性 TCRαβ T 细胞提供了机会。
研究了 20 例成熟 T 细胞肿瘤患者和 44 例无 T 细胞肿瘤证据的患者。通过 9 色流式细胞术评估外周血(51 例)、骨髓(10 例)和淋巴结(3 例)标本,包括 TRBC1(CD2/CD3/CD4/CD5/CD7/CD8/CD45/TCRγδ/TRBC1 和/或 CD2/CD3/CD4/CD5/CD7/CD8/CD26/CD45/TRBC1)。任何免疫表型上明显不同的 CD4 阳性或 CD8 阳性/TCRγδ 阴性 T 细胞亚群上出现单相(克隆性)TRBC1 表达被认为提示克隆性。
20 例 T 细胞恶性肿瘤患者的所有免疫表型异常 T 细胞均出现单相(克隆性)TRBC1 表达(敏感性 100%),包括 17 例>97%或<3%的 TRBC1 阳性事件,以及 3 例单相同质 TRBC1 弱表达。44 例无 T 细胞恶性肿瘤患者的所有免疫表型明显不同的 CD4 阳性和 CD8 阳性/TCRγδ 阴性 T 细胞亚群均显示出预期的 TRBC1 阳性和 TRBC1-阴性亚群的混合物(非克隆性),除了 7 例(16%)非常小的 CD8 阳性 T 细胞亚群表现出单相(克隆性)模式。
在诊断性 T 细胞流式细胞术面板中加入单克隆抗-TRBC1 抗体,除了具有不确定意义的小单型 CD8 阳性亚群外,还可快速识别 T 细胞肿瘤。© 2019 年国际临床细胞化学学会。
