Phenotypic analysis of peripheral T cell lymphoma among the Japanese.

S Nakamura, T Koshikawa, K Koike, K Kitoh, H Suzuki, A Oyama, T Motoori, M Kojima, M Ogura, S Kurita
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引用次数: 45

Abstract

From 1980 to 1990, 174 peripheral T cell lymphomas were studied morphologically and immunophenotypically with a panel of monoclonal antibodies which were reactive with T cell differentiation antigens in cryostat sections and/or cell suspensions. Histologically, 57% of the lymphomas were categorized into low-grade tumors according to the updated Kiel classification, while 41% were high-grade tumors. By immunologic studies, 50% of the lymphomas were of helper/inducer (CD4) phenotype, 6% were of cytotoxic/suppressor (CD8) phenotype, 3% expressed both CD4 and CD8, 3% lacked both CD4 and CD8, and 36% were phenotypically undetermined because of an admixture of a fairly even number of CD4 and CD8-positive cells. The phenotypically undetermined cases were more frequently noted in the low-grade groups than in the high-grade group, and the latter often showed a loss of pan-T antigens, although there was no definite correlation between the histologic category and the immunophenotype. CD25, which is strongly manifested in anti-HTLV-1 antibody-positive cases, was negative or only weakly expressed in anti-HTLV-1 antibody-negative cases. Anaplastic large cell lymphomas (LC-Ana) strongly expressed CD30, which was also detectable in only large blast-like cells in the low-grade tumors. Seventy-one per cent of the lymphomas expressed Ia antigens. In this series, the clinical data were available on 154 patients. For individual markers, the expression of CD30 and HLA-DR were associated with a longer actuarial survival (P < 0.01 and P < 0.05 by the generalized Wilcoxon test). The absence of CD25 or the presence of CD3 on tumor cells correlated with a relatively favorable prognosis, but not significantly. The detection of CD4 and CD8 had relatively little prognostic value. In the cases excluding LC-Ana, a significant difference was also recognized between the groups with and without CD25, CD30 and HLA-DR (P < 0.05 by the generalized Wilcoxon test). These results suggest that the immunophenotypic analysis of peripheral T cell lymphoma provided its use as an adjunct to a histopathologic diagnosis and was related to prognostic prediction.

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日本人外周血T细胞淋巴瘤的表型分析。
从1980年到1990年,用一组单克隆抗体对174例外周血T细胞淋巴瘤进行了形态学和免疫表型研究,这些单克隆抗体在低温切片和/或细胞悬液中与T细胞分化抗原反应。组织学上,根据最新的Kiel分级,57%的淋巴瘤被分类为低级别肿瘤,41%的淋巴瘤被分类为高级别肿瘤。通过免疫学研究,50%的淋巴瘤为辅助/诱导剂(CD4)表型,6%为细胞毒性/抑制因子(CD8)表型,3%既表达CD4又表达CD8, 3%既缺乏CD4又缺乏CD8, 36%的淋巴瘤由于CD4和CD8阳性细胞的混合数量相当均匀而表型不确定。表型不确定的病例在低级别组中比在高级别组中更常见,后者通常表现为泛t抗原的缺失,尽管组织学分类与免疫表型之间没有明确的相关性。CD25在抗htlv -1抗体阳性的病例中表现强烈,而在抗htlv -1抗体阴性的病例中表现为阴性或仅弱表达。间变性大细胞淋巴瘤(LC-Ana)强烈表达CD30,也仅在低级别肿瘤的大胚样细胞中检测到。71%的淋巴瘤表达Ia抗原。在这个系列中,有154例患者的临床资料。对于单个标记物,CD30和HLA-DR的表达与更长的精算生存相关(广义Wilcoxon检验P < 0.01和P < 0.05)。肿瘤细胞上CD25缺失或CD3存在与相对有利的预后相关,但不显著。CD4和CD8检测的预后价值相对较小。在排除LC-Ana的病例中,有CD25、CD30和HLA-DR组与无CD25、CD30组之间也存在显著差异(经广义Wilcoxon检验P < 0.05)。这些结果表明,外周T细胞淋巴瘤的免疫表型分析可以作为组织病理学诊断的辅助手段,并与预后预测有关。
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