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弥漫性大细胞淋巴瘤免疫表型的临床相关性

Clinical relevance of immunologic phenotype in diffuse large cell lymphoma.

作者信息

Horning S J, Doggett R S, Warnke R A, Dorfman R F, Cox R S, Levy R

出版信息

Blood. 1984 May;63(5):1209-15.

PMID:6370335
Abstract

The immunologic phenotypes of 78 diffuse large cell lymphomas were determined by an immunoperoxidase technique using a panel of monoclonal antibodies. The phenotypes were correlated with clinical and morphological parameters by univariate and multivariate analysis. Forty-one lymphomas (53%) expressed immunoglobulin (Ig+). Of the 37 cases that did not express immunoglobulin (Ig-), 9 expressed T cell antigens. Although the T cell phenotypes were antigenically heterogeneous, all cases represented mature T cell phenotypes. The majority of the remaining 28 cases expressed the B cell-associated antigen, B1. At 5 yr, actuarial survival for the Ig- patients was 63%, compared with 15% for the Ig+ patients. A significantly greater proportion of patients with Ig+ lymphomas were over the age of 65 at diagnosis. All of the 9 patients with marrow involvement were Ig+. Multiple factors were analyzed by the Cox regression procedure for their impact on survival, including antigenic profile, histologic grade, morphological classification, and numerous clinical parameters previously recognized to be of prognostic significance. In this analysis, stage, age greater than 65 yr, systemic symptoms, and marrow involvement had the greatest influence on survival. The survival difference between Ig- and Ig+ patients is explained by a higher proportion of Ig+ patients with these unfavorable prognostic factors. With our current immunologic methods, retrospective cell phenotyping analysis has not provided independent prognostic significance in diffuse large cell lymphoma. A prospective evaluation of similarly treated patients is needed to characterize the influence of phenotype fully and to determine its potential usefulness for therapy.

摘要

采用一组单克隆抗体,通过免疫过氧化物酶技术确定了78例弥漫性大细胞淋巴瘤的免疫表型。通过单变量和多变量分析,将这些表型与临床和形态学参数进行关联。41例淋巴瘤(53%)表达免疫球蛋白(Ig+)。在37例不表达免疫球蛋白的病例(Ig-)中,9例表达T细胞抗原。尽管T细胞表型在抗原方面具有异质性,但所有病例均代表成熟T细胞表型。其余28例中的大多数表达B细胞相关抗原B1。5年时,Ig-患者的精算生存率为63%,而Ig+患者为15%。Ig+淋巴瘤患者在诊断时年龄超过65岁的比例明显更高。所有9例有骨髓受累的患者均为Ig+。通过Cox回归程序分析了多种因素对生存的影响,包括抗原谱、组织学分级、形态学分类以及众多先前被认为具有预后意义的临床参数。在该分析中,分期、年龄大于65岁、全身症状和骨髓受累对生存影响最大。Ig-和Ig+患者之间的生存差异是由于Ig+患者中这些不良预后因素的比例较高。使用我们目前的免疫方法,回顾性细胞表型分析在弥漫性大细胞淋巴瘤中尚未提供独立的预后意义。需要对接受类似治疗的患者进行前瞻性评估,以充分描述表型的影响并确定其对治疗的潜在用途。

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