Complex Immunophenotypic Changes as Prognosis Panel in Chronic Lymphocytic Leukemia

Clinical Lymphoma and Myeloma Pub Date : 2009-12-01 DOI:10.3816/CLM.2009.n.099

Horia Bumbea , Sanziana Radesi , Ana-Maria Vladareanu , Viviana Roman , Anamaria Vintilescu

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Abstract

The present study proposes to asses the prognosis with consecrated markers CD38 and the new ZAP-70 related to the various patterns of CLL complex immunophenotype: cyclin D1, CD38, CD20, FMC7, CD23. This particular combination could be used as a prognosis panel in CLL.

Brief Abstract

Background

Chronic lymphocytic leukemia (CLL) has many other prognostic markers established in the past years related to disease and to the patient status, and the most important seem to now be immunophenotypical, genetic, and molecular. CD38 and ZAP-70 are now used in a strong prognosis panel of markers for CLL.

Aims

The present study proposes to assess the prognosis with consecrated markers CD38 and the new ZAP-70 related to the various patterns of CLL immunophenotype.

Patients and Methods

We have analyzed 187 patients diagnosed with CLL in order to find correlations between clinical stage, immunophenotype, and outcome.

Results

We found correlations between expression of CD38 related to clinical outcome, (dr: 0.541; P < .05.), and between ZAP-70 and CD38 (dr: 0.666; P = .018). The expression of BCL-2 was correlated to outcome (dr: 0.533; P < .01) and response to treatment (dr: 0.420; P < .01). Cyclin D1 expression was found in correlation with outcome (P = .014) and BCL-2 expression (P = .034). Lower expression CD23 was associated with poor outcome and expression of CD38 and ZAP-70 (P value < .05; dr: —0.117). We found in patients with cyclin D1 positive comparative to those cyclin D1 negative the association of high intensity CD20⁺ (28% vs. 3%), FMC7⁺ (33% vs. 8%), and lower CD23 (30%-60% vs. > 60%). Also, CD38 was positive in 44% vs. 10% and ZAP-70 in 66% versus 5%. This association defines a “lymphoma”-like immunophenotype for cyclin D1—positive cases. Treatment was chlorambucil, fludarabine/cyclophosphamide (FC), or FC + rituximab (FCR).

Conclusion

Flow cytometry is the most practical method used in CLL for diagnosis and prognosis evaluation. The immunophenotypical markers surrogate for IgVH mutation status, as CD38 and ZAP-70 have a strong correlation with outcome in CLL, and our results found that analysis by flow cytometry of both CD38 and ZAP-70 could be used in the evaluation of patients with CLL as strong prognosis markers. The complex immunophenotype in CLL could be used to define 2 main prognosis patterns: (1) cyclin D1—positive, CD38 positive, CD20 high, FMC7 positive, CD23 weak with poor prognosis; and (2) cyclin D1—negative, CD38 negative, CD20 low, FMC7 negative, CD23 high with good prognosis. These patterns have strong association with expression of ZAP-70 and could be used as prognosis assessment of patients with CLL.

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复杂免疫表型变化作为慢性淋巴细胞白血病的预后指标

本研究拟采用与CLL复合体免疫表型不同模式(cyclin D1、CD38、CD20、FMC7、CD23)相关的特异性标志物CD38和新的ZAP-70来评估预后。这种特殊的组合可以作为CLL的预后指标。摘要背景慢性淋巴细胞白血病(CLL)在过去的几年里已经建立了许多其他与疾病和患者状态相关的预后标志物，现在最重要的似乎是免疫表型，遗传和分子。CD38和ZAP-70现在被用于CLL的强预后标记。目的探讨与CLL不同免疫表型相关的特异性标志物CD38和新的ZAP-70对预后的影响。患者和方法我们分析了187例诊断为CLL的患者，以发现临床分期、免疫表型和预后之间的相关性。结果CD38表达与临床预后相关(dr: 0.541;P & lt;ZAP-70与CD38之间(dr: 0.666;P = .018)。BCL-2的表达与预后相关(dr: 0.533;P & lt;.01)和对治疗的反应(dr: 0.420;P & lt;. 01)。Cyclin D1表达与预后相关(P = 0.014)， BCL-2表达与预后相关(P = 0.034)。CD23的低表达与预后不良及CD38和ZAP-70的表达相关(P值<. 05;博士:-0.117)。我们发现，与cyclin D1阴性患者相比，cyclin D1阳性患者与高强度CD20+(28%比3%)、FMC7+(33%比8%)和低水平CD23(30%-60%比>60%)。CD38和ZAP-70的阳性率分别为44%和10%和66%和5%。这种关联定义了细胞周期蛋白d1阳性病例的“淋巴瘤”样免疫表型。治疗为氯苯、氟达拉滨/环磷酰胺(FC)或FC +利妥昔单抗(FCR)。结论流式细胞术是CLL诊断和预后评价最实用的方法。作为IgVH突变状态的免疫表型标记物，CD38和ZAP-70与CLL的预后有很强的相关性，我们的研究结果发现，流式细胞术分析CD38和ZAP-70可以作为CLL患者的强预后标记物用于评估。CLL的复杂免疫表型可定义两种主要的预后模式:(1)cyclin d1阳性、CD38阳性、CD20高、FMC7阳性、CD23弱且预后差;(2) cyclin d1阴性、CD38阴性、CD20低、FMC7阴性、CD23高，预后良好。这些模式与ZAP-70的表达有较强的相关性，可作为判断CLL患者预后的依据。

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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Clinical Lymphoma and Myeloma

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