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预测 Binet 分期 A 期慢性淋巴细胞白血病的分期进展。

Predicting Stage Progression in Binet Stage a Chronic Lymphocytic Leukemia.

机构信息

Department of Medicine, Kuwait University, State of Kuwait, Kuwait.

Department of Hematology, Kuwait Cancer Center, State of Kuwait, Kuwait.

出版信息

Hematol Oncol Stem Cell Ther. 2024 Mar 22;17(2):137-145. doi: 10.56875/2589-0646.1117.

Abstract

INTRODUCTION

The variable clinical course of chronic lymphocytic leukemia (CLL) and the lack of consensus on follow-up and treatment strategies have necessitated a prognostic model for identifying high-risk patients at the time of diagnosis.

METHODS

We involved a retrospective analysis of demographic and clinical characteristics of 212 patients diagnosed with Binet stage A CLL and thus eligible for risk stratification by both the International Prognostic Score for Early-stage CLL (IPS-E) and the alternative IPS-E (AIPS-E). We evaluated the applicability of these prognostic indices in our young, Middle Eastern cohort (median age 59 at diagnosis).

RESULTS

During the study period with a median follow-up of 3.5 years, 67 patients (32 %) experienced progression to first treatment and cumulative incidence of treatment was 13 % at 1 year and 28 % at 3 years after diagnosis. Sixty-nine (51 % of the 136 with a known value) patients harbored an unmutated immunoglobulin heavy chain gene (IGHV) and 21 (10 %) an 11q or 17p deletion with 11 % lacking FISH results. For each early-stage CLL prognostic index, more patients were identified as high-risk for disease progression (51 % of 124 patients evaluable for IPS-E; 42 % of 109 patients evaluable for AIPS-E) than intermediate-risk and low-risk. Multivariable models involving the IPS-E and AIPS-E components revealed that unmutated IGHV and elevated absolute lymphocyte count were significant predictors of earlier treatment requirement. Both prognostic scores were discriminative of time to first treatment (log-rank p < 0.001; c-statistics of 0.74 for IPS-E and 0.69 for AIPS-E).

CONCLUSION

Although clarity on clinical behavior with regard to initiation of treatment remains elusive, IPS-E and AIPS-E are valuable tools for identifying high-risk patients.

摘要

简介

慢性淋巴细胞白血病(CLL)的临床表现存在差异,且对于随访和治疗策略尚未达成共识,因此需要一种在诊断时能够识别高危患者的预后模型。

方法

我们回顾性分析了 212 例 Binet 分期为 A 期的 CLL 患者的人口统计学和临床特征,这些患者有资格通过国际早期 CLL 预后评分(IPS-E)和替代 IPS-E(AIPS-E)进行风险分层。我们评估了这些预后指标在我们年轻的中东队列中的适用性(诊断时的中位年龄为 59 岁)。

结果

在中位随访 3.5 年的研究期间,67 例患者(32%)发生首次治疗进展,1 年和 3 年时的累积治疗发生率分别为 13%和 28%。69 例(136 例已知值中的 51%)患者存在未突变的免疫球蛋白重链基因(IGHV),21 例(10%)患者存在 11q 或 17p 缺失,11%的患者缺乏 FISH 结果。对于每个早期 CLL 预后指标,更多的患者被确定为疾病进展的高危患者(可评估 IPS-E 的 124 例患者中有 51%;可评估 AIPS-E 的 109 例患者中有 42%),而中危和低危患者较少。涉及 IPS-E 和 AIPS-E 成分的多变量模型显示,未突变的 IGHV 和绝对淋巴细胞计数升高是更早需要治疗的显著预测因素。这两种预后评分均能区分首次治疗时间(对数秩检验 p<0.001;IPS-E 的 C 统计量为 0.74,AIPS-E 的 C 统计量为 0.69)。

结论

尽管在启动治疗方面的临床行为仍不明确,但 IPS-E 和 AIPS-E 是识别高危患者的有用工具。

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