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由临床和生物学标志物组成的预测慢性淋巴细胞白血病(CLL)患者首次治疗时间的多变量模型:单中心经验的初步结果

Multivariable model consisting of clinical and biological markers for time to first treatment in CLL patients: Preliminary results from single centre experience.

作者信息

Trajkova Sanja, Cevreska Lidija, Pivkova-Veljanovska Aleksandra, Ivanovski Martin, Dukovski Dusko, Popova-Simjanovska Marija, Cadievski Lazar, Eftimov Aleksandar, Dimovski Aleksandar, Panovska-Stavridis Irina

机构信息

University Haematology Clinic, Medical Faculty, Ss. Cyril and Methodius University, Skopje, R. Macedonia.

出版信息

Pril (Makedon Akad Nauk Umet Odd Med Nauki). 2013;34(3):39-47.

Abstract

INTRODUCTION

The clinical course for patients with chronic lymphocytic leukaemia (CLL) is extremely heterogeneous; one of the most important challenges in the clinical management of these patients is the decision on initiating their treatment, but there is no available prognostic system that will resolve this issue. Usually, criteria for active disease are used to initiate therapy. Recently, some authors have proposed prognostic models, scoring systems involving a set of clinical and biological risk factors and estimates of individual patient survivals. Here, we report our initial results from a study designed to evaluate the statistical association of the distinct clinical and biological parameters with the prognosis and time to initiating treatment for patients with CLL.

MATERIAL AND METHODS

Our study incorporated 100 consecutive, treatment naive CLL patients. In each patient all traditional laboratory, clinical and biological prognostic factors were evaluated at their first visit to our Institution. We then combined the following independent characteristics: age, β-2 microglobulin, absolute lymphocyte count, sex, Rai stage, and number of involved lymph node groups, which are included in some of the already published CLL prognostics index, in association with the CD38 expression and mutational status of the immunoglobulin heavy chain gene variable region (IGVH). Further, we correlated those factors by multivariable analysis with time to first treatment. This multivariable model was used to develop a nomogram-a weighted tool to calculate 5- and 10-year survival probability and estimate median time to first treatment (TFT).

RESULTS

According to the prognostic index, a classification tree was built that identified three subsets of patients whose scores were 1-3 (low risk - 32 pts - 32%), 4-7 (intermediate risk - 48 pts - 48%) and > 8 (high risk - 20 pts - 20%). Estimated median survival in the low risk subset of patients is 141 years, and 10.7 and 4.6 years respectively in the intermediate and high risk subsets of patients. Projected survival in respectively low, intermediate and high-risk groups are 100%, 100%, 25%, and 43%, 34%, 25% at 5 years and 10 years, respectively. Also, statistical analyses showed that among other things CD38 expression and unmutated IGHV mutation status are associated with a shorter time to first treatment.

CONCLUSION

Our prognostic model that combines and correlates the distinct clinical and biological markers of CLL patients enables identification of patients who are at high risk of progression. This prognostic model may facilitate the clinical decision for initiating treatment.

摘要

引言

慢性淋巴细胞白血病(CLL)患者的临床病程极不均匀;对这些患者进行临床管理时最重要的挑战之一是决定开始治疗,但目前尚无可用的预后系统能解决这一问题。通常,采用疾病活动标准来启动治疗。最近,一些作者提出了预后模型、评分系统,涉及一组临床和生物学风险因素以及对个体患者生存率的估计。在此,我们报告一项研究的初步结果,该研究旨在评估CLL患者不同临床和生物学参数与预后及开始治疗时间之间的统计学关联。

材料与方法

我们的研究纳入了100例连续的、未经治疗的CLL患者。在每位患者首次就诊于我们机构时,对所有传统实验室、临床和生物学预后因素进行评估。然后,我们将以下独立特征相结合:年龄、β2微球蛋白、绝对淋巴细胞计数、性别、Rai分期、受累淋巴结组数量,这些已包含在一些已发表的CLL预后指数中,并与CD38表达及免疫球蛋白重链基因可变区(IGVH)的突变状态相关联。此外,我们通过多变量分析将这些因素与首次治疗时间相关联。该多变量模型用于开发一种列线图——一种加权工具,用于计算5年和10年生存概率,并估计首次治疗的中位时间(TFT)。

结果

根据预后指数,构建了一棵分类树,确定了三个患者亚组,其得分分别为1 - 3分(低风险——32例患者——32%)、4 - 7分(中风险——48例患者——48%)和>8分(高风险——20例患者——20%)。低风险亚组患者的估计中位生存期为141年,中风险和高风险亚组患者分别为10.7年和4.6年。低、中、高风险组在5年和10年时的预计生存率分别为100%、100%、25%以及43%、34%、25%。此外,统计分析表明,除其他因素外,CD38表达和未突变的IGHV突变状态与较短的首次治疗时间相关。

结论

我们结合并关联CLL患者不同临床和生物学标志物的预后模型能够识别出进展风险高的患者。这种预后模型可能有助于临床治疗启动决策。

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