首页> 外文期刊>British Journal of Cancer >Prognostic study of continuous variables (white blood cell count, peripheral blast cell count, haemoglobin level, platelet count and age) in childhood acute lymphoblastic leukaemia. Analysis of a population of 1545 children treated by the French Acute Lymphoblastic Leukaemia Group (FRALLE)
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Prognostic study of continuous variables (white blood cell count, peripheral blast cell count, haemoglobin level, platelet count and age) in childhood acute lymphoblastic leukaemia. Analysis of a population of 1545 children treated by the French Acute Lymphoblastic Leukaemia Group (FRALLE)

机译:儿童急性淋巴细胞白血病连续变量(白细胞计数,外周母细胞计数,血红蛋白水平,血小板计数和年龄)的预后研究。法国急性淋巴细胞白血病小组(FRALLE)治疗的1545名儿童的分析

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Many cutpoints have been proposed to categorize continuous variables in childhood acute lymphoblastic leukaemia (white blood cell count, peripheral blast cell count, haemoglobin level, platelet count and age), and have been used to define therapeutic subgroups. This variation in the choice of cutpoints leads to a bias called the ‘Will Rogers phenomenon'. The aim of this study was to analyse variations in the relative risk of relapse or death as a function of continuous prognostic variables in childhood ALL and to discuss the choice of cutpoints. We studied a population of 1545 children with ALL enrolled in three consecutive protocols named FRALLE 83, FRALLE 87 and FRALLE 89. We estimated the risk of relapse or death associated with different values of each continuous prognostic variable by dividing the sample into quintiles of the distribution of the variables. As regards age, a category of children under 1 year of age was distinguished and the rest of the population was divided into quintiles. The floated variance method was used to calculate the confidence interval of each relative risk, including the reference category. The relation between the quantitative prognostic factors and the risk was monotonic for each variable, except for age. For the white blood cell count (WBC), the relation is log linear. The risk associated with WBC values in the upper quintile was 1.9 times higher than that in the lower quintile. The peripheral blast cell count correlated strongly with WBC (correlation coefficient: 0.99). The risk increased with the haemoglobin level, and the risk in the upper quintile was 1.3 times higher than that in the lower quintile. The risk decreased as the platelet count increased: the risk in the lower quintile was 1.2 times higher than that in the upper quintile. The risk increased gradually with increasing age above one year. The small subgroup of patients (2.5% of the population) under 1 year of age at diagnosis had a risk 2.6 times higher than the reference category of patients between 3 and 4.3 years of age. When the risk associated with a quantitative prognostic factor varies monotonously, the selection of a cutpoint is arbitrary and represents a loss of information. Despite this loss of information, such arbitrary categorization may be necessary to define therapeutic stratification. In that case, consensus cutpoints must be defined if one wants to avoid the Will Rogers phenomenon. The cutpoints proposed by the Rome workshop and the NCI are arbitrary, but may represent an acceptable convention. ? 2000 Cancer Research Campaign http://www.bjcancer.com
机译:已提出许多切点来对儿童急性淋巴细胞白血病的连续变量进行分类(白细胞计数,外周母细胞计数,血红蛋白水平,血小板计数和年龄),并已用于定义治疗亚组。切割点选择的这种变化会导致一种称为“威尔·罗杰斯现象”的偏见。这项研究的目的是分析复发或死亡的相对风险随儿童ALL持续预后变量的变化,并讨论切点的选择。我们研究了1545名ALL儿童,这些儿童参加了名为FRALLE 83,FRALLE 87和FRALLE 89的三个连续方案。我们通过将样本分成分布的五分位数,估算了与每个连续预后变量的不同值相关的复发或死亡的风险的变量。关于年龄,区分了1岁以下儿童的类别,其余人口分为五等分。浮动方差法用于计算每个相对风险(包括参考类别)的置信区间。定量预后因素与风险之间的关系对于每个变量(年龄除外)都是单调的。对于白细胞计数(WBC),该关系为对数线性关系。在上五分之一人群中与WBC值相关的风险比在下五分位数人群中高1.9倍。外周母细胞计数与WBC密切相关(相关系数:0.99)。风险随着血红蛋白水平的升高而增加,上五分位数的风险是下五分位数的1.3倍。随着血小板计数的增加,风险降低:较低的五分之一患者的风险是较高的五分之一患者的1.2倍。随着年龄的增加,这一风险逐渐增加。诊断为1岁以下的一小部分患者(占人口的2.5%)的风险是3至4.3岁年龄段患者的参考类别的2.6倍。当与定量预后因素相关的风险单调变化时,切入点的选择是任意的,代表信息丢失。尽管丢失了信息,但仍可能需要进行此类任意分类以定义治疗分层。在这种情况下,如果要避免威尔·罗杰斯现象,就必须定义共识的切入点。罗马讲习班和NCI提出的削减点是任意的,但可能代表可接受的惯例。 ? 2000年癌症研究运动http://www.bjcancer.com

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