Mihou Dimitra, Katodritou Eirini, Zervas Kostas
Department of Hematology-Oncology, Theagenion Cancer Center, Thessaloniki, Greece.
Hematology. 2007 Dec;12(6):527-31. doi: 10.1080/10245330701384161.
Since the prognostic significance of the combination of beta-2-microglobulin (beta(2)m) and albumin in multiple myeloma (MM) has been recognized, these two easily obtainable parameters were subsequently employed in the staging systems of Bataille et al. (BSS), the South West Oncology Group (SWOG SS) and most recently the International Myeloma Working Group (ISS). There is no consensus, however, regarding the cut off levels of beta(2)m and the stage, early or advanced, at which albumin should be added to the model. At the same time, Weber et al. demonstrated similar results using beta(2)m alone in identical cut-offs with ISS (WSS). The aim of the present study is to apply these four staging systems in 504 MM patients, in order to discern the role of albumin in MM staging and evaluate if, and at which stage, albumin should be added to the model.
Median overall survival (OS) according to BSS, SWOG SS, ISS and WSS was estimated according to the Kaplan-Meier method. OS differences between the stages were assessed using the log-rank test. Patients with beta(2)m < 3.5 mg/l and albumin < 3.5 g/dl, who were classified in stage II according to ISS and in stage I according to WSS, were analyzed separately in order to detect in which prognostic group they practically belong.
BSS and SWOG SS failed to distinguish stage II from stage III patients and stage III from stage IV patients, respectively. ISS and WSS achieved clear stratification of the patients into three distinct prognostic subgroups, but WSS I patients had a lower life expectancy than ISS I patients. This difference was due to false inclusion of patients with beta(2)m < 3.5 mg/l and albumin < 3.5 g/dl in stage I by WSS, while separate analysis of these patients proved that they belong, in fact, in stage II. In an attempt to improve its prognostic impact, WSS was then successfully modified by dividing WSS I patients in two substages, WSS IA: beta(2)m < 2.5 mg/l and WSS IB: 2.5 mg/l < or = beta(2)m < 3.5 mg/l, thus designating a low-risk and a low-intermediate-risk subgroup, respectively.
Albumin appears to lose its prognostic value at high cut-off levels of beta(2)m, while it enhances the prognostic significance of beta(2)m at low cut-off levels of the latter. Albumin cannot be eliminated from the ISS, since it is absolutely necessary in order to identify true low-risk patients. The only possibility for albumin exclusion from the model, could be to decrease the beta(2)m low-risk cut-off from 3.5 to 2.5 mg/l.
由于β2微球蛋白(β2m)与白蛋白联合检测在多发性骨髓瘤(MM)中的预后意义已得到认可,这两个易于获取的参数随后被应用于巴塔伊等人的分期系统(BSS)、西南肿瘤协作组(SWOG SS)以及最近的国际骨髓瘤工作组(ISS)。然而,关于β2m的临界值以及应将白蛋白纳入模型的分期(早期或晚期),目前尚无共识。同时,韦伯等人使用与ISS相同临界值的单独β2m检测(WSS)也得出了类似结果。本研究的目的是将这四种分期系统应用于504例MM患者,以明确白蛋白在MM分期中的作用,并评估是否以及在哪个阶段应将白蛋白纳入模型。
根据Kaplan-Meier法估计BSS、SWOG SS、ISS和WSS的中位总生存期(OS)。使用对数秩检验评估各分期之间的OS差异。对β2m < 3.5 mg/l且白蛋白 < 3.5 g/dl的患者进行单独分析,这些患者根据ISS被归类为II期,根据WSS被归类为I期,以确定他们实际所属的预后组。
BSS无法区分II期与III期患者,SWOG SS则无法区分III期与IV期患者。ISS和WSS成功地将患者分为三个不同的预后亚组,但WSS I期患者的预期寿命低于ISS I期患者。这种差异是由于WSS将β2m < 3.5 mg/l且白蛋白 < 3.5 g/dl的患者错误地纳入I期,而对这些患者的单独分析表明他们实际上属于II期。为了提高其预后影响,随后对WSS进行了成功修改,将WSS I期患者分为两个亚期,WSS IA:β2m < 2.5 mg/l和WSS IB:2.5 mg/l ≤ β2m < 3.5 mg/l,从而分别指定了一个低风险和一个低中风险亚组。
在β2m的高临界值水平时,白蛋白似乎失去了其预后价值,而在β2m的低临界值水平时,它增强了β2m的预后意义。白蛋白不能从ISS中排除,因为为了识别真正的低风险患者,它是绝对必要的。将白蛋白从模型中排除的唯一可能性可能是将β2m的低风险临界值从3.5降至2.5 mg/l。
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