Minimal Residual Disease Evaluation in Childhood Acute Lymphoblastic Leukemia: A Clinical Evidence Review.

Q1 Medicine Ontario Health Technology Assessment Series Pub Date : 2016-03-08 eCollection Date: 2016-01-01
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Abstract

Background: Leukemia accounts for nearly a third of childhood cancers in Canada, with acute lymphoblastic leukemia (ALL) comprising nearly 80% of cases. Identification of prognostic factors that allow risk stratification and tailored treatment have improved overall survival. However, nearly a quarter of patients considered standard risk on the basis of conventional prognostic factors still relapse, and relapse is associated with increased morbidity and mortality. Relapse is thought to result from extremely low levels of leukemic cells left over once complete remission is reached, termed minimal residual disease (MRD). Poor event-free survival (EFS) as well as overall survival for those who are classified as MRD-positive have been substantiated in seminal studies demonstrating the prognostic value of MRD for EFS in the past few decades. This review sought to further elucidate the relationship between MRD and EFS by looking at relapse, the primary determinant of EFS and the biological mechanism through which MRD is thought to act. This evidence review aimed to ascertain whether MRD is an independent prognostic factor for relapse and to assess the effect of MRD-directed treatment on patient-important outcomes in childhood ALL.

Methods: Large prospective cohort studies with a priori multivariable analysis that includes potential confounders are required to draw confirmatory conclusions about the independence of a prognostic factor. Data on the prognostic value of MRD for relapse measured by molecular methods (polymerase chain reaction [PCR] of immunoglobulin or T-cell receptor rearrangements) or flow cytometry for leukemia-associated immunophenotypes or difference-from-normal approach were abstracted from included studies. Relevant data on relapse, EFS, and overall survival were abstracted from randomized controlled trials (RCTs) evaluating the effect of MRD-directed treatment.

Results: A total of 2,832 citations were reviewed, of which 12 studies were included in this review. All cohort studies evaluating MRD as a prognostic factor for relapse found significant independent value when added to various existing prognostic factors. Seven studies showed prognostic value of MRD measured at the end of induction therapy and two at the end of consolidation therapy in de novo ALL, one study in relapsed ALL after re-induction therapy, and three studies before hematopoietic stem cell transplant. One large RCT in standard-risk patients found no compromise to outcomes when reducing treatment in MRD-negative patients, and also showed a 45% reduction in relapse risk and nearly 40% benefit in EFS when escalating treatment in MRD-positive patients.

Conclusions: Minimal residual disease is an independent prognostic factor for relapse in childhood ALL. Relapse is a key determinant of EFS and patients' quality of life. Treatment selected on the basis of MRD status appears to improve outcomes.

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儿童急性淋巴细胞白血病的最小残留病评估:临床证据回顾。
背景:在加拿大,白血病占儿童癌症的近三分之一,其中急性淋巴细胞白血病(ALL)占近 80%。通过对预后因素的识别,可以进行风险分层和有针对性的治疗,从而提高了总生存率。然而,在根据传统预后因素被视为标准风险的患者中,仍有近四分之一的患者会复发,而复发与发病率和死亡率的增加有关。复发的原因被认为是达到完全缓解后残留的白血病细胞水平极低,称为最小残留病(MRD)。在过去几十年中,一些开创性的研究证实了 MRD 对无事件生存期(EFS)和总生存期的预后价值。本综述试图通过研究复发(EFS的主要决定因素)和MRD被认为发挥作用的生物学机制,进一步阐明MRD与EFS之间的关系。本证据综述旨在确定MRD是否是复发的独立预后因素,并评估针对MRD的治疗对儿童ALL患者重要预后的影响:方法:需要开展大型前瞻性队列研究,并进行包括潜在混杂因素在内的先验多变量分析,以得出预后因素独立性的确证结论。通过分子方法(免疫球蛋白或T细胞受体重排的聚合酶链式反应[PCR])或流式细胞术检测白血病相关免疫表型或与正常值的差异方法测量MRD对复发的预后价值,并从纳入的研究中摘录相关数据。从评估MRD定向治疗效果的随机对照试验(RCT)中摘录了复发、EFS和总生存期的相关数据:结果:共查阅了 2,832 条引用文献,其中 12 项研究被纳入本综述。所有将MRD作为复发预后因素进行评估的队列研究发现,MRD与现有的各种预后因素相比具有显著的独立价值。七项研究显示,MRD在新发ALL诱导治疗结束时测量具有预后价值,两项研究在巩固治疗结束时测量具有预后价值,一项研究在复发ALL再次诱导治疗后测量具有预后价值,三项研究在造血干细胞移植前测量具有预后价值。一项针对标准风险患者的大型研究发现,减少对MRD阴性患者的治疗并不会影响疗效,同时还显示,在对MRD阳性患者进行升级治疗时,复发风险降低了45%,EFS获益近40%:结论:最小残留病是儿童 ALL 复发的独立预后因素。结论:最小残留病是儿童 ALL 复发的独立预后因素,复发是决定 EFS 和患者生活质量的关键因素。根据MRD状态选择治疗似乎可以改善预后。
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Ontario Health Technology Assessment Series
Ontario Health Technology Assessment Series Medicine-Medicine (miscellaneous)
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