Abstract

Minimal residual disease, or MRD, is an important prognostic indicator in childhood acute lymphoblastic leukemia. In ALL-IC-BFM 2002 study, we employed a standardized method of flow cytometry MRD monitoring for multiple centers internationally using uniformed gating, and determined the relevant MRD-based risk stratification strategies in our local patient cohort. We also evaluated a novel method of PCR MRD quantitation using peripheral blood plasma. For the bone marrow flow MRD study, patients could be stratified into 3 risk groups according to MRD level using a single time-point at day-15 (Model I) (I-A: <0.1%, I-B: 0.1–10%, I-C: >10%), or using two time-points at day-15 and day-33 (Model II) (II-A: day-15<10% and day-33<0.01%, II-B: day-15≥10% or day-33≥0.01% but not both, II-C: day-15≥10% and day-33≥0.01%), which showed significantly superior prediction of relapse (p = .00047 and <0.0001 respectively). Importantly, patients with good outcome (frequency: 56.0%, event-free survival: 90.1%) could be more accurately predicted by Model II. In peripheral blood plasma PCR MRD investigation, patients with day-15-MRD≥10−4 were at a significantly higher risk of relapse (p = 0.0117). By multivariate analysis, MRD results from both methods could independently predict patients’ prognosis, with 20–35-fold increase in risk of relapse for flow MRD I-C and II-C respectively, and 5.8-fold for patients having plasma MRD of ≥10−4. We confirmed that MRD detection by flow cytometry is useful for prognostic evaluation in our Chinese cohort of childhood ALL after treatment. Moreover, peripheral blood plasma DNA MRD can be an alternative where bone marrow specimen is unavailable and as a less invasive method, which allows close monitoring.

Highlights

  • Despite recent advances in the treatment of childhood acute lymphoblastic leukemia (ALL), the disease remains a major cause of cancer-related mortality in children

  • In 35 of the 43 of B-lineage ALL patients at diagnosis, a population of leukemic cells could be identified by at least one Leukemia-associated immunophenotypes (LAIPs), constituting a coverage rate of 81.4% (35/43). Among these 35 patients of BALL with positive LAIP, only 22.9% (8/35) had 2 or more while the majority 77.1% (27/35) had only 1 LAIP identified for followup

  • minimal residual disease (MRD) detection has become an essential tool for assessment of in vivo treatment response in childhood ALL and flow cytometry (FCM) is one of the most commonly used technologies, which is easy to apply and with fast available results

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Summary

Introduction

Despite recent advances in the treatment of childhood acute lymphoblastic leukemia (ALL), the disease remains a major cause of cancer-related mortality in children. Detection of minimal residual disease (MRD) has become an important assessment and the level of MRD emerged as one of the most powerful indicators of treatment response in vivo, as it corresponds to the resistance of leukemic cells to chemotherapy and the dynamic interactions of complicated therapy[4,5,6]. The FCM method has the advantage over PCR of providing a faster result and is more cost-effective and widely applicable to most patients. It can be applied in multi-center setting using standardized reagents and gating strategies [12,13]. We report our local findings as part of the I-BFM Mini-mini project using FCM for quantitation of MRD [12], and determined the clinically relevant MRD cutoffs for risk stratifying Chinese patients treated under ALL IC-BFM 2002 protocol

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