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微小残留病的免疫表型分析是预测急性髓系白血病患者复发的一种有用方法。

Immunophenotyping investigation of minimal residual disease is a useful approach for predicting relapse in acute myeloid leukemia patients.

作者信息

San Miguel J F, Martínez A, Macedo A, Vidriales M B, López-Berges C, González M, Caballero D, García-Marcos M A, Ramos F, Fernández-Calvo J, Calmuntia M J, Diaz-Mediavilla J, Orfao A

机构信息

Department of Hematology, University Hospital, Salamanca, Spain.

出版信息

Blood. 1997 Sep 15;90(6):2465-70.

PMID:9310499
Abstract

A high complete remission rate is currently achieved in patients with acute myeloid leukemia (AML). However, many patients eventually relapse due to the persistence of low numbers of residual leukemic cells that are undetectable by conventional cytomorphologic criteria (minimal residual disease [MRD]). Using immunophenotypic multiparametric flow cytometry, we have investigated in sequential studies (diagnosis and follow-up) the impact of MRD detection on the outcome of 53 AML patients that had achieved morphologic remission with standard AML protocols and displayed at diagnosis an aberrant phenotype. Patients were studied at diagnosis with a panel of 35 monoclonal antibodies in triple staining combinations for detection of aberrant or uncommon phenotypic features. According to these features, a patient's probe was custom-built at diagnosis for the identification of possible residual leukemic cells during follow-up. The level of MRD at the end of induction and intensification therapy correlated with the number of relapses and relapse-free survival (RFS). Thus, patients with more than 5 x 10(-3) residual cells (5 residual cells among 1,000 normal bone marrow [BM] cells) identified as leukemic by immunophenotyping in the first remission BM showed a significant higher rate of relapse (67% v 20% for patients with less than 5 x 10(-3) residual cells; P = .002) and a lower median RFS (17 months v not reached; P = .01). At the end of intensification, with a cut-off value of 2 x 10(-3) leukemic cells, AML patients also separated into two distinct groups with relapse rates of 69% versus 32% (P = .02), respectively, and median RFS of 16 months versus not reached (P = .04). In addition, overall survival was also significantly related to the level of residual cells in the marrow obtained at the end of induction and particularly after intensification therapy (P = .008). Furthermore, we have explored whether residual disease was related with the functional expression of multidrug resistance (MDR-1) at diagnosis as assessed by the rhodamine123 assay. Patients with > or =5 x 10(-3) residual leukemic cells at the end of induction therapy had a significantly higher rhodamine-123 efflux (mean, 56% +/- 24%) than those with less than 5 x 10(-3) residual cells (mean, 32% +/- 31%; P = .04). Finally, multivariate analysis showed that the number of residual cells at the end of induction or intensification therapy was the most important prognostic factor for prediction of RFS. Overall, our results show that immunophenotypical investigation of MRD strongly predicts outcome in patients with AML and that the number of residual leukemic cells correlates with multidrug resistance.

摘要

目前,急性髓系白血病(AML)患者可实现较高的完全缓解率。然而,许多患者最终会复发,原因是存在少量残留白血病细胞,这些细胞按传统细胞形态学标准无法检测到(微小残留病[MRD])。我们运用免疫表型多参数流式细胞术,在系列研究(诊断和随访)中调查了MRD检测对53例AML患者预后的影响,这些患者采用标准AML方案已实现形态学缓解,且诊断时表现出异常表型。诊断时用一组35种单克隆抗体以三重染色组合方式研究患者,以检测异常或不常见的表型特征。根据这些特征,在诊断时为患者定制探针,以便在随访期间识别可能的残留白血病细胞。诱导和强化治疗结束时的MRD水平与复发次数和无复发生存期(RFS)相关。因此,首次缓解骨髓中经免疫表型鉴定为白血病的残留细胞超过5×10⁻³(每1000个正常骨髓[BM]细胞中有5个残留细胞)的患者,复发率显著更高(残留细胞少于5×10⁻³的患者为20%,前者为67%;P = 0.002),中位RFS更低(分别为17个月和未达到;P = 0.01)。强化治疗结束时,以2×10⁻³白血病细胞为临界值,AML患者也分为两个不同组,复发率分别为69%和32%(P = 0.02),中位RFS分别为16个月和未达到(P = 0.04)。此外,总生存期也与诱导结束时,特别是强化治疗后获得的骨髓中残留细胞水平显著相关(P = 0.008)。此外,我们还探讨了残留病是否与诊断时通过罗丹明123检测评估的多药耐药(MDR - 1)功能表达相关。诱导治疗结束时残留白血病细胞≥5×10⁻³的患者,罗丹明 - 123外排率显著高于残留细胞少于5×10⁻³的患者(平均值分别为56%±24%和32%±31%;P = 0.04)。最后,多变量分析表明,诱导或强化治疗结束时的残留细胞数量是预测RFS的最重要预后因素。总体而言,我们的结果表明,对MRD进行免疫表型研究能有力预测AML患者的预后,且残留白血病细胞数量与多药耐药相关。

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